Patent Publication Number: US-5530197-A

Title: Control of ostrinia

Description:
This application is a divisional of application Ser. No. 08/377,690, filed Jan. 25, 1995, which is a continuation of application Ser. No. 08/164,781, filed Dec. 10, 1993, now abandoned, which is a continuation of application Ser. No. 07/938,362, filed Aug. 31, 1992, now abandoned. 
    
    
     This invention relates to a method to control or combat Ostrinia, particularly Ostrinia nubilalis (Lepidoptera, Pyralidae) or the European corn borer, using a Bacillus thuringiensis (&#34;Bt&#34;) cryIB gene or CryIB protein or using the cryIB gene and the cryIAb or cryIAc gene or their respective proteins. This invention also relates to a method to protect crops, particularly corn, against Ostrinia. 
     This invention further relates to the use of microorganisms, especially plant-associated microorganisms, preferably Clavibacter xyli, and to the use of plants, especially monocotyledonous plants, particularly corn (maize, Zea mays), stably transformed with the cryIB gene alone or with both the cryIB gene and cryIAb or cryIAc gene to control or combat Ostrinia such as O. nubilalis. 
     This invention still further relates to the use of insecticidal formulations containing the CryIB protein or both the CryIB protein and the CryIAb or CryIAc protein to protect plants from Ostrinia. 
     This invention also relates to a plant, especially a monocot, particularly a cereal plant, quite particularly corn, infestable by O. nubilalis and transformed with an expressible cryIB gene or with both an expressible cryIB gene and a cryIAb or cryIAc gene, to combat or control Ostrinia. 
     BACKGROUND OF THE INVENTION 
     Bacillus thuringiensis 
     Bacillus thuringiensis (&#34;Bt&#34;) is a gram-positive soil bacterium, which produces endogenous crystalline inclusions upon sporulation. Early in this century, these bacteria were found to be insecticidal (Berliner, 1915). Some years later, their insecticidal activity was found to reside in the proteins present in their crystals, hereinafter referred to as &#34;insecticidal crystal proteins&#34; or &#34;ICPs&#34;. Since then, the Bt strains, spores, crystals and ICPs have been used as biological insecticides in commercial formulations. 
     The limited spectrum of these insecticidal proteins allows any naturally occurring predators of the target insects to survive. The continued presence of these predators prevents further outbreaks of the insects. Furthermore, these Bt proteins have the advantage that they are rapidly degradable and that no stable residues accumulate in the environment. 
     Cry proteins and cry genes 
     The specificity of the environmentally safe Bt insecticides has provoked a search for new Bt strains, producing toxins against other insect pests. Insecticidal Bt strains toxic to lepidopteran, coleopteran and dipteran insects have been found (Hofte and Whiteley, 1989). Although considerable homology can be found between genes that encode various ICPs toxic to one particular insect class, the sensitivity of specific insects to related Bt gene products is often very different. For instance, Chambers et al (1991) described a large difference in activity of the CryIF protein against Heliothis virescens and Heliothis zea (50% lethal concentrations of respectively 0.31 and &gt;57 ng protoxin/mm 2  diet). 
     The Bt insecticidal crystal (Cry) proteins have been divided into five classes, according to their structural similarities and insecticidal spectra (Hofte and Whiteley, 1989): CryI proteins are toxic to Lepidoptera, CryII proteins are toxic to Diptera and Lepidoptera, CryIII proteins are toxic to Coleoptera and CryIV proteins are toxic to Diptera. A general cytolytic protein (cytA) is classified as a fifth toxic protein, but it has no specific insecticidal activity. The Bt genes coding for the insecticidal Cry proteins (cry genes) show strong homology in some conserved domains. These insecticidal Bt genes are mostly found on large conjugative plasmids, which may explain their observed mobility among Bt strains. One strain can contain several cry genes, and one gene can be found in several strains (Hofte and Whiteley, 1989). 
     Typically, cryI genes encode proteins with a molecular weight of 130 to 140 kD (hereinafter referred to as the &#34;protoxins&#34;), and upon ingestion by a sensitive insect, the protoxins are processed to smaller proteins (hereinafter referred to as the &#34;toxins&#34;) having a molecular weight of 60 to 70 kD. The cryII and cryIII genes encode protoxins with a molecular weight of about 70 kD (except the cryIIIC gene which encodes a protoxin of 129 kD according to PCT publication WO 90/09445). The CryIV genes encode protoxins of either of these molecular weight types. The CryI protoxins constitute the largest group of protoxins, which are found in typical bipyramidal crystals. 
     The cry genes have been used to transform bacteria (e.g., Obukowicz et al, 1986; Stock et al, 1990) and plants (e.g., Vaeck et al, 1987) in order to provide resistance against insect pests. Adequate expression in plants was only obtained when the plants were transformed with a truncated Bt gene (e.g., Vaeck et al, 1987; Fischhoff et al, 1987; Barton et al, 1987). 
     The cryIB gene has been described in European patent publication (&#34;EP&#34;) 408 403 and by Brizzard and Whiteley (1988). It encodes a 137 kD protoxin and a 66 kD toxin. The CryIB toxin has been shown to be insecticidal to insects like Pieris brassicae, Plutella xylostella, Spadoptera littoralis and Spodoptera exigua (Ferre et al, 1991; Visser et al, 
     The CryIAa (Gawron-Burke and Baum, 1991), CryIAb, CryIAc (Macintosh et al, 1990) and CryIF gene products (Chambers et al, 1991) have been described as toxic to O. nubilalis. Moreover, Peferoen (1991) has described the insecticidal activity of the following ICPs against various insects, including O. nubilalis: CryIAa, CryIAb, CryIAc, CryIB, CryID, CryIC and CryIE, and PCT publication WO 92/09696 also has described the insecticidal activity of the cryIAb and cryIB genes against O. nubilalis. 
     PCT publication 90/15139 has described the prevention of insect resistance development with various combinations of Bt genes, such as the cryIAb and cryIB genes (the Bt 2 and Bt 14 genes), against Pieris brassicae, Plutella xylostella, and Phthorimaea operculella. 
     Mode of action of the CryI proteins 
     The ICPs owe their specificity to the presence of specific receptor sites in the midgut brush border membranes of sensitive insects. In vivo, the crystals are solubilized in the alkaline environment of the midgut, and the released protoxins are processed by proteases to yield smaller protease-resistant toxins which bind to, and cause swelling of, the midgut cells (Gill et al, 1992). The C-terminal part of the CryI-type protoxin is probably involved in the formation of its crystal structure, but is thought not to be important in its mode of action (Hofte and Whiteley, 1989). Electrophysiological evidence (Harvey et al, 1983) and biochemical evidence (Knowles and Ellar, 1987) suggest that the toxins generate pores in the midgut brush border cell membranes, thus disturbing the osmotic balance. The intoxicated insects quickly stop feeding and eventually die. The high affinity binding of the toxins has been correlated with their toxicity (Van Rie et al, 1989). 
     Ostrinia nubilalis 
     The European corn borer is a very serious and persistant pest for corn (Davidson and Lyon, 1987; Hudon et al, 1987). The larvae of this insect initially feed on leaf tissue and later enter the stalks, burrowing downwards as the season progresses. O. nubilalis is estimated to be the most important corn pest in Europe and the second most important in the USA. Damage caused by O. nubilalis in the USA is estimated to be over 400 million dollars (U.S.) a year. Estimates for O. nubilalis spraying amount in France to 25 million dollars (U.S.) a year. Up to now, hazardous chemical insecticides have mostly been used to combat this insect. The European corn borer is remarkably polyphagous (Hudon et al, 1987) and has been found to attack other important crops such as wheat, cotton, potato, tomato, beet, oat and soybean plants (Davidson and Lyon, 1987; Hudon et al, 1987). 
     SUMMARY OF THE INVENTION 
     In accordance with this invention, a method is provided to combat and/or control insects of the species Ostrinia, particularly Ostrinia nubilalis (the European corn borer), by the step of contacting these insects with: a) the CryIB protein or an equivalent thereof; or b) both i) the CryIB protein and ii) the CryIAb or the CryIAc, preferably the CryIAb, protein or their equivalents. 
     Also in accordance with this invention, the contacting step can be carried out with an insecticidal composition comprising: the CryIB protein or its equivalent or both the CryIB protein and the CryIAb or CryIAc protein or their equivalents in pure form; or Bt crystals containing these protein(s) or their equivalents; or crystal-spore mixtures of naturally occurring Bt bacteria containing the cryIB gene or its equivalent or both the cryIB gene and the cryIAb or cryIAc gene or their equivalents; or crystal-spore mixtures of Bt bacteria transformed with an expressible cryIB gene or its equivalent or with both an expressible cryIB gene and an expressible cryIAb or cryIAc gene or their equivalents. 
     Further in accordance with this invention, the contacting step can be carried out with a microorganism, preferably a plant-associated microorganism, especially an endophytic microorganism, particularly Clavibacter xyli, transformed with an expressible cryIB gene or its equivalent or with both an expressible cryIB gene and an expressible cryIAb or cryIAc gene or their equivalents, so as to inoculate plants or parts thereof, such as seeds, so that they become resistant to attack by Ostrinia. 
     Furthermore, the contacting of the insects can be with a plant, especially a monocotyledonous plant, particularly a cereal plant, quite particularly corn, stably transformed with an expressible cryIB gene or its equivalent or with both an expressible cryIAb or cryIAc gene and an expressible cryIB gone or their equivalents, so that the transformed plant expresses the CryIB protein or its equivalent or a combination of the CryIB and CryIAb or CryIAc proteins or their equivalents in insecticidally effective amounts. 
     Moreover, a plant, especially a monocotyledonous plant, particularly a cereal plant, quite particularly a corn plant, infested by Ostrinia, is protected from this insect by having been stably transformed with the cryIB gene or its equivalent or with both the cryIB gene and the cryIAb or cryIAc gene or their equivalents. 
     DETAILED DESCRIPTION OF THE INVENTION 
     This invention is based on the result of toxicity assays which were conducted by feeding the European corn borer, Ostrinia nubilalis, an artificial diet containing the purified CryIB toxin and which surprisingly showed that this protein was toxic to the European corn borer (see Example 1). Furthermore, the CryIB toxin was found to bind non-competitively to the midgut membranes of Ostrinia when compared with other Cry toxins which are insecticidally active against this insect as shown in Example 2. Therefore, this active Bt protein can be used to provide maximum protection against this important pest and can prevent or reduce the development of insect resistance to Bt insecticidal formulations in the field. 
     The &#34;CryIB protein&#34; of this invention encompasses the full length protein (protoxin) encoded by the cryIB gene and having the amino acid sequence shown in SEQ ID No.1 of the Sequence Listing and any protein that is substantially the same as the CryIB protoxin of SEQ ID No.1, as well as any insecticidally active fragment thereof, such as the CryIB toxin. An example of substantially the same protein as the protoxin of SEQ ID No.1 is the naturally occurring CryIB protoxin described by Brizzard and Whiteley (1988). The &#34;CryIB protein&#34; of this invention includes proteins in which some amino acids of the protoxin of SEQ ID No.1 are deleted, added or replaced by others without significantly changing the insecticidal activity, particularly against O. nubilalis, for example the modified CryIB protoxin described in EP 408 403 &#34;CryIB toxin&#34; as used herein, means the smallest insecticidally active fragment of the CryIB protoxin, extending from amino acid 145 to amino acid 636 in SEQ ID No.1. In this regard, &#34;insecticidally active fragment of the CryIB protoxin&#34; as used herein, means any part of the CryIB protoxin having insecticidal activity, preferably its toxin. 
     In this invention, &#34;cryIB gene&#34; encompasses the gene with the DNA sequence shown in SEQ ID No.1 of the Sequence Listing or any mutant, synthetic or modified gene encoding a CryIB protein, such as the modified gene described in EP 408 403. Modifications to the gene can include: 1) the replacement of some codons with others coding for the same or for other amino acids, preferably with codons that code for the same amino acids; 2) deleting or adding some codons; and 3) reciprocal recombination as described by Ge et al (1991); provided that such modifications do not substantially alter the properties, especially the insecticidal properties, particularly against O. nubilalis, of the encoded CryIB protein. It is evident that the definition of the cryIB gene comprises any modified gene designed to provide higher expression levels of a CryIB protein in plants. One particularly preferred modified gene is the naturally occurring cryIB gene described by Brizzard and Whiteley (1988), wherein only two nucleotides are different from SEQ ID No.1: in the Brizzard and Whiteley sequence, a T is replaced by a C at position 311, and a C is replaced by a T at position 633. Only the latter change in Brizzard and Whiteley leads to a different amino acid: a His codon is changed to a Tyr codon. &#34;Insecticidally active fragment of the cryIB gene&#34;, as used herein, means any truncated gene encoding an insecticidally active fragment of the CryIB protein, like the gene fragment encoding the CryIB toxin. 
     In accordance with this invention, a cryIB gene can be isolated from a Bt strain, for example Bt. entomocidus HD-110. This strain is publicly available from the Agricultural Research Culture Collection, Northern Regional Research Laboratory, U.S. Dept. of Agriculture, Peoria, Ill. 61604, USA (&#34;NRRL&#34;). The isolation and cloning of the cryIB gene, as well as its modification, are described in EP 408 403. The gene has an open reading frame (ORF) of 3684 bp, encoding a 137 kD protoxin and 66 kD and 55 kD protease-activated fragments. The nucleotide sequence and the corresponding amino acid sequence are shown in SEQ ID No.1. An insecticidally active cryIB gene fragment also can be constructed as described in EP 408 403. For this purpose, a BclI site has been identified downstream of the coding sequence encoding the CryIB toxin. 
     Similarly, the &#34;CryIAb protein&#34; of this invention encompasses a protoxin with the amino acid sequence disclosed in EP 193 259 and shown in SEQ ID No.2 in the Sequence Listing, any protein that is substantially the same as the CryIAb protoxin of SEQ ID No.2, and any insecticidally active fragment thereof, such as the CryIAb toxin. The CryIAb protein includes: naturally occurring variants with substantially the same insecticidal activity, particularly against O. nubilalis, such as the CryIAb protoxin described by Hofte and Whiteley (1989) and in EP 224 331 and the CryIAb protoxin described by Fischhoff et al (1987); and any CryIAb protoxin encoded by a modified or synthetic Bt gene but with substantially the same insecticidal activity as the protoxin of SEQ ID No.2, as described, for example, in PCT publication WO 91/16432 and in European patent applications (&#34;EPA&#34;) 91402920.2 and 92400820.4. &#34;CryIAb toxin&#34;, as used herein, is the protein containing amino acids 29 to 601 of the amino acid sequence shown in SEQ ID No.2 in the Sequence Listing. &#34;Insecticidally active fragment of the CryIAb protein&#34;, as used herein, means any fragment of the CryIAb protoxin having insecticidal activity, preferably the cryIAb toxin. 
     Similarly, the &#34;cryIAb gene&#34; of this invention encompasses the gene with the DNA sequence shown in SEQ ID No.2 or any mutant, synthetic or modified gene encoding a CryIAb protein. Naturally occurring cryIAb genes with minor differences include the gene described in EP 224 331 and the genes listed by Hofte and Whiteley (1989). Modifications, as described above for the cryIB gene, can also be introduced into the cryIAb gene, provided that such modifications do not substantially alter the insecticidal properties, particularly against O. nubilalis, of the encoded CryIAb protein. The isolation and cloning of a cryIAb gene is described in EP 193 259 and by Hofte et al (1986). The gene contains an ORF of 3464 bp, encoding a protoxin of 131 kD and a toxin of 60 kD. The gene can be isolated from the Bt subsp. thuringiensis berliner 1715 strain (Hofte et al, 1986) or from the Bt HD-1 kurstaki strain which is publicly available from the N.R.R.L. 
     Likewise, the &#34;CryIAc protein&#34; of this invention encompasses a protoxin with the amino acid sequence shown in SEQ ID No.3 of the Sequence Listing, any protein that is substantially the same as the CryIAc protoxin of SEQ ID No.3  and any insecticidally active fragment thereof, such as the CryIAc toxin described by Dardenne et al (1990). 
     Likewise, the &#34;cryIAc gene&#34; of this invention encompasses the gene described by Adang et al (1985) with the DNA sequence as shown in SEQ ID No.3 of the Sequence listing or any mutant, synthetic or modified gene, encoding a CryIAc protein. Variants of the cryIAc gene include: the modified or synthetic cryIAc genes described in EP 358 962; and the naturally occurring cryIAc gene described by Dardenne et al (1990), EP 367 474, and PCT publication WO 90/03434 which is a preferred variant differing from the cryIAc DNA sequence of SEQ ID No.3 by 10 nucleotides in the gene part-encoding the toxin (one nucleotide triplet also being deleted in this part, resulting in 3 different amino acids in the toxin and one deleted amino acid). The cryIAc gene can be isolated from the Bt subsp. thuringiensis HD-73 strain, publicly available from the NRRL. 
     In accordance with this invention, one can combat or control Ostrinia species, particularly the European corn borer, by contacting this insect: a) with the CryIB protein or b) with a combination of the CryIB protein and the CryIAb protein or a combination of the CryIB protein and the CryIAc protein, preferably the combination of the CryIB and CryIAb proteins. Such combinations of proteins encompass combinations of the full length protoxins and/or insecticidally active fragments .of such protoxins, achieved for example by co-expression of the corresponding genes and gene fragments in a cell or by expression of a modified gene encoding insecticidally active fragments of both proteins. By &#34;combat&#34; is meant treating plants in a field in such a way as to destroy the Ostrinia (e.g. European corn borers) that are attacking or that would attack the plants such as when a sudden increase in its population would occur; by &#34;control&#34; is meant treating plants in a field in such a way as to limit the Ostrinia&#39;s damage to the plants such as when relatively small numbers of insects are constantly present in the field without causing major damage to the plants; and by &#34;contacting&#34; is meant ensuring that the CryIB protein or a combination of the CryIB and CryIAb or CryIAc proteins is present in a field of plants that is infested, or can be infested, by Ostrinia so that the protein(s) can become ingested by the insects, for example by transforming either the plants, plant-associated microorganisms or other microorganisms, or by applying to the field insecticidal formulations containing the CryIB protein or the combination of the CryIB protein and the CryIAb or CryIAc protein. 
     Contacting Ostrinia with the CryIB protein or a mixture thereof with the CryIAb or CryIAc protein in accordance with this invention can be carried out directly by using an insecticidal composition comprising the CryIB protein or both the CryIB and CryIAb or CryIAc proteins in the form of purified proteins, in the form of Bt strains or their crystals, or in the form of Bt crystal-spore mixtures. By &#34;purified proteins&#34; is meant the CryIB, CryIAb and/or CryIAc proteins purified from their crystal proteins, from transformed microorganisms or from transformed plant cells by methods well known in the art (e.g., as described in EP 193 259). In this regard, such a contacting step can be carried out with naturally occurring or genetically engineered Bt strains, preferably the Bt subsp. entomocidus HD-110, Bt subsp. thuringiensis HD-2 or Bt subsp. thuringiensis 4412 strain (Hofte et al, 1986; Hofte and Whiteley, 1989), containing the cryIB gene or both the cryIB and cryIAb genes. For contacting the insects with both the CryIB and CryIAb protoxins, the Bt subsp. thuringiensis HD-2 strain is preferred, since it has been found to comprise both the cryIB and cryIAb genes (Brizzard et al, 1991). 
     An insecticidal, particularly an anti-Ostrinia, composition comprising the CryIB protein or the CryIB and the CryIAb or CryIAc proteins can be formulated in a conventional manner, together with suitable carriers, diluents, emulsifiers and/or dispersants known in the art. Also, well known methods for stabilizing Cry proteins in the field can be used, such as by delivering the proteins to the field in killed and stabilized microorganisms, or targeting the proteins, synthesized by plants or microorganisms transformed with the cryIB gene or the cryIAb or cryIAc and the cryIB genes to certain intra- or extracellular sites where a higher stability Of the proteins can be obtained. 
     The CryIB protein or the CryIB and CryIAb or CryIAc proteins or killed and stabilized cells of microorganisms containing such proteins can be formulated in insecticidal compositions in a variety of ways, using any number of conventional additives, wet or dry, depending upon the particular use. Additives can include wetting agents, detergents, stabilizers, adhering agents, spreading agents and extenders. Examples of such compositions include pastes, dusting powders, wettable powders, granules, baits and aerosol sprays. Other Bt proteins or killed and stabilized cells of microorganisms containing such proteins and other insecticides, as well as fungicides, biocides, herbicides and fertilizers, can be employed along with the CryIB protein or the CryIB and the CryIAb or CryIAc proteins or killed and stabilized cells containing such proteins to provide additional advantages or benefits. Such an insecticidal composition can be prepared in a conventional manner, and the amount of the CryIB protein or the CryIB and the CryIAb or CryIac proteins employed will depend upon a variety of factors, such as the composition used, the type of area to which the composition is to be applied, and the prevailing weather conditions, but generally the concentration of such proteins will be at least about  0.1% by weight of the formulation, more often from about 0.15% to about 0.8% by weight percent of the formulation. 
     The cryIB gene or the cryIB and the cryIAb or cryIAc genes can, if desired, also be used with their native 5&#39; and 3&#39; signal sequences, to transform microorganisms such as Bt strains, in order to control Ostrinia, particularly O. nubilalis. Of course, other microorganisms can be transformed, such as phages and other viruses, bacteria, fungi and yeasts. Such transformations can be carried out in a conventional manner, preferably by using conventional electroporation methods as described in PCT publication WO 90/06999 or other methods as described by Lereclus et al (1992). To obtain expression in microorganisms other than Bt, such cry genes will have to contain the necessary signal sequences to provide proper expression in such other microorganisms. The BtPGSI387 strain (PCT publication WO 90/06999) is particularly suited for transformation with such cry genes, since this strain is easily fermented by conventional methods (Dulmage, 1981) to provide high yields of cells. The so-transformed microorganism can then be used to produce the CryIB protein or the CryIB and the CryIAb or CryIAc proteins, which could then be formulated for protecting plants from Ostrinia. 
     Contacting Ostrinia, particularly the European corn borer, with the CryIB protein or mixtures thereof in accordance with this invention can also be carried out indirectly, by ensuring that the CryIB protein or the CryIB and the CryIAb or CryIAc proteins are biologically produced at appropriate places by microorganisms or plants expressing the cryIB gene or the cryIAb or cryIAc and the cryIB genes. This can be achieved by inoculating plants or parts of plants, like seeds, with plant-associated microorganisms, transformed with the cryIB gene or the cryIB and the cryIAb or cryIAc genes. By &#34;inoculating&#34; is meant contacting or coating a plant or part of a plant with the microorganisms such that they remain associated with the plant or plant parts. Plant-associated microorganisms, which can be used, include the plant-colonizing (epiphytic) microorganisms like the Pseudomonas bacteria and endophytic plant-colonizing microorganisms like Clavibacter xyli. Transformation of Clavibacter xyli subsp. cynodontis with the cryIB gene or the cryIB and the cryIAb or cryIAc genes can be carried out as described by Turner et al (1991), and these genes are preferably under the control of their original Bt promoter or any other Bt promoter and are flanked by suitable 3&#39; transcription termination signals like the lambda t R  1 transcription terminator sequence (Turner et al, 1991). Stably transforming plants with the cryIB gene or with a combination of the cryIAb or cryIAc and the cryIB genes in accordance with this invention also renders the plants and their progeny resistant to Ostrinia. 
     In order to express the cryIB gene or the cryIB and the cryIAb or cryIAc genes in microorganisms and plants, suitable restriction sites can be introduced, flanking the gene(s). This can be done by site-directed mutagenesis (Stanssens et al, 1989). 
     In order to obtain enhanced expression in plants, it may be preferred to modify the cryIB, cryIAb and/or cryIAc genes as described: in PCT publication WO 91/16432, EPA 91402920.2 and 92400820.4 and by Perlak et al (1991) and Murray et al (1991). A particularly preferred modification to the cryIB gene involves changing the exceptional TTG start codon to the more common ATG start codon by site-directed mutagenesis (Stanssens et al, 1989) as described in EP 408 403. 
     A gene cassette, containing the cryIB gene or the cryIB and the cryIAb or cryIAc genes, can be constructed as described in EP 408 403 in order to express the gene(s) in E. coli and plants. In this regard, insecticidally effective part(s) of such gene(s) can be stably inserted in a conventional manner into the nuclear genome of a single plant cell, and the so-transformed plant cell can be used in a conventional manner to produce a stably transformed plant that is resistant to the European corn borer. In this regard, a disarmed Ti-plasmid, containing the insecticidally effective gene part(s), in Agrobacterium tumefaciens can be used to transform the plant cell using the procedures described, for example, in EP 116 718, EP 270 822, PCT publication WO 84/02913, Deblaere et al (1985), and Gould et al (1991). Preferred Ti-plasmid vectors contain the insecticidally effective gene part(s) between the border sequences, or at least located to the left of the right border sequence, of the T-DNA of the Ti-plasmid. Of course, other types of vectors can be used to transform the plant cell, such as direct gene transfer (as in EP 233 247), pollen-mediated transformation (as in PCT publication WO 85/01856), plant RNA virus-mediated transformation (as in EP 067 553), or liposome-mediated transformation (as in US patent 4,536,475). Other methods described for transforming certain lines of corn (Fromm et al, 1990; Gordon-Kamm et al, 1990) and the more recently described method for transforming monocots generally (PCT publication WO 92/09696) also can be used. 
     The resulting transformed plant can be used in a conventional plant breeding scheme to produce more transformed plants with the same characteristics or to introduce the insecticidally effective gene part(s) in other varieties of the same or related plant species. The seeds, obtained from these plants, contain the respective gene part(s) as stable genomic inserts. Cells of the transformed plant can be cultured to produce the gene products for use in conventional insecticidal compositions. 
     Part(s) of the cryIB or the cryIB and the cryIAb or cryIAc gene(s), encoding insecticidally active fragment(s) of the CryIB or the CryIB and the CryIAb or CryIAC proteins, are inserted in a plant cell genome so that the inserted gene part(s) are downstream (e.g. 3&#39;) of, and under the control of, a promoter which can direct the expression of the gene part(s) in the plant cell; and upstream (e.g. 5&#39;) of suitable 3&#39; end transcription regulation signals (i.e., transcript formation and polyadenylation signals). Preferred promoters include: the strong constitutive 35S promoters of the cauliflower mosaic virus of isolates CM 1841 (Gardner et al, 1981), CabbB-S (Franck et al, 1980) and CabbB-JI (Hull and Howell, 1987); and the TR1&#39; promoter and the TR2&#39; promoter which drive the expression of the 1&#39; and 2&#39; genes, respectively, of the T-DNA (Velten et al, 1984). Alternative promoters are those which are selectively expressed in certain tissues or are inducible promoters (such as the promoter of the ribulose-1,5-bisphosphate carboxylase small subunit gene disclosed in EP 193 259). Preferred polyadenylation and transcript formation signals include those of the octopine synthase gene (Gielen et al, 1984) and the T-DNA gene 7 (Velten and Schell, 1985), which act as 3&#39; untranslated DNA sequences in transformed plant cells. For example, the cryIB gene or the cryIB and the cryIAb or cryIAc genes can be inserted into the pDE110 or pDE108 vector, described in PCT patent publication WO 92/09696, under the control of suitable plant .promoters and flanked by suitable 3&#39; termination sites as described above. These vectors can be used to stably transform corn lines with these genes (e.g., as described in PCT publication WO 92/09696), thus rendering the corn lines resistant to attack by Ostrinia, such as the European corn borer. 
     To achieve co-expression of the cryIB and the cryIAb or cryIAc gene(s) in plants, it is preferred that two plants, each transformed with one of the cry genes, be crossed to obtain a progeny, containing both genes as described, for example, in EP 408 403. The resulting plants are well protected against Ostrinia nubilalis attack by the expression of both the CryIB and the CryIAb or CryIAc proteins in the plant cells. Gene cassettes for co-expression of the cryIB and cryIAb genes in plants are described in EP 408 403. For obtaining enhanced expression in monocots such as corn, the cryIAb or cryIAc and the cryIB genes are preferably modified as described in PCT publication WO 91/16432 and in EPA 91402920.2 and 92400820.4. These modified genes can be transferred to a monocot cell by electroporation as disclosed in PCT publication WO 92/09696 to achieve expression of the genes in monocots after regeneration of the monocot cell to a plant. 
     It is also preferred to provide the transformed plant cells with screenable or selectable marker genes. Suitable marker genes include the neogene (Reiss et al, 1984; EP 242 236), coding for kanamycin resistance. The transformed cells can be provided with a hybrid gene, containing the cry gene(s) and the marker gene under the control of the same promoter. This hybrid gene will be expressed in the transformed cells as a fusion protein (Vaeck et al, 1987). Also hybrid genes, comprising the active fragments of both the cryIB and the cryIAb .or cryIAc genes, can be constructed as described by, for example, Ge et al (1991). 
     The following Examples illustrate the invention. In the Examples, all procedures for making and manipulating DNA are carried out by the standard procedures described by Sambrook et al (1989) Molecular Cloning--A Laboratory Manual, Second Edition, Cold Spring Harbor Laboratory Press, NY, USA. 
    
    
     In the Examples, references are made to the following Figures and Sequence Listing. 
     FIG. 1 shows the binding of iodinated CryIAb toxin to brush border membrane vesicles of O. nubilalis. Membrane vesicles were incubated (30 min.) with iodinated CryIAb toxin in the presence of increasing concentrations of competitor: unlabeled CryIAb (*), CryIAc (∘) and CryIB (□) toxins. The CryIB toxins did not bind to the receptors occupied by the labeled CryIAb toxins, while the CryIAc and CryIAb toxins suppress binding of the LABELLED CryIAb toxins. Curves were predicted by the LIGAND computer program (Munson and Rodbard, 1980). Each point is the mean of three independent experiments (three independently prepared batches of vesicles) . 
    
    
     SEQUENCE LISTING 
     SEQ ID No.1 is the nucleotide sequence of the cryIB gene and the corresponding amino acid sequence of the CryIB protoxin as described in EP 408 403. 
     SEQ ID No.2 is the nucleotide sequence of the cryIAb gene and the corresponding amino acid sequence of the CryIAb protoxin as described in EP 193 259. 
     SEQ ID No.3 is the nucleotide sequence of the cryIAc gene and the corresponding amino acid sequence of the CryIAc protoxin. 
     EXAMPLE 1 
     Insecticidal Activity of the CryIB Toxin 
     The CryIB toxin of SEQ ID No.1, obtained from Bacillus thuringiensis subsp. entomocidus HD-110, was found to be insecticidal to neonate Ostrinia nubilalis (European corn borer) larvae in bio-assays on artificial diet (diet according to Poitout et al, 1972). 
     Multiwell plates were filled with the artificial diet, and sample dilutions of different purified CryI toxins (50 μl) in bovine serum albumin-containing phosphate buffered saline (&#34;PBS-BSA&#34;: 8 mM Na 2  HPO 4 , 2 mM KH 2  PO 4 , 150 mM NaCl and 0.1% BSA) were applied uniformly on the surface of the food and allowed to dry. Mortality was scored after 5 days. The toxicity data were analyzed by probit analysis (Finney, 1962). 
     As shown in Table I below, O. nubilalis is very sensitive to the CryIB toxin. The 50% lethal concentration value is much lower than most other CryI toxins and only the CryIAb toxin is more toxic. Also, the toxicity of the CryIB protoxin against O. nubilalis larvae was found to be comparable to that of the activated toxin, demonstrating that the proteolytical activation of the protoxin in the midgut did not interfere with toxicity. 
     
                       TABLE I                                                     
______________________________________                                    
LC.sub.50 values of solubilized purified CryI toxins to                   
O. nubilalis (LC.sub.50 expressed in ng toxin/cm.sup.2 of                 
diet).                                                                    
CryI Toxin                                                                
        IAa    IAb    IAc  IB   IC    ID    IE                            
______________________________________                                    
LC.sub.50                                                                 
        1247   50     531  105  &gt;1350 &gt;1350 &gt;1350                         
______________________________________                                    
 
    
     Upon spraying of corn plants with the CryIB toxin, the plants are protected from O. nubilalis larvae, which immediately stop feeding upon spraying and do not cause any major damage to the plants. 
     EXAMPLE 2 
     Binding of the CryIB, CryIAb and CryIAc toxins to O. nubilalis Midgut Membranes 
     Receptor binding assays were conducted to compare the binding of the CryIB toxin with that of other CryI toxins. These tests were conducted on Ostrinia midgut brush border membrane vesicles, prepared as described by Wolfersberger et al (1987), using radioligand competition binding experiments as described by Van Rieet al (1989). 
     As shown in FIG. 1, the CryIAb and CryIAc toxins bind to the same receptor sites in the brush border membranes. However, no suppression of CryIAb binding is obtained when adding the CryIB toxin to the assay, indicating that the CryIB toxin binds to a different receptor. 
     Furthermore, immunocytochemical assays, using polyclonal antibodies against the CryIB toxin, showed accumulation of the toxin in the midgut and binding of the toxin to the brush border membranes in previously intoxicated European corn borer larvae. 
     These results show the surprising benefit of using the CryIB protein in combination with the CryIAb protein or the CryIAc protein, particularly with the CryIAb protein, against Ostrinia, particularly O. nubilalis. 
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         __________________________________________________________________________
SEQUENCE LISTING                                                          
(1) GENERAL INFORMATION:                                                  
(iii) NUMBER OF SEQUENCES: 3                                              
(2) INFORMATION FOR SEQ ID NO:1:                                          
(i) SEQUENCE CHARACTERISTICS:                                             
(A) LENGTH: 4074 base pairs                                               
(B) TYPE: nucleic acid                                                    
(C) STRANDEDNESS: double                                                  
(D) TOPOLOGY: linear                                                      
(ii) MOLECULE TYPE: DNA (genomic)                                         
(vi) ORIGINAL SOURCE:                                                     
 (A) ORGANISM: Bacillus thuringiensis                                     
(B) STRAIN: entomocidus HD 110                                            
(ix) FEATURE:                                                             
(A) NAME/KEY: CDS                                                         
(B) LOCATION: 186..3872                                                   
(D) OTHER INFORMATION: /note=&#34;PROPERTIES: CryIB is toxic to               
Ostrinea nubilalis (among others)&#34;                                        
(xi) SEQUENCE DESCRIPTION: SEQ ID NO:1:                                   
AAACTGTGGCTAAGATAAATGGCCCTAAATTATGAAGGTATA TGTGCTAAAGTCCAAAAA60           
GCGGGAGGTAATTCATCAAAAAATTTTACTATACAATTTTCTTAGGTAATGCTGTGTTAA120           
AACTAATCAGTGAAGAAAAGTTAAATAGTTGGTAATATAAGCCCAACATAAAAGGAGGAG180           
TTATATTGACTTCA AATAGGAAAAATGAGAATGAAATTATAAATGCT227                       
MetThrSerAsnArgLysAsnGluAsnGluIleIleAsnAla                                
1510                                                                      
GTATCGAATCATTCCGCACAAAT GGATCTATTACCAGATGCTCGTATT275                      
ValSerAsnHisSerAlaGlnMetAspLeuLeuProAspAlaArgIle                          
15202530                                                                  
GAGGATAGCTTGTGTAT AGCCGAGGGGAACAATATTGATCCATTTGTT323                      
GluAspSerLeuCysIleAlaGluGlyAsnAsnIleAspProPheVal                          
354045                                                                    
AGCGCATCAACAGT CCAAACGGGTATTAACATAGCTGGTAGAATACTA371                      
SerAlaSerThrValGlnThrGlyIleAsnIleAlaGlyArgIleLeu                          
505560                                                                    
GGCGTATTGGGCGT ACCGTTTGCTGGACAACTAGCTAGTTTTTATAGT419                      
GlyValLeuGlyValProPheAlaGlyGlnLeuAlaSerPheTyrSer                          
657075                                                                    
TTTCTTGTTGGTGAATT ATGGCCCCGCGGCAGAGATCAGTGGGAAATT467                      
PheLeuValGlyGluLeuTrpProArgGlyArgAspGlnTrpGluIle                          
808590                                                                    
TTCCTAGAACATGTCGAACAACT TATAAATCAACAAATAACAGAAAAT515                      
PheLeuGluHisValGluGlnLeuIleAsnGlnGlnIleThrGluAsn                          
95100105110                                                               
GCTAGGAATACGGCTCT TGCTCGATTACAAGGTTTAGGAGATTCCTTC563                      
AlaArgAsnThrAlaLeuAlaArgLeuGlnGlyLeuGlyAspSerPhe                          
115120125                                                                 
AGAGCCTATCAACA GTCACTTGAAGATTGGCTAGAAAACCGTGATGAT611                      
ArgAlaTyrGlnGlnSerLeuGluAspTrpLeuGluAsnArgAspAsp                          
130135140                                                                 
GCAAGAACGAGAAG TGTTCTTCATACCCAATATATAGCTTTAGAACTT659                      
AlaArgThrArgSerValLeuHisThrGlnTyrIleAlaLeuGluLeu                          
145150155                                                                 
GATTTTCTTAATGCGAT GCCGCTTTTCGCAATTAGAAACCAAGAAGTT707                      
AspPheLeuAsnAlaMetProLeuPheAlaIleArgAsnGlnGluVal                          
160165170                                                                 
CCATTATTGATGGTATATGCTCA AGCTGCAAATTTACACCTATTATTA755                      
ProLeuLeuMetValTyrAlaGlnAlaAlaAsnLeuHisLeuLeuLeu                          
175180185190                                                              
TTGAGAGATGCCTCTCT TTTTGGTAGTGAATTTGGGCTTACATCGCAG803                      
LeuArgAspAlaSerLeuPheGlySerGluPheGlyLeuThrSerGln                          
195200205                                                                 
GAAATTCAACGCTA TTATGAGCGCCAAGTGGAACGAACGAGAGATTAT851                      
GluIleGlnArgTyrTyrGluArgGlnValGluArgThrArgAspTyr                          
210215220                                                                 
TCCGACTATTGCGT AGAATGGTATAATACAGGTCTAAATAGCTTGAGA899                      
SerAspTyrCysValGluTrpTyrAsnThrGlyLeuAsnSerLeuArg                          
225230235                                                                 
GGGACAAATGCCGCAAG TTGGGTACGGTATAATCAATTCCGTAGAGAT947                      
GlyThrAsnAlaAlaSerTrpValArgTyrAsnGlnPheArgArgAsp                          
240245250                                                                 
CTAACGTTAGGAGTATTAGATCT AGTGGCACTATTCCCAAGCTATGAC995                      
LeuThrLeuGlyValLeuAspLeuValAlaLeuPheProSerTyrAsp                          
255260265270                                                              
ACTCGCACTTATCCAAT AAATACGAGTGCTCAGTTAACAAGAGAAGTT1043                     
ThrArgThrTyrProIleAsnThrSerAlaGlnLeuThrArgGluVal                          
275280285                                                                 
TATACAGACGCAAT TGGAGCAACAGGGGTAAATATGGCAAGTATGAAT1091                     
TyrThrAspAlaIleGlyAlaThrGlyValAsnMetAlaSerMetAsn                          
290295300                                                                 
TGGTATAATAATAA TGCACCTTCGTTCTCTGCCATAGAGGCTGCGGCT1139                     
TrpTyrAsnAsnAsnAlaProSerPheSerAlaIleGluAlaAlaAla                          
305310315                                                                 
ATCCGAAGCCCGCATCT ACTTGATTTTCTAGAACAACTTACAATTTTT1187                     
IleArgSerProHisLeuLeuAspPheLeuGluGlnLeuThrIlePhe                          
320325330                                                                 
AGCGCTTCATCACGATGGAGTAA TACTAGGCATATGACTTATTGGCGG1235                     
SerAlaSerSerArgTrpSerAsnThrArgHisMetThrTyrTrpArg                          
335340345350                                                              
GGGCACACGATTCAATC TCGGCCAATAGGAGGCGGATTAAATACCTCA1283                     
GlyHisThrIleGlnSerArgProIleGlyGlyGlyLeuAsnThrSer                          
355360365                                                                 
ACGCATGGGGCTAC CAATACTTCTATTAATCCTGTAACATTACGGTTC1331                     
ThrHisGlyAlaThrAsnThrSerIleAsnProValThrLeuArgPhe                          
370375380                                                                 
GCATCTCGAGACGT TTATAGGACTGAATCATATGCAGGAGTGCTTCTA1379                     
AlaSerArgAspValTyrArgThrGluSerTyrAlaGlyValLeuLeu                          
385390395                                                                 
TGGGGAATTTACCTTGA ACCTATTCATGGTGTCCCTACTGTTAGGTTT1427                     
TrpGlyIleTyrLeuGluProIleHisGlyValProThrValArgPhe                          
400405410                                                                 
AATTTTACGAACCCTCAGAATAT TTCTGATAGAGGTACCGCTAACTAT1475                     
AsnPheThrAsnProGlnAsnIleSerAspArgGlyThrAlaAsnTyr                          
415420425430                                                              
AGTCAACCTTATGAGTC ACCTGGGCTTCAATTAAAAGATTCAGAAACT1523                     
SerGlnProTyrGluSerProGlyLeuGlnLeuLysAspSerGluThr                          
435440445                                                                 
GAATTACCACCAGA AACAACAGAACGACCAAATTATGAATCTTACAGT1571                     
GluLeuProProGluThrThrGluArgProAsnTyrGluSerTyrSer                          
450455460                                                                 
CACAGGTTATCTCA TATAGGTATAATTTTACAATCCAGGGTGAATGTA1619                     
HisArgLeuSerHisIleGlyIleIleLeuGlnSerArgValAsnVal                          
465470475                                                                 
CCGGTATATTCTTGGAC GCATCGTAGTGCAGATCGTACGAATACGATT1667                     
ProValTyrSerTrpThrHisArgSerAlaAspArgThrAsnThrIle                          
480485490                                                                 
GGACCAAATAGAATCACCCAAAT CCCAATGGTAAAAGCATCCGAACTT1715                     
GlyProAsnArgIleThrGlnIleProMetValLysAlaSerGluLeu                          
495500505510                                                              
CCTCAAGGTACCACTGT TGTTAGAGGACCAGGATTTACTGGTGGGGAT1763                     
ProGlnGlyThrThrValValArgGlyProGlyPheThrGlyGlyAsp                          
515520525                                                                 
ATTCTTCGAAGAAC GAATACTGGTGGATTTGGACCGATAAGAGTAACT1811                     
IleLeuArgArgThrAsnThrGlyGlyPheGlyProIleArgValThr                          
530535540                                                                 
GTTAACGGACCATT AACACAAAGATATCGTATAGGATTCCGCTATGCT1859                     
ValAsnGlyProLeuThrGlnArgTyrArgIleGlyPheArgTyrAla                          
545550555                                                                 
TCAACTGTAGATTTTGA TTTCTTTGTATCACGTGGAGGTACTACTGTA1907                     
SerThrValAspPheAspPhePheValSerArgGlyGlyThrThrVal                          
560565570                                                                 
AATAATTTTAGATTCCTACGTAC AATGAACAGTGGAGACGAACTAAAA1955                     
AsnAsnPheArgPheLeuArgThrMetAsnSerGlyAspGluLeuLys                          
575580585590                                                              
TACGGAAATTTTGTGAG ACGTGCTTTTACTACACCTTTTACTTTTACA2003                     
TyrGlyAsnPheValArgArgAlaPheThrThrProPheThrPheThr                          
595600605                                                                 
CAAATTCAAGATAT AATTCGAACGTCTATTCAAGGCCTTAGTGGAAAT2051                     
GlnIleGlnAspIleIleArgThrSerIleGlnGlyLeuSerGlyAsn                          
610615620                                                                 
GGGGAAGTGTATAT AGATAAAATTGAAATTATTCCAGTTACTGCAACC2099                     
GlyGluValTyrIleAspLysIleGluIleIleProValThrAlaThr                          
625630635                                                                 
TTCGAAGCAGAATATGA TTTAGAAAGAGCGCAAGAGGCGGTGAATGCT2147                     
PheGluAlaGluTyrAspLeuGluArgAlaGlnGluAlaValAsnAla                          
640645650                                                                 
CTGTTTACTAATACGAATCCAAG AAGATTGAAAACAGATGTGACAGAT2195                     
LeuPheThrAsnThrAsnProArgArgLeuLysThrAspValThrAsp                          
655660665670                                                              
TATCATATTGATCAAGT ATCCAATTTAGTGGCGTGTTTATCGGATGAA2243                     
TyrHisIleAspGlnValSerAsnLeuValAlaCysLeuSerAspGlu                          
675680685                                                                 
TTCTGCTTGGATGA AAAGAGAGAATTACTTGAGAAAGTGAAATATGCG2291                     
PheCysLeuAspGluLysArgGluLeuLeuGluLysValLysTyrAla                          
690695700                                                                 
AAACGACTCAGTGA TGAAAGAAACTTACTCCAAGATCCAAACTTCACA2339                     
LysArgLeuSerAspGluArgAsnLeuLeuGlnAspProAsnPheThr                          
705710715                                                                 
TCCATCAATAAGCAACC AGACTTCATATCTACTAATGAGCAATCGAAT2387                     
SerIleAsnLysGlnProAspPheIleSerThrAsnGluGlnSerAsn                          
720725730                                                                 
TTCACATCTATCCATGAACAATC TGAACATGGATGGTGGGGAAGTGAG2435                     
PheThrSerIleHisGluGlnSerGluHisGlyTrpTrpGlySerGlu                          
735740745750                                                              
AACATTACCATCCAGGA AGGAAATGACGTATTTAAAGAGAATTACGTC2483                     
AsnIleThrIleGlnGluGlyAsnAspValPheLysGluAsnTyrVal                          
755760765                                                                 
ACACTACCGGGTAC TTTTAATGAGTGTTATCCGACGTATTTATATCAA2531                     
ThrLeuProGlyThrPheAsnGluCysTyrProThrTyrLeuTyrGln                          
770775780                                                                 
AAAATAGGGGAGTC GGAATTAAAAGCTTATACTCGCTACCAATTAAGA2579                     
LysIleGlyGluSerGluLeuLysAlaTyrThrArgTyrGlnLeuArg                          
785790795                                                                 
GGTTATATTGAAGATAG TCAAGATTTAGAGATATATTTGATTCGTTAT2627                     
GlyTyrIleGluAspSerGlnAspLeuGluIleTyrLeuIleArgTyr                          
800805810                                                                 
AATGCGAAACATGAAACATTGGA TGTTCCAGGTACCGAGTCCCTATGG2675                     
AsnAlaLysHisGluThrLeuAspValProGlyThrGluSerLeuTrp                          
815820825830                                                              
CCGCTTTCAGTTGAAAG CCCAATCGGAAGGTGCGGAGAACCGAATCGA2723                     
ProLeuSerValGluSerProIleGlyArgCysGlyGluProAsnArg                          
835840845                                                                 
TGCGCACCACATTT TGAATGGAATCCTGATCTAGATTGTTCCTGCAGA2771                     
CysAlaProHisPheGluTrpAsnProAspLeuAspCysSerCysArg                          
850855860                                                                 
GATGGAGAAAAATG TGCGCATCATTCCCATCATTTCTCTTTGGATATT2819                     
AspGlyGluLysCysAlaHisHisSerHisHisPheSerLeuAspIle                          
865870875                                                                 
GATGTTGGATGCACAGA CTTGCATGAGAATCTAGGCGTGTGGGTGGTA2867                     
AspValGlyCysThrAspLeuHisGluAsnLeuGlyValTrpValVal                          
880885890                                                                 
TTCAAGATTAAGACGCAGGAAGG TCATGCAAGACTAGGGAATCTGGAA2915                     
PheLysIleLysThrGlnGluGlyHisAlaArgLeuGlyAsnLeuGlu                          
895900905910                                                              
TTTATTGAAGAGAAACC ATTATTAGGAGAAGCACTGTCTCGTGTGAAG2963                     
PheIleGluGluLysProLeuLeuGlyGluAlaLeuSerArgValLys                          
915920925                                                                 
AGGGCAGAGAAAAA ATGGAGAGACAAACGTGAAAAACTACAATTGGAA3011                     
ArgAlaGluLysLysTrpArgAspLysArgGluLysLeuGlnLeuGlu                          
930935940                                                                 
ACAAAACGAGTATA TACAGAGGCAAAAGAAGCTGTGGATGCTTTATTC3059                     
ThrLysArgValTyrThrGluAlaLysGluAlaValAspAlaLeuPhe                          
945950955                                                                 
GTAGATTCTCAATATGA TAGATTACAAGCGGATACAAACATCGGCATG3107                     
ValAspSerGlnTyrAspArgLeuGlnAlaAspThrAsnIleGlyMet                          
960965970                                                                 
ATTCATGCGGCAGATAAACTTGT TCATCGAATTCGAGAGGCGTATCTT3155                     
IleHisAlaAlaAspLysLeuValHisArgIleArgGluAlaTyrLeu                          
975980985990                                                              
TCAGAATTACCTGTTAT CCCAGGTGTAAATGCGGAAATTTTTGAAGAA3203                     
SerGluLeuProValIleProGlyValAsnAlaGluIlePheGluGlu                          
99510001005                                                               
TTAGAAGGTCACA TTATCACTGCAATCTCCTTATACGATGCGAGAAAT3251                     
LeuGluGlyHisIleIleThrAlaIleSerLeuTyrAspAlaArgAsn                          
101010151020                                                              
GTCGTTAAAAAT GGTGATTTTAATAATGGATTAACATGTTGGAATGTA3299                     
ValValLysAsnGlyAspPheAsnAsnGlyLeuThrCysTrpAsnVal                          
102510301035                                                              
AAAGGGCATGTAGAT GTACAACAGAGCCATCATCGTTCTGACCTTGTT3347                     
LysGlyHisValAspValGlnGlnSerHisHisArgSerAspLeuVal                          
104010451050                                                              
ATCCCAGAATGGGAAGCAGA AGTGTCACAAGCAGTTCGCGTCTGTCCG3395                     
IleProGluTrpGluAlaGluValSerGlnAlaValArgValCysPro                          
1055106010651070                                                          
GGGTGTGGCTATA TCCTTCGTGTCACAGCGTACAAAGAGGGATATGGA3443                     
GlyCysGlyTyrIleLeuArgValThrAlaTyrLysGluGlyTyrGly                          
107510801085                                                              
GAGGGCTGC GTAACGATCCATGAAATCGAGAACAATACAGACGAACTA3491                     
GluGlyCysValThrIleHisGluIleGluAsnAsnThrAspGluLeu                          
109010951100                                                              
AAATTTAAA AACCGTGAAGAAGAGGAAGTGTATCCAACGGATACAGGA3539                     
LysPheLysAsnArgGluGluGluGluValTyrProThrAspThrGly                          
110511101115                                                              
ACGTGTAATGA TTATACTGCACACCAAGGTACAGCTGGATGCGCAGAT3587                     
ThrCysAsnAspTyrThrAlaHisGlnGlyThrAlaGlyCysAlaAsp                          
112011251130                                                              
GCATGTAATTCCCGTA ATGCTGGATATGAGGATGCATATGAAGTTGAT3635                     
AlaCysAsnSerArgAsnAlaGlyTyrGluAspAlaTyrGluValAsp                          
1135114011451150                                                          
ACTACAGCA TCTGTTAATTACAAACCGACTTATGAAGAAGAAACGTAT3683                     
ThrThrAlaSerValAsnTyrLysProThrTyrGluGluGluThrTyr                          
115511601165                                                              
ACAGAT GTAAGAAGAGATAATCATTGTGAATATGACAGAGGGTATGTC3731                     
ThrAspValArgArgAspAsnHisCysGluTyrAspArgGlyTyrVal                          
117011751180                                                              
AATTA TCCACCAGTACCAGCTGGTTATGTGACAAAAGAATTAGAATAC3779                     
AsnTyrProProValProAlaGlyTyrValThrLysGluLeuGluTyr                          
118511901195                                                              
TTCCCAG AAACAGATACAGTATGGATTGAGATTGGAGAAACGGAAGGA3827                     
PheProGluThrAspThrValTrpIleGluIleGlyGluThrGluGly                          
120012051210                                                              
AAGTTTATTGTA GATAGCGTGGAATTACTCCTCATGGAAGAATAGGATCATC3879                 
LysPheIleValAspSerValGluLeuLeuLeuMetGluGlu                                
121512201225                                                              
CAAGTATAGCAGTTTAATAAATATTAATTAAA ATAGTAGTCTAACTTCCGTTCCAATTAA3939         
ATAAGTAAATTACAGTTGTAAAAAGAAAACGGACATCACTCTTCAGAGAGCGATGTCCGT3999          
TTTTTATATGGTTTGTGCTAATGATAAGTGTGCACGAAATTTTATTGTCAAAATAGTATT4059          
TACTTGA GAAAAAGA4074                                                      
(2) INFORMATION FOR SEQ ID NO:2:                                          
(i) SEQUENCE CHARACTERISTICS:                                             
(A) LENGTH: 4343 base pairs                                               
(B) TYPE: nucleic acid                                                    
(C) STRANDEDNESS: double                                                  
(D) TOPOLOGY: linear                                                      
(ii) MOLECULE TYPE: DNA (genomic)                                         
(vi) ORIGINAL SOURCE:                                                     
 (A) ORGANISM: Bacillus thuringiensis                                     
(B) STRAIN: berliner 1715                                                 
(ix) FEATURE:                                                             
(A) NAME/KEY: CDS                                                         
(B) LOCATION: 141..3608                                                   
(D) OTHER INFORMATION: /note=&#34;coding sequence for CryIAb                  
insecticidal crystal protein                                              
PROPERTIES: CryIAb is toxic to Ostrinia nubilalis                         
(amongothers)&#34;                                                            
(xi) SEQUENCE DESCRIPTION: SEQ ID NO:2:                                   
CAAAAATTGATATTTAGTAAAATTAGTTGCACTTTGTGCATTTTTTCATAAGATGAGTCA60            
TATGTTTTAAATTGTAGTAATGAAAAACAGTATTATATCATAATGAATTGGTATCTTAAT120           
AAAAGAGATGGAGGTAACTTATGGATAACAATCC GAACATCAATGAATGC170                    
MetAspAsnAsnProAsnIleAsnGluCys                                            
1510                                                                      
ATTCCTTATAATTGTTTAAGTAACCCT GAAGTAGAAGTATTAGGTGGA218                      
IleProTyrAsnCysLeuSerAsnProGluValGluValLeuGlyGly                          
152025                                                                    
GAAAGAATAGAAACTGGTTACACC CCAATCGATATTTCCTTGTCGCTA266                      
GluArgIleGluThrGlyTyrThrProIleAspIleSerLeuSerLeu                          
303540                                                                    
ACGCAATTTCTTTTGAGTGAATTT GTTCCCGGTGCTGGATTTGTGTTA314                      
ThrGlnPheLeuLeuSerGluPheValProGlyAlaGlyPheValLeu                          
455055                                                                    
GGACTAGTTGATATAATATGGGGAATT TTTGGTCCCTCTCAATGGGAC362                      
GlyLeuValAspIleIleTrpGlyIlePheGlyProSerGlnTrpAsp                          
606570                                                                    
GCATTTCTTGTACAAATTGAACAGTTAATTAAC CAAAGAATAGAAGAA410                      
AlaPheLeuValGlnIleGluGlnLeuIleAsnGlnArgIleGluGlu                          
75808590                                                                  
TTCGCTAGGAACCAAGCCATTTCTAGA TTAGAAGGACTAAGCAATCTT458                      
PheAlaArgAsnGlnAlaIleSerArgLeuGluGlyLeuSerAsnLeu                          
95100105                                                                  
TATCAAATTTACGCAGAATCTTTT AGAGAGTGGGAAGCAGATCCTACT506                      
TyrGlnIleTyrAlaGluSerPheArgGluTrpGluAlaAspProThr                          
110115120                                                                 
AATCCAGCATTAAGAGAAGAGATG CGTATTCAATTCAATGACATGAAC554                      
AsnProAlaLeuArgGluGluMetArgIleGlnPheAsnAspMetAsn                          
125130135                                                                 
AGTGCCCTTACAACCGCTATTCCTCTT TTTGCAGTTCAAAATTATCAA602                      
SerAlaLeuThrThrAlaIleProLeuPheAlaValGlnAsnTyrGln                          
140145150                                                                 
GTTCCTCTTTTATCAGTATATGTTCAAGCTGCA AATTTACATTTATCA650                      
ValProLeuLeuSerValTyrValGlnAlaAlaAsnLeuHisLeuSer                          
155160165170                                                              
GTTTTGAGAGATGTTTCAGTGTTTGGA CAAAGGTGGGGATTTGATGCC698                      
ValLeuArgAspValSerValPheGlyGlnArgTrpGlyPheAspAla                          
175180185                                                                 
GCGACTATCAATAGTCGTTATAAT GATTTAACTAGGCTTATTGGCAAC746                      
AlaThrIleAsnSerArgTyrAsnAspLeuThrArgLeuIleGlyAsn                          
190195200                                                                 
TATACAGATCATGCTGTACGCTGG TACAATACGGGATTAGAGCGTGTA794                      
TyrThrAspHisAlaValArgTrpTyrAsnThrGlyLeuGluArgVal                          
205210215                                                                 
TGGGGACCGGATTCTAGAGATTGGATA AGATATAATCAATTTAGAAGA842                      
TrpGlyProAspSerArgAspTrpIleArgTyrAsnGlnPheArgArg                          
220225230                                                                 
GAATTAACACTAACTGTATTAGATATCGTTTCT CTATTTCCGAACTAT890                      
GluLeuThrLeuThrValLeuAspIleValSerLeuPheProAsnTyr                          
235240245250                                                              
GATAGTAGAACGTATCCAATTCGAACA GTTTCCCAATTAACAAGAGAA938                      
AspSerArgThrTyrProIleArgThrValSerGlnLeuThrArgGlu                          
255260265                                                                 
ATTTATACAAACCCAGTATTAGAA AATTTTGATGGTAGTTTTCGAGGC986                      
IleTyrThrAsnProValLeuGluAsnPheAspGlySerPheArgGly                          
270275280                                                                 
TCGGCTCAGGGCATAGAAGGAAGT ATTAGGAGTCCACATTTGATGGAT1034                     
SerAlaGlnGlyIleGluGlySerIleArgSerProHisLeuMetAsp                          
285290295                                                                 
ATACTTAACAGTATAACCATCTATACG GATGCTCATAGAGGAGAATAT1082                     
IleLeuAsnSerIleThrIleTyrThrAspAlaHisArgGlyGluTyr                          
300305310                                                                 
TATTGGTCAGGGCATCAAATAATGGCTTCTCCT GTAGGGTTTTCGGGG1130                     
TyrTrpSerGlyHisGlnIleMetAlaSerProValGlyPheSerGly                          
315320325330                                                              
CCAGAATTCACTTTTCCGCTATATGGA ACTATGGGAAATGCAGCTCCA1178                     
ProGluPheThrPheProLeuTyrGlyThrMetGlyAsnAlaAlaPro                          
335340345                                                                 
CAACAACGTATTGTTGCTCAACTA GGTCAGGGCGTGTATAGAACATTA1226                     
GlnGlnArgIleValAlaGlnLeuGlyGlnGlyValTyrArgThrLeu                          
350355360                                                                 
TCGTCCACTTTATATAGAAGACCT TTTAATATAGGGATAAATAATCAA1274                     
SerSerThrLeuTyrArgArgProPheAsnIleGlyIleAsnAsnGln                          
365370375                                                                 
CAACTATCTGTTCTTGACGGGACAGAA TTTGCTTATGGAACCTCCTCA1322                     
GlnLeuSerValLeuAspGlyThrGluPheAlaTyrGlyThrSerSer                          
380385390                                                                 
AATTTGCCATCCGCTGTATACAGAAAAAGCGGA ACGGTAGATTCGCTG1370                     
AsnLeuProSerAlaValTyrArgLysSerGlyThrValAspSerLeu                          
395400405410                                                              
GATGAAATACCGCCACAGAATAACAAC GTGCCACCTAGGCAAGGATTT1418                     
AspGluIleProProGlnAsnAsnAsnValProProArgGlnGlyPhe                          
415420425                                                                 
AGTCATCGATTAAGCCATGTTTCA ATGTTTCGTTCAGGCTTTAGTAAT1466                     
SerHisArgLeuSerHisValSerMetPheArgSerGlyPheSerAsn                          
430435440                                                                 
AGTAGTGTAAGTATAATAAGAGCT CCTATGTTCTCTTGGATACATCGT1514                     
SerSerValSerIleIleArgAlaProMetPheSerTrpIleHisArg                          
445450455                                                                 
AGTGCTGAATTTAATAATATAATTCCT TCATCACAAATTACACAAATA1562                     
SerAlaGluPheAsnAsnIleIleProSerSerGlnIleThrGlnIle                          
460465470                                                                 
CCTTTAACAAAATCTACTAATCTTGGCTCTGGA ACTTCTGTCGTTAAA1610                     
ProLeuThrLysSerThrAsnLeuGlySerGlyThrSerValValLys                          
475480485490                                                              
GGACCAGGATTTACAGGAGGAGATATT CTTCGAAGAACTTCACCTGGC1658                     
GlyProGlyPheThrGlyGlyAspIleLeuArgArgThrSerProGly                          
495500505                                                                 
CAGATTTCAACCTTAAGAGTAAAT ATTACTGCACCATTATCACAAAGA1706                     
GlnIleSerThrLeuArgValAsnIleThrAlaProLeuSerGlnArg                          
510515520                                                                 
TATCGGGTAAGAATTCGCTACGCT TCTACCACAAATTTACAATTCCAT1754                     
TyrArgValArgIleArgTyrAlaSerThrThrAsnLeuGlnPheHis                          
525530535                                                                 
ACATCAATTGACGGAAGACCTATTAAT CAGGGGAATTTTTCAGCAACT1802                     
ThrSerIleAspGlyArgProIleAsnGlnGlyAsnPheSerAlaThr                          
540545550                                                                 
ATGAGTAGTGGGAGTAATTTACAGTCCGGAAGC TTTAGGACTGTAGGT1850                     
MetSerSerGlySerAsnLeuGlnSerGlySerPheArgThrValGly                          
555560565570                                                              
TTTACTACTCCGTTTAACTTTTCAAAT GGATCAAGTGTATTTACGTTA1898                     
PheThrThrProPheAsnPheSerAsnGlySerSerValPheThrLeu                          
575580585                                                                 
AGTGCTCATGTCTTCAATTCAGGC AATGAAGTTTATATAGATCGAATT1946                     
SerAlaHisValPheAsnSerGlyAsnGluValTyrIleAspArgIle                          
590595600                                                                 
GAATTTGTTCCGGCAGAAGTAACC TTTGAGGCAGAATATGATTTAGAA1994                     
GluPheValProAlaGluValThrPheGluAlaGluTyrAspLeuGlu                          
605610615                                                                 
AGAGCACAAAAGGCGGTGAATGAGCTG TTTACTTCTTCCAATCAAATC2042                     
ArgAlaGlnLysAlaValAsnGluLeuPheThrSerSerAsnGlnIle                          
620625630                                                                 
GGGTTAAAAACAGATGTGACGGATTATCATATT GATCAAGTATCCAAT2090                     
GlyLeuLysThrAspValThrAspTyrHisIleAspGlnValSerAsn                          
635640645650                                                              
TTAGTTGAGTGTTTATCTGATGAATTT TGTCTGGATGAAAAAAAAGAA2138                     
LeuValGluCysLeuSerAspGluPheCysLeuAspGluLysLysGlu                          
655660665                                                                 
TTGTCCGAGAAAGTCAAACATGCG AAGCGACTTAGTGATGAGCGGAAT2186                     
LeuSerGluLysValLysHisAlaLysArgLeuSerAspGluArgAsn                          
670675680                                                                 
TTACTTCAAGATCCAAACTTTAGA GGGATCAATAGACAACTAGACCGT2234                     
LeuLeuGlnAspProAsnPheArgGlyIleAsnArgGlnLeuAspArg                          
685690695                                                                 
GGCTGGAGAGGAAGTACGGATATTACC ATCCAAGGAGGCGATGACGTA2282                     
GlyTrpArgGlySerThrAspIleThrIleGlnGlyGlyAspAspVal                          
700705710                                                                 
TTCAAAGAGAATTACGTTACGCTATTGGGTACC TTTGATGAGTGCTAC2330                     
PheLysGluAsnTyrValThrLeuLeuGlyThrPheAspGluCysTyr                          
715720725730                                                              
TTAACGTATTTATATCAAAAAATAGAT GAGTCGAAATTAAAAGCCTAT2378                     
LeuThrTyrLeuTyrGlnLysIleAspGluSerLysLeuLysAlaTyr                          
735740745                                                                 
ACCCGTTACCAATTAAGAGGGTAT ATCGAAGATAGTCAAGACTTAGAA2426                     
ThrArgTyrGlnLeuArgGlyTyrIleGluAspSerGlnAspLeuGlu                          
750755760                                                                 
ATCTATTTAATTCGCTACAATGCC AAACACGAAACAGTAAATGTGCCA2474                     
IleTyrLeuIleArgTyrAsnAlaLysHisGluThrValAsnValPro                          
765770775                                                                 
GGTACGGGTTCCTTATGGCGCCTTTCA GCCCCAAGTCCAATCGGAAAA2522                     
GlyThrGlySerLeuTrpArgLeuSerAlaProSerProIleGlyLys                          
780785790                                                                 
TGTGCCCATCATTCCCATCATTTCTCCTTGGAC ATTGATGTTGGATGT2570                     
CysAlaHisHisSerHisHisPheSerLeuAspIleAspValGlyCys                          
795800805810                                                              
ACAGACTTAAATGAGGACTTAGGTGTA TGGGTGATATTCAAGATTAAG2618                     
ThrAspLeuAsnGluAspLeuGlyValTrpValIlePheLysIleLys                          
815820825                                                                 
ACGCAAGATGGCCATGCAAGACTA GGAAATCTAGAATTTCTCGAAGAG2666                     
ThrGlnAspGlyHisAlaArgLeuGlyAsnLeuGluPheLeuGluGlu                          
830835840                                                                 
AAACCATTAGTAGGAGAAGCACTA GCTCGTGTGAAAAGAGCGGAGAAA2714                     
LysProLeuValGlyGluAlaLeuAlaArgValLysArgAlaGluLys                          
845850855                                                                 
AAATGGAGAGACAAACGTGAAAAATTG GAATGGGAAACAAATATTGTT2762                     
LysTrpArgAspLysArgGluLysLeuGluTrpGluThrAsnIleVal                          
860865870                                                                 
TATAAAGAGGCAAAAGAATCTGTAGATGCTTTA TTTGTAAACTCTCAA2810                     
TyrLysGluAlaLysGluSerValAspAlaLeuPheValAsnSerGln                          
875880885890                                                              
TATGATAGATTACAAGCGGATACCAAC ATCGCGATGATTCATGCGGCA2858                     
TyrAspArgLeuGlnAlaAspThrAsnIleAlaMetIleHisAlaAla                          
895900905                                                                 
GATAAACGCGTTCATAGCATTCGA GAAGCTTATCTGCCTGAGCTGTCT2906                     
AspLysArgValHisSerIleArgGluAlaTyrLeuProGluLeuSer                          
910915920                                                                 
GTGATTCCGGGTGTCAATGCGGCT ATTTTTGAAGAATTAGAAGGGCGT2954                     
ValIleProGlyValAsnAlaAlaIlePheGluGluLeuGluGlyArg                          
925930935                                                                 
ATTTTCACTGCATTCTCCCTATATGAT GCGAGAAATGTCATTAAAAAT3002                     
IlePheThrAlaPheSerLeuTyrAspAlaArgAsnValIleLysAsn                          
940945950                                                                 
GGTGATTTTAATAATGGCTTATCCTGCTGGAAC GTGAAAGGGCATGTA3050                     
GlyAspPheAsnAsnGlyLeuSerCysTrpAsnValLysGlyHisVal                          
955960965970                                                              
GATGTAGAAGAACAAAACAACCACCGT TCGGTCCTTGTTGTTCCGGAA3098                     
AspValGluGluGlnAsnAsnHisArgSerValLeuValValProGlu                          
975980985                                                                 
TGGGAAGCAGAAGTGTCACAAGAA GTTCGTGTCTGTCCGGGTCGTGGC3146                     
TrpGluAlaGluValSerGlnGluValArgValCysProGlyArgGly                          
9909951000                                                                
TATATCCTTCGTGTCACAGCGTAC AAGGAGGGATATGGAGAAGGTTGC3194                     
TyrIleLeuArgValThrAlaTyrLysGluGlyTyrGlyGluGlyCys                          
100510101015                                                              
GTAACCATTCATGAGATCGAGAACAA TACAGACGAACTGAAGTTTAGC3242                     
ValThrIleHisGluIleGluAsnAsnThrAspGluLeuLysPheSer                          
102010251030                                                              
AACTGTGTAGAAGAGGAAGTATATCCAAACA ACACGGTAACGTGTAAT3290                     
AsnCysValGluGluGluValTyrProAsnAsnThrValThrCysAsn                          
1035104010451050                                                          
GATTATACTGCGACTCAAGAAGAA TATGAGGGTACGTACACTTCTCGT3338                     
AspTyrThrAlaThrGlnGluGluTyrGluGlyThrTyrThrSerArg                          
105510601065                                                              
AATCGAGGATATGACGGAGCC TATGAAAGCAATTCTTCTGTACCAGCT3386                     
AsnArgGlyTyrAspGlyAlaTyrGluSerAsnSerSerValProAla                          
107010751080                                                              
GATTATGCATCAGCCTATGA AGAAAAAGCATATACAGATGGACGAAGA3434                     
AspTyrAlaSerAlaTyrGluGluLysAlaTyrThrAspGlyArgArg                          
108510901095                                                              
GACAATCCTTGTGAATCTAACA GAGGATATGGGGATTACACACCACTA3482                     
AspAsnProCysGluSerAsnArgGlyTyrGlyAspTyrThrProLeu                          
110011051110                                                              
CCAGCTGGCTATGTGACAAAAGAATTA GAGTACTTCCCAGAAACCGAT3530                     
ProAlaGlyTyrValThrLysGluLeuGluTyrPheProGluThrAsp                          
1115112011251130                                                          
AAGGTATGGATTGAGATCGGA GAAACGGAAGGAACATTCATCGTGGAC3578                     
LysValTrpIleGluIleGlyGluThrGluGlyThrPheIleValAsp                          
113511401145                                                              
AGCGTGGAATTACTTCT TATGGAGGAATAATATATGCTTTAAAATGT3625                      
SerValGluLeuLeuLeuMetGluGlu                                               
11501155                                                                  
AAGGTGTGCAAATAAAGAATGATTACTGACTTGTATTGACAGATAAATAAGGAAATTTTT3 685         
ATATGAATAAAAAACGGGCATCACTCTTAAAAGAATGATGTCCGTTTTTTGTATGATTTA3745          
ACGAGTGATATTTAAATGTTTTTTTGCGAAGGCTTTACTTAACGGGGTACCGCCACATGC3805          
CCATCAACTTAAGAATTTGCACTACCCCCAAGTGTCAA AAAACGTTATTCTTTCTAAAAA3865         
GCTAGCTAGAAAGGATGACATTTTTTATGAATCTTTCAATTCAAGATGAATTACAACTAT3925          
TTTCTGAAGAGCTGTATCGTCATTTAACCCCTTCTCTTTTGGAAGAACTCGCTAAAGAAT3985          
TAGGTTTTGTAA AAAGAAAACGAAAGTTTTCAGGAAATGAATTAGCTACCATATGTATCT4045         
GGGTCAGTCAACGTACAGCGAGTGATTCTCTCGTTCGACTATGCAGTCAATTACACGCCG4105          
CCACAGGACCTCTTATGAGTCCAGAAGGACTCAATAAACGCTTTGATAAAAAAGCG GTTG4165         
AATTTTTGAAATATATTTTTTCTGCATTATGGAAAAGTAAACTTTGTAAAACATCAGCCA4225          
TTTCAAGTGCAGCACTCACGTATTTTCAACGAATCCGTATTTTAGATGCGACGATTTTCC4285          
AAGTACCGAAACATTTAGCACATGTATATC CTGGGTCAGGTGGTTGTGCACAAACTGC4343           
(2) INFORMATION FOR SEQ ID NO:3:                                          
(i) SEQUENCE CHARACTERISTICS:                                             
(A) LENGTH: 3537 base pairs                                               
(B) TYPE: nucleic acid                                                    
(C) STRANDEDNESS: double                                                  
(D) TOPOLOGY: linear                                                      
(ii) MOLECULE TYPE: DNA (genomic)                                         
(vi) ORIGINAL SOURCE:                                                     
(A) ORGANISM: Bacillus thuringiensis                                      
 (B) STRAIN: kurstaki HD-73                                               
(ix) FEATURE:                                                             
(A) NAME/KEY: CDS                                                         
(B) LOCATION: 1..3537                                                     
(D) OTHER INFORMATION: /note=&#34;FEATURES: sequence encodes                  
CryIAc insecticidal crystal protein                                       
PROPERTIES: CryIAc is toxic to Ostrinia nubilalis                         
(amongothers)                                                             
(xi) SEQUENCE DESCRIPTION: SEQ ID NO:3:                                   
ATGGATAACAATCCG AACATCAATGAATGCATTCCTTATAATTGTTTA48                       
MetAspAsnAsnProAsnIleAsnGluCysIleProTyrAsnCysLeu                          
151015                                                                    
AGTAACCCTGAA GTAGAAGTATTAGGTGGAGAAAGAATAGAAACTGGT96                       
SerAsnProGluValGluValLeuGlyGlyGluArgIleGluThrGly                          
202530                                                                    
TACACCCCAATC GATATTTCCTTGTCGCTAACGCAATTTCTTTTGAGT144                      
TyrThrProIleAspIleSerLeuSerLeuThrGlnPheLeuLeuSer                          
354045                                                                    
GAATTTGTTCCCGGT GCTGGATTTGTGTTAGGACTAGTTGATATAATA192                      
GluPheValProGlyAlaGlyPheValLeuGlyLeuValAspIleIle                          
505560                                                                    
TGGGGAATTTTTGGTCCCTCT CAATGGGACGCATTTCTTGTACAAATT240                      
TrpGlyIlePheGlyProSerGlnTrpAspAlaPheLeuValGlnIle                          
65707580                                                                  
GAACAGTTAATTAAC CAAAGAATAGAAGAATTCGCTAGGAACCAAGCC288                      
GluGlnLeuIleAsnGlnArgIleGluGluPheAlaArgAsnGlnAla                          
859095                                                                    
ATTTCTAGATTA GAAGGACTAAGCAATCTTTATCAAATTTACGCAGAA336                      
IleSerArgLeuGluGlyLeuSerAsnLeuTyrGlnIleTyrAlaGlu                          
100105110                                                                 
TCTTTTAGAGAG TGGGAAGCAGATCCTACTAATCCAGCATTAAGAGAA384                      
SerPheArgGluTrpGluAlaAspProThrAsnProAlaLeuArgGlu                          
115120125                                                                 
GAGATGCGTATTCAA TTCAATGACATGAACAGTGCCCTTACAACCGCT432                      
GluMetArgIleGlnPheAsnAspMetAsnSerAlaLeuThrThrAla                          
130135140                                                                 
ATTCCTCTTTTTGCAGTTCAA AATTATCAAGTTCCTCTTTTATCAGTA480                      
IleProLeuPheAlaValGlnAsnTyrGlnValProLeuLeuSerVal                          
145150155160                                                              
TATGTTCAAGCTGCA AATTTACATTTATCAGTTTTGAGAGATGTTTCA528                      
TyrValGlnAlaAlaAsnLeuHisLeuSerValLeuArgAspValSer                          
165170175                                                                 
GTGTTTGGACAA AGGTGGGGATTTGATGCCGCGACTATCAATAGTCGT576                      
ValPheGlyGlnArgTrpGlyPheAspAlaAlaThrIleAsnSerArg                          
180185190                                                                 
TATAATGATTTA ACTAGGCTTATTGGCAACTATACAGATTATGCTGTA624                      
TyrAsnAspLeuThrArgLeuIleGlyAsnTyrThrAspTyrAlaVal                          
195200205                                                                 
CGCTGGTACAATACG GGATTAGAACGTGTATGGGGACCGGATTCTAGA672                      
ArgTrpTyrAsnThrGlyLeuGluArgValTrpGlyProAspSerArg                          
210215220                                                                 
GATTGGGTAAGGTATAATCAA TTTAGAAGAGAATTAACACTAACTGTA720                      
AspTrpValArgTyrAsnGlnPheArgArgGluLeuThrLeuThrVal                          
225230235240                                                              
TTAGATATCGTTGCT CTGTTCCCGAATTATGATAGTAGAAGATATCCA768                      
LeuAspIleValAlaLeuPheProAsnTyrAspSerArgArgTyrPro                          
245250255                                                                 
ATTCGAACAGTT TCCCAATTAACAAGAGAAATTTATACAAACCCAGTA816                      
IleArgThrValSerGlnLeuThrArgGluIleTyrThrAsnProVal                          
260265270                                                                 
TTAGAAAATTTT GATGGTAGTTTTCGAGGCTCGGCTCAGGGCATAGAA864                      
LeuGluAsnPheAspGlySerPheArgGlySerAlaGlnGlyIleGlu                          
275280285                                                                 
AGAAGTATTAGGAGT CCACATTTGATGGATATACTTAACAGTATAACC912                      
ArgSerIleArgSerProHisLeuMetAspIleLeuAsnSerIleThr                          
290295300                                                                 
ATCTATACGGATGCTCATAGG GGTTATTATTATTGGTCAGGGCATCAA960                      
IleTyrThrAspAlaHisArgGlyTyrTyrTyrTrpSerGlyHisGln                          
305310315320                                                              
ATAATGGCTTCTCCT GTAGGGTTTTCGGGGCCAGAATTCACTTTTCCG1008                     
IleMetAlaSerProValGlyPheSerGlyProGluPheThrPhePro                          
325330335                                                                 
CTATATGGAACT ATGGGAAATGCAGCTCCACAACAACGTATTGTTGCT1056                     
LeuTyrGlyThrMetGlyAsnAlaAlaProGlnGlnArgIleValAla                          
340345350                                                                 
CAACTAGGTCAG GGCGTGTATAGAACATTATCGTCCACTTTATATAGA1104                     
GlnLeuGlyGlnGlyValTyrArgThrLeuSerSerThrLeuTyrArg                          
355360365                                                                 
AGACCTTTTAATATA GGGATAAATAATCAACAACTATCTGTTCTTGAC1152                     
ArgProPheAsnIleGlyIleAsnAsnGlnGlnLeuSerValLeuAsp                          
370375380                                                                 
GGGACAGAATTTGCTTATGGA ACCTCCTCAAATTTGCCATCCGCTGTA1200                     
GlyThrGluPheAlaTyrGlyThrSerSerAsnLeuProSerAlaVal                          
385390395400                                                              
TACAGAAAAAGCGGA ACGGTAGATTCGCTGGATGAAATACCGCCACAG1248                     
TyrArgLysSerGlyThrValAspSerLeuAspGluIleProProGln                          
405410415                                                                 
AATAACAACGTG CCACCTAGGCAAGGATTTAGTCATCGATTAAGCCAT1296                     
AsnAsnAsnValProProArgGlnGlyPheSerHisArgLeuSerHis                          
420425430                                                                 
GTTTCAATGTTT CGTTCAGGCTTTAGTAATAGTAGTGTAAGTATAATA1344                     
ValSerMetPheArgSerGlyPheSerAsnSerSerValSerIleIle                          
435440445                                                                 
AGAGCTCCTATGTTC TCTTGGATACATCGTAGTGCTGAATTTAATAAT1392                     
ArgAlaProMetPheSerTrpIleHisArgSerAlaGluPheAsnAsn                          
450455460                                                                 
ATAATTGCATCGGATAGTATT ACTCAAATCCCTGCAGTGAAGGGAAAC1440                     
IleIleAlaSerAspSerIleThrGlnIleProAlaValLysGlyAsn                          
465470475480                                                              
TTTCTTTTTAATGGT TCTGTAATTTCAGGACCAGGATTTACTGGTGGG1488                     
PheLeuPheAsnGlySerValIleSerGlyProGlyPheThrGlyGly                          
485490495                                                                 
GACTTAGTTAGA TTAAATAGTAGTGGAAATAACATTCAGAATAGAGGG1536                     
AspLeuValArgLeuAsnSerSerGlyAsnAsnIleGlnAsnArgGly                          
500505510                                                                 
TATATTGAAGTT CCAATTCACTTCCCATCGACATCTACCAGATATCGA1584                     
TyrIleGluValProIleHisPheProSerThrSerThrArgTyrArg                          
515520525                                                                 
GTTCGTGTACGGTAT GCTTCTGTAACCCCGATTCACCTCAACGTTAAT1632                     
ValArgValArgTyrAlaSerValThrProIleHisLeuAsnValAsn                          
530535540                                                                 
TGGGGTAATTCATCCATTTTT TCCAATACAGTACCAGCTACAGCTACG1680                     
TrpGlyAsnSerSerIlePheSerAsnThrValProAlaThrAlaThr                          
545550555560                                                              
TCATTAGATAATCTA CAATCAAGTGATTTTGGTTATTTTGAAAGTGCC1728                     
SerLeuAspAsnLeuGlnSerSerAspPheGlyTyrPheGluSerAla                          
565570575                                                                 
AATGCTTTTACA TCTTCATTAGGTAATATAGTAGGTGTTAGAAATTTT1776                     
AsnAlaPheThrSerSerLeuGlyAsnIleValGlyValArgAsnPhe                          
580585590                                                                 
AGTGGGACTGCA GGAGTGATAATAGACAGATTTGAATTTATTCCAGTT1824                     
SerGlyThrAlaGlyValIleIleAspArgPheGluPheIleProVal                          
595600605                                                                 
ACTGCAACACTCGAG GCTGAATATAATCTGGAAAGAGCGCAGAAGGCG1872                     
ThrAlaThrLeuGluAlaGluTyrAsnLeuGluArgAlaGlnLysAla                          
610615620                                                                 
GTGAATGCGCTGTTTACGTCT ACAAACCAACTAGGGCTAAAAACAAAT1920                     
ValAsnAlaLeuPheThrSerThrAsnGlnLeuGlyLeuLysThrAsn                          
625630635640                                                              
GTAACGGATTATCAT ATTGATCAAGTGTCCAATTTAGTTACGTATTTA1968                     
ValThrAspTyrHisIleAspGlnValSerAsnLeuValThrTyrLeu                          
645650655                                                                 
TCGGATGAATTT TGTCTGGATGAAAAGCGAGAATTGTCCGAGAAAGTC2016                     
SerAspGluPheCysLeuAspGluLysArgGluLeuSerGluLysVal                          
660665670                                                                 
AAACATGCGAAG CGACTCAGTGATGAACGCAATTTACTCCAAGATTCA2064                     
LysHisAlaLysArgLeuSerAspGluArgAsnLeuLeuGlnAspSer                          
675680685                                                                 
AATTTCAAAGACATT AATAGGCAACCAGAACGTGGGTGGGGCGGAAGT2112                     
AsnPheLysAspIleAsnArgGlnProGluArgGlyTrpGlyGlySer                          
690695700                                                                 
ACAGGGATTACCATCCAAGGA GGGGATGACGTATTTAAAGAAAATTAC2160                     
ThrGlyIleThrIleGlnGlyGlyAspAspValPheLysGluAsnTyr                          
705710715720                                                              
GTCACACTATCAGGT ACCTTTGATGAGTGCTATCCAACATATTTGTAT2208                     
ValThrLeuSerGlyThrPheAspGluCysTyrProThrTyrLeuTyr                          
725730735                                                                 
CAAAAAATCGAT GAATCAAAATTAAAAGCCTTTACCCGTTATCAATTA2256                     
GlnLysIleAspGluSerLysLeuLysAlaPheThrArgTyrGlnLeu                          
740745750                                                                 
AGAGGGTATATC GAAGATAGTCAAGACTTAGAAATCTATTTAATTCGC2304                     
ArgGlyTyrIleGluAspSerGlnAspLeuGluIleTyrLeuIleArg                          
755760765                                                                 
TACAATGCAAAACAT GAAACAGTAAATGTGCCAGGTACGGGTTCCTTA2352                     
TyrAsnAlaLysHisGluThrValAsnValProGlyThrGlySerLeu                          
770775780                                                                 
TGGCCGCTTTCAGCCCAAAGT CCAATCGGAAAGTGTGGAGAGCCGAAT2400                     
TrpProLeuSerAlaGlnSerProIleGlyLysCysGlyGluProAsn                          
785790795800                                                              
CGATGCGCGCCACAC CTTGAATGGAATCCTGACTTAGATTGTTCGTGT2448                     
ArgCysAlaProHisLeuGluTrpAsnProAspLeuAspCysSerCys                          
805810815                                                                 
AGGGATGGAGAA AAGTGTGCCCATCATTCGCATCATTTCTCCTTAGAC2496                     
ArgAspGlyGluLysCysAlaHisHisSerHisHisPheSerLeuAsp                          
820825830                                                                 
ATTGATGTAGGA TGTACAGACTTAAATGAGGACCTAGGTGTATGGGTG2544                     
IleAspValGlyCysThrAspLeuAsnGluAspLeuGlyValTrpVal                          
835840845                                                                 
ATCTTTAAGATTAAG ACGCAAGATGGGCACGCAAGACTAGGGAATCTA2592                     
IlePheLysIleLysThrGlnAspGlyHisAlaArgLeuGlyAsnLeu                          
850855860                                                                 
GAGTTTCTCGAAGAGAAACCA TTAGTAGGAGAAGCGCTAGCTCGTGTG2640                     
GluPheLeuGluGluLysProLeuValGlyGluAlaLeuAlaArgVal                          
865870875880                                                              
AAAAGAGCGGAGAAA AAATGGAGAGACAAACGTGAAAAATTGGAATGG2688                     
LysArgAlaGluLysLysTrpArgAspLysArgGluLysLeuGluTrp                          
885890895                                                                 
GAAACAAATATC GTTTATAAAGAGGCAAAAGAATCTGTAGATGCTTTA2736                     
GluThrAsnIleValTyrLysGluAlaLysGluSerValAspAlaLeu                          
900905910                                                                 
TTTGTAAACTCT CAATATGATCAATTACAAGCGGATACGAATATTGCC2784                     
PheValAsnSerGlnTyrAspGlnLeuGlnAlaAspThrAsnIleAla                          
915920925                                                                 
ATGATTCATGCGGCA GATAAACGTGTTCATAGCATTCGAGAAGCTTAT2832                     
MetIleHisAlaAlaAspLysArgValHisSerIleArgGluAlaTyr                          
930935940                                                                 
CTGCCTGAGCTGTCTGTGATT CCGGGTGTCAATGCGGCTATTTTTGAA2880                     
LeuProGluLeuSerValIleProGlyValAsnAlaAlaIlePheGlu                          
945950955960                                                              
GAATTAGAAGGGCGT ATTTTCACTGCATTCTCCCTATATGATGCGAGA2928                     
GluLeuGluGlyArgIlePheThrAlaPheSerLeuTyrAspAlaArg                          
965970975                                                                 
AATGTCATTAAA AATGGTGATTTTAATAATGGCTTATCCTGCTGGAAC2976                     
AsnValIleLysAsnGlyAspPheAsnAsnGlyLeuSerCysTrpAsn                          
980985990                                                                 
GTGAAAGGGCAT GTAGATGTAGAAGAACAAAACAACCAACGTTCGGTC3024                     
ValLysGlyHisValAspValGluGluGlnAsnAsnGlnArgSerVal                          
99510001005                                                               
CTTGTTGTTCCGGA ATGGGAAGCAGAAGTGTCACAAGAAGTTCGTGTC3072                     
LeuValValProGluTrpGluAlaGluValSerGlnGluValArgVal                          
101010151020                                                              
TGTCCGGGTCGTGGCTATA TCCTTCGTGTCACAGCGTACAAGGAGGGA3120                     
CysProGlyArgGlyTyrIleLeuArgValThrAlaTyrLysGluGly                          
1025103010351040                                                          
TATGGAGAAGGT TGCGTAACCATTCATGAGATCGAGAACAATACAGAC3168                     
TyrGlyGluGlyCysValThrIleHisGluIleGluAsnAsnThrAsp                          
104510501055                                                              
GAACTGAAG TTTAGCAACTGCGTAGAAGAGGAAATCTATCCAAATAAC3216                     
GluLeuLysPheSerAsnCysValGluGluGluIleTyrProAsnAsn                          
106010651070                                                              
ACGGTAAC GTGTAATGATTATACTGTAAATCAAGAAGAATACGGAGGT3264                     
ThrValThrCysAsnAspTyrThrValAsnGlnGluGluTyrGlyGly                          
107510801085                                                              
GCGTACACTT CTCGTAATCGAGGATATAACGAAGCTCCTTCCGTACCA3312                     
AlaTyrThrSerArgAsnArgGlyTyrAsnGluAlaProSerValPro                          
109010951100                                                              
GCTGATTATGCGTCA GTCTATGAAGAAAAATCGTATACAGATGGACGA3360                     
AlaAspTyrAlaSerValTyrGluGluLysSerTyrThrAspGlyArg                          
1105111011151120                                                          
AGAGAGAAT CCTTGTGAATTTAACAGAGGGTATAGGGATTACACGCCA3408                     
ArgGluAsnProCysGluPheAsnArgGlyTyrArgAspTyrThrPro                          
112511301135                                                              
CTACC AGTTGGTTATGTGACAAAAGAATTAGAATACTTCCCAGAAACC3456                     
LeuProValGlyTyrValThrLysGluLeuGluTyrPheProGluThr                          
114011451150                                                              
GATA AGGTATGGATTGAGATTGGAGAAACGGAAGGAACATTTATCGTG3504                     
AspLysValTrpIleGluIleGlyGluThrGluGlyThrPheIleVal                          
115511601165                                                              
GACAGC GTGGAATTACTCCTTATGGAGGAATAG3537                                    
AspSerValGluLeuLeuLeuMetGluGlu                                            
11701175                                                                  
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