Patent Publication Number: US-4929734-A

Title: Tetrahydropyridine oxime compounds

Description:
CROSS-REFERENCE TO RELATED APPLICATION 
     This application is a continuation-in-part of United States Ser. No. 32,839 of Mar. 31, 1987, now U.S. Pat. No. 4,798,841. 
    
    
     BACKGROUND OF THE INVENTION 
     The present invention relates to chemical compounds, pharmaceutical compositions, and to a method of treatment employing the compounds and compositions. More particularly, the present invention is concerned with certain 1,2,5,6-tetrahydro-1-substituted 3- or 4-pyridine oximes, to pharmaceutical compositions containing these compounds, and to a pharmaceutical method of treatment. 
     Disorders of cognition are generally characterized by symptoms of forgetfulness, confusion, memory loss, attentional deficits and/or, in some cases, affective disturbances. These symptoms may arise as a result of the general aging process and/or from organic brain disease, cerebrovascular disease, head injury or developmental or genetic defects. 
     The general decrease in cognitive function which accompanies the aging process is well accepted. The same phenomenon has been observed and documented in many lower mammals, including those routinely employed in pharmacological testing programs for screening and predicting usefulness for particular drugs in higher animals, including humans. 
     Although disorders of cognition often accompany the general aging process, presenile and senile primary degenerative dementia are the most common accepted causes of mental deterioration in the elderly. It has been estimated that at least ten percent of persons over sixty years of age will eventually suffer severe mental deterioration. A much larger number will experience cognitive decline of sufficient severity to impede their activities. 
     Many of the symptoms of cognitive disorders, especially impaired memory, are associated with decreased acetylcholine synthesis and the impairment of cholinoreceptive neurons. In the hippocampus and cerebral cortex of patients suffering from primary degenerative dementia for example, the level of the enzyme choline acetyltransferase (CAT) can be reduced by as much as ninety percent. (See Davies et al., The Lancet, 1976 (Vol. 2): 1403; Perry et al., J. Neurol. Sci., 34: 247-265 (1977); and White et al., The Lancet, 1977 (Vol. 1): 668-670). 
     Since CAT catalyzes the synthesis of acetylcholine from its precursors choline and acetyl coenzyme A, the loss of CAT reflects the loss of cholinergic, or acetylcholine-releasing, nerve endings in the hippocampus and cerebral cortex. There is abundant evidence that cholinergic terminals in the hippocampus are critically important for memory formation. 
     The cholinergic hypothesis suggests that drugs which restore acetylcholine levels or which mimic the action of acetylcholine (i.e. are cholinomimetic) are effective in correcting this deficit in neurotransmitter chemical and provide treatment of the memory impairment symptom of cerebral insufficiency. Considerable biochemical, pharmacological, and electrophysiological evidence supports the hypothesis that deficits in the cholinergic system underlie geriatric cognitive dysfunction. (See C. Peterson and G. E. Gibson, Neurobiol. Aging, 4: 25-30 (1983)). Aged humans and non-human primates with decreased cognition show improved memory when they are treated, for example, with acetylcholinesterase inhibitors such as physostigmine. These agents increase the available supply of synaptic acetylcholine by inhibiting its hydrolysis. 
     Aminopyridines such as 3,4-diaminopyridine ameliorate age-related cognitive deficits by increasing the release of acetylcholine from presynaptic nerve terminals, thus increasing synaptic acetylcholine. (See H. P. Davis et al., Exp. Aging Res., 9: 211-214 (1983)). 
     It has been known for some time that the natural alkaloid, muscarine, has the ability to act relatively selectively at autonomic effector cells to produce qualitatively the same effects as acetylcholine. Two related alkaloids, pilocarpine and arecoline, have the same principal sites of action as muscarine and acetylcholine and are thus classified as having &#34;muscarinic&#34; action. Although these naturally occurring alkaloids are of great value as pharmacological tools, present clinical use is largely restricted to the use of pilocarpine as a miotic agent. 
     Arecoline (the methyl ester of 1,2,5,6-tetrahydro-1-methyl-3-pyridinecarboxylic acid) is the chief alkaloid found in betel nuts (Areca catechu). Betel nuts have been chewed by natives of the East Indies since early times as a euphoretic. The present pharmaceutical utility of arecoline, however, has been limited to its use as a veterinary anthelmintic agent. 
     Recently it has been demonstrated that arecoline is effective in ameliorating some of the symptoms of cognitive disorders in patients clinically diagnosed as having presenile primary degenerative dementia. Significant improvement was observed in a test of picture recognition after administration of arecoline to patients in a double blind study. (See Christie et al., Brit. J. Psychiatry, 138: 46-50 (1981)). 
     Certain 3- or 4-ketoximes of 1-(lower alkyl)-1,2,5,6-tetrahydropyridines in which the oxygen is unsubstituted are disclosed in U.S. Pat. No. 3,004,979, having utility as parasympathomimetic agents acting on non-striated muscle. 
     Regarding analgesia, the literature indicates that acetylcholine and muscarine agonists possess antinociceptive activity (see T. T. Chau et al., J. Pharmacol. Exp. Ther., 222: 612-666 (1982),; W. L. Dewey et al., Life Sci., 17: 9-10 (1975); and N. W. Pedigo et al., Neurosci. Lett., 26: 85-90 (1981) and references cited therein). 
     The classification and nomenclature of phencyclidine and sigma receptor sites has been reviewed (Trends Neurosci.  1987, 10: 444-446). See also Clin. Neuropharmacol. 1988, 11: 105. The structural determinants of sigma receptor affinity have been described (Mol. Pharmacol. 1987, 32: 772-784). We have found that a new structural class of chemical compounds, e.g. tetrahydropyridine oximes, have unexpectedly high affinity for the sigma site. 
     Sigma receptor agonists may serve to modulate the actions of a variety of transmitters (Eur. J. Pharmacol. 1988, 149: 399-400). 
     1,3-Disubstituted-guanidine sigma receptor ligands are useful in the diagnosis and treatment of hallucination associated psychotic mental illness (e.g., schizophrenia) and chronic mental depression (U.S. Pat. No. 4,709,094, Trends Neurosci. 1988, 11: 37-40. 
     Since haloperidol and many other antipsychotic drugs exhibit an affinity for sigma receptors which is at least equal to its affinity for dopamine receptors, these data raise the further possibility that sigma receptors are involved in the motor side effects of antipsychotic drugs (Neurology 1988, 38: 961-965). 
     The sigma site plays a role in immune system functioning, for example, as evidenced by steroid binding at sigma receptors and the link between endocrine, nervous, and immune systems (Science 1988, 240: 219-221). See also Eur. J. Pharmacol. 1988; 148: 467-470. Additionally, sigma ligands prevent the proliferative response of T lymphocytes by lowering IL2 production (Biochem. Pharmacol. 1987, 36: 3929-3936). The aforementioned articles suggest activity as antiinflammatories or immunosuppressants. 
     SUMMARY OF THE INVENTION 
     The present invention provides a compound of formula 1: ##STR1## wherein the ##STR2## may be attached to the tetrahydropyridine moiety at either atom number 3 or 4 of the tetrahydropyridine ring system, and the attachment of the OH group to the nitrogen atom is configured either syn- or anti- to the tetrahydropyridine ring. 
     The substituent group R 1  is hydrogen; straight or branched alkyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; straight or branched alkenyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; straight or branched alkynyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; cycloalkyl of from three to eight carbon atoms; ##STR3## where A is a bond or is a hydrocarbon chain of from one to four carbon atoms and when containing two or more carbon atoms may contain one double bond and where R 3  is alkyl of from one to six carbon atoms, optionally substituted with halogen; ##STR4## where n is zero to four and X and Y are independently selected from hydrogen, fluorine, chlorine, bromine, hydroxy, straight or branched alkyl of from one to three carbon atoms, or alkoxyl of from one to four carbon atoms. 
     R 2  is selected from hydrogen; straight or branched alkynyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; cycloalkyl of from three to six carbon atoms; or ##STR5## where n is zero to six and X and Y are independently selected from hydrogen, fluorine, chlorine, bromine, hydroxy, straight or branched alkyl of from one to three carbon atoms, or alkoxyl of from one to four carbon atoms; with the proviso that R 1  and R 2  may not both simultaneously be hydrogen; or a pharmaceutically acceptable acid addition salt thereof. 
     In another aspect, the present invention provides a method of treating depression in a mammal in need of such treatment comprising the administration of an antidepressant effective amount of a compound of formula 1 above in combination with a pharmaceutically acceptable carrier. 
     In another aspect, the present invention provides a method of treating psychoses, e.g. schizophrenia, in a mammal in need of such treatment comprising the administration of an antipsychotic effective amount of a compound of formula 1 above in combination with a pharmaceutically acceptable carrier. 
     In another aspect, the present invention provides a method of treating inflammation in a mammal in need of such treatment comprising the administration of an antiinflammatory effective amount of a compound of formula 1 above in combination with a pharmaceutically acceptable carrier. 
     In another aspect, the present invention provides pharmaceutical compositions for treating depression comprising administering an antidepressant effective amount of a compound of formula 1 above in combination with a pharmaceutically acceptable carrier. 
     In another aspect, the present invention provides pharmaceutical compositions for treating psychoses, e.g. schizophrenia, comprising administering an antipsychotic effective amount of a compound of formula 1 above in combination with a pharmaceutically acceptable carrier. 
     In another aspect, the present invention provides pharmaceutical compositions for treating inflammation comprising administering an antiinflammatory effective amount of a compound of formula 1 above in combination with a pharmaceutically acceptable carrier. 
     DETAILED DESCRIPTION 
     The compounds of the present invention comprise a class of 1,2,5,6-tetrahydro-1-substituted 3- or 4-pyridine oximes and their pharmaceutically acceptable salts which are centrally acting muscarinic agents and which are thus useful as analgesic agents, sleep aids, or therapeutic agents for treating cholinergic deficit states such as senile dementia, Alzheimer&#39;s disease, Huntington&#39;s chorea, tardive dyskinesia, hyperkinesia, mania or similar conditions of cerebral insufficiency characterized by decreased cerebral acetylcholine production or release. 
     The compounds of the present invention are also active at the sigma site and as sigma agents are useful for treating depression, psychoses, e.g. schizophrenia, and inflammatory diseases. 
     The substituent group R 1  in structural formula 1 above is selected from hydrogen; straight or branched alkyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; straight or branched alkenyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; straight or branched alkynyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; cycloalkyl of from three to eight carbon atoms; ##STR6## where A is a bond or a hydrocarbon chain of from zero to four carbon atoms and when containing two or more carbon atoms may contain one double bond and R 3  is alkyl of from one to six carbon atoms, optionally substituted with halogen; or ##STR7## where n is zero to four X and Y are independently selected from hydrogen, fluorine, chlorine, bromine, hydroxy, straight or branched alkyl of from one to three carbon atoms, or alkoxyl of from one to four carbon atoms. 
     The term &#34;alkyl of from one to six carbon atoms&#34; denotes a substituent group derived from a saturated hydrocarbon by removal of a single hydrogen atom. The term includes methyl, ethyl, n-propyl, iso-propyl, n-butyl, sec-butyl, iso-butyl, tert-butyl, and the various isomeric forms of pentyl and hexyl. Likewise, the terms &#34;alkenyl of from one to six carbon atoms&#34; and &#34;alkynyl of from one to six carbon atoms&#34; denote substituent groups derived, respectively, from alkene or alkyne hydrocarbons by the removal of a single hydrogen atom. These terms include ethenyl, ethynyl, propenyl, propynyl, and similar branched and unbranched unsaturated hydrocarbon groups of up to six carbon atoms. 
     The term &#34;cycloalkyl of from three to eight carbon atoms&#34; denotes saturated carbocyclic rings such as cyclopropyl, cyclobutyl, cyclopentyl, cyclohexyl, as well as alkyl substituted carbocyclic rings containing up to eight carbon atoms such as methyl-, dimethyl-, and ethylcyclohexyl. 
     The term &#34;alkoxyl&#34; denotes a substitent group derived by removal of the hydrogen from the oxygen atom of a saturated alcohol and attached to the parent molecular moiety through the oxygen atom. Such groups include methoxyl, ethoxyl, 1- and 2-propoxyl, and similar branched and unbranched alkoxyl groups of up to four carbon atoms. 
     In compounds of the present invention, the substituent group R 2  is selected from hydrogen; straight or branched alkynyl of from one to six carbon atoms optionally substituted with hydroxy or alkoxyl of from one to four carbon atoms; cycloalkyl of from three to six carbon atoms; ##STR8## where n is zero to six and X and Y are independently selected from hydrogen, fluorine, chlorine, bromine, hydroxy, straight or branched alkyl of from one to three carbon atoms, or alkoxyl of from one to four carbon atoms. 
     Preferred compounds for use in the pharmaceutical methods of the present invention are those in which R 1  is alkyl and R 2  is ##STR9## where n is zero to four. 
     The compounds employed in the method of this invention may exist in either of two isomeric forms in which the hydrogen atom of the oxime group may be either syn- or anti- with respect to the tetrahydropyridine ring. The present invention includes both forms of the compounds as well as mixtures of the svn- and anti- forms. Moreover, in those compounds in which there is a double bond in a carbon chain, both the Z (i.e. cis-) and E (i.e. trans) forms are included in the present invention. The terms syn- and anti- as they apply to the compounds of the present invention are illustrated by formulas 1a and 1b: ##STR10## 
     Examples of compounds contemplated as falling within the scope of the present invention include, but are not limited to the following: 
     3-Phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-propanone oxime. 
     1-(1,2,5,6-Tetrahydro-1-methyl-3-pyridinyl)-3-butyn-1-one oxime. 
     Phenyl(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)methanone oxime. 
     3-Phenyl-1-(1,2,5,6-tetrahydro-1-propyl-3-pyridinyl)-1-propanone oxime. 
     1-(1,2,5,6-Tetrahydro-1-methyl-3-pyridinyl)-4-hexyn-1-one oxime. 
     Compounds of the present invention are prepared by the general synthetic method detailed in Reaction Sequence 1, following. 
     Referring to the Reaction Sequence, the starting 3- or 4-ketopyridines, 5, are prepared by one of three alternative methods. In the first method, the known 3- or 4-pyridinecarbonitriles, 2, are reacted in the conventional manner with the desired alkyl lithium compound or the appropriate Grignard reagent in an aprotic solvent such as diethyl ether, tetrahydrofuran, dioxane or the like, followed by hydrolysis in dilute aqueous acid. In the second method, the known 3- or 4-pyridinecarbonyl chlorides, 3, are reacted in the usual manner with the desired alkynyl or aralkyl organometallic compound in the presence of a copper(I) halide. Preferred organometallic compounds are Grignard reagents or organolithium compounds. ##STR11## In the third alternative method, the known 3- or 4-pyridinecarboxaldehydes, 4, from which the aldoximes may be prepared directly, are reacted in the usual manner with the desired Grignard reagent followed by oxidation of the carbinol thus produced by manganese dioxide or by the method of D. Swern, et al., J. Org. Chem., 43: 2480-2482 (1978). 
     The 3- or 4-ketopyridines, 5 thus produced, are reacted with a diol such as ethanediol in the presence of acid to produce the 3- or 4-pyridineketals, 6. The ketals, 6, are converted by the action of the desired alkynyl, or aralkyl halide (preferably the iodide) to the corresponding N-substitutedpyridinium ketals, 7. The N-substitutedpyridinium ketals, 7, are subsequently reduced by the action of an alkali metal hydride, such as sodium borohydride, to produce the N-substituted 3- or 4-ethylenedioxyketal-1,2,5,6-tetrahydropyridines, 8. 
     The 3- or 4-ethylenedioxyketal-1,2,5,6-tetrahydropyridines, 8, are next converted to the corresponding N-substituted 3- or 4-keto-1,2,5,6-tetrahydropyridines, 9, by the action of aqueous acid. The 3- or 4-keto-1,2,5,6-tetrahydropyridines, 9, are then reacted with hydroxylamine hydrochloride in, for example, methanol under reflux for a period sufficient to effect the formation of the corresponding oximes, 10. 
     Alternatively, the unsubstituted oximes, 13, are converted to the corresponding N-substituted pyridinium iodides by reaction with the desired iodide. These pyridinium salts are reduced by the action of sodium borohydride, generally in a mixed water/alcohol medium at ambient temperature, to produce the N-substituted 3- or 4-oximino-1,2,5,6-tetrahydropyridine compounds of the present invention. 
     By virtue of the basic nitrogen atom in the tetrahydropyridine ring, the compounds of the present invention form pharmaceutically acceptable acid addition salts with organic and inorganic acids. Examples of suitable acids for the formation of pharmaceutically acceptable salts are hydrochloric, sulfuric, phosphoric, acetic, benzoic, citric, malonic, salicylic, malic, fumaric, oxalic, succinic, tartaric, lactic, gluconic, ascorbic, maleic, aspartic, benzenesulfonic, methane- and ethanesulfonic, hydroxymethane and hydroxyethanesulfonic, and the like. (See for example, &#34;Pharmaceutical Salts,&#34; J. Pharm. Sci. 66 (1): 1-19 (1977)). 
     In a similar manner, the N-lower-alkyl and lower-dialkyl tetrahydropyridinium salts may be used in the method of this invention as, for example the N-methyl-, N,N-dimethyl- and N-ethyl-1,2,5,6-tetrahydropyridinium halides. 
     The acid addition salts are prepared by contacting the free base form of the compounds of this invention with a sufficient amount of the desired acid to produce the salt in the conventional manner. The free base forms may be regenerated, if desired, by treating the salt form with a base. For example, dilute aqueous solutions of such bases as sodium hydroxide, potassium carbonate, ammonia, and sodium bicarbonate may be utilized for this purpose. 
     The free acid or base forms of the compounds of this invention differ somewhat from their respective salt forms in such physical properties as melting point and solubility in polar solvents, but the salts are otherwise equivalent to their respective free acid or base forms for the purposes of the invention. 
     The compounds of the present invention are sigma receptor agonists and as sigma agents are thus useful as antidepressants for the treatment of depression in mammals including man, as antipsychotics for treating psychoses, e.g. schizophrenia, and as agents for treating inflammatory diseases. 
     The biological activity of compounds of the present invention was evaluated using a number of tests. The activity of compounds of this invention as sigma site agonists was measured by the method described in Mol. Pharmacol. 1987, 32: 772-784. IC 50  values for the sigma site of 0.7 nM and 5 nM were found for 3-phenyl-1-( 1,2,5,6-tetrahydro-1-propyl-3-pyridinyl)propanone oxime and 3-phenyl-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)propanone oxime. 
     3-Phenyl-1-(1,2,5,6-tetrahydro-1-propyl-3-pyridinyl)propanone oxime was also evaluated in a test that measures spontaneous exploratory activity and motor coordination (MAST). The experimental aspects of this test are described in Pharmacol. Biochem. Behav. 1977; 6: 351-353 and Life Sci. 1978; 22: 1067-1076. Administered subcutaneously, the compound produced significant (p&lt;0.05) inhibition of spontaneous activity in rats; the ED 50  was 33.2 mg/kg. Essentially no discoordination was noted in mice or rats. 
     As an example of the compounds of the present invention, 3-phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)propanone oxime was subjected to the self-stimulation test. This test as applied for antidepressant discovery involves the ability of antidepressant drugs to potentiate the stimulatory effect of methamphetamine on intracranial self-stimulation responding in rats. 
     Rats with stimulating electrodes implanted in the lateral hypothalamus were trained to depress a lever in order to deliver rewarding electric current to their brains, as described by Poschel and Ninteman in Life Sciences, vol. 3, pp. 903-910, 1964. Groups of four rats performed self-stimulation (SS) behavior for one hour and were then removed from the test apparatus and given an oral injection of water, the subject compound (10 or 20 mg/kg) or the antidepressant reference agent, imipramine (10 mg/kg). Rats were then returned to the apparatus and allowed to perform SS for another 1.5 hours at which time they were again removed from the box and were given an intraperitoneal injection of methamphetamine (0.25 mg/kg). Rats were then returned to the apparatus and allowed to perform SS for 5.5 hours. The number of lever presses made per 30 minute interval were recorded. Drug effects were compared during the first hour after methamphetamine administration. 
     Antidepressant drugs, such as imipramine, increase the number of lever presses made after methamphetamine treatment. The data in Table 1 demonstrate that 3-phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)propanone oxime showed effects similar to those of imipramine in the SS test. That is, rats given the subject compound or imipramine prior to methamphetamine showed an increased number of SS lever presses as compared to control rats given water prior to methamphetamine. 
     
                       TABLE 1                                                     
______________________________________                                    
Effects of 3-phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-                     
pyridinyl)propanone oxime (compound) and the antidepressant               
drug imipramine on the increase in self-stimulation (SS)                  
responding produced by methamphetamine in rats.                           
                       SS Responses                                       
Treatment              (Mean ± S.E.M.)                                 
______________________________________                                    
Vehicle + Methamphetamine                                                 
                        2317 ± 473                                     
Compound, 10 mg/kg + Methamphetamine                                      
                       4409 ± 630*                                     
Compound, 20 mg/kg + Methamphetamine                                      
                       5149 ± 467*                                     
Imipramine, 10 mg/kg + Methamphetamine                                    
                       4199 ± 259*                                     
______________________________________                                    
 *Significantly different than Vehicletreated group (p &lt; .05)             
 
    
     Finally, 3-phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)propanone oxime, a representative compound of the present invention was subjected to the Porsolt behavioral despair test which involves the ability of antidepressant drugs to reduce the duration of time that rats remain immobile when they are forced to spin in a narrow water-filled cylinder. 
     In this test, rats are placed in a narrow cylinder filled with water for 15 minutes on the day prior to the drug test. Typically, the rats swim for a time in an apparent attempt to escape but eventually cease attempts to escape, remain immobile and float with their snouts above the surface. Rats are then removed from the cylinders, dried under a heat lamp and returned to their home cages. After the swim on day 1 and 30 minutes before testing on the next day, drugs or the vehicle solution are administered intraperitoneally and the rats are again placed in the water-filled cylinders. The duration of immobility is measured during a 5 minute test. Antidepressant drugs are active in the behavioral despair test at doses that do not simulate locomotor activity as reported by Porsolt et al., European Journal of Pharmacology, vol. 47, pp. 379-391, 1978. 
     Groups of 10 rats were treated with saline, the subject compound (30 mg/kg) or imipramine (30 mg/kg) on day 1 and one hour prior the test on day 2. 
     In order to ensure that the effect of the subject compound in the behavioral despair test was not simply due to a general stimulant effect of the compound, the effects of the subject compound (30 mg/kg) and imipramine (30 mg/kg) on locomotor activity was determined in separate groups of rats. For this test, rats were placed in darkened cylindrical chambers and locomotor activity was recorded for 30 minutes by means of photoelectric cells. The number of interruptions of the photocell beam indicated the amount of locomotion. 
     Whereas control rats rapidly become immobile and remain so for about more than half of the test, rats treated with antidepressant drugs continue to swim about the cylinder and thus display less immobility than controls. The data in Table 2 demonstrate that the subject compound, like imipramine, reduced the duration of immobility in the behavioral despair test. Table 2 also shows that neither the subject compound nor imipramine increased spontaneous locomotion in rats when dosed as in the behavioral despair procedure. Thus, the subject compound displayed a profile similar to that seen with the antidepressant imipramine in the Porsolt behavioral despair test. 
     
                       TABLE 2                                                     
______________________________________                                    
Effect of 3-phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-                      
pyridinyl)propanone oxime (compound) and the antidepressant               
drug imipramine in the Porsolt behavioral despair and                     
locomotor activity tests in rats.                                         
              Behavioral     Locomotor                                    
              Despair Test   Activity Test                                
Treatment     (Seconds Immobile)                                          
                             (Counts)                                     
______________________________________                                    
Vehicle        192 ± 9    165 ± 14                                  
Imipramine - 30 mg/kg                                                     
               82 ± 14*    93 ± 17*                                 
Compound - 30 mg/kg                                                       
              121 ± 14*   139 ± 26                                  
______________________________________                                    
 *Significantly different than Vehicle treatment, p &lt; .05                 
 
    
     In therapeutic use as agents for treating depression, psychoses or inflammation, the compounds utilized in the pharmaceutical method of this invention are administered to the patient at dosage levels of from 0.7 to 7000 mg per day. For a normal human adult of approximately 70 kg of body weight, this translates into a dosage of from 0.01 to 100 mg/kg of body weight per day. The specific dosages employed, however, may be varied depending upon the requirements of the patient, the severity of the condition being treated, and the activity of the compound being employed. The determination of optimum dosages for a particular situation is within the skill of the art. 
     For preparing pharmaceutical compositions from the compounds of this invention, inert, pharmaceutically acceptable carriers can be either solid or liquid. Solid form preparations include powders, tablets, dispersable granules, capsules, cachets, and suppositories. 
     A solid carrier can be one or more substances which may also act as diluents, flavoring agents, solubilizers, lubricants, suspending agents, binders, or tablet disintegrating agents; it can also be an encapsulating material. 
     In powders, the carrier is a finely divided solid which is in a mixture with the finely divided active component. In tablets, the active compound is mixed with the carrier having the necessary binding properties in suitable proportions and compacted in the shape and size desired. 
     For preparing suppositories, a low-melting wax such as a mixture of fatty acid glycerides and cocoa butter is first melted, and the active ingredient is dispersed therein by, for example, stirring. The molten homogeneous mixture is then poured into convenient sized molds and allowed to cool and solidify. 
     Powders and tablets preferably contain between about 5 to about 70% by weight of the active ingredient. Suitable carriers are magnesium carbonate, magnesium stearate, talc, lactose, sugar, pectin, dextrin, starch, tragacanth, methyl cellulose, sodium carboxymethyl cellulose, a low-melting wax, cocoa butter, and the like. 
     The term &#34;preparation&#34; is intended to include the formulation of the active compound with encapsulating material as a carrier providing a capsule in which the active component (with or without other carriers) is surrounded by a carrier, which is thus in association with it. In a similar manner, cachets are also included. 
     Tablets, powders, cachets, and capsules can be used as solid dosage forms suitable for oral administration. 
     Liquid form preparations include solutions suitable for oral or parenteral administration, or suspensions, and emulsions suitable for oral administration. Sterile water solutions of the active component or sterile solutions of the active component in solvents comprising water, ethanol, or propylene glycol may be mentioned as examples of liquid preparations suitable for parenteral administration. 
     Sterile solutions may be prepared by dissolving the active component in the desired solvent system, and then passing the resulting solution through a membrane filter to sterilize it or, alternatively, by dissolving the sterile compound in a previously sterilized solvent under sterile conditions. 
     Aqueous solutions for oral administration can be prepared by dissolving the active compound in water and adding suitable flavorants, coloring agents, stabilizers, and thickening agents as desired. Aqueous suspensions for oral use can be made by dispersing the finely divided active component in water together with a viscous material such as natural or synthetic gums, resins, methyl cellulose, sodium carboxymethyl cellulose, and other suspending agents known to the pharmaceutical formulation art. 
     Preferably, the pharmaceutical preparation is in unit dosage form. In such form, the preparation is divided into unit doses containing appropriate quantities of the active component. The unit dosage form can be a packaged preparation, the package containing discrete quantities of the preparation, for example, packeted tablets, capsules, and powders in vials or ampoules. The unit dosage form can also be a capsule, cachet, or tablet itself, or it can be the appropriate number of any of these packaged forms. 
     The following preparative examples are provided to enable one skilled in the art to practice the invention. They are illustrative of the present invention and are not to be read as limiting the scope of the invention as it is defined by the appended claims. 
    
    
     EXAMPLES OF GENERAL SYNTHETIC METHODS AND PREPARATION OF STARTING MATERIALS 
     Example 1 
     Representative Example of the Conversion of a Pyridine Carboxaldehyde to a Ketopyridine--Preparation of 1-(3-Pyridinyl)propanone 
     3-Pyridinecarboxaldehyde (10.71 g, 100 mmol) was dissolved in 200 ml of tetrahydrofuran under a nitrogen atmosphere and cooled to -30° C. Ethylmagnesium bromide (100 mmol, 2.0 molar in tetrahydrofuran) was slowly added, after which the mixture was stirred at -30° C. for one hour. Saturated ammonium chloride solution was added and the mixture was allowed to warm to room temperature. Diethyl ether (200 ml) was added and the organic layer was separated, dried over anhydrous magnesium sulfate, and evaporated to yield the intermediate carbinol as a yellow oil. This material was taken up in 500 ml of toluene, and 26.1 g (300 mmol) of manganese dioxide was added. The resulting mixture was heated under reflux for two hours under a nitrogen atmosphere in a flask fitted with a Dean Stark trap to collect water which was azeotropically removed. 
     The reaction mixture was cooled to room temperature and diluted by the addition of diethyl ether. The reaction mixture is filtered and the solvents were removed from the filtrate under vacuum and the crude product purified by chromatography on a silica gel column, eluting with 1:1 hexane/ethyl acetate to produce 7.09 g of 1-(3-pyridinyl)-1propanone. 
     Example 2 
     Representative Example of the Conversion of a Pyridinecarbonyl Chloride to a Ketopyridine--Preparation of 1-(3-Pyridinyl)pentanone 
     Copper(I) iodide (3.8 g, 2.0 mmol) was suspended in 30 ml of dry tetrahydrofuran which was then cooled to -40° C. n-Butyl lithium solution (16 ml, 2.5 molar in tetrahydrofuran) was added and the mixture further cooled to -78° C. and stirred for one hour. 3-Pyridinecarbonyl chloride hydrochloride (1.78 g, 10 mmol) was quickly added, and the resulting mixture was allowed to slowly warm to room temperature. The reaction was quenched by the addition of 2 ml of methanol, and the mixture partitioned between diethyl ether and 1:1 saturated aqueous ammonium chloride/aqueous ammonia. 
     This mixture was stirred until the aqueous layer became dark blue (copper ammonia complex), after which the layers were separated. The organic layer was washed successively with portions of 10% aqeuous Na 2  S 2  O 3 , water, and brine, and then dried over anhydrous magnesium sulfate. The solvent was removed under vacuum and the crude product chromatographed on silica gel, eluting with 70% hexane in ethyl acetate, to yield 0.80 g of 1-(3-pyridinyl)-1-pentanone. 
     Example 3 
     Representative Example of the Preparation of a Ketopyridine by the Swern Oxidation of an Intermediate Carbinol Prepared via Grignard Reaction - Preparation of 2-Methyl-1-(3-pyridinyl)-1-propanone 
     Oxalyl chloride was distilled under a nitrogen atmosphere immediately prior to use; 10.93 g (86.13 mmol) was dissolved in 200 ml of dichloromethane. This mixture was cooled, under a nitrogen atmosphere, to -50° C. and 13.45 g (12.22 ml, 172.3 mmol) of dry dimethylsulfoxide in 50 ml of dichloromethane were slowly added. The resulting mixture was stirred at -50° C. for ten minutes. α-(1-Methylethyl)-3-pyridinemethanol (11.84 g, 78.3 mmol, previously prepared by reaction of 3-pyridinecarboxaldehyde with isopropylmagnesium bromide) in 50 ml of dichloromethane was added. This mixture was stirred at -50° C. for one hour, after which time 39.6 g (54.57 ml, 391.5 mmol) of triethylamine were added. This mixture was allowed to slowly warm to room temperature. 
     Water (300 ml) was added to the mixture, and the layers were separated. The water layer was extracted twice with dichloromethane, and the organic solutions were combined, washed with successive portions of 10% aqueous sodium carbonate solution, and brine, and then dried over anhydrous magnesium sulfate. The solvents were removed under vacuum, and the crude product was chromatographed over silica gel, eluting with 15% ethyl acetate in chloroform to yield 10.3 g of 2-methyl-1-(3-pyridinyl)-1-propanone. 
     Example 4 
     Representative Example of the Conversion of a Ketopyridine to a Keto-1,2,5,6-tetrahydropyridine--Preparation of 1-(1,2,5,6-Tetrahydro-1-methvl-3-pyridinyl)-1-pentanone 
     1-(3-Pyridinyl)-1-pentanone (4.53 g, 27.75 mmol, prepared as described in Example 2 above), 1,2-ethanediol (2.58 g, 2.32 ml, 41.63 mmol), and p-toluenesulfonic acid (6.3 g, 33.3 mmol) were dissolved in 50 ml of toluene at room temperature. This mixture was heated under reflux for twenty hours in a flask fitted with a Dean Stark trap to collect azeotropically distilled water. 
     After this time, the mixture was cooled and poured into 10% aqueous sodium carbonate solution and the resulting mixture diluted with diethyl ether. The organic layer was separated, dried over anhydrous magnesium sulfate, and evaporated to yield the crude ethylene ketal as an orange oil. The crude product was purified by chromatography over silica gel, eluting with 70% hexane in ethyl acetate to produce 4.22 g of the pure material. 
     The ethylene ketal was mixed with 10 ml of methyl iodide and stirred at room temperature for three days. The excess methyl iodide was removed under vacuum, and the residue triturated with diethyl ether to obtain 6.78 g of the N-methylpyridinium ethylene ketal iodide. 
     The N-methylpyridinium ethylene ketal iodide was dissolved in 60 ml of absolute ethanol under nitrogen, and 0.81 g of sodium borohydride were slowly added, keeping the temperature of the reaction mixture under 25° C. This was followed by addition of another 1.32 g of sodium borohydride. This mixture was stirred at room temperature for 30 minutes, after which time the mixture was heated under reflux for thirty minutes. 
     The reaction mixture was cooled to room temperature and 21 ml of 6 M aqueous hydrochloric acid were slowly added. After addition of the acid was complete, the resulting mixture was heated under reflux for one hour and then cooled to room temperature. The alcohol was removed under vacuum leaving a yellowish slurry. 
     Fifty ml of water were added, followed by the slow addition of 20 g of potassium carbonate. The resulting mixture was extracted twice with diethyl ether and the extract was dried over anhydrous magnesium sulfate. The ether was evaporated and the residue was purified by column chromatography over silica gel, eluting with 5% methanol in diethyl ether, to yield 2 g of 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-pentanone as a yellow oil. This material was reacted with oxalic acid to yield 1.3 g of the ethanedioate salt, mp 171° -172° C. 
     Example 5 
     Representative Example of the Preparation of a 1,2,5,6-Tetrahydropyridine Oxime by the Oximination of a Keto-1,2,5,6-tetrahydropvridine--Preparation of 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-pentanone Oxime 
     To a solution of 1.09 g (6.01 mmol) of 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-pentanone (prepared as described in Example 4 above) in 6 ml of methanol were added 0.42 g (6.1 mmol) of hydroxylamine hydrochloride. The resulting mixture was heated under reflux for 12 hours, cooled, and stirred at room temperature for three days. The solvent was removed under vacuum and chloroform and dilute aqueous ammonium hydroxide solution were added. The chloroform layer was separated, washed with water until it tested neutral, and dried over anhydrous magnesium sulfate. The chloroform was removed under vacuum and the residual dark oil was taken up in diethyl ether. This solution was filtered through silica gel and the ether removed under vacuum. The residue was reacted with oxalic acid to produce 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-pentanone oxime, ethanedioate salt, mp 91° -95° C. 
     Example 6 
     Representative Example of the Conversion of a Ketopyridine to a 1-Methyl-ketoxime-1,2,5,6-tetrahydropyridine via the Ketopyridine Oxime--Preparation of 1-(1,2,5,6-tetrahydro-1-methylpyridinyl)ethanone Oxime 
     Step 1--Preparation of 1-(3-pyridinyl)ethanone oxime 
     A mixture of 50 g (0.41 mol) of 1-(3-pyridinyl)ethanone and 29 g (0.42 mol) of hydroxylamine hydrochloride in 250 ml of methanol was heated under reflux for five hours. Upon cooling to room temperature, a white solid separated from the reaction mixture. This material was collected by filtration and the filtrate was concentrated to yield additional white solid. The combined solids were dissolved in water and the solution was made weakly basic by the addition of sodium bicarbonate solution while cooling. The white precipitate which formed was separated by filtration to yield 55.4 g of 1-(3-pyridinyl)ethanone oxime, mp 115° -117° C. 
     Step 2--Preparation of 1-(3-pyridinyl)ethanone oxime methiodide 
     1-(3-pyridinyl)ethanone oxime (8.8 g, 0.073 mol) was dissolved in 500 ml of acetonitrile and 10 ml (0.16 mol) of methyl iodide were added. The resulting mixture was heated under reflux for four hours and then cooled to room temperature. The white precipitate was collected by filtration to yield 16.45 g of 1-(3-pyridinyl)ethanone oxime methiodide, mp 219° -220° C. 
     Step 3--Preparation of 1-(1,2,5,6-tetrahydro-1methylpyridinyl)ethanone oxime 
     To a suspension of 5 g of sodium borohydride in 100 ml of 50:50 water/methanol was added, in a dropwise manner, 50 ml of a solution of 19.5 g (0.07 mol) of 1-(3-pyridinyl)ethanone oxime methiodide dissolved in 50 ml of 50:50 water/methanol while maintaining the temperature between -5° C. and 0° C. 
     The mixture was then allowed to warm to room temperature and was diluted with 200 ml of water. This mixture was stirred for a few minutes and the light yellow precipitate which formed was collected by filtration to yield 7.83 g of 1-(1,2,5,6-tetrahydro-1-methylpyridinyl)ethanone oxime, mp 154° -157° C. 
     PREPARATIVE EXAMPLES FOR COMPOUNDS OF THE PRESENT INVENTION 
     Example 7 
     Preparation of 3-Phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)propanone Oxime 
     Step 1--Preparation of 3-phenyl-1-(3-pyridinyl)-1-propanone 
     Employing the general method of Example 1 above, 21.42 g (0.225 mol) of pyridine-3-carboxaldehyde and 27.3 ml (0.200 mol) of 2-phenylethyl bromide were converted by Grignard reaction to 40 g (94%) of (2-phenyl-3-pyridinyl)methanol and then oxidized by the action of manganese dioxide to yield a mixture of 3-phenyl-1-(3-pyridinyl)-1-propanone and 3-phenyl-1-(3-pyridinyl)-2-propen-1-one. This mixture was reduced by hydrogen over Raney nickel to produce 17.1 g of 3-phenyl-1-(3-pyridinyl)-1-propanone. 
     Step 2--Preparation of 3-phenyl-1-(1,2,5,6-tetrahydromethyl-3-pyridinyl)-1-propanone oxime 
     Employing the general methods of Examples 4 and 6 above, 10 g (47.3 mmol) of 3-phenyl-1-(3-pyridinyl)-1-propanone were first converted by the action of methyl iodide to the N-methylpyridinium iodide and then reduced by the action of sodium borohydride to produce 3-phenyl-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-propanone which was isolated as the hydrochloride salt (5.2 g, 58%), mp 195° -197° C. 
     Example 8 
     Preparation of 1-(1,2,5,6-Tetrahydro-1-methyl-3-pyridinyl)-3-butyne-1-one Oxime 3-butyne-1-one Oxime 
     Step 1--Preparation of 4-trimethylsilyl-3-butyne-1-ol 
     A solution of 2 mol of ethyl magnesium bromide (2.0 molar solution in tetrahydrofuran) is cooled in an ice bath and a solution of 50.5 g of 3-butyn-1-ol (0.72 mol) in 50 ml of tetrahydrofuran is slowly added. After addition is complete, the mixture was allowed to warm to room temperature and was stirred overnight. The mixture was then cooled in an ice bath and 254 ml (2 mol) of chlorotrimethylsilane was slowly added. This mixture was heated under reflux for two hours and then cooled to 20° C. and 800 ml of 1.4 M aqueous sulfuric acid were added. The mixture was extracted with diethyl ether and the ether solution was dried and concentrated under vacuum. The residue was distilled to yield 72.8 g of 4-trimethylsilyl-3-butyne-1-ol, bp 43° -48° C. at 1 mm Hg. 
     Step 2--Preparation of 4-Bromo-1-trimethylsilyl-1-butyne 
     4-Trimethylsilyl-3-butyne-1-ol (14.2 g, 0.1 mol) and 0.2 ml of pyridine were dissolved in 50 ml of diethyl ether under a nitrogen atmosphere. Phosphorus tribromide (3.8 ml, 0.04 mol) was slowly added and the mixture was heated under reflux for two hours. Isolation of the product by conventional means yielded 9.6 g of 4-bromo-1-trimethylsilyl-1-butyne as a clear liquid, bp 35° -38° C. at 1 mm Hg. 
     Step 3--Preparation of (4-trimethylsilylbutyn-3-yl-3-pyridinyl)methanol 
     Employing the general method of Example 1 above, 10.7 g (0.1 mol) of pyridine-3-carboxaldehyde and 20.5 g (0.1 mol) of 4-bromo-1-trimethylsilyl-1-butyne were converted by Grignard reaction to 5.9 g (25%) of (4-trimethylsilylbutyn-3-yl-3-pyridinyl)methanol which was employed without further purification. 
     Step 4--Preparation of (3-butynyl-3-pyridinyl)methanol 
     Four ml of a 1.0 M solution of tetrabutylammonium fluoride in tetrahydrofuran was added to 0.75 g (3.21 mmol) of (4-trimethylsilylbutyn-3-yl-3-pyridinyl)methanol in 3 ml of tetrahydrofuran and the resulting mixture was stirred at room temperature for 30 minutes. Isolation of the product yielded 0.12 g of (3-butynyl-3-pyridinyl)methanol as a brown oil. 
     Step 5--Preparation of 1-(3-pyridinyl)-3-butyn-1-one 
     Employing the Swern oxidation method of Example 3 above, 4.8 g (29.9 mmol) of (3-butynyl-3-pyridinyl)methanol was oxidized to 2.95 g (62%) of 1-(3- pyridinyl)-3-butyn-1-one. 
     Step 6--Preparation of 1-(3-pyridinyl)-3-butyne-1-one oxime 
     Employing the general method of Example 5 above, 2.95 g (18.5 mmol) of 1-(3-pyridinyl)-3-butyne-1-one was converted to 2.1 g (66%) of the corresponding oxime by reaction with hydroxylamine hydrochloride. 
     Step 7--Preparation of 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-3-butyne-1-one oxime 
     Employing the general method of Example 6 above, 2.95 g (12.2 mmol) of 1-(3-pyridinyl)-3-butyne-1-one oxime were converted to the corresponding 1-methyl pyridinium iodide and subsequently reduced by the action of sodium borohydride to produce 1.2 g of 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-3-butyne-1-one oxime which was isolated as the ethanedioate salt, mp 55° -57° C. 
     Example 9 
     Preparation of 4-Methoxy-1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-1-butanone Oxime 
     Step 1--Preparation of 4-Chloro-1-methoxybutane 
     4-Chloropropanol (47.3 g, 0.5 mol) and 62.2 ml (1 mol) of methyl iodide were dissolved in 300 ml of tetrahydrofuran and the resulting solution was cooled in an ice bath. A suspension of 40 g (1 mol) of sodium hydride in oil was slowly added. When addition was complete, the reaction mixture was allowed to warm to room temperature and was stirred overnight. 
     The mixture was again cooled in an ice bath and 150 ml of water were added to quench the reaction. The organic layer was separated, dried over anhydrous magnesium sulfate, and the solvent evaporated under vacuum. The residue was distilled to yield 27.6 g of 4-chloro-1-methoxybutane, bp 111° -113° C. 
     Step 2--Preparation of 3-(Methoxypropyl)-3-pyridinylmethanol 
     Following the general method of Example 1, 21.7 g (0.2 mol) of 4-chloro-1-methoxypropane and 21.4 g (0.2 mol) of pyridine-3-carboxaldehyde were converted to 18.87 g (52%) of (4-methoxypropyl-3-pyridinyl)methanol. 
     Step 3--Preparation of 4-methoxy-1-(1-methyl-3-pyridinyl)butanone 
     Employing the Swern oxidation method of Example 3, 25.67 g (0.142 mol) of (4-methoxypropyl-3-pyridinyl)methanol were converted to 17.6 g (69%) of 4-methoxy-1-(1-methyl-3-pyridinyl)butanone as a yellow oil which was used without further purification. 
     Step 4--Preparation of 4-methoxy-1-(1-methyl-3-pyridinyl)butanone oxime 
     Employing the general method of Example 5, 8.96 g (50 mmol) of 1-(1-methyl-3-pyridinyl)butanone was converted to the corresponding oxime by reaction with 3.82 g (55 mmol) of hydroxylamine hydrochloride. The product (9.5 g, 98%) was isolated as a thick reddish oil which was used without further purification. 
     Step 5--Preparation of 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-4-methoxybutanone oxime 
     Employing the general method of Example 6 above, 9.5 g (49 mmol) of 4-methoxy-1-(1-methyl-3-pyridinyl)butanone oxime were first converted to 16.5 g of the N-methyl pyridinium iodide salt and then reduced to 1-(1,2,5,6-tetrahydro-1-methyl-3-pyridinyl)-4-methoxybutanone oxime by the action of sodium borohydride. 
     The title compound was isolated as the ethanedioate salt, mp 114° -116° C. 
     Employing the methods detailed above, the following additional compounds were prepared: 
     
                       TABLE 4                                                     
______________________________________                                    
Example Compound Name         M.P.                                        
______________________________________                                    
10      1,2,5,6-Tetrahydro-1-methyl-                                      
                              249-251° C.                          
        3-pyridinecarboxaldehyde oxime                                    
        (Isolated as the monohydrochloride)                               
11      2-Methyl-1-(1,2,5,6-tetrahydro-                                   
                               98-102° C.                          
        1-methyl-3-pyridinyl)-1-propanone                                 
        oxime                                                             
        (Isolated as the ethanedioate)                                    
12      1-(1,2,5,6-Tetrahydro-1-methyl-                                   
                              70-75° C.                            
        3-pyridinyl)-4-penten-1-one oxime                                 
        (Isolated as the monohydrochloride)                               
13      1-[1,2,5,6-Tetrahydro-1-(1-methyl-                                
                              110-111° C.                          
        ethyl)-3-pyridinyl]ethanone oxime                                 
14      1-(1-Ethyl-1,2,5,6-tetrahydro-                                    
                              &gt;250° C.                             
        3-pyridinyl)ethanone oxime                                        
        (Isolated as the monohydrochloride)                               
15      1-[1,2,5,6-Tetrahydro-1-(2-                                       
                              102-104° C.                          
        propenyl)-3-pyridinyl]ethanone                                    
        oxime                                                             
16      Phenyl(1,2,5,6-tetrahydro-                                        
                              225-228° C.                          
        1-methyl-3-pyridinyl)methanone                                    
        oxime                                                             
        (Isolated as the monohydrochloride)                               
17      1-[1-Cyclopentyl-1,2,5,6-                                         
                              268-270° C.                          
        tetrahydro-3-pyridinyl]ethanone                                   
        oxime                                                             
        (Isolated as the monohydrochloride)                               
18      3-Phenyl-1-(1,2,5,6-tetrahydro-                                   
                              200-210° C.                          
        1-propyl-3-pyridinyl)-1-propanone                                 
                              (Dec.)                                      
        oxime                                                             
        (Isolated as the monohydrochloride)                               
19      1-(1,2,5,6-Tetrahydro-3-                                          
                              227-228° C.                          
        pyridinyl)ethanone oxime                                          
                              (Dec.)                                      
        (Isolated as the hydrochloride)                                   
20      1-(1,2,5,6-Tetrahydro-1-methyl-                                   
                              177-178° C.                          
        3-pyridinyl)-4-hexyn-1-one oxime                                  
        (Isolated as the monohydrochloride)                               
21      1-(1,2,3,6-Tetrahydro-4-pyridinyl)-                               
                              165-166° C.                          
        ethanone oxime                                                    
______________________________________