Abstract:
The present invention relates to novel use of the extracts of  Cassia tora  plant species. The present invention particularly relates to novel use of the extracts of  Cassia tora  leaves, which show antianxiety activity. The present invention also relates to a process for the preparation of novel herbal extract of  Cassia tora  species with antianxiety activity and also to the use thereof for the treatment of anxiety.

Description:
FIELD OF THE INVENTION 
       [0001]    The present invention relates to a process for the preparation of herbal extract of  Cassia tora  leaves, useful for the treatment of anxiety disorders. The present invention particularly relates to a novel extract of  Cassia tora  leaves, which show anti-anxiety activity. The present invention also relates to a process for the preparation of a novel extract from  Cassia tora  leaves and more particularly this invention relates to the to preparation of active extract from leaves of  Cassia tora  plant belonging to Caesalpiniaceae family and Leguminaceae sub-family The extract so obtained is a new source of anti-anxiety drug, which can be isolated and identified. The active extract consists of constituents active against anxiety and useful for the treatment of neurological disease like anxiety. 
       BACKGROUND OF THE INVENTION 
       [0002]    Anxiety disorders, the most prevalent psychiatric illness in the general community, are present in 15-20% of medical clinic patients. Anxiety can be defined as an emotional state, unpleasant in nature, uneasiness, discomfort and concern or fear about some defined or undefined future threat or can be a component of, or reaction to, a primary medical disease [Reus V. I. (2005). Mental Disorders. In (16 th  Edition) Harrison&#39;s Principles of internal medicine (pp 2457-2552). Mc-Graw Hill]. Though fear and anxiety are nature&#39;s first-line of defense, as the ability to sense potential danger before it strikes is an evolutionary key to survival. But when it is excessive and becomes disproportionate to the situation, and interferes with a person&#39;s ability to function effectively, then it leads to clinical anxiety and panic disorders which requires treatment. 
         [0003]    The primary anxiety disorders are classified according to their duration and course and the nature of precipitants. Most common of them is the generalized anxiety and the panic disorder. Generalized anxiety disorder is a chronic state of anxiety wherein the patient feels apprehensive, highly alert with an overactive sympathetic system without any reason, whereas panic disorder can be defined by the presence of recurrent and unpredictable panic attacks, which are distinct episode of intense fear and discomfort associated with a variety of physical symptoms, including palpitations, sweating, trembling, shortness of breath, chest pain, dizziness and a fear of impending doom or death. [Reus V. I. (2005). Mental Disorders. In (16 th  Edition) Harrison&#39;s Principles of internal medicine (pp 2457-2552). Mc-Graw Hill] 
         [0004]    Currently, the benzodiazepines are the most commonly employed medicinal treatments for the common clinical anxiety disorders, despite the potential for drug dependence and side effects. Virtually all effects of benzodiazepines results from their depressant actions on central nervous system (CNS). The most prominent of these effects are sedation, hypnosis, anxiolytic, muscle relaxation, anterograde amnesia and anticonvulsant activity. [Charney D. S., Mihic S. J., and Harris R. A. (2006) Hypnotics and Sedatives. In (11 th  Edition) Goodmann and Gillmann&#39;s the pharmacological basis of therapeutics (pp 401-427). Mc-Graw Hill, Baldessarini R. J. (2006) Drug therapy of Depression and Anxiety Disorders. In (11 th  Edition) Goodmann and Gillmann&#39;s the pharmacological basis of therapeutics (pp 429-459). Mc-Graw Hill]. 
         [0005]    However, at the time of peak concentration in plasma, hypnotic doses of benzodiazepines can be expected to cause varying degrees of side effects including lightheadedness, lassitude, increased reaction time, motor incoordination, impairment of mental and motor functions, confusion and anterograde amnesia. [Charney D. S., Mihic S. J., and Harris R. A. (2006) Hypnotics and Sedatives. In (11 th  Edition) Goodmann and Gillmann&#39;s the pharmacological basis of therapeutics (pp 401-427). Mc-Graw Hill] 
         [0006]    Chronic benzodiazepine use poses a risk of development of dependence and abuse [Wood, J. H., Katz, J. L and Winger G. (1992) Benzodiazepines: Use,abuse, and consequences  Pharmacol. Rev.,  1992, 44:151-347]. After chronic use, the proportion of patients who become tolerant increases, and reducing the dose or stopping the medication produces withdrawal symptoms which may include temporary intensification of the problems that originally prompted their use (e.g., insomnia or anxiety). Dysphoria, irritability, sweating, unpleasant dreams, tremors, anorexia and faintness or dizziness may also occur, especially when withdrawal of the benzodiazepine occurs abruptly [Petursson, H. (1994). The benzodiazepine withdrawal syndrome.  Addiction.  89:1455-1459]. Some patients may increase their dose overtime because tolerance definitely develops to the sedative effects. Mild dependency may develop in many patients who have taken therapeutic doses of benzodiazepines on a regular basis for prolonged periods. Abuse by the pregnant mother can result in the withdrawal symptom of the newborn. [Baldessarini R. J. (2006) Drug therapy of Depression and Anxiety Disorders. In (11 th  Edition) Goodmann and Gillmann&#39;s the pharmacological basis of therapeutics (pp 429-459). Mc-Graw Hill] 
         [0007]    Benzodiazepines causes drug interactions by potentiate the effect of other CNS depressants such as alcohol, hypnotics, and neuroleptics. Further aminophyllines antagonizes the action of benzodiazepines and enzyme inhibitors like cimitidine and ketoconazole enhances benzodiazepine actions. Therefore, there is an urgent need of drug which possess a greater efficacy lesser undesirables effect with no tolerance and dependence. [Charney D. S., Mihic S. J., and Harris R. A. (2006) Hypnotics and Sedatives. In (11 th  Edition) Goodmann and Gillmann&#39;s the pharmacological basis of therapeutics (pp 401-427). Mc-Graw Hill] 
         [0008]    The use of plants for alleviation of human suffering is perhaps as old as human themselves. Herbal drugs are playing an important role in health care programs and there is resurgence of interest in herbal medicine for treatment of various ailments including neuropsychiatric disorders. Because of their wide biological activities, higher safety margins and lesser costs, herbal medicines are in great demand in the developed as well as developing countries for primary healthcare. 
         [0009]    The current Invention relates to the biological efficacy of the leaves part of the plant  Cassia tora  against neurological disorder-anxiety. Anti anxiety activity of the plant has not been reported so far. The crude alcoholic extract of the leaves of the plant revealed significant antianxiety activity. Further, the antianxiety activity was found to be localized in a non-toxic extract of leaves part of the plant  Cassia tora.    
         [0010]    Bhawarlal Jain Babulal in a PCT Patent entitled “A Process for manufacturing an herbal composition for relieving pain from joints and bones” vide Patent No. WO 2008/015697 A3 describes a process for manufacturing an herbal composition comprising of different extracts of various herbs in the different percentage by weight including fruit extract of  Cassia tora  (15%). The composition is said to be useful for relieving pain from joints and bones. Cited reference does not suggest the use of extract of  Cassia tora  for the treatment of anxiety. 
         [0011]    Cherng J M et al, in a research paper entitled “Anthraquinones of edible wild vegetable  Cassia tora  stimulate proliferation of human CD4(+) T lymphocytes and secretion of interferon-gamma or interleukin 10” published in Food Chemistry, Vol. 107 (4) pp. 1576-1580 (April 2008) describes the immunostimulatory activities of four anthraquinones of  Cassia tora  on human peripheral blood mononuclear cell (PBMC). The results of the studies showed that at non-cytotoxic concentrations, the tested anthraquinones were effective in stimulating the proliferation of resting human PBMC and/or secretion of IFN-gamma. However, at the concentration of 10 mu gm/mL (35 M), rhein significantly stimulated proliferation of resting human PBMC (stimulation index (SI)=1.53), but inhibited IFN-gamma secretion (74.5% of control). Cited reference does not expressly describe the anti-anxiety activity in the  Cassia tora  plant. 
         [0012]    Crane Philip in a PCT Patent entitled “Modified polysaccharides for depressing to floatable gangue minerals” vide Patent No. WO 2008/020311 A3 describes a class of non-sulfide, silicate gangue material depressants based on naturally occurring galactomannans having a galactose-to-mannose ratio of less than 1:2.1, exemplified by modified products of the seed gums:  Cassia tora  gum, Sesbania gum, Kalonji gum, Ceratonia siliqua gum and/or  Tamarindus indica  gum and methods of making and using them. Cited reference does not teach the usage of alcoholic extract of  Cassia tora  leaves for the treatment of anxiety. 
         [0013]    Kim Kwang Soo in a PCT Patent entitled “Beverage composition using Sea weed Fusiforme and onion for the prevention of Hypertension” vide Patent No. WO 2008/032958 A1 describes about the beverage composition for the prevention of Hypertension comprising Hizikia fusiforme, Allium cepa, Acanthopanax senticosus, 
         [0014]    Lycii fructus,  Cassia tora  extract and vinegar. It also descloses the preparation of extracts as well their evaluation for anti-hypertensive activity. Cited reference does not expressly describe the anti-anxiety activity in any of the plant species mentioned above except  Cassia tora  and does not pertain to the present invention. 
         [0015]    Qi, Guoyi, in a Chinese patent entitled “Mongolian medicinal composition containing Liquidambar and Terminalia and others for treating psoriasis” vide Patent No. CN 101167908 A 30 Apr. 2008, 8 pp. (Chinese) describes the Mongolian medicinal compn. for treating psoriasis composed of Boehmeria nivea seed 35,  Cassia  seed 35, Liquidambar formosana 35, Terminalia chebula 35,  Lotus  seed 35, Gardenia jasminoides 35, Xanthoceras sorbifolia 30, Acorns gramineus 30, Trogopterus xanthipes feces 35, crystal salt 35, Viola yedoensis 30, Rhododendron molle 30,  Eugenia caryophyllata  dried flower bud 30, artificial bezoar 35, buffalo horn powder 35, bear bile 10, Crocus sativus 20, musk 5, baked mercury 10, and baked sulfur 10 wt. part. Cited reference does not teach the anti anxiety activity of  Cassia tora  leaves. Yan, Liang et al, in a Chinese patent entitled “A Chinese medicinal composition for relieving eye diseases in the middle-aged and senile patients, and preparation method thereof” vide Patent No. CN 101167954 A 30 Apr. 2008, 4 pp. (Chinese) describes the preparation of Chinese medicinal compn (by wt. parts) Lycium barbarum fruit 10-25, Rhizoma Polygonati 5-20, Semen Cassiae ( Cassia obtusifolia  and/or  Cassia tora ) 10-25, Moms alba fruit 10-25, glue of Equus asinus hide 5-20 and Chrysanthemum morifolium flower 5-20. The prepn. method comprises mixing the water soln. of the fine powder of glue of Equus asinus hide with the concd. water decoction of the rest medicinal materials, adding proper amt. of starch, dextrin and stevioside, granulating with ethanol, drying, sieving and bagging. It has good therapeutic effects on visual deterioration and presbyopia in senile patients. It can improve vision effectively; and has auxiliary functions in relieving asthenopia, protecting the functions of eye tissues, and preventing, relieving and eliminating eye diseases such as myopia, presbyopia and amblyopia. It has no adverse side effect on human bodies. Cited reference does not disclose the anti anxiety activity of  Cassia tora  leaves. 
         [0016]    Li, Shutang, in a Chinese patent entitled “Antihypertensive hypolipidemic healthcare tea” vide Patent No. CN 101120708 A 13 Feb. 2008, 7 pp. (Chinese) describes the antihypertensive hypolipidemic healthcare tea which comprises (by wt. %): Saliva miltiorrhiza 20-40,  Ginkgo biloba  leaves 15-35, Gynostemma pentaphyllum 15-35, Semen Cassiae 10-25, Semen Persicae 5-20, and  Carthamus tinctorius  5-15. The tea is prepd. by mixing and bagging. The tea can nurse lungs, eyes, livers and kidneys, promote the decompn. of serum cholesterin, triglyceride and low d. lipoprotein, and prevent cardiovascular and cerebrovascular diseases. Cited reference does not disclose the anti anxiety activity of  Cassia tora  leaves extract. 
         [0017]    Wang, Zhihua, in a Chinese patent entitled “Health oral liquid for fat and weight reduction, skin care and gastrointestinal function regulation” vide Patent No. CN 101112457 A 30 Jan. 2008, 7 pp. (Chinese) describes the preparation of health oral liq. from Semen Cassiae ( Cassia obtusifolia  and/or  Cassia tora ) 15-25, Radix Et Rhizoma Rhei 15-25, oligosaccharide 3-15, honey 10-15 , Cynomorium songaricum  20-30, and tea leaf 2-3%, by decocting Semen Cassiae and  Cynomorium songaricum  in pure water for 45 min, filtering, soaking tea leaf preferably longjing tea in the filtrate for 30 min, filtering again, cooling the filtrate down to 15, adding the rest of materials, stirring for 10 min, filtering, and bottling. The oral liq. is effective in reducing lipids, cholesterols, triglycerides and low d. lipoproteins in blood, and has anti-arteriosclerotic and antiaging effects. Cited reference does not teach the anti anxiety activity of  Cassia tora  leaves. 
         [0018]    Yang, Rongping et al., in a Chinese patent entitled “New formulations of traditional Chinese medicine for treating fatty liver” vide Patent No. CN 101112432 A 30 Jan. 2008, 19 pp. (Chinese) describes the chinese medicinal prepn. for treating primary and secondary fatty liver, which is prepd. from (by wt. parts) Semen Cassiae (Cassia to obtusifolia and/or  Cassia tora ) 9-15,  Crataegus pinnatifida  9-15, and  Panax quinquefolium  3-9, by reflux-extg. the above materials with 30-90% ethanol soln., removing ethanol, sepg. by macroporous resin column chromatog., eluting with ethanol, collecting ethanol eluate, concg., adding adjuvant, and processing into various pharmaceutically acceptable forms. The invention has the advantages of definite therapeutic effect, low adverse side effect, controllable quality and low cost. Cited reference does not disclose the anti anxiety activity of  Cassia tora  leaves. Zheng, Jimi, in a Chinese patent entitled “Chinese medicinal granule for treating retinal hemorrhage and vitreous opacity.” vide Patent No. CN 101112468 A 30 Jan. 2008, 4 pp. (Chinese) describes the Chinese medicinal granule preparation for treating retinal hemorrhage and vitreous opacity, which comprises (by wt. parts) Salvia miltiorrhiza 30 , Radix Puerariae  ( Pueraria lobata  and/or  Pueraria thomsonii ) 15 , Semen Cassiae  ( Cassia obtusifolia  and/or  Cassia tora ) 15 , Cuscuta chinensis  seed 15, Pollen Typhae ( Typha angustifolia  and/or  Typha orientalis ) 10 , Rhizoma Atractylodis  ( Atractylodes lancea  and/or  Atractylodes chinensis ) 10,  Sargassum  ( Sargassum pallidum  and/or  Sargassum fusiforme ) 10 , Thallus Laminariae  and/or  Thallus Eckloniae  10,  Scutellaria baicalensis  6, and powder of  Panax notoginseng  2. The granule is administered orally and is rich in puerarin which is a flavonoid compd. effective in improving microcirculation, enhancing erythrocyte deformability, increasing blood flow rate, and inhibiting platelet aggregation. The granule has the advantages of reasonable formula and marked therapeutic effect. Cited reference does not suggest the anti anxiety activity of  Cassia tora  leaves. 
         [0019]    Nishikawa, Masashi et al., in Japanese patent entitled “ Cassia tora  seed extracts, their manufacture, method for reduction of diarrhea-inducing activity of the extracts, and foods and beverages containing them” vide patent No. JP 2008007473 A 17 Jan. 2008, 12 pp. (Japanese) describes the manufacture of  Cassia tora  seed exts., useful for prevention and treatment of fatigue, contain (A) emodin, Aloe-emodin, chrysophanol, physcion, aurantioobtusin, and their glycosides, and (B) rubrofusarin (I) or its glycosides in wt. ratio A/B £2.00, preferably £1.90.  Cassia occidentalis  may be also used instead of  C. tora . Thus, 90° water ext. of pulverized  C. tora  seeds (A/B=1.619) was orally administered to mice, resulting in causing no diarrhea. Beverage contg. the ext. at 106.7 mg/day as I for 3 days raised plasma GSH level from ˜1.5 mM to ˜2.3 mM in healthy volunteers with no adverse effects on digestive functions. Cited to reference does not describe the anti anxiety activity of  Cassia tora  leaves. 
         [0020]    Zhang, Y et al, in a research paper entitled “Chemical components and antioxidant activity of the volatile oil from  cassia tora  L. seed prepared by supercritical fluid extraction” published in Journal Of Food Lipids, Vol. 14 (4) pp. 411-423 (December 2007) describes the extraction of volatile oil from seeds of  Cassia tora  L. by employing supercritical fluid extraction using carbon dioxide and its analysis by gas chromatography (GC) and GC-mass spectrometry. This volatile oil was characterized by a high content of aliphatic acids (75.90%) and anthraquinones (7.26%). In the antioxidant assays, the volatile oil from  C. tora  L. seed demonstrated 2,2′-diphenyl-1-picryhydrazyl radical-scavenging activity in the concentration range from 20 to 500 mu g/mL, with the 50% inhibitory concentration (IC50) value at 137 mu g/mL; it also showed a significant inhibitory effect against hydroxyl radicals with an IC50 value of 67 mu g/mL, lower than that of quercetin (IC50=8.15 mu g/mL), but superior to that of 4-terpineol (IC50=87.5 mu g/mL). The observed antioxidant activity of this volatile oil is probably caused by the presence of high levels of chrysophanol and, possibly, (Z,Z)-9,12-octadecadienoic acid. Cited reference does not pertain to the anti-anxiety activity in the extract of  Cassia tora  leaves. 
         [0021]    Jang D S et al, in a research paper entitled “Anthraquinones from the seeds of  Cassia  tora with inhibitory activity on protein glycation and aldose reductase” published in Biological &amp; Pharmaceutical Bulletin, Vol. 30 (11) pp. 2207-2210 (November 2007) describes the in-vitro bioassay study of nine anthraquinones isolated from an EtOAc-soluble extract of the seeds of  Cassia tora  to evaluate their inhibitory activity against advanced glycation end products (AGEs) formation and rat lens aldose reductase (RLAR). Among the isolates, compounds 6 and 8 exhibited a significant inhibitory activity on AGEs formation with observed IC50 values of 118 and 28.9 mu M, respectively, in an AGEs-bovine serum albumin (BSA) assay by specific fluorescence. Furthermore, compounds 6 and 8 inhibited AGEs-BSA formation more effectively than aminoguanidine, an AGEs inhibitor, by indirect AGEs-ELISA. N-epsilon-Carboxymethyllysine (CML)-BSA formation was also inhibited by compounds 6 and 8. 
         [0022]    Whereas compounds 1, 4, and 6 showed a significant inhibitory activity on RLAR with IC50 values of 13.6, 8.8, and 15.9 mu M, respectively. Cited reference does not teach the anti-anxiety activity in the extract of  Cassia tora  leaves. 
         [0023]    El-Halawany, A M et al, in a research paper entitled “Estrogenic and anti-estrogenic activities of  cassia tora  phenolic constituents” published in Chemical &amp; Pharmaceutical Bulletin, Vol. 55 (10) pp. 1476-1482 (October 2007) describes an estrogenic activity bioassay-guided fractionation of the 70% ethanolic extract of  Cassia tora  seeds. Two new phenolic triglucosides, along with seven known compounds were isolated and the structures of the new compounds were elucidated. The estrogenic activity of the fractions and the isolated compounds were investigated using the estrogen-dependent proliferation of MCF-7 cells. In addition, the yeast two hybrid assay expressing estrogen receptor alpha (ER alpha) and beta (ER beta) and the ERa competitor screening assay (ligand binding screen) were used to verify the binding affinities of the isolated compounds to ER. Furthermore, a naringinase pre-treatment of the 70% alcoholic extract of  Cassia tora  seeds resulted in a significant increase in its estrogenic activity. From the naringinase pre-treated extract six compounds were isolated, among which 6-hydroxymusizin and aurantio-obtusin showed the most potent estrogenic activity, while torachrysone, rubrofusarin and toralactone showed a significant anti-estrogenic activity. Finally, from the structure activity relationship studies it was found that the basic nucleus 1,3,8-trihyroxy-naphthalene (T3HN) plays a principal role in the binding affinity of these compounds to ER. Cited reference does not disclose the anti-anxiety activity of the extract from  Cassia tora  leaves. Jia, Z B et al, in a research paper entitled “Antioxidant properties of extracts from juemingzi ( Cassia tora  L.) evaluated in vitro” published in LWT-Food Science And Technology, Vol. 40 (06) pp. 1072-1077 (2007) describes the antioxidant activity of three different fractions of methanol extract from juemingzi ( Cassia tora  L.) was evaluated using different antioxidant tests, including inhibition of peroxidation of linoleic acid, reducing power, free-radical scavenging and ferrous ions chelating activity. In the above four assays, all the fractions showed antioxidant potential to varying degrees. Among these fractions, ethyl acetate fraction exhibited more antioxidant potency than other fractions. Furthermore, ethyl acetate fraction was found to be more effective in protecting LDL against oxidation in a concentration-dependent manner. The data suggest that juemingzi especially ethyl acetate-soluble fraction may have a preventive effect against atherosclerosis by inhibiting LDL oxidation. Cited reference does not describe the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0024]    Cho, I J et al, in a research paper entitled “Hypolipidemic effect of soluble fiber isolated to from seeds of  Cassia tora  Linn. in rats fed a high-cholesterol diet” published in Journal Of Agricultural And Food Chemistry, Vol. 55 (04) pp. 1592-1596 (21 Feb. 2007) describes hypolipidemic effect of soluble fiber isolated from seeds of  Cassia tora  Linn. in rats fed a high-cholesterol diet. In this study the effects of SFC on lipid metabolism were investigated. Male Sprague-Dawley rats were fed one of three experimental diets, a normal diet, a high-cholesterol diet, or a high-cholesterol diet with 5% SFC, for 5 weeks. The serum concentration of total cholesterol in rats fed SFC was 27% lower (p&lt;0.05) compared to that of the control group, but the serum high-density lipoprotein cholesterol level was increased in the SFC group. Liver total cholesterol and triglyceride levels were reduced significantly (p&lt;0.05) in rats fed the SFC diet. In addition, fecal bile acid and lipid excretion was significantly increased by SFC consumption. These results indicate that SFC enhances fecal lipid excretion and may cause a reduction in serum and hepatic lipid concentrations in rats. Cited reference does not expressly describe the anti-anxiety activity of the extract from  Cassia tora  leaves. Eladevi Mahendra Shah, in a US Patent entitled “Novel base material for pharmaceutical and/or cosmetic cream (Herbal composition for itchy or infected skin)” vide Patent No. US 2007/0014749 A1 describes the preparation and use of compositions for the treatment of skin disorders itchy and/or infected skin such as impetigo, acne and fungal infection of skin and nails. The compositions are based on extracts from the plants  Cassia tora, Centratherum anthelminticum  and/or  Melia azadirachta . The herbs may be in powdered form of suitable for preparing decoctions in hot water. Cited reference does not describe the Anti-anxiety activity of the extract of  Cassia tora.    
         [0025]    Kaneda Yoshihisa et al., in a PCT Patent entitled “Composition having physical endurance improving effect and/or anti-fatigue effect” vide Patent No. WO 2007/004570 A1 describes for a composition comprising a natural product derived component, which comprises an active ingredient different from that in a conventionally known amino acid composition, is effective in the improvement in physical endurance and the alleviation or recovery of the decline in physical activity and fatigue, and is safe for oral administration. A composition having a physical endurance-improving effect and/or an anti-fatigue effect and comprising an active ingredient, a substance extracted from a seed cassiae semen (A seed of a plant  Cassia obtusifolia  or  Cassia tora ) with water, an organic solvent compatible with water or a mixture of water with the organic solvent at any given ratio. Cited reference does not expressly teach the Anti-anxiety activity in the extract of  Cassia tora  leaves. 
         [0026]    Nam, Jong Hyun in a PCT Patent entitled “Natural plant extract composition for prevention and recovery of hyperlipidemia and stroke, natural tea containing the same as active ingredient and method for preparing the natural tea” vide Patent No. WO 2007/111401 A1 describes a natural plant extract composition contains a  Cassia tora  extract and an  Albizzia julibrissin  extract which can lower the blood cholesterol level to prevent arteriosclerosis and stroke. And it is effective for the prevention and treatment of hyperlipidemia and stroke. Cited reference does not expressly describe the Anti-anxiety activity of the extract of  Cassia tora  leaves. 
         [0027]    Dutta, Tuhina et al, in a research paper entitled “Identification of antifungal activity in different species of  Cassia ” published in Indian Journal of Environment and Ecoplanning, 12(3), 661-663 (English)  2006  describes the antifungal activity in three different species of  Cassia  viz.  Cassia fistula, Cassia sophera  and  Cassia tora . The crude 50% aq. ethanolic leaf ext. of the three species were tested for their antifungal effect by the std. Agar cup method. Antifungal activity was located in the crude exts. of all the tested plant exts. against  Fusarium oxysporum  and  Phytophthora  sp. The antifungal property was also evaluated by studying the effects of the leaf exts. on healthy and fungal infected seeds of  Phaseolus aureus  in different doses (2 mg/mL, 2.4 mg/mL, 2.8 mg/mL and 3.2 mg/mL). Maximum inhibitory effect was exhibited by  Cassia sophera  (3.2 mg/mL dose). Cited reference does not expressly describe the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0028]    Guo Xinfu, in a PCT Patent entitled “A composition for treating or preventing hyperlipemia, hypertension and hepatic adipose infiltration” vide Patent No. WO 2006/081739 A1 describes the preparation of a composition for treating or preventing hyperlipemia, hypertension and hepatic adipose infiltration. The composition contains various herbs including semen of  Cassia tora  L. which has no toxic side effect and have good effects on regulating fats, can significantly reduce cholesterol, triglyceride, low density lipo-protein in the blood, have apparent effects on treating and preventing hypertension, hepatic adipose infiltration, and can be used in preparing drugs or health food for treating and preventing hyperlipemia, hypertension and hepatic adipose to infiltration Cited reference does not suggest the anti-anxiety activity in the extract of  Cassia tora  leaves. 
         [0029]    Kim S. Y. et al in a Korean Patent entitled “Composition for preventing and treating anxiety symptom associated with brain nervous system comprising extract of  cinnamomum cassia  presl. Having anti-anxiety activity” vide Patent No. KR2006030535-A; KR646594-B1, describes the preparation of extract of  cinnamomum cassia  presl. Using a polar solvent selected from water, C1-C4 lower alcohol and their mixed solvent for preventing and treating anxiety symptom associated with brain nervous system. Cited reference does not disclose in-vitro &amp; in-vivo antianxiety activity of extract obtained from  Cassia tora  of Caesalpiniaceae family. Cho, S H et al, in a research paper entitled “Effects of  Cassia tora  fiber supplement on serum lipids in Korean diabetic patients” published in Journal Of Medicinal Food, Vol. 8 (3) pp. 311-318 (2005) describes the effects of  Cassia tora  fiber supplement on serum lipids in Korean diabetic patients.  Cassia tora  fiber supplement consisting of 2 g of soluble fiber extracted from  Cassia  semen ( C. tora  L.), 200 mg of a-tocopherol, 500 mg of ascorbic acid, and 300 mg of maltodextrin was formulated in a pack, and given to 15 type II diabetic patients with instructions to take two packs per day for 2 months. Lifestyle factors and dietary intakes of the patients were not altered during the 2-month period. Serum total cholesterol was moderately (P&lt;0.1) decreased in the  C. tora  group compared with the age- and gender-matched placebo group, as was the ratio of apolipoprotein B to apolipoprotein A1 (P&lt;0.1). Levels of serum triglycerides and low-density lipoprotein-cholesterol tended to decrease more in the  C. tora -supplemented group than in the placebo group. Serum a-tocopherol was increased (P&lt;0.01) but lipid peroxides were not significantly lower in the  C. tora  group. Fasting blood glucose, hemoglobin A I c, blood urea nitrogen, creatinine, and activities of serum aspartate aminotransferase and alanine aminotransferase were not changed by the fiber supplement. It was concluded that  C. tora  supplements can help to improve serum lipid status in type II diabetic patients without serious adverse effects. Cited reference does not teach the anti-anxiety activity of the extract from  Cassia tora  leaves. Lee, C H &amp; Lee, H S, in a research paper entitled “Antifungal property of dihydroxyanthraquinones against phytopathogenic fungi” published in Journal Of Microbiology And Biotechnology, Vol. 15 (2) pp. 442-446 (April 2005) describes the fungicidal activities of  Cassia obtusifolia  extracts and their active principles against to  Botrytis cinerea, Erysiphe graminis, Phytophthora infestans, Puccinia recondita, Pyricularia grisea , and  Rhizoctonia solani , and compared with synthetic fungicides and two dihydroxyanthraquinones. Cited reference does not describe the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0030]    Utz, Ferdinand et al., in a PCT Patent and U.S. patent entitled “Cationic  Cassia  derivatives and applications therefor” vide Patent No. WO 2004/112733 A1 and US 2008/0004340 A1 U.S. Pat. No. 7,262,157 B2 describes the cationically derivatized polygalactomannans obtained from  Cassia tora  and  Cassia obtusifolia  and their use in personal care, household care and institutional care composition. In addition, these polymers are useful for improving the psychosensory and aesthetic properties of cosmetic formulations. Cited reference does not expressly teach the Anti-anxiety activity of the extract of  Cassia tora  leaves. 
         [0031]    Chi-Hao Wu and Gow-Chin Yen, in a research paper entitled “Antigenotoxic properties of  Cassia  tea ( Cassia tora  L.): Mechanism of action and the influence of roasting process” published in Life Sciences, Vol. 76 (1) pp. 85-101 (November 2004) describes the Antigenotoxic properties and the possible mechanisms of water extracts from  Cassia tora  L. (WECT) treated with different degrees of roasting (unroasted and roasted at 150 and 250° C.). The individual anthraquinone content in extracts of  C. tora  was measured by HPLC. Three anthraquinones, chrysophanol, emodin and rhein, have been detected under experimental conditions. The anthraquinone content decreased with increased roasting temperature. In conclusion, our data suggest that the decrease in antigenotoxic potency of roasted  C. tora  was related to the reduction in their anthraquinones. Cited reference does not disclose the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0032]    Kim, Y M et al., in a research paper entitled “Anthraquinones isolated from  Cassia tora (Leguminosae) seed show an antifungal property against phytopathogenic fungi” published in Journal Of Agricultural And Food Chemistry, Vol. 52 (20) pp. 6096-6100 (6 Oct. 2004) describes the fungicidal activities of  Cassia tora  extracts and their active principles against  Botrytis cineria, Erysiphe graminis, Phytophthora infestans, Puccinia recondita, Pyricularia grisea , and  Rhizoctonia solani  using a whole plant method in vivo and compared with synthetic fungicides and three commercially available anthraquinones. Little or no activity was observed for anthraquinone and anthraquinone-2-carboxylic acid when tested at 1 g/L. Chlorothalonil and dichlofluanid as synthetic fungicides were active against  P. infestans  and  B. cinerea  at 0.05 g/L, respectively. The results demonstrate the fungicidal actions of emodin, physcion, and rhein from  C. tora . Cited reference does not teach the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0033]    Hebbar, S S et al., in a review article entitled “Ethnomedicine of Dharwad district in Karnataka, India—plants used in oral health care” published in Journal Of Ethnopharmacology, Vol. 94 (2-3) pp. 261-266 (October 2004) describes the ethnomedicine survey of the Dharwad district of Karnataka in southern India. It was revealed that 35 plants belonging to 26 families are being used to treat different types of oral ailments like toothache, plaque and caries, pyorrhea and aphthae. Sixteen of these plants were new claims for the treatment of oral ailments not previously reported in the ethnomedicinal literature of India.  Basella alba, Blepharis repens, Capparis sepiaria, Oxalis corniculata  and  Ricinus communis  are used for the treatment of aphthae;  Azima tetracantha, Caesalpinia coriaria, Cleome gynandra, Gossypium herbacium, Leucas aspera, Merremia chryseides, Pergularia daemia, Prosopis juliflora  and  Solanum nigrum  are used to treat tooth ache and  Cassia hirsuta  and  Cassia tora  are used in the treatment of plaque and caries. Cited reference does not pertain to the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0034]    Park, T H et al., in a research paper entitled “Peroxynitrite scavenging mode of alaternin isolated from  Cassia tora ” published in Journal Of Pharmacy And Pharmacology, Vol. 56 (10) pp. 1315-1321 (October 2004) describes a potent oxidant Peroxynitrite (ONOO) which contributes to the oxidation of various cellular constituents, including lipids, amino acids, sulfhydryls and nucleotides. It can cause cellular injury, such as DNA fragmentation and apoptotic cell death. ONOO— toxicity is also reported to be involved in inflammatory and neurodegenerative diseases, such as Alzheimer&#39;s disease, Parkinson&#39;s disease and atherosclerosis. Moreover, the necessity for a strong ONOO-scavenger is important because of the lack of endogenous enzymes that protect against the damage caused by ONOO—. The aim of the study was to evaluate the ability of natural products to scavenge ONOO—. They have tested various plant extracts for their ONOO— scavenging activity. Among them, extract from  Cassia tora  showed potent ONOO— scavenging activity. Further analysis identified the phenolic active components, alaternin and nor-rubrofusarin glucose, as potent ONOO— scavengers. The alaternin and nor-rubrofusarin glucose led to a decrease in the ONOO-mediated nitration of tyrosine through electron donation. In bovine serum albumin, alaternin, but not nor-rubrofusarin glucose, showed significant inhibition of ONOO-mediated nitration in a dose-dependent manner. Therefore, it was assumed that alaternin can be developed as an effective ONOO— scavenger for the prevention of ONOO-associated diseases. Cited reference does not disclose the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0035]    Patil, U K et al., in a research paper entitled “Hypolipidemic activity of seeds of  Cassia  tora Linn” published in Journal Of Ethnopharmacology, Vol. 90 (2-3) pp. 249-252 (February 2004) describes the hypolipidemic activity of ethanolic extract of seeds of  Cassia tora  L. and its fractions on triton induced hyper-lipidemic profile. Ethanolic extract and its ether soluble and water soluble fraction decreased serum level of total cholesterol on the other hand increased the serum HDL-cholesterol level. Ethanolic extract, ether fraction and water fraction decreased triglyceride level and reduced the LDL-cholesterol level. Cited reference does not expressly describe the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0036]    Lee, H S. in a research paper entitled “Inhibitory effects of quinizarin isolated from  Cassia tora  seeds against human intestinal bacteria and Aflatoxin B-1 biotransformation” published in Journal Of Microbiology And Biotechnology, Vol. 13 (4) pp. 529-536 (August 2003) describes the growth-inhibitory activity in vitro of  Cassia tora  seed-derived materials against seven intestinal bacteria and compared with that of anthraquinone, anthraflavine, anthrarufin. and 1-hydroxyanthraquinone. The active constituent of  C. tora  seeds was characterized as quinizarin. The growth responses varied depending on the compound, dose, and bacterial strain tested. At 1 mg/disk, quinizarin exhibited a strong inhibition of  Clostridium perfringens  and moderate inhibition of  Staphylococcus aureus  without any adverse effects on the growth of  Bifidobacterium adolescentis, B. bifidum, B. longum , and  Lactobacillus casei . Furthermore, the isolate at 0.1 mg/disk showed moderate and no activity against  C. perfringens  and  S. aureus . The structure-activity relationship revealed that anthrarufin, anthraflavine, and quinizarin moderately inhibited the growth of  S. aureus. However, anthraquinone and  1-hydroxyanthraquinone did not inhibit the human intestinal bacteria tested. As for the morphological effect of 1 mg/disk quinizarin. most strains of  C. perfringens  were damaged and disappeared. indicating that the strong activity of quinizarin was morphologically exhibited against  C. perfringens . The inhibitory effect on aflatoxin B-1 biotransformation by anthraquinones revealed that anthrarufm (IC50, 11.49 muM), anthraflavine (IC50, 26.94 muM), and quinizarin (IC50, 4.12 muM) were potent inhibitors of aflatoxin B-1-8,9-epoxide formation. However, anthraquinone and 1-hydroxyanthraquinone did not inhibit the mouse liver microsomal sample to convert aflatoxin B, to aflatoxin B,-8,9-epoxide. These results indicate that the two hydroxyl groups on A ring of anthraquinones may be essential for inhibiting the formation of aflatoxin B-1-8,9-epoxide. Accordingly, as naturally occurring inhibitory agents, the  C. tora  seed-derived materials could be useful as a preventive agent against diseases caused by harmful intestinal bacteria, such as clostridia, and as an inhibitory agent for the mouse liver microsomal conversion of aflatoxin B-1 to aflatoxin B-1-8,9-epoxide. Cited reference does not disclose the anti-anxiety activity of the extract from  Cassia tora  leaves. 
         [0037]    Takagi Chiyoshi et al., in a PCT and EP Patents entitled “Flavor deterioration inhibitor and inhibitor for the generation of citral deterioration smell” vide Patent No. WO 03/105599 A1, EP 01554938 B1 &amp; EP 01554938 Aldescribes for a flavor deterioration inhibitor which comprises an extract obtained by extracting  Angelica keiskei , avocado,  Cassia tora, Plantago asiatica  L, hawthorn, fermented tea leaves with water, an organic polar solvent or a mixture thereof; and a deterioration smell inhibitor for citral or a citral—containing product. In particular, a remarkable inhibitory effect can be achieved on deterioration due to light. Cited reference does not describe the Anti-anxiety activity in the extract of  Cassia tora  leaves. 
         [0038]    Chidume, F C et al., in a research publication entitled “Antinociceptive and smooth muscle contracting activities of the methanolic extract of  Cassia tora  leaf” published in Journal Of Ethnopharmacology, Vol. 81 (2) pp. 205-209 (July 2002) describes the antinociceptive and smooth muscle contracting activities of the methanolic extract of  Cassia tora  leaf. The leaves of  Cassia tora  Linn. (Family: Caesalpiniaceae) were soxhlet extracted with methanol. The spasmogenic effects of the extract were evaluated on guinea pig ileum, rabbit jejunum and mice intestinal transit. Antinociceptive activity of the extract was also evaluated in the mice. The LD50 values of the extract in mice were &gt;2000 mg/kg i.p. and p.o. The extract contracted smooth muscles of guinea pig ileum and rabbit jejunum in a concentration-dependent manner. Atropine reversibly blocked this activity. Mepyramine also reduced the contractile amplitude due to the extract in a concentration-dependent manner. The extract increased intestinal transit in mice dose to dependently.  C. tora  extract significantly (P&lt;0.05) reduced the number of acetic acid induced abdominal constrictions in mice and the effect was comparable to that of aspirin (150 mg/kg i.p.). The extract also significantly (P&lt;0.05) reduced the nociceptive response of mice to increased force (g). The effects were dose-dependent. The studies suggest that the use of  C. tora , traditionally, as a purgative and in the treatment of other ailments is justifiable. Cited reference does not expressly teach the anti-anxiety activity of methanolic extract of  Cassia tora  leaves at ambient temperature. Yen, G C et al., in a research publication entitled “Antioxidant properties of water extracts from  Cassia tora  L. in relation to the degree of roasting” published in Journal Of Agricultural And Food Chemistry, Vol. 48 (7) pp. 2760-2765 (July 2000) describes the antioxidant properties of water extracts from  Cassia tora  L. in relation to the degree of roasting. The antioxidant properties of water extracts from  Cassia tora  L. (WECT) prepared under different degrees of roasting were investigated. The water extracts of unroasted  C. tora  L. (WEUCT) showed 94% inhibition of peroxidation of linoleic acid at a dose of 0.2 mg/mL, which was higher than that of alpha-tocopherol (82%). Water extracts prepared from  C. tora  L. roasted at 175 degrees C. for 5 min and at 200 degrees C. for 5 min exhibited 83% and 2%, respectively, inhibition of linoleic acid peroxidation. This result indicated that the antioxidant activities of WECT decreased with longer roasting time or higher roasting temperature. In conclusion, the decrease in the antioxidant activity of water extracts from roasted  C. tora  L. might have been due to the degradation of Maillard reaction products and the decrease of polyphenolic compounds. Cited reference does not disclose the anti-anxiety activity of  Cassia tora  leaves. El-Tahir, A et al., in a research publication entitled “Antiplasmodial activity of selected sudanese medicinal plants with emphasis on  Acacia nilotica”  published in Phytotherapy Research, Vol. 13 (6) pp. 474-478 (September 1999) describes the antiplasmodial activity of selected sudanese medicinal plants with emphasis on  Acacia nilotica . Twenty-two plant organs from eleven plants comprising five families were extracted and screened for antiplasmodial activity in vitro against  Plasmodium falciparum  3D7 (chloroquine sensitive) and Dd2 (chloroquine resistant and pyrimethamine sensitive). Fifty nine percent of plant extracts from 22 extracts exerted activity on  P. falciparum  strain 3D7 with an IC50 less than 50 mu g/mL, whereas 43% of plant extracts showed to an IC50 value within 50 mu g/mL on Dd2 strains. Plant extracts from  Gardenia lutea, Haplophyllum tuberculatum, Cassia tora, Acacia nilotica  and  Aristolochia bracteolata  possessed IC50 values less than 5 mu g/mL on both tested strains, Bioassay guided fractionation of  A. nilotica  revealed that the ethyl acetate extract possessed the highest activity (IC50=1.5 mu g/mL). Fraction 2 (R-f=0.75) prepared by preparative chromatography showed the highest activity on  P. falciparum  (IC50=1.7 mu g/mL). 
         [0039]    Phytochemical analysis indicated that the most active phase contained terpenoids and tannins and was devoid of alkaloids and saponins, The effect of plant extracts on lymphocyte proliferation showed low toxicity to the human cells. This plant has been subjected to long term clinical trials in folk medicine and is a promising plant. Cited reference does not expressly describe the anti-anxiety activity of  Cassia tora  leaves. 
         [0040]    Hatano, T et al., in a research publication entitled “Phenolic constituents of  cassia  seeds and antibacterial effect of some naphthalenes and anthraquinones on methicillin-resistant  Staphylococcus aureus ” published in Chemical &amp; Pharmaceutical Bulletin, Vol. 47 (8) pp. 1121-1127 (August 1999) describes the isolation of thirteen phenolic glycosides including six new compounds from seeds of  Cassia tora  (Leguminosae). 
         [0041]    The effects of the phenolic glycosides, their aglycones and several other compounds structurally related to them on  Escherichia coli  K12,  Pseudomonas aeruginosa  PAO1 and some strains of  Staphylococcus aureus  were examined. Among them, torachrysone (15), toralactone (16), aloe-emodin (18), rhein (19) and emodin (20) showed noticeable antibacterial effects on four strains of methicillin-resistant  Staphylococcus aureus  with a minimum inhibitory concentration of 2-64 mu g/ml. On the other hand, the phenolic compounds tested did not show strong antibacterial effects on  E. coli  and  P. aeruginosa . Cited reference does not suggest the anti-anxiety activity of  Cassia tora  leaves. 
         [0042]    Agarkar, S V et al., in a review article entitled “Phytochemical and pharmaco-logical investigations of genus  Cassia : A review” published in Asial Journal Of Chemistry, Vol. 11 (2) pp. 295-299 (April-June 1999) describes the phytochemical and pharmacological investigations of genus  Cassia . About 26 species of genus  Cassia  have been reported to contain anthracene derivatives. The more important species among them are  Cassia alata, Cassia angustifolia vahl, Cassia autifolia, Cassia cinnamon, Cassia fistula Cassia nodosa Cassia obtusifolia, Cassia sophera, Cassia tora  and  Cassia zeylanicum . Diuretic, antidiabetic, antibiotic, antifungal, antipyretic, anthlemintic, antibacterial, antirheumatic, anti-eczema, antiherpetic, antiasthmatic, anti-leprosy, anti-typhoid and anti-bronchitis activities have been reported from some of these species. Cited reference does not suggest the anti-anxiety activity of  Cassia tora  leaves Maity, T K et al., in a research paper entitled “Studies on antiinflammatory effect of  Cassia tora  leaf extract (fam. Leguminosae)” published in Phytotherapy Research, Vol. 12 (3) pp. 221-223 (May 1998) describes the antiinflammatory effect of the methanol extract of the leaves of  Cassia tora  against carrageenin, histamine, serotonin and dextran-induced rat hind paw oedema, It exhibited significant antiinflammatory activity against all these agents, The extract (400 mg/kg) showed maximum inhibition of oedema of 40.33%, 31.37%, 53.57% and 29.15% at the end of 3 h with carrageenin, dextran, histamine and serotonin-induced rat paw oedema, respectively. Using a chronic test, the granuloma pouch in rats, the extract exhibited a 48.13% reduction in granuloma weight. Cited reference does not disclose the anti-anxiety activity of methanolic extract of  Cassia tora  leaves. 
         [0043]    Yen, G C et al., in a research paper entitled “Extraction and identification of an antioxidative component from Jue Ming Zi ( Cassia tora  L.)” published in Journal Of Agricultural And Food Chemistry, Vol. 46 (3) pp. 820-824 (March 1998) describes the antioxidant activity of  Cassia tora  L. and  Cassia occidentalis  L. The results indicated that methanolic extracts from  C. tora  L. (MECT) and  C. occidentalis  L. (MECO) produced stronger antioxidant activity and gave higher yields of extract than other organic solvents, The MECT showed stronger antioxidant activity than did the MECO on peroxidation of linoleic acid. MECT at 200 ppm was stronger than 200 ppm of alpha-tocopherol, but weaker than 200 ppm of butylated hydroxyanisole. Amberlite XAD-2 column chromatography separated MECT into eight fractions. Of the eight fractions, fraction V possessed significant antioxidant activity and showed 85.8% inhibition on peroxidation of linoleic acid. Subsequently, fraction V was separated into two subfractions, Va and Vb, by Toyoperal HW-40 F gel filtration chromatography. The subfraction Vb exhibited stronger antioxidant activity than did subfraction Va and was identified as 1,3,8-trihydroxy-6-methyl-9,10-anthracenedione (emodin). Cited reference does not expressly describe the anti-anxiety activity of methanolic extract of  Cassia tora  leaves. 
         [0044]    Pandey, V N et al., in a research paper entitled “Synergistic activity of extracted plant oils against  Pythium aphanidermatum  and P-debaryanum” published in Tropical Agriculture, Vol. 74 (2) pp. 164-167 (April 1997) describes the synergistic activity of to extracted plant oils against  Pythium aphanidermatum  and  P - debaryanum . The leaves of  Cassia tora, Hyptis suaveolens, Murraya koenigii, Ocimum canum , and  Ranunculus arvensis  showed absolute volatile toxicity against  Pythium aphanidermatum  and  P. debaryanum . The volatile antifungal fractions of  H. suaveolens, M. koenigii , and  O. canum  were isolated in the form of essential oils. The oils were tested individually as well as in four mixtures. The fungitoxic activity of the four mixtures of the three oils was found to be several times enhanced than that of the individual oils except for  O. canum  which exhibited absolute fungitoxicity at 1000 ppm. Cited reference does not disclose the anti-anxiety activity of methanolic extract of  Cassia tora  leaves. 
         [0045]    Choi, J S et al., in a research paper entitled “In vitro antimutagenic effects of anthraquinone aglycones and naphthopyrone glycosides from  Cassia tora ” published in Planta Medica, Vol. 63 (1) pp. 11-14 (February 1997) describes the antimutagenic activity of a methanol extract of  Cassia tora  seeds against aflatoxin B-1(AFB(1)) with the  Salmonello typhimurium  assay. The MeOH extract was then sequentially partitioned with CH2Cl2. n-BuOH and H2O. The CH 2 Cl 2  and n-BuOH fractions possessed antimutagenic activity but the H2O fraction was inactive. Neither the MeOH extract nor its fractions were capable of inhibiting the direct-acting mutagen N-methyl-N′-nitro-N-nitrosoguanidine suggesting that these fractions may prevent the metabolic activation of AFB(1) or scavenge the electrophilic intermediate capable of inducing mutations. The pure chrysophanol, chryso-obtusin, and aurantio-obtusin obtained from the CH 2 Cl 2  fraction and cassiaside and rubro-fusarin gentiobioside obtained from the n-BuOH fraction demonstrated significant antimutagenic activity. Cited reference does not suggest the anti-anxiety activity of methanolic extract of  Cassia tora  leaves. 
         [0046]    Mukherjee, P K et al., in a research paper entitled “Antifungal activities of the leaf extract of  Cassia tora  Linn (Fam Leguminosae)” published in Phytotherapy Research, Vol. 10 (6) pp. 521-522. (September 1996) describes the antifungal activities of the leaf extract of  Cassia tora  Linn. The antifungal activity of the dealcoholized extract of leaves of  Cassia tora  L, was determined on five different fungal organisms. The crude leaf extract significantly inhibited the growth of  C. albicans, A. niger, S. cerevisiae  and  T. mentagophytes  when tested by turbidity and spore germination methods in a concentration dependent fashion. The effects produced by the extract were compared with a standard antifungal agent griseofulvin. Cited reference does not teach the anti-to anxiety activity of methanolic extract of  Cassia tora  leaves. 
         [0047]    Sui-Ming Wong et al., in a research paper entitled “New Antihepatotoxic Naphtho-pyrone Glycosides from the Seeds of  Cassia tora   1 ” published in Planta Medica, Vol. 55 (3) pp. 276-280. (June 1989) describes the isolation of new antihepatotoxic naphtho-pyrone glycosides from the seeds of  Cassia tora . Their structures were elucidated on the basis of chemical and spectral data. The naphtho-γ-pyrone glycosides were found to have significant hepato-protective effects against galactosamine damage, which were higher than that of silybin from  Silybum marianum . Cited reference does not disclose the anti-anxiety activity of  Cassia tora  leaves. 
         [0048]    Sui-Ming Wong et al., in a research paper entitled “Anthraquinone glycosides from the seeds of  Cassia tora ” published in Phytochemistry, Vol. 28 (1) pp. 211-214. (1989) describes the isolation of three new anthraquinone glycosides from the seeds of  Cassia tora . Their structures were elucidated on the basis of chemical and spectral data. The first two compounds exhibited a weak protective effect on primary cultured hepatocytes against carbon tetrachloride toxicity. Cited reference does not suggest the anti-anxiety activity of  Cassia tora  leaves. 
         [0049]    Bayerlein et al., in a US patent entitled “Derivatives of  Cassia tora  polysaccarides and their use” vide U.S. Pat. No. 4,753,659 dated Jun. 28, 1988 describes about new alkyl ethers and phosphoric acid esters of  Cassia tora  polygalactomannans and their use, alone or in combination with other thickening agents, as thickening agents. Cited reference does not describe the Anti-anxiety activity or any type of activity in  Cassia  tora. 
         [0050]    Park H. Y. in a Korean Patent entitled “Eye bandage for sleeping which is made out of fabric dyed by loess, and filled with  cassia tora  and siberian chrysanthemum, etc” vide Patent No. KR712055-B1 describes the eye bandage for sleeping comprises: a bandage cover, made by sewing a fabric dyed by the loess through the immersion in the loess solution in such a manner that it is filled with fillers, and having an eye covering member which has a length enough to cover user&#39;s both eyes, and an ear covering member which is formed respectively in both sides of the eye covering member; and a filler, composed of the  Cassia tora  which is filled into the eye covering member. Cited reference does not teach about the antianxiety activity of extract obtained from the  Cassia tora.    
       Object of the Invention 
       [0051]    The main object of the present invention is to provide a plant extract for treating anxiety disorders, which obviates the drawbacks as detailed above. 
         [0052]    Another object of the present invention is to provide an active extract from a herbal source. 
         [0053]    Still another object of the present invention is to prepare  Cassia tora  leaves extract in solvent mixture having different polarity for antianxiety activity. 
         [0054]    Yet another object of the present invention is to show that the leaves of  Cassia tora  plant species possess antianxiety activity. 
         [0055]    Yet another object of the present invention is to utilize alcohol: water combination for complete extraction. 
         [0056]    Yet another object of the present invention is to show that the plant material retains the activity when stored under ambient condition and the extract prepared from the leaves has high shelf life without loss of activity. 
         [0057]    Still another object of the present invention is to subject the extract for biological screening, both in-vitro and in-vivo. 
         [0058]    Still another object of the present invention is to provide an antianxiety extract of  Cassia tora  leaves. 
       SUMMARY OF THE INVENTION 
       [0059]    Accordingly the present invention provides a process for the preparation of herbal extract of  Cassia tora  leaves, useful for the treatment of anxiety disorders, comprising the steps of:
       i. collecting  Cassia tora  plant material;   ii. drying the plant material at ambient temperature in the range of 25 to 37° C. while maintaining the moisture in the range of 0.5-1.5 percent;   iii. pulverizing the plant material dried in step (ii) and selecting the material in the size range of 16-20 mesh sieve;   iv. soaking the pulverized plant material obtained in (iii) in 95:05 (v/v) alcohol-water mixture in static condition at ambient temperature followed by draining &amp; collecting the extract solution;   v. repeating the soaking step described in step (iv) above five times with fresh solvent mixture at an interval of 24 hours;   vi. concentrating the extract solution obtained in step (v) by known methods;   vii. freeze drying the concentrated extract obtained in step (vi) at a temperature in the range of − 50  to −60° C. for a period in the range of 8 to 16 hours;   viii. testing the extract in-vitro and in-vivo for anti-anxiety activities.       
 
         [0068]    In an embodiment of the invention, the plant part used for extraction is leaves of  Cassia  tora. 
         [0069]    In another embodiment of the invention, the said extract is active on benzodiazepine receptors. 
         [0070]    Yet another embodiment of the invention provides a herbal extract of  Cassia tora  leaves prepared by the said process. 
         [0071]    In another embodiment of the invention, the extract exhibits inhibition for binding to benzodiazepine receptors even at concentration as low as 1.56 μg. 
         [0072]    In yet an embodiment of the invention, the extract is administered in a form selected from tablets, lozenges, capsules, powder, solution, intravenously and orally. Still another embodiment of the invention provides use of herbal extract obtained from  Cassia tora  species in treating anxiety disorders. 
     
    
     DETAILED DESCRIPTION OF THE INVENTION 
       [0073]    The plant was identified and required material was collected from the natural vegetation. The extraneous matter was removed from the collected material. The cleaned plant material was dried at room temperature for a period of 3 to 4 weeks. The plant material was pulverized and sieved to obtain 16 to 20-mesh size powder and then soaked in methanol-water mixture under static condition at ambient temperature. The extraction cycle was repeated for five times using fresh alcohol:water (95:05 v/v) mixture. Each extract filtrate was combined, and concentrated using rotary evaporator to obtain crude concentrated extract. The concentrated extract was dispersed in deionised water and again concentrated on rotary evaporator to obtain an extract, free from traces of alcohol. This alcohol-free concentrated extract was freeze dried to obtain moisture-free crude extract in powder form. The crude extract was initially tested in-vitro and after positive test the extract was tested for in-vivo anti-anxiety activity. 
       In Vitro Radioligand Receptor Binding to Assess the Effect of Extract on Frontocortical Benzodiazepine Receptors: 
       [0074]    Role of benzodiazepine receptors in anxiety is well documented. Keeping in view of this, potential of  Cassia tora  leaves extract on frontocortical benzodiazepine receptors was assessed involving in vitro assays of 3H-Flunitrazepam to rat frontocortical membranes, known to label benzodiazepine receptors. 
       Preparation of Crude Synaptic Membrane: 
       [0075]    Albino rats of Wistar strain obtained from the animal breeding colony of Indian Institute of Toxicology Research (IITR), Lucknow were used through out these studies. Rats were sacrificed and their brain removed immediately. The brain was dissected into regions to take out frontal cortex following the standard protocol (Glowinski and Iverson 1966). Crude synaptic membrane from frontal cortex was prepared (Khanna et al 1994). Briefly, frontal cortex was weighed and homogenized in 19 vols. of TRIS-HCl buffer (5 mM, pH 7.4). The homogenate was centrifuged at 50,000×g for 20 minutes at 4° C. The supernatant was removed and the pellet was suspended in the same buffer followed by centrifugation at 50,000×g for 20 minutes at 4° C. to remove endogenous amines and for cell lysis. The pellet thus obtained was finally suspended in the same volume of TRIS-HCl buffer (40 mM, pH 7.4) and used for benzodiazepine receptor assay. Protein estimation was carried out following the procedure of Lowry et al (1951) using bovine serum albumin as a reference standard. 
       Radioligand Receptor Binding Assay: 
       [0076]    Assay for benzodiazepine receptors was carried out in 96 well multiscreen plates HTS FB (Millipore, USA) using 4 tip robotic liquid handling system (Multi Probe II EX, Perkin Elmer, USA). Assay mixture in a final volume of 250 ul contained TRIS-HCl buffer (40 mM, pH 7.4, 140 ul), fronto-cortical membrane (50 ul), radioligand (3H-Flunitrazepam, 0.5×10 −9  M, Specific Activity 82 Ci/mmole, Perkin Elmer, USA, 40 ul) and  Cassia tora  leaves extract, concentrations ranging from 1.56-200 ug in 20 ul) in multiwell plates in triplicate. To assess the total binding, the assay mixture did not contain test compound and thus volume of the TRIS-HCl buffer was 160 ul. In parallel assay, the reaction mixture contained diazepam (1×10 −6  M) instead of test compound. Diazepam in that case served as a positive competitor. The contents in the plate were mixed thoroughly and incubated for 15 minutes at 37° C. using plate incubator (Heidolph, Titramax 100). Following incubation, the contents of the plates were filtered over vacuum manifold attached with the robotic liquid handling system. The plates were washed twice with cold TRIS-HCl buffer (40 mM, pH 7.4, 250 ul) to remove unbound radioligand. The plates were dried over vacuum and left on the deck overnight. Following this, scintillation fluid (Microscint O, 60 ul, Perkin Elmer, USA) was added to each well. The plates were stabilized by leaving them overnight and counted on plate counter (TOPCOUNT NXT, Perkin Elmer, USA) for tritium. Percent inhibition of receptor binding was calculated in presence and absence of extract by the following formulae, 
         [0000]    1 
         [0000]    
       
         
           
             
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                     extract 
                   
                 
                 
                   Binding 
                    
                   
                       
                   
                    
                   in 
                    
                   
                       
                   
                    
                   absence 
                    
                   
                       
                   
                    
                   of 
                    
                   
                       
                   
                    
                   leaves 
                    
                   
                       
                   
                    
                   extract 
                 
               
               × 
               100 
             
           
         
       
     
       Material and Method for In Vivo Evaluation of the Extract: 
     Materials: 
       [0077]    1. Animals: Swiss Albino male mice 20-25 gm body weights were procured from Laboratory Animal Services Division of Central Drug Research Institute, Lucknow. All animals were kept in polyacrylic cage in environmentally controlled rooms (temperature 24-27° C. and humidity 60-65% with 12:12 light:dark cycle). Food was provided in the form of dry pellets and water ad libitum. Each animal was used only once in the behavioral tests and were habituated with the experimental room one day prior to the experiment All experiments involving animals complies with the ethical standards of animal handling and approved by Institutional Animal Ethics Committee. 
         [0078]    2. Drugs: Diazepam,[Ranbaxy, India] as a positive control. 
       Methods: 
       [0079]    Treatment of animals: Diazepam was diluted in distilled water, administered by intraperitoneally. The extract was dissolved in 0.5% gum acacia suspension and administered by oral route. 
         [0080]    Elevated plus maze test in mice: This test was used to evaluate the anti-anxiety activity. The test is based on the principal of conflict between exploration and fear of open/or closed arms. Apparatus consists of a raised stainless steel maze of four arms arranged in ‘+’ sign. Two of opposite arms are enclosed by raised walls whereas other arms are kept open. All the four arms consist of infrared beams at regular distance. The movement of animal across the arms is calculated by interruption of beams, which was analyzed by Maze Tracking Software (M/s. Columbus Instruments, USA). The trial was started by placing an animal on the central platform of the maze facing an open arm. Animals were given a period of 2 min to acclimatize with its surroundings. The time spent in each of the two types of arm was recorded during the next 5 min test period. The percentage open arm time were used as index of anxiety. The apparatus was cleaned thoroughly between trials with damp and dry towels. 
         [0081]    Diazepam (1.5 mg/kg) and the  Cassia  Lora leaves extract (100 mg/kg) was orally administered one hour prior to the experiment. 
       Locomotor Activity Monitor (for Positive Symptoms): 
       [0082]    Gross open field activity is studied using Digiscan Infrared Photocell system [Test Box model: RXYZCM (16 TAO)]; Omnitech Electronics, Columbus, Ohio] in 42×42×30 cm Plexiglass arenas, fitted into infrared beam containing metallic grid. Activity of animals will be observed by the interruption of infrared beams. All cages are connected with a counting module, which counts the number of interruptions. Prior to the experiment, animals both treated and the controls, are habituated in the Test Box for 15 minutes. After the initial habituation process, the activity of the treated and control animals is studied for duration of 2 hours (which can vary depending on experimental requirements). Gross locomotor activity of animals is studied in terms of: horizontal activity, total distance traveled (cm), number of movements, movement time (sec), rest time (sec), vertical activity, number of vertical movements, vertical time (sec), stereotypy counts, number of stereotypy, stereotypy time (sec), clockwise revolutions, anti-clockwise revolutions, margin time (sec), centre time (sec), time spent in corners(sec)—Left-Front, Right-Front, Left-Rear, Right-Rear. Data will be automatically generated through the associated software. Data is presented as Means±SEM. Parametric data is analyzed by Student&#39;s T test or analysis of variance (ANOVA). 
         [0083]    Rota rod test in mice: Rota rod test is commonly used for evaluation of neurotoxicity or neurological deficit in mice treated with various plant extracts used in the study. The protocol as described by Dunham and Miya is based on the assumption that an animal with normal motor efficiency (and not reduced muscular tone) is able to maintain its equilibrium on a rotating rod. Basically the Rota rod consists of a rod which is coated to with rubber or polypropylene foam to provide friction and to prevent animals from slipping off the rod. The distance between the rod and floor is kept 15 cm to avoid intentional jumping of mice. The rod is driven by a motor and the rotational speed can be regulated which is maintained at 80 rpm in our study. Animals were trained on the Rota rod for duration of 2 minutes per trial, with 4 trials per day for two days. On the third day, mice were tested before and one hour after the treatment of extract. 
         [0084]    The following examples are given by way of illustration and should not be construed to limit the scope of the invention. 
       Example-1 
       [0085]    The plant material was collected from Bhavnagar city area of Bhavnagar district of Gujarat, located at 12° 75′ N Latitude &amp; 72° 15′ E Longitude at altitude of 00 m sea level. It was further processed to separate necessary part (leaves) and it was cleaned to remove extraneous matter. The cleaned leaves were air dried at 28° C. and powdered in mini grinding mill to obtain powder form of the mesh size of 16μ. The powdered plant material was then further processed for crude extract preparation with solvent system i.e., methanol-water (95:05) at 28° C. The extract was concentrated by conventional techniques using Rotary Evaporator and removed the solvent to the maximum extent. The concentrated extract was freeze dried at the temperature range of −60° C. for a period of 16 hours to obtain the crude dried extract. The crude extract was tested for in vitro anti-anxiety activity. The activity results are as given below (Table: 1): 
         [0000]    
       
         
               
             
               
               
               
             
               
               
               
             
           
               
                 TABLE 1 
               
             
             
               
                   
               
               
                 In vitro radioligand receptor binding effect of extract 
               
               
                 on frontocortical benzodiazepine receptors 
               
             
          
           
               
                   
                 Leaves Extract 
                 % Inhibition in 
               
               
                 Sr. No. 
                 (Concentration in μg) 
                 3H-Flunitrazepam binding 
               
               
                   
               
             
          
           
               
                 1 
                 100 
                 86 
               
               
                 2 
                 50 
                 82 
               
               
                 3 
                 25 
                 73 
               
               
                 4 
                 12.5 
                 80 
               
               
                 5 
                 6.25 
                 69 
               
               
                 6 
                 3.12 
                 69 
               
               
                 7 
                 1.56 
                 62 
               
               
                   
               
             
          
         
       
     
       Example-2 
       [0086]    The in-vitro active extract of Example-1 i.e., the methanol:water::95:05 extract of leaves was tested for in-vivo anti-anxiety activity in mice. Rota rod test is commonly used for evaluation of neurotoxicity or neurological deficit in mice treated with various plant extracts used in the study. 
         [0087]    Results: The results are shown in Table 2 and  FIG. 1 . Both original and repeat extract to (100 mg/kg p.o.) and Diazepam (1.5 mg/kg p.o.) resulted in a significant increase in the percentage of time spent in open arms (P&lt;0.01) in comparison to saline treated control mice. 
         [0000]    
       
         
               
               
               
               
               
             
               
               
               
               
               
             
           
               
                 TABLE 2 
               
               
                   
               
               
                   
                 Dose 
                 Time spent in open 
                 % time 
                   
               
               
                   
                 (mg/kg 
                 arms (secs) out of 
                 spent in 
                 Significance 
               
               
                 DRUG 
                 p.o.) 
                 300 secs* 
                 open arms 
                 P value** 
               
               
                   
               
             
             
               
                   
               
             
          
           
               
                 Control 
                 — 
                 18.35 ± 0.79 
                 6.35 
                 — 
               
               
                 Original extract 
                 100 
                 50.57 ± 4.50 
                 16.85 
                 P &lt; 0.01 
               
               
                 Repeat extract 
                 100 
                 56.47 ± 6.97 
                 18.82 
                 P &lt; 0.01 
               
               
                 Diazepam 
                 1.5 
                 70.16 ± 4.09 
                 23.38 
                 P &lt; 0.01 
               
               
                   
               
               
                 *Values are expressed as Mean ± SEM. 
               
               
                 **Statistical analysis is done using One way Anova followed by Dunnett&#39;s Multiple Comparison Test 
               
             
          
         
       
     
       ADVANTAGES OF THE INVENTION 
       [0000]    
       
         
           
             1. Plant material retains the activity when stored under ambient condition. 
             2. The extract prepared from the leaves has high shelf life without loss of activity.