SOME PROPERTIES OF VARIOUS FRACTIONS OF THE SEEDS OF ARISTOLOCHIA BRACTEATA

Document Type : Research article

Authors

1 Sudan University of Science and Technology, College of Veterinary Medicine and Animal Production.

2 Sudan University of Science and Technology, College of Veterinary Medicine and Animal Production

Abstract

Paper chromatography of different fractions of the seeds of A. bracteata was carried out. The Rf values were recorded and the spots were exposed to U.V. light. The alcohol extract gave five spots. Four yellow spots were seen in U.V. light, and one spot fluorescing blue in the same U.V. light. This result indicated the presence of alkaloid. Evaporation of the ether gave a yellow acidic residue which was found to contain two non-alkaloidal compounds. Three alkaloids were detected in the quaternary alkaloid chloride.

Keywords


Assiut Vet. Med. J. Vol. 52 No. 109 April 2006

Sudan University of Science and Technology, College of Veterinary Medicine and Animal Production.

SOME PROPERTIES OF VARIOUS FRACTIONS OF THE SEEDS OF ARISTOLOCHIA BRACTEATA

(With One Table)

By S.E.M. BARAKAT and I.M.T. FADLALLA

(Received at 2/3/2006)

خواص الأجزاء المختلفة لبذور نبات عرق العقرب

بعض

سيف الدولة مصطفى برکات،عماد محمد طاهر فضل الله في هذه الدراسة تم اجراء کروماتوقرافيا الورق للأجزاء المختلفة لبذور نبات أم جلاجل

النقاط للأشعة فوق البنفسجية.

عرق العقرب) وتم تسجيل قيم معامل العرقلة وتعريض أعطى المستخلص الکحولي خمسة نقاط أربعة منها صفراء اللون تمت معاينتها بالأشعة فوق البنفسجية اضافة إلى منطقة واحدة ذات أشعاع أزرق هذه النتيجة أشارت إلى وجود قلويد. تبخر الايثر اعطى راسب حمضي أصفر اللون ثبت احتواءه على مرکبين غير قلويديين. تم

عن ثلاثة قلويدات في کلوريد القلويد الرباعي

الکشف

SUMMARY

Paper chromatography of different fractions of the seeds of A. bracteata was carried out. The Rf values were recorded and the spots were exposed to U.V. light. The alcohol extract gave five spots. Four yellow spots were seen in U.V. light, and one spot fluorescing blue in the same U.V. light. This result indicated the presence of alkaloid. Evaporation of the ether gave a yellow acidic residue which was found to contain two non-alkaloidal compounds. Three alkaloids were detected in the quaternary alkaloid chloride.

Key words: Paper chromatography, aristolochia bracteata, alkaloids.

Rf values.

INTRODUCTION

Aristolochia species (Aristolochiaceae) are recorded in a list of plants used in Kenya, Ethiopia, Tanzania and Sudan for the treatment of infestation with nematodes. Worldwide, A. bracteata is used against

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snake bites and scorpion stings (Morton, 1975; Hazlett, 1986; Houghton and Osibogun, 1993; Coe and Anderson, (1996).

Aristolochia trilobata is used for stomach pain and its leaf tinctures are used for the treatment of diarrhoea (Giron et al, 1991). It has been shown that aristolochic acid inhibits inflammation induced by immune complexes and non-immunological agents Moreno, 1993). Moreover, aristolochic acid inhibits the activity of snake venom phospholipase (PLA) by forming 1:1 complex (Lans, 2001).

In the Sudan, Aristolochia bracterata, locally known as Um Galagel or Erg Elagrab, is widely distributed in central, eastern and western areas and is used as antidote to scorpion bites and as an anthelmintic (Brown and Massey, 1929).

Chemical constitution of toxic substances in plants is important. Alkaloids produce varying degrees of physiological reactions when introduced into animals (Schacental, 1963, 1970, Bull et al., 1968). There is, as yet, little information available regarding the toxic properties of poisonous plants in the Sudan.

In our previous repot, (Barakat, et al., 1983) we have shown the toxicity of A. bracteata in Nubian goats. In addition the combined toxicity of A. bracteata and Rotundifolia to Nubian goats was investigated (Eldirdiri, et al., 1987).

Plants of the genus Aristolochus such as A. clematis and A. densivenia contain an alkaloid, aristolochine and probably other substances (Watt and Breyer-Brandwijk, 1962; Clarke and Clarke, 1967). It has been found that A. bracteata contains Aristolochic acid, fixed oils and an orange yellow compound (Watt and Breyer-Brand wijk, 1962).

Aristolochia Bracteata is used in traditional medicines as a gastric stimulant and in the treatment of cancer, lung inflammation, dysentery and snake bites (Lans, et al., 2001).

Antibacterial activity of dried extracts of roots of A. bracteata was evaluated against a few gram-positive and gram-negative bacteria. All the erude extracts showed a broad spectrum of antibacterial activity (Negi et al., 2003).

El Tahir et al., (1999) investigated the antiplasmodial activity of extracts from Gardenia lutea, cassia tora, Acacia nilotica and Aristolochia bracteolate.

The ethanol extract of the shade-dried leaves of Aristolochia bracteolate was studied for its effect on wound healing in rats. The plant showed a definite positive effect on wound healing, with a significant

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increase of the level of two powerful antioxidant enzymes (Shirwaikar, et al., 2003).

The Sudanese species A. bracteata is of considerable interest. There are no reports on the chemical constituents of this species. The purpose of the present preliminary investigation was to throw light on some properties of the different fractions of the fully-ripe seeds of A. bracteata.

MATERIALS and METHODS Preparation of Various Extracts of Aristolochia Seeds:

A sample of 500g of Aristolochia seeds was dried in the sun, finely ground in a mortar, defatted with petroleum ether and extracted with 95 percent alcohol. The extractives were then fractionated. The petroleum ether was evaporated in vacuum to give a residue (Fraction I). The defatted seeds were then extracted with 95% alcohol. The alcohol extract was concentrated to a thick syrup which was poured slowly with continuous stirring into warm diluted HCI at pH2. The mixture was refrigerated overnight and the supernatant was decanted. The decantate was concentrated, rendered alkaline with ammonia and extracted with ether. The ethereal extract was evaporated to give a residue (Fraction II).

The remaining aqueous alkaline solution was extracted with methylene chloride and evaporated to give a residue (Fraction III). The aqueous alkaline solution was then acidified (PH2) and treated with a freshly prepared saturated aqueous solution of ammonia reineckate. The reineckates were converted to chloride by means of HC1. Paper chromatography:

Paper chromatography of the different fractions of the seeds of A. bracteata was carried out using the solvent system B.A.W. (butanol, ammonia and water, 50-8-1) and B.Ac. W. (butanol, acetic acid and water, 5-1-4). The Rf values were recorded and the spots were exposed to ultra-violet light. Preparation of Dragendorff's reagent:

Preparation of Dragendorff's reagent is the most commonly used reagent for alkaloids which appear as orange spots on the lighter to orange to yellow background. The limit of detectability with Dragendorff's reagent lies usually between 3 and 10 ug>Dragendorff's reagent was prepared as follows: Solution A: Bismuth subnitrate (850g), H20 (40 ml) and AcOH (10ml). Solution B: KI (8g), H20 (20 ml).

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Stock solution: Solution A and B were mixed and strored in a dark bottle. Spry solution: stock (10 ml), ACOH (20 ml) and H20 (100 ml), stable for several weeks.

RESULTS Properties of Fractions of Aristolochia Seeds:

Paper chromatographic results of the alcohol extract and fractions using the solvent system (B.AC.W) and (B.A.W) are given in Table (1).

The alcohol extract gave sports. Two yellow sports were seen in both the ordinary and long wave ultra-violet (U.V.) light, two spots fluorescing yellow and one spot fluorescing blue in the same U.V. light. The blue fluorescing spot was stained heavily orange following spraying with Dragendorff's reagent.

This result indicated the presence of an alkaloid. Evaporation of the ether gave a yellow acidic residue which was found, by paper chromatography, to contain two non-alkaloidal compounds. Three alkaloids (A, B and C) were detected in the quaternary alkaloid chloride. Due to the small amount of the material used, detection of the alkaloid was achieved by streaking a methanolic solution of this fraction on Whattman filter paper No. 17 which was then chromatographed and separated zones were obtained: A/Blue fluorescing zone stained with Dragendorff's reagent. B/ Yellow zone stained with Drragendorff's spray reagent. C/ Yellow zone stained with Dragendorff s reagent.

The results indicated the presence of three alkaloids in the quaternary alkaloid fraction. Evaporation of petroleum ether resulted in a greenish brown oily residue and was found to contain no alkaloids. Table 1: Paper Chromatography of Fractions of Aristolochia seeds:

Fraction

No. of Colour in Fluorescence

Rf value | sports ordinary light in U.V. light | B. Ac. W. B.A.W. Alcohol

Blue

0.03 Yellow

Yellow

0.91

0.08 Yellow

0.50

0.21 Yellow

Yellow

0.53 10.39 Yellow

0.78

| 0.54 Ether

Yellow

Yellow

0.91 Yellow

0.78

0.54 Methylene chloride

Blue

0.71

0.03 Quaternary

Blue

| 0.71 10.03 Yellow

Yellow

0.53

0.21 _ D Yellow

Yellow

0.50

0.39

15

0.71

10.08

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DISCUSSION

It has been suggested that the roots of A. bracteata contain Aristolochic acid and aristolochine and probably other compounds (Watt and Breyer-Brandwijk, 1962).

Paper chromatography procedure for the deternination of alkaloids in the aqueous extract of the seeds of A. bracteata has been developed. Neither the petroleum ether nor the ether extract contained alkaloids. However, The latter contained two non-alkaloidal compound. It is evident that the three alkaloids designated A, B and C were found in the quaternary alkaloid fraction of the seeds of Sudanese species of S. bracteata.

It has been shown that plants of the genus Aristolochia contain different toxic extracts. Lee et al. (2002) reported that the major component in Aristolochia fangchi was Aristolochic acid I, and the level ranged from 437 to 668 ppm. Aristolochic acid II was the major component of Aristolochia contorta and its range was <115ppm.

Rastrelli et al. (1997) found that five new protopine type alkaloids, and a novel 8-benzylberberine-type alkaloid, were isolated

Three new compounds, Aristolochic acid 111a-6-0-beta-D glucosidal, cepharanone-A N-beta-D-glucoside and 2-hydrozy-8 methyloxy cepharanone-A were isolated togther with eight known compounds from methanolic extracts of fresh roots of Aristolochia cinnabarina (Li et al., 1994).

The aqueous extract of the seeds of the plant has toxic effects in laboratory animals. Barakat, and Fadalla, 11h Sci. Cong. 2004, Fac. Vet. Med. Assiut. Univ., Egypt.

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London. Bull, L.B.; Culvenor, C.C.J. and Dick, A.T. (1968): The pyrrolizidine

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Assiut Vet. Med. J. Vol. 52 No. 109 April 2006

Clarke, E.G. and Clarke, M.L. (1967): Carnerss Veterinary Toxicology,

3rd ed., Bailliere Tindall and Cassell itd., London. Coe, F.G. and Anderson, G.J. (1996): Screening of medicinal plants

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Toxicity of Aristolochia bracteata and Cababa rotundifolia to

goats. Vet. Hum. Toxicol. 29 (2). El-Tahir, A.; Satti, G.M. and Khalid, S.A. (1999): Antiplasmodial

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botanical survey of the medicinal flora used by the Caribs of

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339-352. Houghton, P.J. and Obsibogun, I.M. (1993): Flowering plants used

against snakebites. Review article. J. Ethno-Pharmacology, 39:

1-29. Lans, C.; Harper, T.; Georges, K. and Bridgewaler, E. (2001):

Meddicinal and elhnoveterinary remedies of hunters in Trinidad. BMC complementary and Alternative Medicine, 1

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169-174. Levi, M.; Guchelaor, H.J.; Woerdenbag, H.J. and Zhu, Y.P. (1998):

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report - pharm. World Sci. 20 (1): 43-44. Li, H.; Sakagami, Y.; Marumo, S. and Chen, X. (1994): Eleven

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Phytochemistry. 37-239. Liu, M.C.; Marumo, S.; Mizuno, M.; Morita, Y.; Hanaki, S.; Yuzama, Y.

and Matsuo, S. (2004): The nephrotoxicily of Alristolohia manshuriensis in oats is attributable to its aristolochia acids. Chin. Exp. Nephrol. 7(3): 186-194.

404

Assiut Vet. Med. J. Vol. 52 No. 109 April 2006

Moreno, J.J. (1993): Effect of Aristolochic acid on arachidonic acid

cascade and in vivo models of inflammation.

Immunopharmacology, 26: 1-9. Morton, J.F. (1975): Current folk remedies of northern Venezuela.

Quarterly J. of Crude Drug Research, 13: 97-121. Negi, P.S.; Anandharamakeishnan, C. and Jayaprakasha, G.K. (2003):

Antibuitriel activity of Aristolochia bracteata root extracte, J.

Med. Food, 6(4): 401-403. Nortier, J.L. and Vanherweghem, J.L. (2002): Renal interstitial fibrosis

and urothelial carcinoma associalied with the use of Chinese

herb (Aristolochia fangchin). Toxicology. 181-182: 577-580. Radeleff, R.D. (1964); Veterinary Toxicology, Lea and Febiger

Philadelphia. Rastrelli, L.; Lapasso, A.; Pizza, C.; De Tommasi, N. and Sorrentino, L.

(1997): New protopine and benzyltrahydroprotaberine alkalaids from Aristolochia contrieta and their activity on

isoeted guinea - pigileum. J. Nat. Prod., 60 (11): 1065-1069. Schoental, R. (1963): Liver disease and natural hepatotoxins. Bulletin of

WHO, 29: 823-833. Schoental, R. (1970): Hepatotoxic activity of retrosine, senkirkine, and

hydroxy-senkirkine in new-born rats and the role of epoxides in carcinogenesis by pyrrolizidine alkaloids and aflatoxins.

Nature, London, 227:401-402. Shi, L.S.; Kuo, P.C., Tsai, Y.L., Damu, A. G. and Wu, T.S. (2004): The

alkalads and other coristitutents from the roots and stem of

Aristolochia elegans. Bioorg. Med. Chem., 12 (2): 439-446. Shirwaikar, A.; Somashekar, A.P.; Udupa, A.L., Udupa, S.L. and

Somashar, S. (2003): Wound healing studies of Aristotchia bracteolate Lam. With supportine action of antioxidant

enzymes phylimedicine, 10(6-7): 558-562. Watt, J.M. and Breyer. Brandwijk, N.G. (1962): Medicinal and

poisonons plants of Southern and Eastern Africa, 2nd ed. Livingstone, Edinburgh.

405

Arlt, V.M.; Ptohl-Lezkowicz, A.; Cosyns, J. and Schmeiser, H.H. (2001):
Mutal-Res. 494 (1-2): 143-150. Barakat, S.E.M.; Wasfi, I.A. and Adam, S.E.I. (1983): The toxicity of
Aristolochia bracteata in goats. Vet. Pathol. 20: 611-616. Brown, A.E. and Massey, R.E. (1929): Flora of the Sudan, Unrby,
London. Bull, L.B.; Culvenor, C.C.J. and Dick, A.T. (1968): The pyrrolizidine
alkaloids: Their chemistry, pathogenecity and other Biological properties, North-Tholl and Pubishing co-Amessterdam.
403
Assiut Vet. Med. J. Vol. 52 No. 109 April 2006
Clarke, E.G. and Clarke, M.L. (1967): Carnerss Veterinary Toxicology,
3rd ed., Bailliere Tindall and Cassell itd., London. Coe, F.G. and Anderson, G.J. (1996): Screening of medicinal plants
used by the Garifuna of Eastern Nicaragua for bioactive
compounds. J. Ethno-pharmacology, 53: 29-50. Eldirdiri, N.I.; Barakat, S.E.M. and Adam, S.E.1. (1987): The Combined
Toxicity of Aristolochia bracteata and Cababa rotundifolia to
goats. Vet. Hum. Toxicol. 29 (2). El-Tahir, A.; Satti, G.M. and Khalid, S.A. (1999): Antiplasmodial
activity of selected Sudanese medicinal plants with emphasis
on Acacia nilotica. Phytothther. Res., 13(6): 474-478. Giron, L.M.; Freire, V.; Alonzo, A. and Caceres, A. (1991): Ethno
botanical survey of the medicinal flora used by the Caribs of
Guatemala. J. Ethno-pharmacology, 34: 173-187. Hazlett, D. (1986): Ethno-botanical observations from Cabecar and
Guaymi settlements in Central America. Economic Botany, 40:
339-352. Houghton, P.J. and Obsibogun, I.M. (1993): Flowering plants used
against snakebites. Review article. J. Ethno-Pharmacology, 39:
1-29. Lans, C.; Harper, T.; Georges, K. and Bridgewaler, E. (2001):
Meddicinal and elhnoveterinary remedies of hunters in Trinidad. BMC complementary and Alternative Medicine, 1
(1): 10. Lee, T.Y., Wu, M.L.; Deng, J.F. and Hwang, D.F. (2002): High.
Performance liguid chromatographic determination for aristolochic acid medicinal plants and slimming products. J. chromatogr. B. Hnalyt. Technol. Biomed. Life Sci., 766 (1):
169-174. Levi, M.; Guchelaor, H.J.; Woerdenbag, H.J. and Zhu, Y.P. (1998):
Acute hepatitis in a patieut using a Chinese herbal tea - a case
report - pharm. World Sci. 20 (1): 43-44. Li, H.; Sakagami, Y.; Marumo, S. and Chen, X. (1994): Eleven
aristolochic acid derivatives from Aristolochia cinnabarina.
Phytochemistry. 37-239. Liu, M.C.; Marumo, S.; Mizuno, M.; Morita, Y.; Hanaki, S.; Yuzama, Y.
and Matsuo, S. (2004): The nephrotoxicily of Alristolohia manshuriensis in oats is attributable to its aristolochia acids. Chin. Exp. Nephrol. 7(3): 186-194.
404
Assiut Vet. Med. J. Vol. 52 No. 109 April 2006
Moreno, J.J. (1993): Effect of Aristolochic acid on arachidonic acid
cascade and in vivo models of inflammation.
Immunopharmacology, 26: 1-9. Morton, J.F. (1975): Current folk remedies of northern Venezuela.
Quarterly J. of Crude Drug Research, 13: 97-121. Negi, P.S.; Anandharamakeishnan, C. and Jayaprakasha, G.K. (2003):
Antibuitriel activity of Aristolochia bracteata root extracte, J.
Med. Food, 6(4): 401-403. Nortier, J.L. and Vanherweghem, J.L. (2002): Renal interstitial fibrosis
and urothelial carcinoma associalied with the use of Chinese
herb (Aristolochia fangchin). Toxicology. 181-182: 577-580. Radeleff, R.D. (1964); Veterinary Toxicology, Lea and Febiger
Philadelphia. Rastrelli, L.; Lapasso, A.; Pizza, C.; De Tommasi, N. and Sorrentino, L.
(1997): New protopine and benzyltrahydroprotaberine alkalaids from Aristolochia contrieta and their activity on
isoeted guinea - pigileum. J. Nat. Prod., 60 (11): 1065-1069. Schoental, R. (1963): Liver disease and natural hepatotoxins. Bulletin of
WHO, 29: 823-833. Schoental, R. (1970): Hepatotoxic activity of retrosine, senkirkine, and
hydroxy-senkirkine in new-born rats and the role of epoxides in carcinogenesis by pyrrolizidine alkaloids and aflatoxins.
Nature, London, 227:401-402. Shi, L.S.; Kuo, P.C., Tsai, Y.L., Damu, A. G. and Wu, T.S. (2004): The
alkalads and other coristitutents from the roots and stem of
Aristolochia elegans. Bioorg. Med. Chem., 12 (2): 439-446. Shirwaikar, A.; Somashekar, A.P.; Udupa, A.L., Udupa, S.L. and
Somashar, S. (2003): Wound healing studies of Aristotchia bracteolate Lam. With supportine action of antioxidant
enzymes phylimedicine, 10(6-7): 558-562. Watt, J.M. and Breyer. Brandwijk, N.G. (1962): Medicinal and
poisonons plants of Southern and Eastern Africa, 2nd ed. Livingstone, Edinburgh.
405