Bacopa and Heart
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    Bacopa Monniera

Bacopa and Heart

No clinical trials have been conducted to test the cardiovascular benefits of Bacopa that have been touted by Ayurvedic medicine for cetnturies. However, in vitro research, agaiun conducted by Dar and Channa, and involving the aorta and pulmonary arteries of rabbits revealed that bacopa extract exerted a vasodilatory effect on calcium chloride-induced contraction in both tissues (Dar A, Channa S. Calcium antagonistic activity of Bacopa monniera on vascular and intestinal smooth muscles of rabbit and guinea-pig. J Ethnopharmacol 1999;66:167-174).

Research Abstracts:

Antioxidant activity of DHC-1, an herbal formulation, in experimentally-induced cardiac and renal damage.

Phytother Res. 2005 Mar;19(3):216-21. 

* Bafna PA, * Balaraman R.

Pharmacy Department, Faculty of Technology and Engineering, The M.S. University of Baroda, Baroda -390

001, Gujarat, India.

DHC-1, an herbal formulation derived from the popular plants Bacopa monniera, Emblica officinalis, Glycyrrhiza glabra, Mangifera indica and Syzygium aromaticum was studied for its antioxidant activity. The protective effect of DHC-1 in isoproterenol-induced myocardial infarction and cisplatin-induced renal damage were studied. A significant reduction in the serum markers of heart and kidney damage and the extent of lipid peroxidation with a concomitant increase in the enzymatic (SOD and CAT) and non-enzymatic antioxidants (reduced glutathione) were observed in DHC-1 pretreated animals compared with the isoproterenol or cisplatin alone treated animals. Thus it can be concluded that DHC-1 possesses a protective effect against both damaged heart and kidneys in rats. This beneficial effect may be attributed, at least in part, to its antioxidant activity. Copyright 2005 John Wiley & Sons, Ltd.

PMID: 15934019 [PubMed - indexed for MEDLINE]

Broncho-vasodilatory activity of fractions and pure constituents isolated from Bacopa monniera.

J Ethnopharmacol. 2003 May;86(1):27-35. 

* Channa S, * Dar A, * Yaqoob M, * Anjum S, * Sultani Z, * Atta-ur-Rahman.

Pharmacology Section, HEJ Research Institute of Chemistry, University of Karachi, 75270, Pakistan. shabnachanna@hotmail.com

The present study demonstrates that various fractions and sub-fractions isolated from Bacopa monniera produced significant inhibition of carbachol-induced bronchoconstriction, hypotension and bradycardia in anaesthetized rats. All these showed more potency towards inhibition of tracheal pressure compared to either blood pressure or heart rate. The sub-sub fraction and compound 1 caused greater inhibition of tracheal pressure and heart rate compared to blood pressure. Thus, overall bioassay-directed fractionation of B. monniera improved the bronchodilatory activity in various fractions and compound 1 (2-219x) in anaesthetized rats. In vitro, the KCl-induced contraction was equally inhibited by crude extract, petroleum ether and methanol fractions on trachea suggesting bronchodilatory activity remained the same in fractions. On pulmonary artery petroleum ether, dichloromethane and methanol fractions produced 2-2.6 times more vasodilatation compared to crude extract of B. monniera. Subsequent sub-fractions failed to show the existence of broncho-vasodilatory activity, however, the CHCl(3)/MeOH sub-fraction significantly reduced the acetylcholine-induced contraction on ileum. Both the methanol fraction and CHCl(3)/MeOH sub-fraction caused marked reduction of barium chloride-, potassium chloride- and calcium chloride-induced contraction on guinea-pig ileum, indicating their interference with Ca(2+) ion movement. Thus, it may be concluded that various fractions derived from B. monniera possess broncho-vasodilatory activity, which is attributed mainly to inhibition of calcium ions.

PMID: 12686438 [PubMed - indexed for MEDLINE]

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