PHYTOCHEMICAL SCREENING AND ANTIMYCOBACTERIAL POTENTIALS OF Syzygium guineense WILD DC. AND Mimosa pigra LINN
Date
2014-09
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Abstract
The prevalence of multi-drug resistant tuberculosis is an increasing health challenge.
Attention has therefore been shifted to the use of ethno-medicines in combating this
disease. Traditionally, Syzygium guineense (stem-bark) and Mimosa pigra (aerial parts) are
used in the treatment of respiratory tract infections with no scientific justification. This
study was designed to identify the constituents of Syzygium guineense and Mimosa pigra
that may be active against Mycobacterium tuberculosis.
The S. guineense (stem-bark) and M. pigra (aerial parts) were obtained from farmlands in
Abuja and authenticated at the herbarium of National Institute for Pharmaceutical Research
and Development, Abuja. The S. guineense (1.0 kg) was extracted successively with
chloroform and methanol. The extracts were separately fractionated with n-hexane
followed by acetone. Mimosa pigra (0.5 kg) was extracted with methanol and partitioned
with diethylether and n-butanol. The fractions were purified using chromatographic
techniques. The extracts, fractions and isolated compounds were subjected to antimycobacterial
assay with Mycobacterium tuberculosis (ZMC 050 and 303) strains using
the Lowenstein-Jensen and mycobacterium growth indicator tube methods. Streptomycin,
isoniazid, rifampicin, and ethambutol were used as standard drugs and dimethylsulphoxide
as negative control. The structures of the isolated compounds were elucidated using infrared,
ultra-violet/visible, nuclear magnetic resonance and mass spectroscopic techniques.
The chloroform extract of S. guineense yielded 4.1 g n-hexane fraction and 5.2 g acetone
fraction A while the methanol extract gave 5.2 g acetone fraction B and 98.0 g residue.
Crude methanol extract of M. pigra gave 40.1, 4.6 and 12.3 g of diethylether, n-butanol
and residue fractions respectively. Two new triterpenoids were isolated from S. guineense
namely: 12-hydroxy-27-demethylfriedelan-3-one and betulinic acid methylenediol ester, in
addition to the two known triterpenoids: betulinic acid, and friedelan-3-one. One new
flavonoid, 8-hydroxy-3-phenyl-4-benzopyrone rhamnoside was isolated from M. pigra.
The two plants‘ methanol extracts, n-butanol fraction, acetone fraction A, and isolated
compounds: betulinic acid, betulinic acid methylenediol ester and 8-hydroxy-3-phenyl-4-
benzopyrone rhamnoside were active against ZMC 050 strain with Minimum Inhibitory
Concentrations (MIC) of 5.0, 5.0, 2.0, 0.6, 0.6, 0.15 and 0.5 mg/mL respectively. The
ZMC 303 strain also gave similar MIC values as ZMC 050 strain. Spectroscopic analysis
of 12-hydroxy-27-demethylfriedelan-3-one provided evidence for δH signals: 0.8-1.2
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(7CH3), 1.2-1.8 (10CH2), and 2.2-2.4 (5CH), δC signals: 29.9-41.7 (5C), 72.8 (1CHOH)
and 213.4 (1C=O) with a molecular ion of 428 corresponding to C29H48O2. The betulinic
acid methylenediol ester showed δH and δC signals similar to betulinic acid except for the
downfield methylenedioxy carbinol (OCH2O) δC signal at 79.0 and molecular ion of 486
correspond to C31H50O4. Betulinic acid and friedelan-3-one signals are similar to published
spectra. The 8-hydroxy-3-phenyl-4-benzopyrone rhamnoside showed δH signals: 0.9 (3Hd,
J=5.8 Hz), 3.1-3.8 (overlapping glycone multiplet) and 5.2 (anomeric) typical of a
rhamnose moiety, with δH 6.2 (1H), 6.4 (1H), 6.9 (5H) and δC 178.0 (1C=O) of the
flavonoid ring.
The bioactive compounds obtained from Syzygium guineense and Mimosa pigra exhibited
anti-mycobacterial activities. They have potentials for the development of drugs for the
management of tuberculosis. The new triterpenoids and flavonoids are addition to the
library of compounds.
Keywords: Syzygium guineense, Mimosa pigra, Antimycobacterial activity, Triterpenoids
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Description
A Thesis in the Department of Chemistry, Submitted to the Faculty of Science in partial fulfillment of the requirements for the Degree of DOCTOR OF PHILOSOPHY of the UNIVERSITY OF IBADAN
Keywords
Syzygium guineense, Mimosa pigra, Antimycobacterial activity, Triterpenoids