In-Vitro Pharmacological Profile f Partially Purified Leaves of Alseodaphne Perakensis
Alseodaphne perakensis (AP) is a moderately sized tree that is widely distributed throughout Peninsular Malaysia. There are no reports of this tree in traditional folk medicine although tests have shown its leaves are rich in alkaloids. Initial experimental work carried out on this species led to...
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| Format: | Thesis |
| Language: | English |
| Published: |
2005
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| Online Access: | http://psasir.upm.edu.my/id/eprint/6334/1/FPSK%28M%29_2005_11.pdf http://psasir.upm.edu.my/id/eprint/6334/ |
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| Summary: | Alseodaphne perakensis (AP) is a moderately sized tree that is widely distributed
throughout Peninsular Malaysia. There are no reports of this tree in traditional folk
medicine although tests have shown its leaves are rich in alkaloids. Initial
experimental work carried out on this species led to the isolation of a major
compound N-methy1-2,3,6-trimethoxymorphinandien-7-onea,n alkaloid with a
morphinandienone skeleton which is similar in structure with Omethylflavinanthine;
and a minor
trimethoxymorphinandien-7-one-N-oxide. Another compound 7-hydroxy-2,3,6-
trimethoxy phenantherenel has also been isolated. All these three compounds
isolated from AP have no reported biological activity. However, the alkaloid Omethylflavinanthine
has been previously isolated from other plants and its analgesic
properties has been reported by other researchers.
polar alkaloid N-methyl-2,3,6-
In this study, the crude methanol extract (CMLE) and semi-pure alkaloids were
extracted by steeping the air-dried leaves of AP in methanol for 48hrs. The solvent
methanol containing CMLE were evaporated using the rotary evaporator at 45OC
leaving a blackish viscous CMLE. The alkaloid in CMLE were extracted using the
sulphuric acid, sodium carbonate, and methylene chloride (DCM) to obtain DCM
'A' and DCM 'B' and de-alkaloid fractions (residue after alkaloid extraction).
Alkaloid test (Meyer's reagent) done on these extracts CMLE and DCM 'A' and
DCM 'B' fractions confirmed the presences of alkaloid;' the residue after alkaloid
extraction tested negative for alkaloid.
These extracts CMLE, DCM 'A' and DCM 'B' from the leaves of AP were tested
on stimulated and unstimulated guinea pig ileum (GPI), rat vas deferentia (RVD)
and mouse vas deferentia (MVD) preparations.
The CMLE (100 p1,O. 1 g/ml) inhibited the electrically induced twitches on the GPI
preparation. On its own, CMLE has no effect on the unstimulated GPI.
Contractions induced by histamine and acetylcholine on the unstimulated GPI
preparation were antagonised in a non-competitive manner by CMLE (100 p1 0.1
g/ml). DCM 'A' (100 pl0.1 glml) was also found to inhibit the electrically induced
twitches on the GPI preparation. On its own, DCM 'A' had no effect on the
unstimulated GPI. DCM 'A' also antagonised the contraction induced by histamine
and acetylcholine on the unstimulated GPI in a non-competitive manner.
The CMLE (1 00 p1 0.1 g/ml) inhibited the electrically induced twitches on the RVD
preparation. On its own, CMLE had no effect on the unstimulated RVD.
Contractions induced by phenylepherine on the unstimulated RVD preparation was
antagonised in a competitive manner by CMLE (100 p1 0.1 glml). Like CMLE,
DCM 'A' (100 yl 0.1 glml) inhibited the electrically induced twitches on the RVD
preparation. On its own, DCM 'A' had no effect on the unstimulated RVD. DCM
'A' also antagonized contractions induced by phenylepherine on the unstimulated
RVD. Like phenylepherine antagonist phentolamine, both CMLE and DCM 'A'
competitively inhibited contraction induced by phenylepherine on RVD.
CMLE and DCM'A' inhibited the electrically induced twitch on the stimulated
MVD; they did not have any effect on the unstimulated MVD. The inhibition by
CMLE and DCM'A' fraction on the stimulated MVD was reversed by naloxone.
DCM 'B' fraction did not have any effect on the stimulated GPI, RVD and MVD
preparation. It also did not have any effect on the unstimulated RVD and MVD,
however, DCM 'B' fraction induced contractions in a dose dependent manner on the
unstimulated GPI. These contractions were antagonised competitively by
mepyramine. The dealkaloid (dAK) fractions did not show any physiological
effect on the stimulated and unstimulated GPI, stimulated and unstimulated RVD
and stimulated and unstimulated MVD.
CMLE and DCM 'A' fractions from the leaves of AP seem to possess;
antihistaminergic, antimuscarinic, antiadrenergic, morphine-like activity. DCM 'B'
fraction exhibited histaminergic activity. |
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