26 NS-EA 51 successfully prevented the histaminic effects on gastric juice volume, pH, acid-output, ulcer formation and pepsin activity in the PL rats (Table 1). Additionally, it inhibited gastric ulcer formation induced by hypothermic-restrained stress (Table 2). However, the fraction did not alter significantly gastric mucus secretions in the rats having either histamine plus PL or hypothermic and restraint stress-induced gastric ulcers (Table 1 and Table 2). Famotidine, a reference drug also caused similar anti-ulcer effects in the experimental animals. But
data pointed out clearly, NS-EA 51 to be the stronger anti-ulcer agent in comparison to the Famotidine (Table 1 and Table 2). The above presented data, has suggested that the purified fraction under experiment lacks any cytoprotective activity and its anti-ulcer DAPT molecular weight effects might be caused by the inhibition of gastric aggressive factors i.e. acid and pepsin which is also in accordant to our previous report. 9 Famotidine, a well-established check details H2-receptor antagonist showed anti-ulcer effects in both histaminic plus PL
and hypothermic-restrained stress models due to the inhibition of gastric histaminic receptors. Therefore, it may be speculated that the fraction may interfere with the histaminic pathway like Famotidine. It is conceivable; therefore, that the mechanism of anti-ulcerogenic action of NS-EA 51, i.e. attenuation of the effects of histamine on gastric juice volume, pH, acid out-put, ulcer index and pepsin activity as well as inhibition of the effect of hypothermic-restraint stress on ulcer index in addition
to the lipid peroxidation prevention, 9 could possibly be related to its interference with the histaminic pathway. In conclusion, the reported results have validated the anti-ulcer activity of the NS-EA 51 fraction isolated from NS. Further pharmacological investigations are still required to elucidate the precise mode(s) of anti-ulcer actions. All authors have none to declare. The authors would like to thank the Islamia University of Bahawalpur-PAKISTAN for provision of research facilities. “
“A homoisoflavanone, (3R)-5,7-dimethoxy-(4′-hydroxybenzyl)-4-chromanone Adenylyl cyclase of the compound (R)-5, was previously isolated from Scilla nervosa (Burch.) Jessop 1 as well as from Drimiopsis burkei Bak. 2 The traditional use of S. nervosa for rheumatic fever indicates possible anti-inflammatory properties of its constituents. 3 Subsequent studies showed strong inhibition of prostaglandin synthesis in microsomal cells by the isolated homoisoflavanone, supporting the traditional use of S. nervosa. 4 Studies indicate that stereoselectivity plays an important role in the anti-inflammatory activities of non-steroidal anti-inflammatory drugs. 5 The decision to employ either a racemate or a pure enantiomer for therapeutic purposes is usually based on the diverse mechanisms of actions of the enantiomers.