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MD Pharmacology NMC syllabus ~5 min read Recent advances last updated on 2026-07-02

Screening of Antidiarrhoeal Drugs

Validated animal models, diarrhoeogens, endpoints & reference standards for preclinical antidiarrhoeal screening

Introduction & two-limb framework

  • Definition — Antidiarrhoeal screening = the battery of in vivo and in vitro preclinical assays that detect and quantify a compound's ability to normalise experimentally-induced diarrhoea, acting on one or both of the two limbs generating diarrhoea — intestinal hypersecretion (fluid/electrolyte) and hypermotility (accelerated propulsion).
  • Two diarrhoeogen families — the model must match the mechanism probed — secretory inducers (prostaglandins/PGE2 & 16,16-dimethyl-PGE2, castor oil → ricinoleic acid, MgSO4, bile salts, cholera toxin, carbachol) vs motility/propulsion accelerators (sennosides & stimulant laxatives that speed large-intestinal transit).
  • Two-limb readout — a valid assay should discriminate the antisecretory component from the antipropulsive (antimotility) component — a drug can be antipropulsive without being antisecretory (some opioids); the castor-oil rat test was explicitly proposed as an in vivo method able to evaluate both (Niemegeers 1984).
  • Three functional headings (Vogel Part XI) — assays cluster as Intestinal Secretion (laxative activity, enteropooling, Ussing-chamber Cl- secretion), Composite antidiarrhoeal effect (castor-oil, cecectomised-rat, cold-restraint) and Gut motility (isolated ileum, charcoal-meal transit, colon motility).
  • Scope — this is experimental evaluation & screening only — models, apparatus, inducers, endpoints, reference standards; the clinical pharmacotherapy of antidiarrhoeals (drug classes, doses, ADRs) is a separate clinical topic and is deliberately out of scope.
Figure 1 — Two-limb antidiarrhoeal-screening framework
Figure 1 — Two-limb antidiarrhoeal-screening framework
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Screening Antidiarrhoeal Drugs

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