Gastrointestinal drugs

Gastrointestinal drugs Department of pharmacology Liming zhou 2010,spring

classification • Drugs for treatment of peptic ulcers • Drugs for adjusting the function of digestion • Drugs promoting gastrointestinal motility • Antiemetic drugs • laxatives

Drugs for peptic ulcers Classification of peptic ulcer: • Duodenal (DU) Gastric (GU) • Role of pepsin in peptic ulcer disease: • Secreted gastric acid plus effects of pepsin promote tissue injury

Peptic ulcer disease: an imbalance between aggressive factors (gastric acid pepsin bacteria) and protective factors (gastric mucus, bicarbonate, prostaglandins) • Regulation of gastric acid secretion-- many factors (chemical, neural, hormonal)

Stimulation: • Gastrin-most potent stimulant • Activation of postganglionic vagal fibers

Drugs for peptic ulcers-----antacidsAction • Neutralize secreted acid • Reduce gastric acidity Pepsin inactive Reduce destroy factors

Drugs for peptic ulcers-----antacids • A magnesium hydroxide(氢氧化镁) • B magnesium trislilicate（三硅酸镁） • C aluminum hydrocide（氢氧化铝） • D Calcium carbonate（碳酸钙） • F Sodium bicarbonate（碳酸氢钠）

1 NaHCO3+HCl NaCl+H2O+CO2 • 2 Al（OH）3 aluminium hydroxide • Al（OH）3+3HCl AlCl3 +3H2O • 3 Mg（OH）2 magnesium hydroxide • Mg（OH）2+2HCl MgCl2 +2H2 O • 4 Mg2Si3O8 magnesium trisilicate • Mg2Si3O8+4HCl 2MgCl2+3SiO2+2H2O • 5 CaCO3 calcium carbonate • CaCO3+2HCl CaCl2+H2O+CO2

Gastric antisecretory drugs • antagonisit of H2 receptor ↓ • decrease the H+ secretion • Basal gastric acid food-stimulated gastric acid

H2 Receptor Antagonists • A cimetidine (西米替丁) + • B ranitidine （雷米替丁）++ • C famotidine（法莫替丁）+++ • Effective inhibitor of stimulated and non-stimulated gastric acid secretion • Healing rates: similar between antacids and H2 receptor antagonists

Effective inhibitor of stimulated and non-stimulated gastric acid secretion • Healing rates: similar between antacids and H2 receptor antagonists

Mucosal protective agents • Prostaglandins • reduction in basal and stimulated gastric acid secretion; • enhanced mucosa resistance to injury (PGE1/PGE2).

Mucosal protective agents • Bismuth compounds • Mechanism of Action • cytoprotective effects • compounds bind to the ulcer base, stimulating mucus and prostaglandin production • antibacterial effect • inhibition of proteolytic, lipolytic, and urease activities • Coating and protecting the ulcer crater

Clinical use of Bismuth compounds • In monotherapy: • ------- eradicate H. pylori in about 20% of patients • combination with antibiotics • -------eradicate H. pylori in up to 95% of patients.

Sucralfate • binds to ulcer bed (granulation tissue, not to gastric or duodenal mucosa) • decreases proton diffusion to the ulcer base • may increase endogenous tissue prostaglandins and may bind epidermal growth factors and other growth factors-- improving mucosal defense

antimicrobials • activity against H.pylori • clarithromycin, amoxicillin, tetracycline

Drugs for adjusting the function of digestion • drugs of aid digestive • A pepsin • B pancreatin • C lactasin

antiemetic drugs and drugs promoting gastrointestinal motility • antiemetic drugs: • H-1 receptor blocker : diphenhydramine • Chloropromazine • M-receptor blocker : scopolamine

drugs promoting gastrointestinal motility • Metoclopramide (甲氧氯普胺)： • domperidone （多潘立酮）blocking D2-receptor • Cisapride(西沙比利）

Metoclopramide (甲氧氯普胺) • Blocking the DA2 receptor in CTZ • Blocking the DA2 receptor in Gastrointestinal

domperidone （多潘立酮） • blocking DA2-receptor in Gastrointestinal

Cisapride(西沙比利） • Increase release of the Ach

antidiarrheal drugs • opium preparation • Laxative Drugs magnesium sulfate sodium sulfate

Gastrointestinal drugs