Acute gastritis by Dr. Evelyn Mbugua
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Nov 29, 2011
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About This Presentation
Gastritis is the inflammation of the inner lining of the stomach. Dr Evelyn Mbugua's presentation provides the latest management of Gastritis
Slide Content
GASTRITIS DR. EVELYN MBUGUA
GASTRIC SECRETIONS HCl and Pepsinogen Acid secretion occurs under Basal, and Stimulated conditions.
Basal gastric acid production Basal acid production occurs in a circadian pattern, with highest levels occurring during the night and lowest levels during the morning hours. Cholinergic input via the vagus nerve and histaminergic input from local gastric sources are the principal contributors to basal acid secretion.
Stimulated gastric acid production Stimulated gastric acid secretion occurs primarily in three phases based on the site where the signal originates :- cephalic, gastric, intestinal.
Cephalic phase - Sight, smell, and taste of food stimulates gastric secretion via the vagus nerve. Gastric phase - Activated once food enters the stomach. Driven by nutrients ( esp amino acids and amines) that directly stimulate the G cell to release gastrin , which in turn activates the parietal cell via direct and indirect mechanisms. Distention of the stomach wall also leads to gastrin release and acid production. Luminal phase - The last phase of gastric acid secretion is initiated as food enters the intestine and is mediated by luminal distention and nutrient assimilation.
GASTRODUODENAL MUCOSAL DEFENCE SYSTEMS Exposure to noxious stimuli :- HCl acid, bile acids, ?pepsin, ?pancreatic enzymes, bacteria, drugs Mucosal integrity is maintained by a highly intricate system that provides mucosal defense and repair. The mucosal defense system can be envisioned as a three-level barrier:- preepithelial , epithelial, subepithelial elements
Gastritis Acute gastritis often due to chemical injury (alcohol drugs) Chronic gastritis: Helicobacter pylori infection Chemical damage (bile reflux, drugs) Autoimmune (associated with vitamin B12 malabsorption (pernicious anaemia)
Acute gastritis Drugs: NSAIDs Alcohol cause acute erosion Severe haemorrhage Acute Helicobacter infection: Prominent neutrophil infiltrate
Chronic gastritis ABC A – autoimmune B – bacterial ( helicobacter ) C - chemical
Autoimmune chronic gastritis Autoantibodies to gastric parietal cells Hypochlorhydria/achlorhydria Loss of gastric intrinsic factor leads to malabsorption of vitamin B12 with macrocytic,megaloblastic anaemia
Cag A Cytotoxin associated gene A — Histopathologic changes in H. pylori gastritis correlate with the presence of an H. pylori-derived cytotoxic protein encoded for by a gene called cytotoxin associated gene A ( Cag A). Approximately 60 percent of H. pylori isolates possess the Cag A gene and express the toxin . Cag A toxin correlates with a number of features that suggest a more severe form of infection, including : A larger number of H. pylori organisms A greater degree of acute and chronic inflammation More severe epithelial injury A higher likelihood of associated peptic ulceration (duodenal and gastric) An increased risk for developing gastric gland atrophy, intestinal metaplasia G astric adenocarcinoma
Treatment of H. Pylori PPI , amoxicillin 1 gm , clarithromycin 500 mg all twice daily for 7-14 days 1st line treatment regimen of choice Bismuth 525 mg, metronidazole 500 mg, tetracycline 500 mg all four times daily with a PPI twice daily for 7-14 days PPI , amoxicillin 1 gm , metronidazole 500 mg all twice daily for 14 days
RESCUE THERAPY PPI, levofloxacin 250 mg, amoxicillin 1 gm all twice daily for 14 days "Rescue" therapy for those failing two course of above treatments PPI , rifabutin 150 mg, amoxicillin 1 gm all twice daily for 14 days Alternative "rescue" therapy PPI twice daily plus amoxicillin 1 three times daily for 14 days Alternative "rescue" therapy
CONFIRMATION OF ERRADICATION Confirmation of eradication has been recommended by a European consensus panel. A 2007 guideline from the American College of Gastroenterology recommends confirming eradication in the following settings : Any patient with an H. pylori-associated ulcer Individuals with persistent dyspeptic symptoms despite the test-and-treat strategy Those with H. pylori-associated MALT lymphoma Individuals who have undergone resection of early gastric cancer
The Tests… Urea breath testing performed at least four weeks after treatment has been promoted as the test of choice to confirm eradication of infection. Stool antigen testing is a more widely available alternative, but it may be less accurate. Until further data are available, the stool antigen test should not be performed sooner than four to six weeks after completion of treatment because of both false-positive and false-negative results in this time period Antibiotics and bismuth should be discontinued for at least four weeks and PPIs at least one week if possible prior to testing done to confirm H. pylori cure (with urea breath test, stool antigen testing, or endoscopic testing) to reduce the chance of false-negative results. Serologic testing is not useful for follow-up since many patients continue to have antibodies for months or even years after eradication therapy.
TAKE HOME POINTS
THE END THANK YOU
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