5. Peptic ulcer refers to an erosion of the mucosal
layer anywhere in the GI tract; however, it
usually refers to erosions in the stomach or
duodenum.
Over 80% of peptic ulcers are caused by
Infection with the bacterium Helicobacter pylori.
7. DUODENAL GASTRIC
INCIDENCE More common Less common
ANATOMY First part of duodenum –
anterior wall
Lesser curvature of
stomach
DURATION Acute or chronic Chronic
MALIGNANCY Rare Benign or malignant
8.
9. HELICOBACTER PYLORI Infection
Non Steroidal Anti-inflammatory Drugs
Steroid therapy
Smoking
Excess alcohol intake
Genetic factors
Zollinger Ellison syndrome – rare syndrome caused by
gastrin-secreting tumour
Blood group O
Hyperparathyroidism
10. Nausea – Vomiting – Anorexia
Epigastric pain after meal and during meal
Intolerance of fatty food
Heartburn
Loss of weight
Oral flatulence, bloating
Pain radiating to the back
13. Bacteria
Gram Negative spiral bacterium
40% of patients >60 years are +ve for H.pylori
Transmitted: possibly person to person
Most common cause of antral gastritis
Mechanism of gastric injury
Adherence to epithelial cells
Infects mucosa of stomach > inflammatory response >
gastritis > increased gastrin secretion > gastric
metaplasia > damage to mucosa > ulceration
Cytotoxin
21. Mechanism of action
Irreversible inhibition of proton pump (H+/ K+
ATPase) that is responsible for final step in
gastric acid secretion from the parietal cell.
PP inhibitors include:
Omperazole
Lansoprazole
Pantoprazole
Rabeprazole
22. They are prodrugs – taken orally.
Are given as enteric coated capsules
They are activated in the acidic medium of the
secretory parietal cell canaliculus.
They are inactivated if (combined with H2
receptor blockers).
Have long duration of action (> 18 -24 hr).
Bioavailability is reduced by food.
Given 1 hr before meal.
23. PPIs are quite safe but may occur:
GIT disturbances: nausea, vomiting, diarrhoea
Achlorhydria: increase the risk of enteric
infections due to Shigella, salmonella
Hypergastrinaemia
Gastric hyperplasia
24. Mechanism of action
They competitively and reversibly block to H2
receptors on the parietal cells thus reduce gastric
secretion. They include:
H2 Receptor inhibitors include:
Cimetidine
Ranitidine
Famotidine
Nizatidine
25. Good oral absorption
Plasma half life (1-3 h).
Duration (4-12 h).
First pass metabolism (50% Except Nizatidine
100 % bioavailability).
Given before meals.
Metabolized by liver.
Excreted mainly in urine.
Cross placenta & excreted in milk
26. These are extremely safe drugs but may occur:
nausea, vomiting,
bradycardia and hypotension (rapid
I.V.)
Gynecomasteia, impotence in male
Galactorrhea in female on long term use
of cimitidine
Decrease metabolism of oral anticoagulant,
phenytoin, benzodiazepines.
29. Treatment
Combined therapy is usually used.
Clarithromycin, tetracycline, amoxicillin
Proton pump inhibitors or H2 receptor
blockers
Bismuth compounds
Metronidazole
Resistance may develop to antibiotics so the
better eradication is obtained using proton
pump inhibitors, clarithromycin &
Amoxicillin.
30. The BEST among all the Triple therapy regimen is
Omeprazole/Lansoprazole - 20/30 mg bd
Clarithromycin - 500 mg bd
Amoxycillin/Metronidazole -1gm/500 mg bd
Given for 14 days followed by P.P.I for 4 – 6 weeks.
Short regimens for 7 – 10 days not very effective.
33. Sucralfate (aluminum hydroxide + sucrose)
Form a sticky like gel over ulcer crater to
protect gastrointestinal mucosa and stimulates
prostaglandin synthesis
It promote mucosal repair and ulcer healing
It has no acid neutralising action and delay
gastric emptying
Dose: 1 g QID
34. Misoprostol is a prostaglandin E1 analog that
stimulates the secretion of mucus and
bicarbonates and inhibits acid secretion to a
minor degree.
The drug has significant side effects, primarily
mild to moderate diarrhoea
Is too costly to be used by most patients.
35. Drugs used to relief gastric pain associated with
hypersecretion of HCL and neutralize the gastric acid.
Mechanism of Action
Neutralization of HCL
Inhibition of pepsin (inactive at PH 5)
1. Systemic Antacids
Sodium bicarbonate
Calcium Carbonate
2. Non Systemic Antacids
Aluminum Hydroxide Gel
Magnesium Trisilicate
36. Sodium bicarbonate
Calcium Carbonate
NaHCO3 + HCL → NaCL + CO2
Disadvantages
Rebound hyperacidity
Stomach distension due to CO2 liberation
→ pain sensation
Sodium load → salt and water retention
( # in cardiac patients)
Systemic alkalosis
37. Aluminum Hydroxide Gel
Magnesium Trisilicate
Al (OH)3 + HCL → HCL3 + H2O
Advantages
Longer duration of action.
Gradual neutralization of HCL → No rebound
hyperacidity.
Adsorbs pepsin.
No stomach distention
38. Due to the benign nature of duodenal ulcers
When patients with duodenal ulcers require
surgery, it is usually one of three procedures:
Vagotomy,
Vagotomy with antrectomy,
Pyloroplasty
39. A peptic ulcer is a break in superficial epithelial
cells penetrating down to muscularis mucosa
Duodenal > gastric ulcers
H pylori is a predominant risk factor
H pylori diagnosed by c urea breath test, stool
antigen or if validated serology, treated with
PAC500 or PMC250 regimen
Complications of PUD can lead to acute
emergency of upper GI bleed
