Peptic ulcers

Question 1

What is a peptic ulcer?

Answer 1

• break in the lining of the mucosa (down to submucosa)
• of stomach or proximal duodenum
• more than 5mm in diameter
• can also occur in distal oesophagus

Question 2

What are symptoms of peptic ulcers?

Answer 2

• recurrent burning epigastric pain
  
  • duodenal ulcer - pain gets better on eating
  • gastric ulcer - pain gets worse on eating
• heartburn/chest (retrosternal) pain
• bleeding -> anaemia, melaena, haematemesis
• belching, bloating, intolerance to fatty foods
• can present w complications of perforation or obstruction

patient can sometimes show site of pain with one finger

Question 3

Are duodenal or gastric ulcers more common?

Answer 3

duodenal ulcers are 4x more common than gastric ulcers

Question 4

What signs may be elicited on examination for peptic ulcers?

Answer 4

• epigastric tenderness
• peritonitic if perforated
  
  • generalised abdo pain
  • guarding
  • rebound tenderness
  • patient prostrated lying still
  • positive cough test

Question 5

What are the differential diagnoses for epigastric pain?

Answer 5

• Peptic ulcer disease
• Pancreatitis
• Appendicitis
• AAA
• Small bowel obstruction
• Mesenteric ischaemia
• Inferior wall MI
• Pericarditis
• Cholecystitis
• Cholangitis
• Oesophagitis
• Gastritis

Question 6

What are the major risk factors for the formation of peptic ulcers?

Answer 6

• H. Pylori infection
• NSAIDs + Aspirin
• Smoking
• Inc age
• FHx/Hx of PUD
• Intensive care patient
• Rarer causes: hyperparathyroidism, Zollinger-Ellison syndrome, gastric ischaemia, infections + Crohn’s

DUs are almost always associated w/ H. Pylori inifection, and GUs with NSAID use

Question 7

Generally speaking, why/how do peptic ulcers form?

Answer 7

• result from imbalance between defence mechanisms and attack mechanisms
• defence factors = mucin, cellular mucus, bicarb, mucosal blood flow, cell turnover/formation
• attack factors = acid, pepsin, H.pylori, bile salts, NSAIDs

Question 8

Helicobacter pylori is a spiral shaped bacterium that has been identified as being carcinogenic. It can cause acute gastritis and is thought to be spread via contaminated food + water.

What is the pathogenesis of H. Pylori infection causing peptic ulcers?

Answer 8

• increases gastric acid secretion (by inc gastrin and reduced somatostatin) -> increasing acidity of gastric contents that flow into duodenum
• disrupts the protective mucosal layer
• reduces duodenal bicarbonate production
• produces virulent factors eg. VacA, CagA, urease
• longstanding H.Pylori infection + severe inflammation -> results in disruption of epithelial tight junctions + cell death -> leading to gastric ulcers

Question 9

What is the pathophysiology of NSAIDs causing peptic ulcers?

Answer 9

By primarily weakening the mucosa’s protective mechanisms

• inhibit COX-1 so PG synthesis is reduced so blood flow + alkaline secretions are reduced
• involve trapping hydrogen ions
• irritates mucosa
• impairs mucosal repair mechanisms
• increase risk of bleeding through anti-platelet actions

Question 10

Which duodenal ulcers bleed and which perforate?

Answer 10

• posterior duodenal ulcers bleed
• anterior duodenal ulcers perforate
• due to the gastroduodenal artery which comes down behind duodenum

Question 11

How do you investigate peptic ulcer disease?

Answer 11

• non-invasive H. Pylori testing in pts <55yrs w/out ALARMS
• OGD - pts with ALARMS or >55yrs
• FBC - looking for microcytic anaemia
• Stool heme test

Question 12

Describe the non-invasive methods to diagnose H. Pylori infection

Answer 12

• Serological tests - detect IgG antibodies against H. Pylori, useful in diagnosis and epidemiological studies. IgA can also be found in saliva - but not as specific + sensitive as serology.
• ¹³C-Urea breath test - quick, screening tool, pts swallow urea containing isotope + it can be detected in next 30 mins from exhaled breath - indicates presence of urease which H. Pylori secreted in order to survive. Pt must be off PPIs + Abx for accuracy. (THIS IS FIRST LINE NOW)
• Stool antigen test - if positive, faeces will contain H. Pylori antigens, detected by immunoassay. Pt must be off PPIs + Abx for accuracy.

Question 13

Describe the invasive methods done at endoscopy to diagnose H. Pylori infection

Answer 13

• Rapid urease test (CLO) - biopsy of mucosa taken from antrum of stomach, placed into medium containing urea + an indicator of phenol red. If H. Pylori present, it hydrolyses the urea -> ammonia, increasing pH of medium causing a colour change.
• Histology - blood taken from OGD, put under microscope + visualised by giemsa staining, if infected H. Pylori will be seen. Again, best to be off PPIs.

Question 14

What is the epidemiology of H. Pylori infection?

Answer 14

• high prevalence in developing countries (80-90%)
• lower in developed countries (20-50%)
• infection rates highest in lower-income groups
• infection usually acquired in childhood
• faecal-oral or oral-oral

Question 15

What is the association of H. Pylori with gastric cancer?

Answer 15

• The incidence of distal (but not proximal) gastric cancer parallels H. Pylori infection in countries w/ a high incidence of gastric cancer
• Serological studies show ppl infected w/ H. Pylori have a higher incidence of distal gastric carcinoma
• Over 70% of gastric B-cell lymphoma pts have H. Pylori
• H. Pylori gastritis has been shown to contain the clonal B cell that eventually gives rise to MALT lymphoma

Question 16

How would you treat acute peptic ulcers?

Answer 16

• Active bleeding ulcer:
  
  • OGD to confirm dx + identify cause of bleeding + stop bleeding, adrenaline is injected into bleeding site with cautery +/- clip as well
  • blood transfusion
  • PPI
  • If perforated or above ineffective -> surgery
• No active bleeding + H. Pylori negative:
  
  • treat underlying cause (eg. stop NSAIDs)
  • start on oral PPIs (or H₂ antagonist)
• No active bleeding + H. Pylori positive:
  
  • H Pylori eradication therapy

Question 17

What does H. Pylori eradication therapy consist of?

Answer 17

• several treatment regimens available
• generally a triple therapy (PPI + 2 Abx)
  
  • omeprazole 20mg + clarithryomycin 500mg + amoxicillin 1g (or metronidazole 400g if allergic) - all twice daily
• can be any PPI (doesn’t have to be omeprazole)
• given for 7 or 14 days
• quadruple therapy may have better eradication rates

Question 18

What is the mechanism of action of NSAIDs?

Answer 18

• inhibit synthesis of PGs from AA by inhibiting COX
• COX exists as COX-1 (constitutive form) + COX-2 (inducible form, stimulated by cytokines)
• COX-1 stimulates PG synthesis to preserve integrity of gastric mucosa; maintain renal perfusion; and inhibit thrombus formation at vascular endothelium
• COX-2 stimulates PGs that cause inflammation + pain
• benefits of NSAIDs principally mediated by COX-2 inhibition
• adverse effects mediated by COX-2 inhibition
• selective COX-2 inhibitors developed to reduce adverse effects of NSAIDs

Question 19

What are the adverse effects of NSAIDs and how do the more selective COX-2 inhibitors’ adverse effects differ?

Answer 19

• GI toxicity
• renal impairment
• inc risk of CV events
• hypersensitivity reactions
• fluid retention

COX-2 inhibitors cause fewer GI side effects than non-selective NSAIDs, but are associated with an increased risk of CV events. All NSAIDs including COX-2 inhibitors can cause renal impairment.

COX-2 specifics should therefore only be used in those with high GI risk and minimal CVS risk.

Question 20

What are examples of COX-2 selective inhibitors?

Answer 20

• etoricoxib
• celebcoxib
• valdcoxib

the ‘coxibs’

Question 21

In which patients should you avoid NSAIDs in, generally speaking?

Answer 21

• severe renal impairment
• heart failure or CV disease
• liver failure
• NSAID hypersensitivity
• Peptic ulcer disease or GI bleeding

Try to use safest NSAID at lowest effective dose for shortest possible time if NSAID is unavoidable in above patients