H.pylori
- Spiral-shaped (helical) Gram Negative Bacteria
- Colonizes gastric mucosa or epithelial lining
- Acquired in early childhood via fecal-oral transmission
- Helicobacter pylori is strongly linked to peptic ulcer disease and is classified as a group 1 carcinogen
- socioeconomic level seems to be the major determinant of risk of infection
- Prevalence: ~30% in Australian adults; higher among:
- Migrants (esp. from East Asia, Mediterranean)
- Institutionalised persons
- Lower socioeconomic groups
- People with a family history of PUD or gastric cancer
- Transmission: Fecal–oral or oral–oral; usually acquired in childhood
Associated conditions
- Active chronic gastritis (universal in infected)
- Dyspepsia
- Peptic Ulcer Disease (15–20% lifetime risk)
- Duodenal Ulcers: 95% related to H. pylori
- Gastric Ulcers: 70-80% related to H. pylori
- Stomach Cancer (epithelial or lymphoid) (~2% lifetime risk)
- Mucosa-associated Lymphoid Tissue (MALT)
- Gastric adenocarcinoma
Clinical
- Reflux symptoms
- Dyspepsia – Chronic or recurrent Epigastric Pain, burning, early satiety or post-prandial fullness
- Epigastric discomfort
- Pain
- Bloating
Indications for Diagnosis and treat
- Proven indications for the diagnosis and treatment
- Peptic ulcer disease (active or confirmed history)
- Dyspepsia
- Low grade gastric MALT lymphoma
- After endoscopic resection of early gastric cancer
- First degree relatives of patients with gastric cancer
- Conditions where evidence is inconclusive for diagnosis and treatment
- Investigated nonulcer dyspepsia (ie. ’functional dyspepsia’: dyspepsia patients who have no ulcer at endoscopy)
- With NSAID use
- Gastro-oesophageal reflux disease (GORD)
- There is no clear evidence that eradication of H. pylori infection causes gastro-oesophageal reflux disease (GORD) or exacerbates GORD
- Helicobacter pylori eradication therapy should not be withheld due to concerns of creating or worsening GORD.
- Routine testing for H. pylori is not recommended in GORD.
- However, in patients receiving long term maintenance treatment with PPIs, H. pylori testing should be considered.
- Profound acid suppression affects the pattern and distribution of gastritis favouring corpus dominant gastritis and may lead to atrophic gastritis.
- Helicobacter pylori eradication halts the progression of atrophic gastritis and may reverse the process of atrophy therefore decreasing cancer risk
- Populations at higher risk for gastric cancer (Japan and parts of China)
- definite evidence on whether H. pylori eradication can reduce the risk of developing gastric adenocarcinoma is lacking.
- It is likely that cancer risk persists for several years after the bacterium is gone
- Unexplained iron deficiency anaemia in adults
- Idiopathic thrombocytopenic purpura
- NSAID and H. pylori eradication
- H. pylori eradication is of value in chronic NSAID users but is insufficient to prevent NSAID related ulcer disease completely
- In naive NSAID users H. pylori eradication may prevent peptic ulcer and bleeding
- For patients with a history of an ulcer complication who require subsequent therapy with an NSAID or aspirin, PPI maintenance treatment is better than H. pylori eradication in preventing ulcer recurrence and/or bleeding. Co-therapy may be an option
- Patients taking long term aspirin and who bleed should be tested for H. pylori, and be treated for the infection if positive
| Test | Mechanism | Notes |
| Invasive | ||
| Rapid urease test | Biopsy specimen is combined with urea and pH is measured H. pylori converts urea to ammonia (NH3) + CO2 Test is positive for H. pylori if pH of the medium becomes more alkaline, indicated by colour change | Highly sensitive and specificn ( >90% ) quick diagnosis Not suitable for monitoring post-eradication because that would entail further gastroscopy |
| Endoscopy & Histology & Culture | Offers additional information on degree and pattern of inflammation | Expensive Histology: Sensitivity and specificity >95%; confirms – gastritis – malignancy – early changes of MALT lymphoma |
| Non-invasive | ||
| Serology | Presence of H. pylori-specific IgG antibodies | Sensitivity: ~85%; Specificity: ~79% (if no previous infection) Use: Past exposure only; not useful for test-of-cure Inexpensive and widely available. Positive predictive value (NPV) 50% — Positive in low titre indicates past exposure to H. pylori and not necessarily active colonisation — Positive in high titre reflects active colonisation — Serology can also remain positive for months to years after successful eradication negative predictive value (NPV) 98% – negative result = almost rules out current infection Not suitable for monitoring post-eradication because successful treatment does not alter IgG levels immediately |
| Urea breath test | Uses principle of urea metabolism by H. pylori Patient ingests radio-labelled (13c) urea followed by a measurement of the concentration of isotope-labelled CO2 exhaled Positive for H. pylori if isotope-labelled CO2 present | Sensitivity/Specificity: >95% Use: First-line for diagnosis and test-of-cure High positive predictive value High negative predictive value Use: First-line for diagnosis and test-of-cure |
| Stool antigen test | Presence of H. pylori antigen in the stool | Sensitivity: 91–96%; Specificity: 93–97% Use: Alternative first-line and test-of-cure option Limitations: ↓ sensitivity during GI bleeding specimens are sensitive to room temperature and must be immediately frozen after collection may be useful in children who are unable to perform a UBT |
✅ Standard Triple Therapy
- Esomeprazole 20 mg orally, twice daily
- Amoxicillin 1 g orally, twice daily
- Clarithromycin 500 mg orally, twice daily
- Duration: 7 to 14 days (14 days preferred for higher eradication rates)
🔹 FIRST-LINE IN PENICILLIN-ALLERGIC PATIENTS
- PPI (standard dose) orally, twice daily
- Esomeprazole 20 mg or
- Lansoprazole 30 mg or
- Omeprazole 20 mg or
- Pantoprazole 40 mg or
- Rabeprazole 20 mg
- Metronidazole 400 mg orally, twice daily
- Clarithromycin 500 mg orally, twice daily
- Duration: 7–14 days (preferably 14 for higher efficacy)
Note: Eradication rates ~80%, lower if metronidazole resistance present
Resistance is increasing markedly
🟡 Avoid repeating if failed once (due to clarithromycin resistance risk)
- Metronidazole resistance is very common
- Clarithromycin resistance is growing (8-12%)
| First and second line therapies | ||||
| 7 days | PPI standard dose bd | clarithromycin 500 mg bd | amoxicillin 1000 mg bd | |
| 7 days | PPI (any) PO BD | clarithromycin 500 mg bd | metronidazole 500 mg bd | |
| 14 days | PPI (any) PO BD | Colloidal bismuth subcitrate 120 mg four times daily (empty stomach) (Bismuth-based quadruple therapy) | Tetracycline 500 mg four times daily **# (empty stomach) (cannot be replaced with doxycycline because of different pharmacokinetics) | Metronidazole 400 mg three times daily with food * All agents available via SAS in Australia |
| 10 days | PPI (any) PO BD | amoxicillin 1000 mg bd | Levofloxacin 250 mg PO BD or 500 mg PO daily (SAS only) OR Moxifloxacin 400 mg PO daily (Quinolone-based triple therapy (10 days)) | |
| third line (‘rescue/salvage’) therapies (Any subsequent eradication regimen used after failure of the initial treatment) | ||||
| 10 days | PPI (any) PO BD | Amoxicillin 1 g PO BD | Rifabutin 150 mg PO BD (off-label use) (Rifabutin-based triple therapy) | Eradication: ~65–80% |
| NEED TGA-SAS approval for: – Colloidal bismuth subcitrate (De-Nol), – Tetracycline (SAS-category B). To prescribe or obtain these drugs for treating H. pylori infection, follow these three steps: • obtain the SAS form from the TGA website (www.tga.gov.au/docs/pdf/unapproved/sascata.pdf) • fax the completed form to the TGA for approval (it will befaxed back to you by the TGA after 1 week) • deliver the SAS form to the drug supplier to be filled | ||||
| Standard PPI doses: – esomeprazole 40 mg/day BD – lansoprazole 30 mg/day BD – omeraprazole 20 mg/day BD – pantoprazole 40 mg/day BD – rabeprazole 20 mg/day BD | ||||
| Common side effects PPIs – Headache and diarrhoea Clarithromycin – Gastrointestinal (GI) upset, diarrhoea, and altered taste Amoxicillin – GI upset, diarrhoea, and headache – Metronidazole Tends to be dose related, a metallic taste, dyspepsia, a disulfiram-like reaction with alcohol consumption Tetracycline – GI upset, photosensitivity Bismuth subcitrate – Darkening of the tongue and stool, nausea, and GI upset Furazolidone – Nausea, vomiting, headache, and malaise in up to a third of patients. – Less frequently hypersensitivity, hypotension, a disulfiram-like reaction with alcohol consumption, and mild reversible haemolytic anaemia Rifabutin – Red discoloration of urine while using the drug. Rash, diarrhoea, nausea, vomiting, dyspepsia. -Small but serious risk of myelotoxicity and ocular toxicity. – Can select for resistance among mycobacteria | ||||
POST-ERADICATION ASSESSMENT
- Test-of-cure is mandatory in:
- Complicated ulcers (bleeding, perforation)
- Before stopping long-term PPI
- Medico-legal assurance
- Preferred test: urea breath test
- Stop PPIs ≥1–2 weeks
- H₂ blockers can continue
- Stop antibiotics ≥4 weeks
- Avoid: Serology (remains positive long-term)
- May need repeat scopes if ulcer/malignancy/assess healing if complicated
- Consider PPI when using NSAIDs in the future
MAINTENANCE THERAPY (If needed)
Use if:
- H. pylori eradication unsuccessful
- Ongoing NSAID requirement
- High-risk of recurrence
PPI options (once daily):
- Esomeprazole 20 mg
- Lansoprazole 30 mg
- Omeprazole 20 mg
- Pantoprazole 40 mg
- Rabeprazole 20 mg
PAEDIATRIC H. PYLORI MANAGEMENT
Prevalence: <5% in Australia
Testing NOT recommended for:
- Functional abdominal pain
- Without alarm symptoms
If testing needed:
- Stool antigen (preferred)
- Urea breath test: false positives common in children
Refer to paediatric gastroenterology
Avoid empirical treatment