Gastroenterological Society of Australia
The Gastroenterological Society of Australia (GESA) sets, promotes and continuously improves the standards of practice, training and research in gastroenterology and hepatology in Australia.
The membership includes Fellows and members of the RACP and the Royal Australasian College of Surgeons interested in the study of gastroenterology. It also extends to medical graduates, trainees, pathologists, radiologists, scientists, allied health professionals, dietitians, and others interested in the science, study or practice of gastroenterology.
Download the Gastroenterological Society of Australia's Top-5 recommendations (PDF)
Top-5 recommendations on low-value practices
1. Do not repeat colonoscopies more often than recommended by the National Health and Medical Research Council (NHMRC) endorsed guidelines.
Rationale and evidence
Rationale
Colonoscopy, with or without polypectomy, is an invasive procedure with a small but not insignificant risk of complications, including perforation or major haemorrhage postpolypectomy, depending on size of lesion. Surveillance colonoscopies place a significant burden on endoscopy services. Consequently, surveillance colonoscopy should be targeted at those who are most likely to benefit and at the minimum frequency required to provide adequate protection against the development of cancer.
Cancer Council Australia guidelines, endorsed by NHMRC, state that if 1 to 2 adenomas less than 1cm in diameter are removed via a high quality colonoscopy, a follow up interval of 5 years is recommended. For larger adenomas, 3 or more adenomas or adenomas containing villous features or high grade dysplasia, which are removed via a high quality colonoscopy, the recommended follow-up period is 3 years.
Evidence
Cancer Council Australia. Clinical Practice Guidelines for Surveillance Colonoscopy. December 2011.
Winawer et al. Randomized comparison of surveillance intervals after colonoscopic removal of newly diagnosed adenomatous polyps. The National Polyp Study Workgroup. N Engl J Med. 1993;328(13): 901-906.
2. Do not undertake faecal occult blood testing in patients who report rectal bleeding, or require investigation for iron deficiency or gastrointestinal symptoms.
Rationale and evidence
Rationale
The faecal occult blood test (FOBT) was developed for use in the outpatient setting for colorectal cancer screening in asymptomatic patients with average risk of colorectal carcinoma.
Studies suggest that it has limited positive impact for hospitalised patients who report rectal bleeding or require investigation for iron deficiency or gastrointestinal symptoms, as it is unlikely to change patient management and may in fact delay investigations while waiting for the results of the test.
Inappropriate use of the FOBT may lead to unnecessary additional investigations (e.g. colonoscopy), which also carries risks and may limit the availability of such investigations for more appropriate indications.
Evidence
Friedman et al. Use and Abuse of Faecal Occult blood tests in an acute hospital patient setting. Int Med Journal Vol 40, Issue 2 pages 107 - 111, Feb 2010.
Ip et al. Use of fecal occult blood testing in hospitalized patients: Results of an audit. Can J Gastroenterol Hepatol. 2014 Oct; 28(9): 489–494.
Sharma et al. An audit of the utility of in-patient fecal occult blood testing. Am J Gastroenterol. 2001 Apr; 96(4): 1256-60.
3. Do not continue prescribing long term proton pump inhibitor (PPI) medication to patients without attempting to reduce the medication down to the lowest effective dose or cease the therapy altogether.
Rationale and evidence
Rationale
While proton pump inhibitors (PPIs) are effective drugs for the treatment of gastroesophageal reflux disease (GERD), their use has been linked to increased risk of fractures, pneumonia, enteric infections, vitamin and mineral deficiencies, and acute interstitial nephritis, particularly among older people who make up the largest proportion of PPI users.
While there is insufficient evidence to establish causation, these reports deserve consideration when prescribing long term PPI use. This is especially because some patients may be able to stop PPI use immediately after the initial course of therapy without experiencing symptoms. Even though GERD is often a chronic condition, over time the disease may not require acid suppression and it is important that patients do not take drugs that are no longer necessary.
Evidence
Choudhry et al. Overuse and inappropriate prescribing of proton pump inhibitors in patients with Clostridium difficile-associated disease. QJM. 2008;101: 445–8.
Hollingworth et al 2010. Marked increase in proton pump inhibitors use in Australia. Pharmacoepidemiol Drug Saf 2010;19: 1019–24.
NICE. Gastro-oesophageal reflux disease and dyspepsia in adults: investigation and management. Clinical guideline 3 September 2014.
4. Do not undertake genetic testing for coeliac genes as a screening test for coeliac disease.
Rationale and evidence
Rationale
The value of testing for coeliac genes is primarily as a negative test – if the gene test is negative then coeliac disease may be excluded. However, as a coeliac gene can be found in approximately one-third of the population, a positive result does not make coeliac disease a certainty.
Serological testing, in a patient consuming an appropriate amount of gluten, is the appropriate first line screening test for coeliac disease. A small bowel biopsy is then required if serology is positive.
Evidence
Fasano and Catassi. Celiac disease. NEJM. 367:2419 Dec 20 2012.
Megiorni and Pezutti. HLA-DQA1 and HLA-DQB1 in Celiac disease predisposition: practical implications of the HLA molecular typing. J Biomed Sci. 2012; 19(1): 88.
5. Do not perform a follow-up endoscopy less than 3 years after 2 consecutive findings of no dysplasia from endoscopies with appropriate 4 quadrant biopsies for patients diagnosed with Barrett's Oesophagus.
Rationale and evidence
Rationale
Barrett’s Oesophagus (or Barrett’s mucosa) is the term given to a change which occurs in the lining of the lower oesophagus. It occurs in a small proportion of patients with longstanding gastro-oesophageal reflux. The condition requires surveillance because of an increased risk of oesophageal adenocarcinoma (EAC). This usually develops slowly over a period of some years and can be predicted by the finding of pre-cancerous changes (dysplasia) on biopsies.
However, systematic surveillance of Barrett’s Oesophagus patients has not been shown to be cost-effective, and no randomised controlled trials have been conducted to compare surveillance with the natural history of Barrett’s Oesophagus. According to currently-accepted guidelines, it is appropriate and safe to examine the oesophagus and check for dysplasia every three years, as cellular changes occur very slowly.
Evidence
Spechler and Souza. Barrett’s Esophagus. NEJM. 371:836 August 28, 2014.
Shaheen et al. ACG Clinical Guideline: Diagnosis and Management of Barrett’s Esophagus. Am J Gastroenterol. 2015 Nov 3.