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Gastro-oesophageal reflux disease

By Theresa Lowry Lehnen - 01st Jan 2024

Gastro-oesophageal reflux disease

Gastro-oesophageal reflux disease (GORD) is a common, chronic, progressive, and relapsing gastrointestinal (GI) disorder characterised by the regurgitation of gastric contents into the oesophagus.1 A higher incidence occurs in people living in western countries, affecting up to 20 per cent of the population. GORD is defined as symptoms or complications due to the reflux of gastric contents into the oesophagus or beyond, the oral cavity (including larynx), or lung.2

GORD is caused by multiple different mechanisms which can be intrinsic, structural, or both. The most common cause is defective functioning of the lower oesophageal sphincter, leading to excessive acid exposure in the lower oesophagus.

In healthy people, the angle of His (where the oesophagus enters the stomach) creates a valve that prevents bile, digestive enzymes, and stomach acid from travelling back into the oesophagus which can cause burning and inflammation of sensitive oesophageal tissue.3

Symptoms

Most patients with GORD present with the classic symptoms of heartburn and acid regurgitation, reporting a burning feeling in the retrosternal area, rising into the chest, and radiating toward the neck, throat, and occasionally the back. It is estimated that between 20-to-40 per cent of patients with heartburn will have a diagnosis of GORD. Symptoms occur particularly after ingestion of fatty, spicy, citrus foods, and alcohol. The columnar epithelium lining of the oesophagus cannot withstand acid, and this leads to inflammation. It can also present in an atypical fashion with oropharyngeal and respiratory symptoms, such as chest pain, dental erosions, halitosis, anorexia, dysphagia, chronic cough, laryngitis, or asthma.1,4

Left untreated, GORD can cause considerable discomfort and a poor quality-of-life. Medical attention should be sought and symptoms investigated when GORD is severe, occurs several times a week, over-the-counter medications fail, dysphagia or symptoms, such as vomiting, haematemesis, anaemia, or unexplained weight loss occur.1,4

Risk factors

Several factors may increase the risk of developing GORD. First-degree relatives of patients with GORD are four times more likely to develop symptoms, raising the possibility of a strong genetic contribution to the aetiology.5 Medicines, such as calcium-channel blockers, nitrates, and non-steroidal anti-inflammatory drugs (NSAIDs) can cause GORD or make the symptoms worse.4 Risk factors for complications include advanced age, obesity, alcohol, and tobacco use.

There is no clear association between gender and oesophageal stricture; however, men are at greater risk of developing erosive oesophagitis, Barrett’s oesophagus, and oesophageal adenocarcinoma than women.The presence of a hiatus hernia increases the likelihood of GORD due to mechanical and motility factors.

There is substantial overlap between symptoms of GORD and those of eosinophilic oesophagitis, functional dyspepsia, and gastroparesis, often posing a challenge for patient management.

Co-existent dysphagia is considered an alarm symptom, requiring investigation and evaluation. GORD may lead to Barrett’s oesophagus, which in turn is a precursor condition for oesophageal cancer.

The risk of progression from Barrett’s to dysplasia is estimated at around 20 per cent. Oesophageal cancer typically affects people aged between 60 and 80 years, with the greatest risk factors being severe, long-standing GORD, smoking, and heavy alcohol consumption.6

Diagnosis

There is no gold standard for diagnosing GORD. A presumptive diagnosis can be made based on the typical symptoms of heartburn and acid regurgitation. Heartburn is described as a burning, retrosternal, rising sensation associated with meals, although this definition is often poorly understood by the general population.Practitioners need to clarify the nature of the symptoms being discussed when the term ‘heartburn’ is used by patients.3

Investigative tests for GORD include endoscopy, barium swallow or meal, manometry, 24-hour pH monitoring, and blood tests. A full blood count should be taken to assess for anaemia, which could be a sign of internal bleeding.7

GORD can be classified according to the presence or absence of erosions on endoscopic examination. Absence of erosions are classified as non-erosive reflux disease (NERD), whereas GORD symptoms with erosions is classified as erosive oesophagitis.The primary role of endoscopy is to look for complications and to exclude other diagnoses. Endoscopy is not generally required in the presence of typical GORD symptoms. However, it is recommended for patients who are at higher risk of Barrett’s oesophagus due to it being a precursor for developing adenocarcinoma.8

Manometry is used to assess how well muscle at the distal end of the oesophagus is functioning. A tube containing pressure sensors can measure the pressures in the oesophagus and help determine whether surgery may be necessary.7

A barium swallow, or barium meal, may be required to assess swallowing ability and look for any blockages or abnormalities in the oesophagus.7

For some patients, 24-hour pH monitoring may be necessary to measure the acidity level in the oesophagus and confirm a diagnosis of GORD. It is the most objective test to diagnose the reflux disease and allows monitoring of GORD patients in their response to medical or surgical treatment.7

A urea breath test is the examination of choice for patients under the age of 50 years presenting with dyspepsia. It is recommended as a non-invasive test for active Helicobacter pylori infection, but does not confirm or establish a diagnosis of GORD.8

A short-term treatment with proton-pump inhibitors (PPIs) and subsequent improvement in symptoms is suggestive of a positive diagnosis. Short-term treatment with PPIs may help predict abnormal 24-hr pH monitoring results among patients with symptoms suggestive of GORD.1

Other causes of chest pain should be outruled before making the diagnosis.Laryngopharyngeal reflux (LPR) or extra-oesophageal reflux disease is another type of acid reflux, which causes respiratory and laryngeal symptoms. Unlike GORD, LPR rarely produces heartburn, and is sometimes called ‘silent reflux’.1

Treatment and management

Treatment and management of GORD includes pharmacotherapy, dietary and lifestyle changes, and in some cases, surgery. Initial treatment is guided by the severity of symptoms and treatment is adjusted according to response. The extent of healing depends on disease severity, treatments chosen, and the duration of therapy. Patients should be advised about lifestyle changes, avoidance of excess alcohol, and consumption of aggravating foods such as fats. Other measures include smoking cessation and weight reduction if applicable, raising the head of the bed when sleeping, and the avoidance of wearing tight-fitting clothing and bending down after a meal.8,9

Pharmacological therapy for GORD is targeted at symptom reduction and minimising mucosal damage from acid reflux. Initial management for mild symptoms may include the use of antacids and alginates, which reduce reflux and protect the oesophageal mucosa. Histamine H2-receptor antagonists such as ranitidine may be used to relieve symptoms and permit reduction in antacid consumption. For more severe symptoms and patients with oesophagitis, oesophageal ulceration, oesophagopharyngeal reflux, and Barrett’s oesophagus, treatment involves the use of PPIs.

There are a wide range of PPIs available, including omeprazole, pantoprazole, lansoprazole, rabeprazole, and esomeprazole. Esomeprazole, the S-isomer of omeprazole, has been found to show more improvement than all other PPIs in several studies. Research has also shown that the treatment of reflux oesophagitis with esomeprazole is more cost-effective than treatments using any other PPI, therefore, providing a greater healing rate at a lower cost.

After a review of available evidence the HSE Medicines Management Programme found minimal differences between PPIs and recommends pantoprazole as the preferred PPI for the treatment of GORD (Figure 1).

Pantoprazole is the Preferred PPI for the Treatment of GORD

Indication Dose Duration Note
Symptomatic GORD 20 mg daily 2-4 weeks If symptom relief/healing is not sufficient, continue treatment for a further four weeks.
Treatment of reflux oesophagitis 40 mg daily 4 weeks
Prophylaxis of reflux oesophagitis 20 mg daily Continuous Increase to 40 mg daily for healing if a relapse occurs before reducing to 20 mg daily.
With reoccurring symptoms, an on-demand regimen of 20 mg once daily when required can be used. Continuous therapy may be considered in patients with unsatisfactory symptom control using an on-demand regimen.

Tips When Prescribing PPIs

  • Address lifestyle issues including advice on healthy eating, weight reduction where appropriate, and smoking cessation.
  • Advise patients to avoid known precipitants associated with their dyspepsia symptoms such as smoking, alcohol, coffee, chocolate, and fatty foods.
  • Review medications for possible causes of dyspepsia such as calcium channel blockers, nitrates, bisphosphonates, corticosteroids, and NSAIDs.
  • Prescribe at the lowest effective dose for the shortest treatment duration.
  • Review patients after the initial course of treatment and at least annually for patients on long-term treatment reducing or stopping PPI treatment symptoms are well controlled, unless there is a recognised indication for long term treatment.

Safety Concerns with PPIs

Gastric cancer: Particular care is required in patients presenting with alarm symptoms (e.g., significant unintentional weight loss); in such cases gastric malignancy should be ruled out before treatment.

Cautions with PPI Use

Bone fracture: PPIs may increase the risk of bone fracture of the hip, wrist and spine, particularly when used at high doses for over a year in older people. Patients at risk of osteoporosis should have an adequate intake of vitamin D and calcium.

Vitamin B12 deficiency: PPIs may reduce absorption of vitamin B12 with long-term treatment.

Hypomagnesaemia: measurement of serum magnesium concentrations should be considered before and during prolonged treatment with a PPI, especially when used with other drugs that cause hypomagnesaemia or with digoxin.

Gastrointestinal infections: PPIs may increase the risk of gastrointestinal infections caused by bacteria such as Salmonella, Campylobacter, Clostridium difficile.

Subacute cutaneous lupus erythematosus: PPIs are associated with very infrequent cases of subacute cutaneous lupus erythematosus.

** Caution is required when prescribing PPIs long-term in older people, as side-effects are likely to be enhanced. List not exhaustive; please consult the Summary of Product Characteristics (SmPC) for full information.

An evaluation report is available at www.hse.ie/yourmedicines

References
  • All Wales Medicines Strategy Group. Safe use of proton pump inhibitors (2018).
  • National Institute for Health and Care Excellence (NICE). Guidance CG184: Gastro-oesophageal reflux disease and dyspepsia in adults: investigation and management (2014).
  • British National Formulary (BNF) March 2018 4 Summary of Product Characteristics (SmPCs) Protium 20mg & 40mg 5. Prescribing PPIs. Drugs and Therapeutic Bulletin 2017; 55(10): 117-120
Abbreviations

GORD: gastro-oesophageal reflux disease, NSAIDs: non-steroidal anti-inflammatory drugs, PPI: proton pump inhibitor.

FIGURE 1: PPIs for the treatment of gastro-oesophageal reflux disease(GORD)

Patients should take their PPI medication first thing in the morning before food. If a morning dose is not enough to control symptoms, a second dose in the evening may be required. If symptoms persist after four-to-six weeks of treatment with a PPI, the patient will need to be reassessed. Non-response to PPIs may suggest an alternative diagnosis, such as peptic ulcer disease, upper gastrointestinal malignancy, functional dyspepsia, eosinophilic oesophagitis, or achalasia. When symptoms resolve or abate with PPIs, treatment can be titrated down to a level that retains remission. This can involve reducing the dose, giving it intermittently, or substituting it with a histamine H2–receptor antagonists. However, for endoscopically confirmed erosive or stricturing disease, or Barrett’s oesophagus, treatment with a PPI usually needs to be maintained at the minimum effective dose.10

If GORD is unresponsive to diet and lifestyle changes in pregnant women, antacids or alginates can be used. If this is ineffective, ranitidine, the H2-receptor antagonist may also be taken. Omeprazole is reserved for pregnant women with severe or complicated reflux disease.

GORD is common in infancy, but most symptoms resolve without treatment between 12 and 18 months. Mild to moderate reflux without complications in infants can usually be managed by changing the frequency and volume of feed, or a thickened formula feed can be used if advised by a dietician. If necessary, suitable alginate preparations can be used instead of thickened feeds.For older children, lifestyle changes may be helpful, followed if necessary by an alginate-containing preparation.

Infants or children who do not respond to these measures, or who have complications such as oesophagitis or a respiratory disorder, need to be referred to hospital, as a H2-receptor antagonist may be required to reduce acid secretion. Omeprazole may be required if the oesophagitis is resistant to the H2-receptor blockade.10

Antacids containing aluminium or magnesium compounds can often relieve symptoms in ulcer, dyspepsia, and non-erosive GORD. Antacids are best given when symptoms occur or are expected — usually between meals and at bedtime. Conventional doses of liquid magnesium aluminium antacids three-to-four times daily promote ulcer healing, but are not as effective as antisecretory medication. Magnesium-containing antacids tend to be laxative in nature, while aluminium-containing antacids can be constipating. Antacid products containing both magnesium and aluminium can reduce these colonic side-effects.

Sodium bicarbonate should no longer be prescribed alone for the relief of dyspepsia, but is present as an ingredient in many indigestion remedies. Bismuth-containing antacids are not recommended, as absorbed bismuth can be neurotoxic. Calcium-containing antacids can induce rebound acid secretion, and prolonged high doses can cause hypercalcemia and alkalosis. Simeticone added to an antacid is an anti-foaming agent to relieve flatulence, and can be useful for the relief of hiccups in palliative care. Antacids should not be taken at the same time as other medication, as they may impair absorption and damage the enteric coating of other drugs.10

Caution must always be maintained with the use of H2-receptor antagonists and PPIs as they can mask the symptoms of gastric cancer. Care is required in patients presenting with alarm features. In such cases, malignancy should be outruled before treatment commences. Side-effects of H2-receptor antagonists include diarrhoea, headache, and dizziness, and the H2-receptor antagonist cimetidine should be avoided in patients stabilised on warfarin, phenytoin, and theophylline.

Side-effects of PPIs include GI disturbances, dizziness, headache, and sleep disturbances. Patients at risk of osteoporosis on PPIs should maintain an adequate intake of calcium and vitamin D, and if necessary, receive other preventative therapy. Long-term use of PPIs has been linked to complications, such as vitamin and mineral malabsorption, pernicious anaemia, gastrointestinal infections, gastric cancer, and dementia.8,10

Surgical treatment for severe GORD, recommended only for those who do not improve with PPIs, includes Nissen fundoplication, LINX (an implanted device around the lower end of the oesophagus), magnetic sphincter augmentation, and transoral incisionless fundoplication. The Nissen fundoplication procedure involves the upper part of the stomach being wrapped around the lower oesophageal sphincter to strengthen the sphincter, prevent acid reflux, and to repair a hiatal hernia. Uncertainty surrounds the benefits of surgery versus long-term medical management with PPIs, and GORD patients with no response to PPIs are less likely to do better after surgery.1,11

Key points

GORD is a common disorder, affecting up to 33 per cent of the population worldwide.12 It is one of the most frequent conditions encountered in primary care. Treatment and management of symptoms is important, and early intervention has the potential to reduce serious complications. The prevalence of GORD continues to rise with increasing obesity levels globally. The mainstay of treatment involves lifestyle modifications, including weight loss, dietary changes, and mealtime practices. Patients in whom lifestyle modifications are ineffective in controlling GORD symptoms can benefit from pharmacologic therapy.13

The goal of treatment is to effectively control symptoms, prevent complications, and improve the patient’s quality-of-life. The goal of anti-reflux treatment is to effectively control GORD symptoms, prevent complications of GORD, and improve quality-of-life. Special attention should focus on reducing the rate of refractory GORD and complications such as Barrett’s oesophagus and adenocarcinoma.

Knowledge and understanding of the safe and effective use of medications in the treatment of GORD, especially PPIs, prevents inappropriate use, and addresses their adverse reactions and interactions with other medications. The clinical benefits and risks of using PPIs should be evaluated for each patient. Assessment, monitoring, audit, and evaluation for disease activity, progression, and effects of the therapeutic regime on a patient with GORD is important, and a continuous process.

For patients requiring long-term PPI therapy the clinical effects should be reviewed regularly and treatment adjusted as required. The lowest dose of a PPI that controls symptoms should be used. Implementing person-centred care, monitoring and evaluating symptoms, outcomes, and responses to therapy plays a pivotal role in managing the illness and improving the patient’s quality-of-life.

References

  1. Antunes C, Aleem A, Curtis S. Gastro-oesophageal reflux disease. USA: StatPearls Publishing; 2022. Available at: www.ncbi.nlm.nih.gov/books/NBK441938/.
  2. Zuckerman M, Carrion A. Gastro-oesophageal reflux disease. BMJ Best Practice. Available at: www.bestpractice.bmj.com/topics/en-gb/82.
  3. Keung C, Hebbard G. The management of gastro-oesophageal reflux disease. Aust Prescr. 2016 Feb;39(1):6-10.
  4. Nidirect. Heartburn and gastro-oesophageal reflux disease (GORD). UK: NHS; 2020. Available at: www.nidirect.gov.uk/conditions/heartburn-and-gastro-oesophageal-reflux-disease-gord.
  5. O Morain C.Management of GORD. Ireland: Medical Independent; 2019. Available at: www.medicalindependent.ie/clinical-news/management-of-gord/.
  6. Richter JE, Rubenstein JH. Presentation and epidemiology of gastroesophageal reflux disease. Gastroenterology. 2018;154(2):267-276.
  7. NHS Inform. Gastro-oesophageal reflux disease (GORD). UK: NHS; 2020. Available at: www.nhsinform.scot/illnesses-and-conditions/stomach-liver-and-gastrointestinal-tract/gastro-oesophageal-reflux-disease-gord/.
  8. National Health Service. Heartburn and acid reflux. UK: NHS; 2022. Available at: www.nhs.uk/conditions/heartburn-and-acid-reflux/.
  9. Health Service Executive. Heartburn and acid reflux. Ireland: HSE; 2021. Available at: www2.hse.ie/conditions/heartburn-and-acid-reflux.
  10. Joint Formulary Committee. Gastro-oesophageal reflux disease. British National Formulary 86, September 2023 – March 2024. UK: British Medical Association, Royal Pharmaceutical Society.
  11. Clarrett DM, Hachem C. Gastroesophageal reflux disease (GERD). Mo Med. 2018;115(3):214-218.
  12. Zhang T, Zhang B, Tian W, et al. Trends in gastroesophageal reflux disease research: A bibliometric and visualised study. Front Med (Lausanne). 2022;9:994534.
  13. Kröner PT, Cortés P, Lukens FJ. The medical management of gastroesophageal reflux disease: A narrative review. Journal of Primary Care & Community Health. 2021;12.
  14. Health Service Executive. Proton pump inhibitors (PPIs) for the treatment of gastro-oesophageal reflux disease (GORD). Ireland: HSE; 2019. Available at: www.hse.ie/eng/services/publications/clinical-strategy-and-programmes/ppis-for-treatment-of-gord-prescribing-tips-and-tools.pdf.

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