Metformin is an oral antihyperglycaemic medicine of the biguanide class and is considered first-line pharmacotherapy for type 2 diabetes mellitus (T2DM) in most European guidelines when diet and exercise alone are insufficient. Its glucose-lowering effect is primarily mediated by a reduction in hepatic gluconeogenesis (decreased hepatic glucose output), along with improved peripheral insulin sensitivity (increased glucose uptake in skeletal muscle and adipose tissue) and a modest effect on intestinal glucose absorption. Unlike sulfonylureas or insulin, metformin does not stimulate insulin secretion and therefore has a very low risk of hypoglycaemia when used alone. It is weight-neutral or associated with mild weight loss, and has favourable effects on surrogate markers such as fasting glucose, HbA1c, and lipid parameters (often small reductions in LDL and triglycerides).
Mechanistically, metformin activates AMP-activated protein kinase (AMPK) and influences cellular energy balance, mitochondrial respiratory chain activity, and signalling pathways involved in glucose and lipid metabolism. Clinically meaningful HbA1c reductions are commonly in the range of ~0.8–1.5% as monotherapy, with additive benefits when combined with other agents (GLP-1 receptor agonists, SGLT2 inhibitors, DPP-4 inhibitors, basal insulin, etc.). Beyond glycaemia, metformin may confer cardiovascular and renal benefits when used as part of comprehensive risk reduction including blood pressure/lipid management, smoking cessation, and weight optimisation.
Metformin is available as immediate-release (IR) tablets typically dosed two or three times daily with meals, and as modified-release (MR/XR) formulations dosed once daily (often with the evening meal) to improve GI tolerability and adherence. Gastrointestinal side effects are common at initiation but usually improve with slow titration and meal-time dosing. The most serious but rare adverse event is lactic acidosis; appropriate patient selection (especially by renal function) and peri-procedure precautions minimise this risk.
Metformin is not a substitute for lifestyle therapy. All patients benefit from nutrition counselling, regular physical activity, sleep optimisation, and management of comorbidities (hypertension, dyslipidaemia). Individualised HbA1c targets should be set (often ≤7.0% for many adults, with looser or tighter targets based on age, comorbidity, and hypoglycaemia risk).
Clinicians typically recheck HbA1c at ~3 months after initiation/titration. If targets are not met, options include further titration, switching to MR, or adding another class (GLP-1 RA or SGLT2 inhibitor often preferred when weight loss or cardiorenal benefit is needed).
Metformin’s safety profile is well established. The majority of adverse effects are gastrointestinal and dose-dependent, usually transient with gradual titration. Serious events are uncommon with appropriate patient selection.
Hypoglycaemia: Metformin alone rarely causes hypoglycaemia. The risk increases when combined with insulin or insulin secretagogues (e.g., sulfonylureas); in combined therapy, counsel on recognition and management of hypoglycaemia.
Patients should receive sick-day guidance: maintain hydration, monitor blood glucose more closely, and seek advice early if vomiting, diarrhoea, or fever lead to reduced intake; temporary dose interruption may be advised.
Metformin is renally eliminated (tubular secretion). It is not metabolised by CYP450, so pharmacokinetic interactions are fewer than with many agents. Clinically relevant interactions arise via effects on renal function/secretion, glycaemic control, or lactic acidosis risk.
Always provide an up-to-date medication and supplement list to your clinician and pharmacist. Check new medicines for OCT/MATE transporter and renal effects.
Missed dose: Take it as soon as remembered if within a few hours of the scheduled time and with food. If it is close to the next dose, skip the missed dose and resume your normal schedule. Do not double doses.
Accidental double dose: Often causes GI upset (nausea, diarrhoea) but is usually not dangerous if renal function is normal. Maintain hydration, monitor glucose, and contact a pharmacist/clinician if symptoms are troublesome. Do not take extra doses to compensate.
Large overdose / toxicity: Risk of lactic acidosis rises, particularly with renal impairment or co-morbid hypoxia/sepsis. Symptoms: profound fatigue, muscle pain, rapid breathing, abdominal pain, hypothermia, hypotension, confusion. Emergency care is required. Management is supportive; severe cases may require haemodialysis to remove metformin and correct acidosis. Bring the container to hospital.
Always read the label and follow your prescriber’s instructions. Seek urgent help for red-flag symptoms (progressive vomiting, dehydration, laboured breathing, chest pain, severe weakness).
The information provided on this website is for general educational purposes only and is not a substitute for professional medical advice, diagnosis, or treatment. Always seek the advice of your doctor, pharmacist, or other qualified health provider with any questions you may have regarding a medical condition or medication. Do not disregard professional medical advice or delay seeking it because of something you have read here. We do not take responsibility for any loss, damage, or injury caused by this information.