ARBs (Angiotensin Receptor Blockers)
Also known as: angiotensin receptor blockers, ARB
Medically reviewed by Nano Health Insights Editorial Team · Last reviewed 2026-06-24
ARBs are blood pressure medicines that block the angiotensin II type 1 receptor and are not safe in pregnancy.
What it is
ARBs are blood pressure medicines that block the angiotensin II type 1 receptor and are not safe in pregnancy. Angiotensin receptor blockers, also called angiotensin II receptor blockers, are a drug class used mainly for hypertension, heart failure, and chronic kidney disease, especially when kidney protection is needed. A key practical fact is that ARBs are contraindicated during pregnancy because drugs acting on the renin-angiotensin system can harm the fetus.
ARBs are often chosen when a person cannot tolerate an ACE inhibitor, especially because ACE inhibitors more commonly cause a dry cough. Common ARBs include losartan, valsartan, telmisartan, olmesartan, candesartan, and irbesartan. They lower blood pressure and can reduce protein loss in urine in some people with kidney disease, including diabetic kidney disease.
A quick comparison:
| Feature | ARBs |
|---|---|
| Main target | Angiotensin II type 1 (AT1) receptor |
| Main uses | Hypertension, heart failure, chronic kidney disease |
| Common advantage vs ACE inhibitors | Less cough |
| Important risks | High potassium, low blood pressure, kidney function changes |
| Major contraindication | Pregnancy |
In India, ARBs are widely used in routine hypertension care along with other first-line drug classes. Choice of medicine depends on blood pressure level, kidney function, diabetes status, heart disease, age, and cost.
How it works
ARBs block the action of angiotensin II at the AT1 receptor. Angiotensin II is part of the renin-angiotensin-aldosterone system, which helps regulate blood pressure, blood vessel tone, sodium balance, and fluid retention.
When angiotensin II binds to the AT1 receptor, it causes blood vessels to constrict and stimulates aldosterone release from the adrenal glands. Aldosterone makes the kidneys retain sodium and water and excrete potassium. By blocking this pathway, ARBs:
- Relax blood vessels, which lowers blood pressure.
- Reduce aldosterone effects, which can decrease sodium and water retention.
- Lower pressure inside the kidney's filtering units, which may reduce albumin or protein in urine.
- Reduce strain on the heart in some patients with heart failure.
Unlike ACE inhibitors, ARBs do not block the breakdown of bradykinin. That is one reason cough is generally less common with ARBs. However, ARBs can still cause serious adverse effects, including hyperkalemia and worsening kidney function in susceptible patients.
Evidence and uses
ARBs are established medicines with strong evidence for several cardiovascular and kidney-related uses. Their blood pressure-lowering effect is broadly comparable to other major antihypertensive classes, and they are commonly used alone or in combination with a calcium channel blocker or thiazide-type diuretic.
Main evidence-based uses include:
| Condition | Role of ARBs |
|---|---|
| Hypertension | First-line option in many adults |
| Heart failure with reduced ejection fraction | Used in selected patients, especially if ACE inhibitors are not tolerated |
| Chronic kidney disease with albuminuria | Can reduce proteinuria and slow progression in some patients |
| Diabetic nephropathy | Often used when albuminuria is present |
For hypertension, ARBs lower blood pressure effectively and are generally well tolerated. For chronic kidney disease, especially when albuminuria is present, they can help protect kidney function over time. For heart failure, some ARBs have outcome data supporting reduced hospitalization or symptom improvement in appropriate patients.
Not all ARBs are identical in approved indications, dosing schedules, or trial evidence. For example, losartan has uricosuric effects that may matter in some patients with gout, while telmisartan has a long half-life. These differences can influence prescribing, but the overall class effect remains similar for blood pressure control.
ARBs should not usually be combined with an ACE inhibitor or with the direct renin inhibitor aliskiren in many patients because dual blockade increases the risk of kidney injury, hypotension, and hyperkalemia without clear added benefit for most people.
Safety and interactions
ARBs are usually well tolerated, but they still require monitoring. The most important safety issues are high potassium, low blood pressure, and changes in kidney function.
Common or important adverse effects include:
- Dizziness or lightheadedness
- Low blood pressure, especially after starting treatment or increasing the dose
- Hyperkalemia
- Rise in serum creatinine or reduced kidney function
- Rare angioedema
People at higher risk of complications include those with chronic kidney disease, dehydration, older age, heart failure, bilateral renal artery stenosis, or those taking other medicines that raise potassium.
Important interactions include:
| Interacting medicine or product | Why it matters |
|---|---|
| Potassium supplements or salt substitutes with potassium | Can raise potassium too much |
| Potassium-sparing diuretics such as spironolactone | Higher hyperkalemia risk |
| NSAIDs such as ibuprofen or diclofenac | Can worsen kidney function and blunt blood pressure control |
| Lithium | Lithium levels can rise |
| ACE inhibitors or aliskiren | Higher risk of kidney injury, hypotension, hyperkalemia |
Patients should tell their clinician about over-the-counter pain medicines, supplements, and low-sodium salts, because many salt substitutes use potassium chloride. In India and elsewhere, this is an easy interaction to miss.
Pregnancy safety is a major issue. ARBs should be stopped and reviewed urgently if pregnancy occurs or is planned. People who are breastfeeding or trying to conceive should discuss alternatives with a clinician.
When to see a clinician
See a clinician promptly if you develop fainting, severe dizziness, swelling of the face or tongue, very low urine output, or symptoms that could suggest high potassium such as marked weakness or palpitations. Routine follow-up is also important after starting an ARB or increasing the dose.
Clinicians commonly check:
- Blood pressure response
- Serum creatinine or estimated kidney function
- Serum potassium
These blood tests are often checked soon after starting therapy or after a dose change, then repeated based on the person's risk profile. Do not stop or double the medicine on your own unless a clinician tells you to, but seek advice if you have vomiting, diarrhea, dehydration, or an acute illness because temporary medicine review may be needed.
Limitations and open questions
ARBs are effective, but they are not the best choice for every patient. Some people need a different first-line drug or a combination regimen to reach blood pressure targets. Class members also differ in trial evidence, approved indications, and duration of action, so they are not perfectly interchangeable.
Evidence is strong for hypertension, selected heart failure settings, and kidney disease with albuminuria, but less certain for some proposed benefits beyond these uses. Reviews have discussed possible differences among individual ARBs, yet head-to-head superiority claims are often limited by study design and indirect comparisons.
Another limitation is that ARBs can initially raise creatinine, which may be expected in some cases but can also signal harm in others. That is why lab monitoring matters. For patients, the practical message is simple: ARBs are widely used and often well tolerated, but they should be taken under medical supervision, with attention to pregnancy risk, kidney function, potassium, and drug interactions.
FAQs
What are common examples of ARBs?
Common ARBs include losartan, valsartan, telmisartan, olmesartan, candesartan, and irbesartan. Different countries may have different brand names, but these generic names identify the drug itself. They all block the AT1 receptor, though they differ in dosing, half-life, and approved uses.
How are ARBs different from ACE inhibitors?
Both drug classes act on the renin-angiotensin system and are used for hypertension, heart failure, and kidney disease. ARBs block the angiotensin II type 1 receptor, while ACE inhibitors reduce formation of angiotensin II. A practical difference is that ARBs are less likely to cause the dry cough commonly associated with ACE inhibitors.
Do ARBs protect the kidneys?
They can, especially in people with chronic kidney disease and albuminuria, including diabetic kidney disease. ARBs reduce pressure within the kidney's filtering units and may lower urine protein. Kidney function and potassium still need monitoring because these medicines can also raise creatinine or potassium, particularly after starting treatment.
Can I take painkillers like ibuprofen with an ARB?
Use caution and ask a clinician or pharmacist first. NSAIDs such as ibuprofen and diclofenac can reduce the blood pressure-lowering effect of ARBs and increase the risk of kidney injury, especially in older adults, people with dehydration, or those with chronic kidney disease. The risk can be higher if a diuretic is also being used.
Are ARBs safe during pregnancy?
No. ARBs are contraindicated in pregnancy because they can injure the developing fetus, particularly later in pregnancy, and may affect fetal kidneys and amniotic fluid. If you are pregnant, planning pregnancy, or think you may be pregnant, contact your clinician promptly to review safer alternatives.