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Telmisartan & Metoprolol in Hypertension & CV Care Continuum: 5 Key Points on India's Most Widely Utilized ARB & Beta Blocker

Written By : NAVANIL BISWAS Published On 2026-07-14T10:45:18+05:30  |  Updated On 14 July 2026 11:27 AM IST
Telmisartan & Metoprolol in Hypertension & CV Care Continuum: 5 Key Points on Indias Most Widely Utilized ARB & Beta Blocker
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If there is one mistake we continue to make with hypertension, it is reducing it to a number. In practice, hypertension rarely presents as isolated BP elevation; it reflects broader cardiovascular disruption involving vascular dysfunction, sympathetic overactivity, metabolic risk, and evolving coronary disease. Accordingly, therapy has shifted from BP lowering alone to overall risk modification. In India, fixed-dose combinations support adherence, 1 with emerging evidence for telmisartan–metoprolol efficacy and tolerability. 2

Prescribing patterns mirror this logic: telmisartan remains a preferred ARB, while metoprolol continues to be widely used. 3, 4 The following five key points highlight where telmisartan and metoprolol stand today and why they continue to matter in real-world clinical practice:

1. Telmisartan–Metoprolol: A Widely Utilized ARB–BB Approach in Young Hypertensive Patients in India

Hypertension in young adults in India is increasingly recognized, often characterized by heightened sympathetic activity and early cardiometabolic risk. 5 In this setting, telmisartan and metoprolol are among the preferred choices within their classes, reflecting their combined utility in addressing blood pressure, heart rate and metabolic components. 6 Indian Physician clinical surveys further indicate frequent use of the telmisartan–metoprolol combination in younger patients, particularly when hypertension coexists with early cardiovascular risk or markers of sympathetic overdrive. This underscores a broader move toward phenotype-driven therapy, where treatment is aligned with the patient’s evolving cardiovascular risk profile rather than addressing BP values alone. 5, 6

Prospective multi-centric Indian evidence (n≈90) supports use of telmisartan–metoprolol FDC in essential hypertension, showing clinic and ambulatory BP reductions of ~18–22/10–12 mmHg over 8–12 weeks. ABPM confirmed improved 24-hour control, with reduced variability index and increased smoothness index (SI >1), indicating sustained BP lowering. The regimen was well tolerated with no major safety concerns. 2

2. Telmisartan–Metoprolol: Standing the Test of Time in 2026

The sustained relevance of the telmisartan–metoprolol combination is supported by both real-world utilization and clinical evidence.

Metoprolol: Preferred Beta Blocker in 2026: Indian physician-based data from the ROBUST survey (JAPI, 2026), involving 1000 HCPs, demonstrated sustained β-blocker preference across the cardiovascular continuum. >70% of respondents reported routine β-blocker use, with metoprolol emerging as a preferred agent across indications, including hypertension with coexisting ischemic heart disease. A substantial proportion also identified metoprolol as a first-line or early add-on option, reflecting its established efficacy and real-world versatility. 7

Telmisartan: High Physician Rated Efficacy in 2026: The TACT-India study, a prospective multicenter evaluation of the telmisartan–amlodipine fixed-dose combination across 982 centers (n=5,363), demonstrated significant BP reductions over 8 weeks, with SBP decreasing from 155.1 to 136.0 mmHg and DBP from 104.5 to 88.4 mmHg (P<0.0001). Approximately 70% of patients achieved target BP <140/90 mmHg, with high physician-rated efficacy and tolerability (>99%). These findings support the effectiveness of telmisartan-based combination therapy in routine Indian practice. 8

3.Relevance in the Cardio-Metabolic Interface

The coexistence of hypertension with metabolic dysfunction, particularly metabolic dysfunction–associated steatotic liver disease (MASLD), is increasingly recognized as a major cardiovascular risk driver. In this context, telmisartan has emerged as a clinically differentiated ARB. A large retrospective, propensity score–matched cohort analysis using the TriNetX global network (ACC 2026, JACC poster presentation) evaluated CV outcomes in patients with MASLD treated with telmisartan versus other ARBs over a ~5-year follow-up, with matching for demographics, comorbidities, and background therapies. Telmisartan use was associated with an approximately 45% reduction in MACE, with consistent reductions across IHD (~36%), arrhythmia (~44%), stroke (~43%), and heart failure (~41%). 9

Mechanistically, telmisartan’s partial PPAR-γ agonistic activity confers additional metabolic effects, linking RAAS blockade with improved insulin sensitivity and lipid regulation; relevant in India’s growing burden of obesity, diabetes, and dyslipidemia. 10

4. Metoprolol: Most Utilized Beta-Blocker in the Landmark BETAMI–DANBLOCK Trial

The landmark BETAMI–DANBLOCK trial (NEJM, 2025) re-evaluated the role of beta-blockers in post–myocardial infarction patients with preserved or mildly reduced left ventricular ejection fraction (LVEF ≥40%). In this randomized study of ~5,500 patients, long-term beta-blocker therapy—predominantly metoprolol—was compared with no beta-blocker use. Over a median follow-up of ~3.5 years, beta-blocker therapy resulted in a significant reduction in the composite of death or major adverse cardiovascular events (14.2% vs 16.3%), with a notable reduction in recurrent myocardial infarction. 11

The predominant use of metoprolol in this trial reinforces its continued clinical relevance, supporting β1-selective blockade as an effective strategy in contemporary post-MI management.

5. Metoprolol: Emerging Safety Signals Across Specific Clinical Scenarios

Recent pharmacovigilance and comparative data have appraised the safety profile of metoprolol across high-risk settings. A FAERS database analysis (2025) evaluating >250,000 β-blocker–related adverse events, including ~4,100 asthma-related cases, demonstrated class heterogeneity, with metoprolol showing a lower reporting odds ratio for asthma-related events compared with agents such as bisoprolol. 12

Similarly, recent comparative data on beta blockers in atrial fibrillation patients on oral anticoagulation indicate a more favorable safety profile with metoprolol versus bisoprolol, particularly with respect to bleeding and composite adverse outcomes. 13

Together, these findings support a shift toward molecule-specific safety considerations, reinforcing the clinical relevance of metoprolol in complex and high-risk patient populations.

Key Takeaways

Hypertension management needs to extend beyond BP reduction to a phenotype-based approach, where consideration of widely accepted combinations such as telmisartan and metoprolol helps address vascular, metabolic, and sympathetic components together, supporting more consistent cardiovascular risk control in routine practice.

** BP: blood pressure, ARB: angiotensin receptor blocker, BB: beta blocker, FDC: fixed dose combination, ABPM: ambulatory blood pressure monitoring, HCP: healthcare professionals, MACE: major adverse cardiovascular events, IHD: ischemic heart disease, PPAR-γ: peroxisome proliferator-activated receptor gamma, MI: myocardial infarction, RAAS: renin angiotensin-aldosterone system

References:
  • 1. Central Drugs Standard Control Organization (CDSCO). (2011). Approved Fixed Dose Combinations (FDC) List. Directorate General of Health Services, Ministry of Health and Family Welfare, Government of India. -
  • 2.Ahire, Prachi1; Sharma, Kamal2; Chhaya, Gaurav3; Chopda, Manoj4; Kaul, Upendra5; Agarwal, Manish6; Dorairaj, Prabhakar7; Dharmadhikari, Shruti1; Bharathi, Prakadeesh1; Khandhedia, Chintan1; Markandeywar, Neeraj1; Mane, Amey1; Mehta, Suyog1; Joglekar, Sadhna8. EFFICACY AND SAFETY OF METOPROLOL+TELMISARTAN FDC IN ESSENTIAL HYPERTENSION: TREATMENT ON VARIABILITY INDEX AND SMOOTHNESS INDEX ANALYSES ASSESSED BY AMBULATORY BP MONITORING. Journal of Hypertension -
  • 3.Kathiresan, M., Saxena, A., Tripathy, P., Tripathi, S., & Upendra, G. (2023). Management of hypertensive patients with ischemic heart disease and the role of a fixed-dose combination of telmisartan and metoprolol: a physician-based research survey. International Journal of Advances in Medicine 10 -
  • 4.Rajadhyaksha GC, Reddy H, Singh AK, et al. The Indian REgistry on Current Patient PrOfiles and TReatment TrenDs in Hypertension (RECORD): Final Outcomes of the Real-World Observational Study. J Assoc Physicians India -
  • 5.Jadhav U, Tiwaskar M, Khan A, Kalmath BC, Ponde CK, Sawhney JP, Tripathy MP, Hazra PK, Sahoo PK, Routray SN, Chandra S. Hypertension in young adults in India: Perspectives and therapeutic options amongst clinician's in a cross sectional observational study. The Journal of the Association of Physicians of India. 69-
  • 6.Jadhav U, Solanki D, Kumar S, Hazra P, Alexander T, Gupta A, Ghatge S, Revankar S. Obesity and Sympathetic Overactivity in Young Individuals With Hypertension: Clinical Perspective of Indian Healthcare Providers. 11 16 -
  • 7.Hiremath J, Dasbiswas A, Sawhney J, et al. Role of β-Blockers Across the Cardiovascular Continuum: A Real-World Perception Survey (ROBUST). J Assoc Physicians India 74 -
  • 8.Das AK, Tiwaskar M, Abdullakutty J, Pande A, Kumar V, Francis F, Zalte N, Sugumaran A, Sawant S, Mohanasundaram S. Evaluation of Effectiveness and Safety of Telmisartan and Amlodipine Fixed-Dose Combination in Indian Patients with Hypertension: TACT-India Study. Drugs Real World Outcomes. 13 -
  • 9.Sivakumar, N., Danpanichkul, P., & Sripusanapan, A. (2026). cardiovascular benefits of telmisartan in metabolic dysfunction associated steatotic liver disease. JACC -
  • 10.Imenshahidi M, Roohbakhsh A, Hosseinzadeh H. Effects of telmisartan on metabolic syndrome components: a comprehensive review. Biomedicine & pharmacotherapy. Biomedicine and Pharmacotherapy -
  • 11.Munkhaugen J, Kristensen AMD, Halvorsen S, Holmager T, Olsen MH, Bakken A, Sehested TSG, Ruddox V, Mæng M, Vikenes K, Jensen SE, Steigen T, Lambrechtsen J, Jortveit J, Bovin A, Schirmer H, Christiansen MK, Wiseth R, Mikkelsen D, Larsen AI, Lyngby Kjærgaard C, Andresen K, Gustafsson I, Tuseth V, Larsen ML, Deeg PS, Veien K, Bøhmer E, Bøtker HE, Brattrud AO, Brønnum-Schou J, Pettersen AR, Bang LE, Øie E, Engstrøm T, Borg EB, Kristensen K, Nymo SH, Gislason G, Vethe NT, Abdulla JAM, Dammen T, Mouridsen MR, Bendz B, Bertelsen MLN, Hove JD, Schierbeck L, Snoer M, Davidsen C, Egholm G, Thomsen KK, Jadou G, Poenaru M, Krarup NT, Böttcher M, Stæhr PB, Zwisler AD, Edvardsen T, Torp-Pedersen C, Otterstad JE, Lange T, Fagerland MW, Atar D, Prescott E; BETAMI–DANBLOCK Investigators. Beta-blockers after myocardial infarction in patients without heart failure. New England Journal of Medicine. 393 -
  • 12.Cazzola M, Ora J, Calzetta L, Rogliani P, Matera MG. β-Blockers and Asthma: Surprising findings from the FAERS database. Respiratory Medicine. -
  • 13.Ömür SE, Tapar GG, Zorlu Ç, Karaman K, Demirezen Y. Effect of metoprolol and bisoprolol on bleeding rates in patients with atrial fibrillation. Cardiovasc J Afr. 36 -
metosartantelmisartanmetoprololcardiovascularbeta blockersangiotensin receptor blockerarbhypertension
NAVANIL BISWAS
NAVANIL BISWAS

    Dr Navanil Biswas is an Interventional Cardiologist based in Kolkata with expertise in complex coronary interventions, chronic total occlusions (CTO), and imaging-guided PCI using OCT, IVUS, and FFR/iFR. Trained at premier institutes, including Mount Sinai, New York, he is actively involved in cardiovascular research and education, with multiple international publications, book chapters, and presentations at leading global cardiology conferences such as ACC, ESC, and TCT.

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