MK-677 vs Telmisartan

Well Studied vs FDA Approved

avoid Mechanism-based · 64% Both MK-677 and Telmisartan carry hepatotoxic risk. Combining hepatotoxic compounds significantly increases liver damage potential. If unavoidable, include liver support (TUDCA/NAC) and monitor ALT/AST frequently.

Molecular Data

MK-677 Telmisartan

Weight 624.77 Da 514.62 Da

Half-life ~24 hours ~24 hours

Type Non-peptide ghrelin receptor agonist Benzimidazole derivative (C33H30N4O2)

Key Benefits

MK-677

01 97% increase in 24-hour growth hormone secretion

02 40-72% elevation in IGF-1 levels

03 Enhanced sleep quality with improved REM patterns

04 Preferential lean tissue gains of 1.1-2.7kg over 8-12 months

05 15% basal metabolic rate increase within 2 weeks

06 Oral administration (no injections required)

Telmisartan

01 Potent 24-hour blood pressure reduction with once-daily dosing

02 Protection against AAS-induced left ventricular hypertrophy and cardiac remodeling

03 Nephroprotection through reduced intraglomerular pressure and proteinuria

04 Unique partial PPAR-gamma agonism improving insulin sensitivity and lipid metabolism

05 No negative impact on exercise performance, VO2 max, or recovery

06 Reduction of pathological vascular remodeling and arterial stiffness

07 Longest half-life of all ARBs ensuring consistent 24-hour coverage

08 Well-tolerated with a low incidence of side effects compared to ACE inhibitors (no dry cough)

Side Effects

MK-677

Appetite stimulation (>50% of users)

Water retention (30-40%)

Lethargy (20-30%)

Fasting glucose elevation (5-15mg/dL)

Note on testosterone suppression: at doses up to 20 mg daily, MK-677 is unlikely to cause significant testosterone suppression on its own. Above 20 mg daily, the likelihood of suppression and other side effects (insulin resistance, water retention, lethargy) increases. The case report documenting 85.7% testosterone suppression involved co-administration with LGD-4033, a SARM known to be profoundly suppressive, making the SARM the likely primary driver of that suppression.

Telmisartan

Dizziness or lightheadedness, particularly during the first few days or after dose increases

Mild hypotension, especially in volume-depleted individuals or those on concurrent antihypertensives

Upper respiratory tract infection symptoms (sinusitis, pharyngitis) - reported in clinical trials at rates similar to placebo

Back pain and myalgia (uncommon but reported)

Fatigue

Contraindications

Heart disease or congestive heart failure

Diabetes or pre-diabetes

Active cancer

Severe cardiovascular disease

Pregnancy or breastfeeding

Pregnancy (Category D - can cause fetal injury and death; discontinue immediately if pregnancy is detected)

Bilateral renal artery stenosis

Known hypersensitivity to telmisartan or any excipients

Concurrent use with aliskiren in patients with diabetes or renal impairment (eGFR <60)

Severe hepatic impairment or biliary obstruction (telmisartan is eliminated primarily via biliary excretion)

Research Evidence

MK-677 Telmisartan

Status Well Studied FDA Approved

References 7 studies 5 studies

Latest July 2024 2023

FDA Approved No Yes

Full MK-677 profile Full Telmisartan profile MK-677 calculator Telmisartan calculator

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This comparison is for educational and research purposes only. Consult a healthcare professional before use.