Fimasartan acts on the kidney's rennin-angiotensin cascade, which begins when renin release from the kidney causes the breakdown of angiotensinogen into angiotensin I. Angiotensin-converting enzyme then catalyzes the reaction that forms angiotensin II, which acts on AT1 receptors on the blood vessels, heart, and kidneys. On blood vessels, the AT1 receptor is coupled to an intracellular pathway that causes smooth muscle contraction of blood vessels. In blocking the AT1 receptor, fimasartan inhibits vasoconstriction, favouring vasodilation. At the kidney and adrenal gland, AT1 blockage and prevention of aldosterone formation increase excretion of water and salt by the kidneys, which decreases overall blood volume. At the heart, AT1 blockage decreases contractility and the stimulatory effects of the sympathetic nervous system. Collectively, fimasartain leads to a reduction in blood pressure and alleviation of hypertensive symptoms. ARBs like fimasartan have also shown to be protective against stroke, myocardial infarction, and heart failure. Fimasartan has been shown to reduce cardiac hypertrophy, fibrosis, remodelling, and unnecessary cell proliferation via blockage of AT1 activation conceivably through decreased Endothelin 1 production, a result of AT1 activation. Fimastartan can also block TGF-β1 production, which contributes to fibrosis and ventricular damage post-infarct. After ARB administration, mice showed improved prognosis after a myocardial infarction, though further studies still need to be done to assess fimasartan's specific effects on decreasing cardiovascular damage.
Side effects
Side effects In clinical trials, fimasartan was well tolerated in all patients. However, higher dosing was accompanied by increased dizziness and headaches in a low number of patients. Other side effects such as diarrhea, syncope, and cold feet were also experienced in a low number of subjects, which all resolved without medical intervention.
Pharmacology
Fimasartan is rapidly absorbed and has minimal accumulation in the body 7 days after administration. Fimasartan possesses a half-life of 9 to 16 hours, appropriate for daily dosing. Fimasartan was found to be effective in fasted or fed states, with a variety of dosing regimens. In trials, the maximum effects of the drug occurred slightly after the maximum plasma concentration was achieved, which occurs 30 minutes to 3 hours after dosing. Fimasartan was found mostly in unmetabolized form in the plasma and in bile excretions. Urinary elimination of the drug was low, at less than 3% 24 hours after administration, entailing that the fimasartan does not undergo renal excretion.
