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Pathway Description
Candesartan Action Pathway (New)
Homo sapiens
Drug Action Pathway
Candesartan is angiotensin receptor blocker (ARB) which block the action of angiotensin II by binding to the type 1 angiotensin II receptor. Angiotensin II is a critical circulating peptide hormone that has powerful vasoconstrictive effects and increases blood pressure. Candesartan is used to treat hypertension as it reduces blood pressure. Angiotensin has many vasoconstrictive effects by binding to angiotensin II type 1 receptors (AT1) in blood vessels, kidneys, hypothalamus, and posterior pituitary.
In blood vessels AT1 receptors cause vasoconstriction in the tunica media layer of smooth muscle surrounding blood vessels increasing blood pressure. Blocking this AT1 receptor lowers the constriction of these blood vessels. AT1 receptors in the kidney are responsible for the production of aldosterone which increases salt and water retention which increases blood volume. Blocking AT1 receptors reduces aldosterone production allowing water retention to not increase. AT1 receptors in the hypothalamus are on astrocytes which inhibit the excitatory amino acid transporter 3 from up-taking glutamate back into astrocytes. Glutamate is responsible for the activation of NMDA receptors on paraventricular nucleus neurons (PVN neurons) that lead to thirst sensation. Since AT1 receptors are blocked, the inhibition of the uptake transporter is not limited decreasing the amount of glutamate activating NMDA on PVN neurons that makes the individual crave drinking less. This lowers the blood volume as well.
Lastly, the AT1 receptors on posterior pituitary gland are responsible for the release of vasopressin. Vasopressin is an anti-diuretic hormone that cases water reabsorption in the kidney as well as causing smooth muscle contraction in blood vessels increasing blood pressure. Lowering angiotensin II action on activating vasopressin release inhibits blood pressure from increasing.
All these effects of candesartan contribute to an overall lowered blood pressure.
The most common side effects of taking candesartan are symptomatic hypotension, abnormal renal function, and hyperkalemia. Other reported side effects include headache, back pain, angioedema, and upper respiratory tract infections, but these are very rare clinically.
References
Candesartan Pathway (New) References
Bulsara KG, Makaryus AN: Candesartan
Pubmed: 30137786
Reid I. A, Schwartz J, Maselli B. J, Keil L. C, Interactions Between Vasopressin and the Renin-Angiotensin System. The Neurohypophysis 60: 475-491, 1983.
Johren O, Golsch C, Dendorfer A, Qadri F, Hauser W, Dominiak P. Deifferential Expression of AT1 Receptors in the Pituitary and Adrenal Gland of SHR and WKY. Hypertension 31 (4): 984-990, 2003.
Mendelowitz D. How Does Angiotensin Activate Hypothalamic Neurons Essential for Controlling Sympathetic Activity and Blood Pressure?. Hypertension 68 (6): 1340-1341, 2016.
Reactome. Glutamate uptake by astrocytes. Reactome. Retrieved: https://reactome.org/content/detail/R-HSA-210439
Wishart DS, Feunang YD, Guo AC, Lo EJ, Marcu A, Grant JR, Sajed T, Johnson D, Li C, Sayeeda Z, Assempour N, Iynkkaran I, Liu Y, Maciejewski A, Gale N, Wilson A, Chin L, Cummings R, Le D, Pon A, Knox C, Wilson M: DrugBank 5.0: a major update to the DrugBank database for 2018. Nucleic Acids Res. 2018 Jan 4;46(D1):D1074-D1082. doi: 10.1093/nar/gkx1037.
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