CELL DEATH REGULATION BY MAMS: FROM MOLECULAR MECHANISMS TO THERAPEUTIC IMPLICATIONS IN CARDIOVASCULAR DISEASES

Cell death regulation by MAMs: from molecular mechanisms to therapeutic implications in cardiovascular diseases

Cell death regulation by MAMs: from molecular mechanisms to therapeutic implications in cardiovascular diseases

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Abstract The endoplasmic qn85q80aafxza reticulum (ER) and mitochondria are interconnected intracellular organelles with vital roles in the regulation of cell signaling and function.While the ER participates in a number of biological processes including lipid biosynthesis, Ca2+ storage and protein folding and processing, mitochondria are highly dynamic organelles governing ATP synthesis, free radical production, innate immunity and apoptosis.Interplay between the ER and mitochondria plays a crucial role in regulating energy metabolism and cell fate control under stress.The mitochondria-associated membranes (MAMs) denote physical contact sites between ER and mitochondria that mediate bidirectional communications rosaliac ar intense visible facial redness serum between the two organelles.Although Ca2+ transport from ER to mitochondria is vital for mitochondrial homeostasis and energy metabolism, unrestrained Ca2+ transfer may result in mitochondrial Ca2+ overload, mitochondrial damage and cell death.

Here we summarize the roles of MAMs in cell physiology and its impact in pathological conditions with a focus on cardiovascular disease.The possibility of manipulating ER-mitochondria contacts as potential therapeutic approaches is also discussed.

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