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Publication : Succinate Can Shuttle Reducing Power from the Hypoxic Retina to the O<sub>2</sub>-Rich Pigment Epithelium.

First Author  Bisbach CM Year  2020
Journal  Cell Rep Volume  31
Issue  5 Pages  107606
PubMed ID  32375026 Mgi Jnum  J:293105
Mgi Id  MGI:6445298 Doi  10.1016/j.celrep.2020.107606
Citation  Bisbach CM, et al. (2020) Succinate Can Shuttle Reducing Power from the Hypoxic Retina to the O2-Rich Pigment Epithelium. Cell Rep 31(5):107606
abstractText  When O2 is plentiful, the mitochondrial electron transport chain uses it as a terminal electron acceptor. However, the mammalian retina thrives in a hypoxic niche in the eye. We find that mitochondria in retinas adapt to their hypoxic environment by reversing the succinate dehydrogenase reaction to use fumarate to accept electrons instead of O2. Reverse succinate dehydrogenase activity produces succinate and is enhanced by hypoxia-induced downregulation of cytochrome oxidase. Retinas can export the succinate they produce to the neighboring O2-rich retinal pigment epithelium-choroid complex. There, succinate enhances O2 consumption by severalfold. Malate made from succinate in the pigment epithelium can then be imported into the retina, where it is converted to fumarate to again accept electrons in the reverse succinate dehydrogenase reaction. This malate-succinate shuttle can sustain these two tissues by transferring reducing power from an O2-poor tissue (retina) to an O2-rich one (retinal pigment epithelium-choroid).
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