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Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway
Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway
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Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway
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Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway
Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway

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Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway
Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway
Paper

Intramembrane protease SPP defines a cholesterol-regulated switch of the mevalonate pathway

2021
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Overview
Intramembrane proteolysis regulates important processes such as signaling and transcriptional and posttranslational abundance control of proteins with key functions in metabolic pathways. This includes transcriptional control of mevalonate pathway genes, thereby ensuring balanced biosynthesis of cholesterol and other isoprenoids. Our work shows that, at high cholesterol levels, signal peptide peptidase (SPP) cleaves squalene synthase (SQS), an enzyme that defines the branching point for allocation of isoprenoids to the sterol and non-sterol arms of the mevalonate pathway. This intramembrane cleavage releases SQS from the membrane and targets it for proteasomal degradation. Regulation of this mechanism is achieved by the E3 ubiquitin ligase TRC8 that, in addition to ubiquitinating SQS in response to cholesterol levels, acts as an allosteric activator of SPP-catalyzed intramembrane cleavage of SQS and other substrates. Hence, SPP-TRC8 mediated abundance control of SQS acts as a metabolic switch within the mevalonate pathway.