Increased Transport of Acetyl-CoA into the Endoplasmic Reticulum Causes a Progeria-like Phenotype

Overview

Journal Aging Cell

Specialties Cell Biology
Geriatrics

Date 2018 Jul 28

PMID 30051577

Citations 31

Authors

Yajing Peng

Samantha L Shapiro

Varuna C Banduseela

Inca A Dieterich

Kyle J Hewitt

Emery H Bresnick

Guangyao Kong

Jing Zhang

Kathryn L Schueler

Mark P Keller

Alan D Attie

Timothy A Hacker

Ruth Sullivan

Elle Kielar-Grevstad

Sebastian I Arriola Apelo

Dudley W Lamming

Rozalyn M Anderson

Luigi Puglielli

Affiliations

Soon will be listed here.

Abstract

The membrane transporter AT-1/SLC33A1 translocates cytosolic acetyl-CoA into the lumen of the endoplasmic reticulum (ER), participating in quality control mechanisms within the secretory pathway. Mutations and duplication events in AT-1/SLC33A1 are highly pleiotropic and have been linked to diseases such as spastic paraplegia, developmental delay, autism spectrum disorder, intellectual disability, propensity to seizures, and dysmorphism. Despite these known associations, the biology of this key transporter is only beginning to be uncovered. Here, we show that systemic overexpression of AT-1 in the mouse leads to a segmental form of progeria with dysmorphism and metabolic alterations. The phenotype includes delayed growth, short lifespan, alopecia, skin lesions, rectal prolapse, osteoporosis, cardiomegaly, muscle atrophy, reduced fertility, and anemia. In terms of homeostasis, the AT-1 overexpressing mouse displays hypocholesterolemia, altered glycemia, and increased indices of systemic inflammation. Mechanistically, the phenotype is caused by a block in Atg9a-Fam134b-LC3β and Atg9a-Sec62-LC3β interactions, and defective reticulophagy, the autophagic recycling of the ER. Inhibition of ATase1/ATase2 acetyltransferase enzymes downstream of AT-1 restores reticulophagy and rescues the phenotype of the animals. These data suggest that inappropriately elevated acetyl-CoA flux into the ER directly induces defects in autophagy and recycling of subcellular structures and that this diversion of acetyl-CoA from cytosol to ER is causal in the progeria phenotype. Collectively, these data establish the cytosol-to-ER flux of acetyl-CoA as a novel event that dictates the pace of aging phenotypes and identify intracellular acetyl-CoA-dependent homeostatic mechanisms linked to metabolism and inflammation.

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