The MTORC1/4E-BP Pathway Coordinates Hemoglobin Production with L-leucine Availability

Overview

Journal Sci Signal

Specialties Cell Biology
Physiology
Science

Date 2015 Apr 16

PMID 25872869

Citations 42

Authors

Jacky Chung

Daniel E Bauer

Alireza Ghamari

Christopher P Nizzi

Kathryn M Deck

Paul D Kingsley

Yvette Y Yien

Nicholas C Huston

Caiyong Chen

Iman J Schultz

Arthur J Dalton

Johannes G Wittig

James Palis

Stuart H Orkin

Harvey F Lodish

Richard S Eisenstein

Alan B Cantor

Barry H Paw

Affiliations

Soon will be listed here.

Abstract

In multicellular organisms, the mechanisms by which diverse cell types acquire distinct amino acids and how cellular function adapts to their availability are fundamental questions in biology. We found that increased neutral essential amino acid (NEAA) uptake was a critical component of erythropoiesis. As red blood cells matured, expression of the amino acid transporter gene Lat3 increased, which increased NEAA import. Inadequate NEAA uptake by pharmacologic inhibition or RNAi-mediated knockdown of LAT3 triggered a specific reduction in hemoglobin production in zebrafish embryos and murine erythroid cells through the mTORC1 (mammalian target of rapamycin complex 1)/4E-BP (eukaryotic translation initiation factor 4E-binding protein) pathway. CRISPR-mediated deletion of members of the 4E-BP family in murine erythroid cells rendered them resistant to mTORC1 and LAT3 inhibition and restored hemoglobin production. These results identify a developmental role for LAT3 in red blood cells and demonstrate that mTORC1 serves as a homeostatic sensor that couples hemoglobin production at the translational level to sufficient uptake of NEAAs, particularly L-leucine.

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