Litcius/Paper detail

Biphasic regulation of glutamine consumption by WNT during osteoblast differentiation

Leyao Shen, Deepika Sharma, Yilin Yu, Fanxin Long, Courtney M. Karner

2020Journal of Cell Science62 citationsDOIOpen Access PDF

Abstract

Osteoblasts are the principal bone forming cells. As such, osteoblasts have enhanced demand for amino acids to sustain high rates of matrix synthesis associated with bone formation. The precise systems utilized by osteoblasts to meet these synthetic demands are not well understood. WNT signaling is known to rapidly stimulate glutamine uptake during osteoblast differentiation. Using a cell biology approach, we identified two amino acid transporters, Slc7a7 and Slc1a5, as the primary transporters of glutamine in response to WNT. Slc1a5 mediates the majority of glutamine uptake, whereas Slc7a7 mediates the rapid increase in glutamine uptake in response to WNT. Mechanistically, WNT signals through the canonical/β-catenin dependent pathway to rapidly induce Slc7a7 expression. Conversely, Slc1a5 expression is regulated by the transcription factor ATF4 downstream of the mTORC1 pathway. Targeting either Slc1a5 or Slc7a7 using shRNA reduced WNT induced glutamine uptake and prevented osteoblast differentiation. Collectively these data highlight the critical nature of glutamine transport for WNT induced osteoblast differentiation.

Topics & Concepts

BiologyWnt signaling pathwayGlutamineOsteoblastConsumption (sociology)Cell biologyBiochemistrySignal transductionAmino acidIn vitroSocial scienceSociologyGenetics and Neurodevelopmental DisordersWnt/β-catenin signaling in development and cancerCancer-related gene regulation