Elena L. Rudashevskaya scite author profile

Cell growth and proliferation are tightly linked to nutrient availability. The mechanistic target of rapamycin complex 1 (mTORC1) integrates the presence of growth factors, energy levels, glucose and amino acids to modulate metabolic status and cellular responses1-3. mTORC1 is activated at the surface of lysosomes by the RAG GTPases and the Ragulator complex through a not fully understood mechanism monitoring amino acid availability in the lysosomal lumen and involving the vacuolar H+ -ATPase 4-8. Here we describe the uncharacterized human member 9 of the solute carrier family 38 (SLC38A9) as a lysosomal membrane-resident protein competent in amino acid transport. Extensive functional proteomic analysis established SLC38A9 as an integral part of the Ragulator/RAG GTPases machinery. Gain of SLC38A9 function rendered cells resistant to amino acid withdrawal, while loss of SLC38A9 expression impaired amino acid-induced mTORC1 activation. Thus SLC38A9 is a physical and functional component of the amino acid-sensing machinery that controls the activation of mTOR.

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LAMTOR/Ragulator is a negative regulator of Arl8b- and BORC-dependent late endosomal positioning

Filipek

Araújo

Vogel

et al. 2017

101

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Elena L. Rudashevskaya

SLC38A9 is a component of the lysosomal amino acid sensing machinery that controls mTORC1

LAMTOR/Ragulator is a negative regulator of Arl8b- and BORC-dependent late endosomal positioning

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