Regulated dynamic subcellular GLUT4 localization revealed by proximal proteome mapping in human muscle cells.
Anuttoma RayJennifer WenLucie YammineJeff CulverIsabella Supardi ParidaJeonifer GarrenLiang XueKatherine HalesQing XiangMorris J BirnbaumBei B ZhangMara MonettiTimothy E McGrawPublished in: Journal of cell science (2023)
Regulation of glucose transport, which is central for control of whole-body metabolism, is determined by the amount of GLUT4 glucose transporter (also known as SLC2A4) in the plasma membrane (PM) of fat and muscle cells. Physiologic signals [such as activated insulin receptor or AMP-activated protein kinase (AMPK)] increase PM GLUT4. Here, we show that the distribution of GLUT4 between the PM and interior of human muscle cells is dynamically maintained, and that AMPK promotes PM redistribution of GLUT4 by regulating exocytosis and endocytosis. Stimulation of exocytosis by AMPK is mediated by Rab10 and the Rab GTPase-activating protein TBC1D4. APEX2 proximity mapping reveals that GLUT4 traverses both PM-proximal and PM-distal compartments in unstimulated muscle cells, further supporting retention of GLUT4 by a constitutive retrieval mechanism. AMPK-stimulated translocation involves GLUT4 redistribution among the same compartments traversed in unstimulated cells, with a significant recruitment of GLUT4 from the Golgi and trans-Golgi network compartments. Our comprehensive proximal protein mapping provides an integrated, high-density, whole-cell accounting of the localization of GLUT4 at a resolution of ∼20 nm that serves as a structural framework for understanding the molecular mechanisms regulating GLUT4 trafficking downstream of different signaling inputs in a physiologically relevant cell type.
Keyphrases
- induced apoptosis
- skeletal muscle
- particulate matter
- air pollution
- protein kinase
- cell cycle arrest
- heavy metals
- endothelial cells
- polycyclic aromatic hydrocarbons
- type diabetes
- signaling pathway
- high resolution
- adipose tissue
- oxidative stress
- minimally invasive
- metabolic syndrome
- cell proliferation
- blood glucose
- insulin resistance
- bone marrow
- amino acid