PLoS Biology (Nov 2018)

Intramembrane ionic protein-lipid interaction regulates integrin structure and function.

  • Jun Guo,
  • Youhua Zhang,
  • Hua Li,
  • Huiying Chu,
  • Qinshu Wang,
  • Shutan Jiang,
  • Yan Li,
  • Hongbin Shen,
  • Guohui Li,
  • Jianfeng Chen,
  • Chenqi Xu

DOI
https://doi.org/10.1371/journal.pbio.2006525
Journal volume & issue
Vol. 16, no. 11
p. e2006525

Abstract

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Protein transmembrane domains (TMDs) are generally hydrophobic, but our bioinformatics analysis shows that many TMDs contain basic residues at terminal regions. Physiological functions of these membrane-snorkeling basic residues are largely unclear. Here, we show that a membrane-snorkeling Lys residue in integrin αLβ2 (also known as lymphocyte function-associated antigen 1 [LFA-1]) regulates transmembrane heterodimer formation and integrin adhesion through ionic interplay with acidic phospholipids and calcium ions (Ca2+) in T cells. The amino group of the conserved Lys ionically interacts with the phosphate group of acidic phospholipids to stabilize αLβ2 transmembrane association, thus keeping the integrin at low-affinity conformation. Intracellular Ca2+ uses its charge to directly disrupt this ionic interaction, leading to the transmembrane separation and the subsequent extracellular domain extension to increase adhesion activity. This Ca2+-mediated regulation is independent on the canonical Ca2+ signaling or integrin inside-out signaling. Our work therefore showcases the importance of intramembrane ionic protein-lipid interaction and provides a new mechanism of integrin activation.