Structural determinants for membrane binding of the EGFR juxtamembrane domain

Author:

Wu Ziwei12,Li Ling3,Zhu Lina12,Wang Runhan14,Dong Yingkui14,Zhang Yaoyao12,Wang Yujuan12ORCID,Wang Junfeng124ORCID,Zhu Lei12ORCID

Affiliation:

1. High Magnetic Field Laboratory, CAS Key Laboratory of High Magnetic Field and Ion Beam Physical Biology, Hefei Institutes of Physical Science Chinese Academy of Sciences Hefei China

2. University of Science and Technology of China Hefei China

3. Institute of Health and Medical Technology, Hefei Institutes of Physical Science Chinese Academy of Sciences Hefei China

4. Institute of Physical Science and Information Technology Anhui University Hefei China

Abstract

Overactivation of the epidermal growth factor receptor (EGFR) is critical for the development of multiple cancers. Previous studies have shown that the cell membrane is a key regulator of EGFR kinase activity through its interaction with the EGFR juxtamembrane domain (JM). However, the lipid recognition specificity of EGFR‐JM and its interaction details remain unclear. Using lipid strip and liposome pulldown assays, we showed that EGFR‐JM could specifically interact with PI(4,5)P2‐or phosphatidylserine‐containing membranes. We further characterized the JM–membrane interaction using NMR‐titration‐based chemical shift perturbation and paramagnetic relaxation enhancement analyses, and found that residues I649 − L659 comprised the membrane‐binding site. Furthermore, the membrane‐binding region contains the predicted dimerization motif of JM, 655LRRLL659, suggesting that membrane binding may affect JM dimerization and, therefore, regulate kinase activation.

Funder

National Natural Science Foundation of China

Publisher

Wiley

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