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- W2938474552 abstract "The family of Angiomotin (Amot) proteins regulate several biological pathways associated with cellular differentiation, proliferation, and migration. These adaptor proteins target proteins to the apical membrane, actin fibers, or the nucleus. A major function of the Amot coiled-coil homology (ACCH) domain is to initiate protein interactions with the cellular membrane, particularly those containing phosphatidylinositol lipids. The work presented in this article uses several ACCH domain lysine/arginine mutants to probe the relative importance of individual residues for lipid binding. This identified four lysine and three arginine residues that mediate full lipid binding. Based on these findings, three of these residues were mutated to glutamates in the Angiomotin 80 kDa splice form and were incorporated into human mammary cell lines. Results show that mutating three of these residues in the context of full-length Angiomotin reduced the residence of the protein at the apical membrane. These findings provide new insight into how the ACCH domain mediates lipid binding to enable Amot proteins to control epithelial cell growth." @default.
- W2938474552 created "2019-04-25" @default.
- W2938474552 creator A5018935283 @default.
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- W2938474552 date "2019-04-12" @default.
- W2938474552 modified "2023-10-14" @default.
- W2938474552 title "Identification of Specific Lysines and Arginines That Mediate Angiomotin Membrane Association" @default.
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- W2938474552 doi "https://doi.org/10.1021/acsomega.9b00165" @default.
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