The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK

The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK

Focal adhesion (FA) proteins, kindlin‐2 and integrin‐linked kinase (ILK), regulate cell adhesion and migration. ILK interacts with and promotes kindlin‐2 targeting to FAs. Leu353 and Leu357 in kindlin‐2 have been reported to be important for the interaction between kindlin‐2 and ILK. However, the bi...

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Main Authors: Tan, Hui-Foon, Guan, Si-Yu, Chng, Choon-Peng, Ong, Li-Teng, Tan, Suet-Mien, Law, Alex Sai Kit
Other Authors: School of Biological Sciences
Format: Article
Language:English
Published: 2019
Subjects:
Cell Adhesion
Integrin-linked Kinase
DRNTU::Science::Biological sciences
Online Access:https://hdl.handle.net/10356/105829
http://hdl.handle.net/10220/48755
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Institution: Nanyang Technological University
Language: English
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spelling sg-ntu-dr.10356-1058292023-02-28T17:06:39Z The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK Tan, Hui-Foon Guan, Si-Yu Chng, Choon-Peng Ong, Li-Teng Tan, Suet-Mien Law, Alex Sai Kit School of Biological Sciences Cell Adhesion Integrin-linked Kinase DRNTU::Science::Biological sciences Focal adhesion (FA) proteins, kindlin‐2 and integrin‐linked kinase (ILK), regulate cell adhesion and migration. ILK interacts with and promotes kindlin‐2 targeting to FAs. Leu353 and Leu357 in kindlin‐2 have been reported to be important for the interaction between kindlin‐2 and ILK. However, the binding interface between kindlin‐2 and ILK remains unclear. Using molecular modeling and molecular dynamics simulations, we show that Asp344, Asp352, and Thr356 in kindlin‐2 and Arg243 and Arg334 in ILK kinase domain (KD) are important in kindlin‐2/ILK complex formation. Mutations that disrupt these interactions abrogate kindlin‐2 and ILK colocalization in HeLa cells. The interactions are direct based on data from pull‐down assays using purified recombinant kindlin‐2 F2‐pleckstrin homology and ILK KDs. These data provide additional insights into the binding interface between kindlin‐2 and ILK. ASTAR (Agency for Sci., Tech. and Research, S’pore) MOE (Min. of Education, S’pore) Accepted version 2019-06-14T04:14:13Z 2019-12-06T21:58:48Z 2019-06-14T04:14:13Z 2019-12-06T21:58:48Z 2018 Journal Article Guan, S.-Y., Chng, C.-P., Ong, L.-T., Tan, H.-F., Law, A. S. K., & Tan, S.-M. (2018). The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK. FEBS Letters, 592(1), 112-121. doi:10.1002/1873-3468.12938 0014-5793 https://hdl.handle.net/10356/105829 http://hdl.handle.net/10220/48755 10.1002/1873-3468.12938 en FEBS Letters © 2017 Federation of European Biochemical Societies. All rights reserved. This paper was published in FEBS Letters and is made available with permission of Federation of European Biochemical Societies. 10 p. application/pdf
institution Nanyang Technological University
building NTU Library
continent Asia
country Singapore
Singapore
content_provider NTU Library
collection DR-NTU
language English
topic Cell Adhesion
Integrin-linked Kinase
DRNTU::Science::Biological sciences
spellingShingle Cell Adhesion
Integrin-linked Kinase
DRNTU::Science::Biological sciences
Tan, Hui-Foon
Guan, Si-Yu
Chng, Choon-Peng
Ong, Li-Teng
Tan, Suet-Mien
Law, Alex Sai Kit
The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK
description Focal adhesion (FA) proteins, kindlin‐2 and integrin‐linked kinase (ILK), regulate cell adhesion and migration. ILK interacts with and promotes kindlin‐2 targeting to FAs. Leu353 and Leu357 in kindlin‐2 have been reported to be important for the interaction between kindlin‐2 and ILK. However, the binding interface between kindlin‐2 and ILK remains unclear. Using molecular modeling and molecular dynamics simulations, we show that Asp344, Asp352, and Thr356 in kindlin‐2 and Arg243 and Arg334 in ILK kinase domain (KD) are important in kindlin‐2/ILK complex formation. Mutations that disrupt these interactions abrogate kindlin‐2 and ILK colocalization in HeLa cells. The interactions are direct based on data from pull‐down assays using purified recombinant kindlin‐2 F2‐pleckstrin homology and ILK KDs. These data provide additional insights into the binding interface between kindlin‐2 and ILK.
author2 School of Biological Sciences
author_facet School of Biological Sciences
Tan, Hui-Foon
Guan, Si-Yu
Chng, Choon-Peng
Ong, Li-Teng
Tan, Suet-Mien
Law, Alex Sai Kit
format Article
author Tan, Hui-Foon
Guan, Si-Yu
Chng, Choon-Peng
Ong, Li-Teng
Tan, Suet-Mien
Law, Alex Sai Kit
author_sort Tan, Hui-Foon
title The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK
title_short The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK
title_full The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK
title_fullStr The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK
title_full_unstemmed The binding interface of kindlin-2 and ILK involves Asp344/Asp352/Thr356 in kindlin-2 and Arg243/Arg334 in ILK
title_sort binding interface of kindlin-2 and ilk involves asp344/asp352/thr356 in kindlin-2 and arg243/arg334 in ilk
publishDate 2019
url https://hdl.handle.net/10356/105829
http://hdl.handle.net/10220/48755
_version_ 1759858383018524672

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