| Literature DB >> 27278019 |
Thankiah Sudhaharan1, Kai Ping Sem1, Hwi Fen Liew1, Yuan Hong Yu1, Wah Ing Goh2, Ai Mei Chou1, Sohail Ahmed3.
Abstract
Rif induces dorsal filopodia but the signaling pathway responsible for this has not been identified. We show here that Rif interacts with the I-BAR family protein IRTKS (also known as BAIAP2L1) through its I-BAR domain. Rif also interacts with Pinkbar (also known as BAIAP2L2) in N1E-115 mouse neuroblastoma cells. IRTKS and Rif induce dorsal membrane ruffles and filopodia. Dominant-negative Rif inhibits the formation of IRTKS-induced morphological structures, and Rif activity is blocked in IRTKS-knockout (KO) cells. To further define the Rif-IRTKS signaling pathway, we identify Eps8 and WAVE2 (also known as WASF2) as IRTKS interactors. We find that Eps8 regulates the size and number of dorsal filopodia and membrane ruffles downstream of Rif-IRTKS signaling, whereas WAVE2 modulates dorsal membrane ruffling. Furthermore, our data suggests that Tir, a protein essential for enterohemorrhagic Escherichia coli infection, might compete for Rif for interaction with the I-BAR domain of IRTKS. Based on this evidence, we propose a model in which Rho family GTPases use the I-BAR proteins, IRSp53 (also known as BAIAP2), IRTKS and Pinkbar, as a central mechanism to modulate cell morphology.Entities:
Keywords: Dorsal filopodia; Dorsal ruffles; Eps8; IRTKS; WAVE2
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Year: 2016 PMID: 27278019 DOI: 10.1242/jcs.179655
Source DB: PubMed Journal: J Cell Sci ISSN: 0021-9533 Impact factor: 5.285