| Literature DB >> 31112396 |
Constanza Blanco1,2, Danna Morales3,2, Ignacio Mogollones1,2, Ariela Vergara-Jaque3,4,5, Carla Vargas1,2, Alhejandra Álvarez1,2, Denise Riquelme6, Elías Leiva-Salcedo6, Wendy González2,5, Diego Morales1,2, Diego Maureira1,2, Ismael Aldunate1, Mónica Cáceres1,2,7, Diego Varela3,2, Oscar Cerda1,2,7.
Abstract
Transient receptor potential melastatin 4 (TRPM4) is a Ca2+-activated nonselective cationic channel involved in a wide variety of physiologic and pathophysiological processes. Bioinformatics analyses of the primary sequence of TRPM4 allowed us to identify a putative motif for interaction with end-binding (EB) proteins, which are microtubule plus-end tracking proteins. Here, we provide novel data suggesting that TRPM4 interacts with EB proteins. We show that mutations of the putative EB binding motif abolish the TRPM4-EB interaction, leading to a reduced expression of the mature population of the plasma membrane channel and instead display an endoplasmic reticulum-associated distribution. Furthermore, we demonstrate that EB1 and EB2 proteins are required for TRPM4 trafficking and functional activity. Finally, we demonstrated that the expression of a soluble fragment containing the EB binding motif of TRPM4 reduces the plasma membrane expression of the channel and affects TRPM4-dependent focal adhesion disassembly and cell invasion processes.-Blanco, C., Morales, D., Mogollones, I., Vergara-Jaque, A., Vargas, C., Álvarez, A., Riquelme, D., Leiva-Salcedo, E., González, W., Morales, D., Maureira, D., Aldunate, I., Cáceres, M., Varela, D., Cerda, O. EB1- and EB2-dependent anterograde trafficking of TRPM4 regulates focal adhesion turnover and cell invasion.Entities:
Keywords: EB proteins; ER export; TRP channels
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Year: 2019 PMID: 31112396 DOI: 10.1096/fj.201900136R
Source DB: PubMed Journal: FASEB J ISSN: 0892-6638 Impact factor: 5.191