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Lamin A/C and PI(4,5)P2-A Novel Complex in the Cell Nucleus

S. Escudeiro-Lopes, VV. Filimonenko, L. Jarolimová, P. Hozák

. 2024 ; 13 (5) : . [pub] 20240225

Language English Country Switzerland

Document type Journal Article

Grant support
19-05608S Czech Science Foundation
18-19714S Czech Science Foundation
17-09103S Czech Science Foundation
16-03346S Czech Science Foundation
15-08738S Czech Science Foundation
68378050 Czech Academy of Sciences, Institute of Molecular Genetics: RVO:
LTC19048 Ministry of Education Youth and Sports
LTC20024 Ministry of Education Youth and Sports
CA19105 action COST: EpiLipidNET
LM2018129 Ministry of Education Youth and Sports
LM2023050 Ministry of Education Youth and Sports
CZ.02.1.01/0.0/0.0/16_013/0001775 European Regional Development Fund
CA15214 action COST: EuroCellNet

Lamins, the nuclear intermediate filaments, are important regulators of nuclear structural integrity as well as nuclear functional processes such as DNA transcription, replication and repair, and epigenetic regulations. A portion of phosphorylated lamin A/C localizes to the nuclear interior in interphase, forming a lamin A/C pool with specific properties and distinct functions. Nucleoplasmic lamin A/C molecular functions are mainly dependent on its binding partners; therefore, revealing new interactions could give us new clues on the lamin A/C mechanism of action. In the present study, we show that lamin A/C interacts with nuclear phosphoinositides (PIPs), and with nuclear myosin I (NM1). Both NM1 and nuclear PIPs have been previously reported as important regulators of gene expression and DNA damage/repair. Furthermore, phosphorylated lamin A/C forms a complex with NM1 in a phosphatidylinositol-4,5-bisphosphate (PI(4,5)P2)-dependent manner in the nuclear interior. Taken together, our study reveals a previously unidentified interaction between phosphorylated lamin A/C, NM1, and PI(4,5)P2 and suggests new possible ways of nucleoplasmic lamin A/C regulation, function, and importance for the formation of functional nuclear microdomains.

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