Litcius/Paper detail

LAP2alpha maintains a mobile and low assembly state of A-type lamins in the nuclear interior

Nana Naetar, Konstantina Georgiou, Christian Knapp, I. N. Bronshtein, Elisabeth Zier, Petra Fichtinger, Thomas Dechat, Yuval Garini, Roland Foisner

2021eLife38 citationsDOIOpen Access PDF

Abstract

Lamins form stable filaments at the nuclear periphery in metazoans. Unlike B-type lamins, lamins A and C localize also in the nuclear interior, where they interact with lamin-associated polypeptide 2 alpha (LAP2α). Using antibody labeling, we previously observed a depletion of nucleoplasmic A-type lamins in mouse cells lacking LAP2α. Here, we show that loss of LAP2α actually causes formation of larger, biochemically stable lamin A/C structures in the nuclear interior that are inaccessible to lamin A/C antibodies. While nucleoplasmic lamin A forms from newly expressed pre-lamin A during processing and from soluble mitotic lamins in a LAP2α-independent manner, binding of LAP2α to lamin A/C during interphase inhibits formation of higher order structures, keeping nucleoplasmic lamin A/C in a mobile state independent of lamin A/C S22 phosphorylation. We propose that LAP2α is essential to maintain a mobile lamin A/C pool in the nuclear interior, which is required for proper nuclear functions.

Topics & Concepts

LaminNuclear laminaCell biologyBiologyMitosisInner membraneInterphaseCell nucleusNuclear proteinChemistryNucleusGeneticsGeneTranscription factorMitochondrionNuclear Structure and FunctionRNA Research and SplicingGenomics and Chromatin Dynamics