| Literature DB >> 33396475 |
Jinsook Ahn1, Soyeon Jeong1, So-Mi Kang2, Inseong Jo1, Bum-Joon Park2, Nam-Chul Ha1.
Abstract
Intermediate filaments (IFs) commonly have structural elements of a central α-helical coiled-coil domain consisting of coil 1a, coil 1b, coil 2, and their flanking linkers. Recently, the crystal structure of a long lamin A/C fragment was determined and showed detailed features of a tetrameric unit. The structure further suggested a new binding mode between tetramers, designated eA22, where a parallel overlap of coil 1a and coil 2 is the critical interaction. This study investigated the biochemical effects of genetic mutations causing human diseases, focusing on the eA22 interaction. The mutant proteins exhibited either weakened or augmented interactions between coil 1a and coil 2. The ensuing biochemical results indicated that the interaction requires the separation of the coiled-coils in the N-terminal of coil 1a and the C-terminal of coil 2, coupled with the structural transition in the central α-helical rod domain. This study provides insight into the role of coil 1a as a molecular regulator in the elongation of IF proteins.Entities:
Keywords: EDMD; assembly mechanism; eA22 interaction; filament assembly; intermediate filament; laminopathies; molecular regulator; nuclear lamin A/C; structural transition
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Year: 2020 PMID: 33396475 PMCID: PMC7824274 DOI: 10.3390/cells10010055
Source DB: PubMed Journal: Cells ISSN: 2073-4409 Impact factor: 6.600