Literature DB >> 20563238

Stabilization of the spectrin-like domains of nesprin-1α by the evolutionarily conserved "adaptive" domain.

Zhixia Zhong1, Siwei A Chang, Agnieszka Kalinowski, Katherine L Wilson, Kris Noel Dahl.   

Abstract

Nesprins are located at the outer and inner membranes of the nuclear envelope and help link the cytoskeleton to the nucleoskeleton. Nesprin-1α, located at the inner nuclear membrane, binds to A-type lamins and emerin and has homology to spectrin-repeat proteins. However, the mechanical and thermodynamic properties of the spectrin-like repeats (SLRs) of nesprin-1α and the potential structural contributions of the unique central domain were untested. In other spectrin superfamily proteins, tandem spectrin-repeat domains undergo cooperatively coupled folding and unfolding. We hypothesized that the large central domain, which interrupts SLRs and is conserved in other nesprin isoforms, might confer unique structural properties. To test this model we measured the thermal unfolding of nesprin-1α fragments using circular dichroism and dynamic light scattering. The SLRs in nesprin-1α were found to have structural and thermodynamic properties typical of spectrins. The central domain had relatively little secondary structure as an isolated fragment, but significantly stabilized larger SLR-containing molecules by increasing their overall helicity, thermal stability and cooperativity of folding. We suggest this domain, now termed the 'adaptive' domain (AD), also strengthens dimerization and inhibits unfolding. Further engineering of the isolated AD, and AD-containing nesprin molecules, may yield new information about the higher-order association of cooperative protein motifs.

Entities:  

Year:  2010        PMID: 20563238      PMCID: PMC2885798          DOI: 10.1007/s12195-010-0121-3

Source DB:  PubMed          Journal:  Cell Mol Bioeng        ISSN: 1865-5025            Impact factor:   2.321


  51 in total

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2.  Dynamic light scattering investigations of human erythrocyte spectrin.

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  13 in total

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3.  The nesprin-cytoskeleton interface probed directly on single nuclei is a mechanically rich system.

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4.  Molecular mechanisms underlying the impact of mutations in SOD1 on its conformational properties associated with amyotrophic lateral sclerosis as revealed with molecular modelling.

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Review 5.  Beyond lamins other structural components of the nucleoskeleton.

Authors:  Zhixia Zhong; Katherine L Wilson; Kris Noel Dahl
Journal:  Methods Cell Biol       Date:  2010       Impact factor: 1.441

6.  Nesprin-1 impact on tumorigenic cell phenotypes.

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7.  Lamin A/C Is Required for ChAT-Dependent Neuroblastoma Differentiation.

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8.  Centrifugal Displacement of Nuclei Reveals Multiple LINC Complex Mechanisms for Homeostatic Nuclear Positioning.

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