Literature DB >> 26778550

BioID Identification of Lamin-Associated Proteins.

Aaron A Mehus1, Ruthellen H Anderson1, Kyle J Roux2.   

Abstract

A- and B-type lamins support the nuclear envelope, contribute to heterochromatin organization, and regulate a myriad of nuclear processes. The mechanisms by which lamins function in different cell types and the mechanisms by which lamin mutations cause over a dozen human diseases (laminopathies) remain unclear. The identification of proteins associated with lamins is likely to provide fundamental insight into these mechanisms. BioID (proximity-dependent biotin identification) is a unique and powerful method for identifying protein-protein and proximity-based interactions in living cells. BioID utilizes a mutant biotin ligase from bacteria that is fused to a protein of interest (bait). When expressed in living cells and stimulated with excess biotin, this BioID-fusion protein promiscuously biotinylates directly interacting and vicinal endogenous proteins. Following biotin-affinity capture, the biotinylated proteins can be identified using mass spectrometry. BioID thus enables screening for physiologically relevant protein associations that occur over time in living cells. BioID is applicable to insoluble proteins such as lamins that are often refractory to study by other methods and can identify weak and/or transient interactions. We discuss the use of BioID to elucidate novel lamin-interacting proteins and its applications in a broad range of biological systems, and provide detailed protocols to guide new applications.
© 2016 Elsevier Inc. All rights reserved.

Entities:  

Keywords:  BioID; Biotinylation; Labeling; Lamins; Protein–protein interactions; Proximity

Mesh:

Substances:

Year:  2015        PMID: 26778550      PMCID: PMC4821506          DOI: 10.1016/bs.mie.2015.08.008

Source DB:  PubMed          Journal:  Methods Enzymol        ISSN: 0076-6879            Impact factor:   1.600


  54 in total

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Review 4.  Nuclear lamins: laminopathies and their role in premature ageing.

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Journal:  Physiol Rev       Date:  2006-07       Impact factor: 37.312

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  10 in total

1.  Towards improving proximity labeling by the biotin ligase BirA.

Authors:  Luke T Oostdyk; Leonard Shank; Kasey Jividen; Natalia Dworak; Nicholas E Sherman; Bryce M Paschal
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3.  Analysis of K-Ras Interactions by Biotin Ligase Tagging.

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4.  Mapping Proximity Associations of Core Spindle Assembly Checkpoint Proteins.

Authors:  Yenni A Garcia; Erick F Velasquez; Lucy W Gao; Ankur A Gholkar; Kevin M Clutario; Keith Cheung; Taylor Williams-Hamilton; Julian P Whitelegge; Jorge Z Torres
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5.  An improved smaller biotin ligase for BioID proximity labeling.

Authors:  Dae In Kim; Samuel C Jensen; Kyle A Noble; Birendra Kc; Kenneth H Roux; Khatereh Motamedchaboki; Kyle J Roux
Journal:  Mol Biol Cell       Date:  2016-02-24       Impact factor: 4.138

6.  Proximal Protein Interaction Landscape of RAS Paralogs.

Authors:  Benoît Béganton; Etienne Coyaud; Estelle M N Laurent; Alain Mangé; Julien Jacquemetton; Muriel Le Romancer; Brian Raught; Jérôme Solassol
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7.  Mapping the micro-proteome of the nuclear lamina and lamina-associated domains.

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9.  A method to map the interaction network of the nuclear lamina with genetically encoded photo-crosslinkers in vivo.

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Review 10.  A Perspective on the Experimental Techniques for Studying Lamins.

Authors:  Ilaria Pecorari; Daniele Borin; Orfeo Sbaizero
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  10 in total

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