Literature DB >> 26542351

Secondary structural analysis of the carboxyl-terminal domain from different connexin isoforms.

Gaëlle Spagnol1, Mona Al-Mugotir1, Jennifer L Kopanic1, Sydney Zach1, Hanjun Li1, Andrew J Trease1, Kelly L Stauch1, Rosslyn Grosely1, Matthew Cervantes1, Paul L Sorgen1.   

Abstract

The connexin carboxyl-terminal (CxCT) domain plays a role in the trafficking, localization, and turnover of gap junction channels, as well as the level of gap junction intercellular communication via numerous post-translational modifications and protein-protein interactions. As a key player in the regulation of gap junctions, the CT presents itself as a target for manipulation intended to modify function. Specific to intrinsically disordered proteins, identifying residues whose secondary structure can be manipulated will be critical toward unlocking the therapeutic potential of the CxCT domain. To accomplish this goal, we used biophysical methods to characterize CxCT domains attached to their fourth transmembrane domain (TM4). Circular dichroism and nuclear magnetic resonance were complementary in demonstrating the connexin isoforms that form the greatest amount of α-helical structure in their CT domain (Cx45 > Cx43 > Cx32 > Cx50 > Cx37Cx40Cx26). Studies compared the influence of 2,2,2-trifluoroethanol, pH, phosphorylation, and mutations (Cx32, X-linked Charcot-Marie Tooth disease; Cx26, hearing loss) on the TM4-CxCT structure. While pH modestly influences the CT structure, a major structural change was associated with phosphomimetic substitutions. Since most connexin CT domains are phosphorylated throughout their life cycle, studies of phospho-TM4-CxCT isoforms will be critical toward understanding the role that structure plays in regulating gap junction function.
© 2015 Wiley Periodicals, Inc.

Entities:  

Keywords:  circular dichroism; gap junctions; intrinsically disordered; nuclear magnetic resonance

Mesh:

Substances:

Year:  2016        PMID: 26542351      PMCID: PMC5178975          DOI: 10.1002/bip.22762

Source DB:  PubMed          Journal:  Biopolymers        ISSN: 0006-3525            Impact factor:   2.505


  76 in total

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4.  Characterization of the connexin45 carboxyl-terminal domain structure and interactions with molecular partners.

Authors:  Jennifer L Kopanic; Mona H Al-mugotir; Fabien Kieken; Sydney Zach; Andrew J Trease; Paul L Sorgen
Journal:  Biophys J       Date:  2014-05-20       Impact factor: 4.033

5.  Purification and reconstitution of the connexin43 carboxyl terminus attached to the 4th transmembrane domain in detergent micelles.

Authors:  Admir Kellezi; Rosslyn Grosely; Fabien Kieken; Gloria E O Borgstahl; Paul L Sorgen
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7.  Altered gating properties of functional Cx26 mutants associated with recessive non-syndromic hearing loss.

Authors:  Gülistan Meşe; Eric Londin; Rickie Mui; Peter R Brink; Thomas W White
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8.  Low-conductivity buffers for high-sensitivity NMR measurements.

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10.  Phosphorylation at S365 is a gatekeeper event that changes the structure of Cx43 and prevents down-regulation by PKC.

Authors:  Joell L Solan; Lucrecia Marquez-Rosado; Paul L Sorgen; Perry J Thornton; Philip R Gafken; Paul D Lampe
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  5 in total

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Review 2.  The Roles of Calmodulin and CaMKII in Cx36 Plasticity.

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Journal:  Int J Mol Sci       Date:  2021-04-25       Impact factor: 5.923

Review 3.  Gap junction structure: unraveled, but not fully revealed.

Authors:  Eric C Beyer; Viviana M Berthoud
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4.  Acetylation of C-terminal lysines modulates protein turnover and stability of Connexin-32.

Authors:  Sarah R Alaei; Charles K Abrams; J Chloë Bulinski; Elliot L Hertzberg; Mona M Freidin
Journal:  BMC Cell Biol       Date:  2018-09-29       Impact factor: 4.241

Review 5.  Peptidic Connexin43 Therapeutics in Cardiac Reparative Medicine.

Authors:  Spencer R Marsh; Zachary J Williams; Kevin J Pridham; Robert G Gourdie
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