BaseSpace
Correlation Engine 2.0
Import Your Data
Literature

FAQ

More FAQs

Back to top
Clear Search sequence regions
(e.g. Leukocyte, Avian flu virus, Aspirin, rs2476601, CXCL2, Angiogenesis, Ischemia)
Bookmark Forward

Register-shift" insulin analogs uncover constraints of proteotoxicity in protein evolution.

Nischay K Rege, Ming Liu, Balamurugan Dhayalan, Yen-Shan Chen, Nicholas A Smith, Leili Rahimi, Jinhong Sun, Huan Guo, Yanwu Yang, Leena Haataja, Nelson F B Phillips, Jonathan Whittaker, Brian J Smith, Peter Arvan, Faramarz Ismail-Beigi, Michael A Weiss

The Journal of biological chemistry 2020 Mar 06


filter terms:
  • amino acid motifs (1)
  • cellular (1)
  • growth factors (1)
  • humans (1)
  • insulin (9)
  • insulins like growth factors (1)
  • IR (2)
  • native (3)
  • proinsulin (3)
  • rat (2)
  • receptor (2)
  • receptor insulin (2)
  • reticulum (1)
  • vertebrate (2)
    • Sizes of these terms reflect their relevance to your search.

    Globular protein sequences encode not only functional structures (the native state) but also protein foldability, i.e. a conformational search that is both efficient and robustly minimizes misfolding. Studies of mutations associated with toxic misfolding have yielded insights into molecular determinants of protein foldability. Of particular interest are residues that are conserved yet dispensable in the native state. Here, we exploited the mutant proinsulin syndrome (a major cause of permanent neonatal-onset diabetes mellitus) to investigate whether toxic misfolding poses an evolutionary constraint. Our experiments focused on an invariant aromatic motif (PheB24-PheB25-TyrB26) with complementary roles in native self-assembly and receptor binding. A novel class of mutations provided evidence that insulin can bind to the insulin receptor (IR) in two different modes, distinguished by a "register shift" in this motif, as visualized by molecular dynamics (MD) simulations. Register-shift variants are active but defective in cellular foldability and exquisitely susceptible to fibrillation in vitro Indeed, expression of the corresponding proinsulin variant induced endoplasmic reticulum stress, a general feature of the mutant proinsulin syndrome. Although not present among vertebrate insulin and insulin-like sequences, a prototypical variant ([GlyB24]insulin) was as potent as WT insulin in a rat model of diabetes. Although in MD simulations the shifted register of receptor engagement is compatible with the structure and allosteric reorganization of the IR-signaling complex, our results suggest that this binding mode is associated with toxic misfolding and so is disallowed in evolution. The implicit threat of proteotoxicity limits sequence variation among vertebrate insulins and insulin-like growth factors. © 2020 Rege et al.

    Citation

    Nischay K Rege, Ming Liu, Balamurugan Dhayalan, Yen-Shan Chen, Nicholas A Smith, Leili Rahimi, Jinhong Sun, Huan Guo, Yanwu Yang, Leena Haataja, Nelson F B Phillips, Jonathan Whittaker, Brian J Smith, Peter Arvan, Faramarz Ismail-Beigi, Michael A Weiss. Register-shift" insulin analogs uncover constraints of proteotoxicity in protein evolution. The Journal of biological chemistry. 2020 Mar 06;295(10):3080-3098

    Expand section icon Mesh Tags

    Expand section icon Substances


    PMID: 32005662

    View Full Text
    • Copyright © 2024 Illumina Inc. All rights reserved.