Bulletin of the American Physical Society
APS March Meeting 2021
Volume 66, Number 1
Monday–Friday, March 15–19, 2021; Virtual; Time Zone: Central Daylight Time, USA
Session P12: Physics of Proteins III
3:00 PM–5:48 PM,
Wednesday, March 17, 2021
Sponsoring
Unit:
DBIO
Chair: Dongping Zhong, Ohio State University - Columbus; Wei Wang, Nanjing Univ
Abstract: P12.00007 : Did proteins evolve structural asymmetry for faster co-translational folding?*
4:36 PM–4:48 PM
Live
Presenter:
John McBride
(Institute for Basic Science)
Authors:
John McBride
(Institute for Basic Science)
Tsvi Tlusty
(Institute for Basic Science)
Proteins are translated from the N- to the C-terminal, raising the basic question of how this innate directionality affects their evolution. To explore this question, we analyze 16,200 structures from the protein data bank (PDB). We find remarkable enrichment of α-helices at the C terminal and β-sheets at the N terminal. Furthermore, this α-β asymmetry correlates with sequence length and contact order, both known determinants of folding rate. Hence, we discuss our proposed ‘slowest-first’ scheme, whereby protein sequences evolved structural asymmetry to accelerate co-translational folding (CTF): the slowest-folding elements (e.g. β-sheets) are positioned near the N terminal so they have more time to fold during translation. We predict that CTF can be accelerated, up to double the rate,when folding time matches translation time; analysis of the PDB reveals that structural asymmetry is indeed maximal in this regime. This is greater in prokaryotes, which generally require faster protein production. Altogether, this indicates that accelerating CTF is a substantial evolutionary force whose interplay with stability and functionality is encoded in sequence asymmetry.
https://arxiv.org/abs/2009.13900
*
This work was supported by the Institute for Basic Science, Project Code IBS-R020-D1.
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