Literature DB >> 29433413

The Work of Titin Protein Folding as a Major Driver in Muscle Contraction.

Edward C Eckels1,2, Rafael Tapia-Rojo1, Jamie Andrés Rivas-Pardo1, Julio M Fernández1.   

Abstract

Single-molecule atomic force microscopy and magnetic tweezers experiments have demonstrated that titin immunoglobulin (Ig) domains are capable of folding against a pulling force, generating mechanical work that exceeds that produced by a myosin motor. We hypothesize that upon muscle activation, formation of actomyosin cross bridges reduces the force on titin, causing entropic recoil of the titin polymer and triggering the folding of the titin Ig domains. In the physiological force range of 4-15 pN under which titin operates in muscle, the folding contraction of a single Ig domain can generate 200% of the work of entropic recoil and occurs at forces that exceed the maximum stalling force of single myosin motors. Thus, titin operates like a mechanical battery, storing elastic energy efficiently by unfolding Ig domains and delivering the charge back by folding when the motors are activated during a contraction. We advance the hypothesis that titin folding and myosin activation act as inextricable partners during muscle contraction.

Entities:  

Keywords:  force spectroscopy; muscle contraction; polymer physics; protein folding; single molecule; titin

Mesh:

Substances:

Year:  2018        PMID: 29433413      PMCID: PMC5957538          DOI: 10.1146/annurev-physiol-021317-121254

Source DB:  PubMed          Journal:  Annu Rev Physiol        ISSN: 0066-4278            Impact factor:   19.318


  122 in total

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Authors:  Anthony L Hessel; Stan L Lindstedt; Kiisa C Nishikawa
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  11 in total

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7.  X-ray Diffraction Analysis to Explore Molecular Traces of Eccentric Contraction on Rat Skeletal Muscle Parallelly Evaluated with Signal Protein Phosphorylation Levels.

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8.  Protein Unfolding: Denaturant vs. Force.

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