PLoS Biology (Apr 2021)

Molecular basis of F-actin regulation and sarcomere assembly via myotilin.

  • Julius Kostan,
  • Miha Pavšič,
  • Vid Puž,
  • Thomas C Schwarz,
  • Friedel Drepper,
  • Sibylle Molt,
  • Melissa Ann Graewert,
  • Claudia Schreiner,
  • Sara Sajko,
  • Peter F M van der Ven,
  • Adekunle Onipe,
  • Dmitri I Svergun,
  • Bettina Warscheid,
  • Robert Konrat,
  • Dieter O Fürst,
  • Brigita Lenarčič,
  • Kristina Djinović-Carugo

DOI
https://doi.org/10.1371/journal.pbio.3001148
Journal volume & issue
Vol. 19, no. 4
p. e3001148

Abstract

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Sarcomeres, the basic contractile units of striated muscle cells, contain arrays of thin (actin) and thick (myosin) filaments that slide past each other during contraction. The Ig-like domain-containing protein myotilin provides structural integrity to Z-discs-the boundaries between adjacent sarcomeres. Myotilin binds to Z-disc components, including F-actin and α-actinin-2, but the molecular mechanism of binding and implications of these interactions on Z-disc integrity are still elusive. To illuminate them, we used a combination of small-angle X-ray scattering, cross-linking mass spectrometry, and biochemical and molecular biophysics approaches. We discovered that myotilin displays conformational ensembles in solution. We generated a structural model of the F-actin:myotilin complex that revealed how myotilin interacts with and stabilizes F-actin via its Ig-like domains and flanking regions. Mutant myotilin designed with impaired F-actin binding showed increased dynamics in cells. Structural analyses and competition assays uncovered that myotilin displaces tropomyosin from F-actin. Our findings suggest a novel role of myotilin as a co-organizer of Z-disc assembly and advance our mechanistic understanding of myotilin's structural role in Z-discs.