Cell Reports (Aug 2024)

Optogenetic control of kinesin-1, -2, -3 and dynein reveals their specific roles in vesicular transport

  • Sahil Nagpal,
  • Karthikeyan Swaminathan,
  • Daniel Beaudet,
  • Maud Verdier,
  • Samuel Wang,
  • Christopher L. Berger,
  • Florian Berger,
  • Adam G. Hendricks

Journal volume & issue
Vol. 43, no. 8
p. 114649

Abstract

Read online

Summary: Each cargo in a cell employs a unique set of motor proteins for its transport. To dissect the roles of each type of motor, we developed optogenetic inhibitors of endogenous kinesin-1, -2, -3 and dynein motors and examined their effect on the transport of early endosomes, late endosomes, and lysosomes. While kinesin-1, -3, and dynein transport vesicles at all stages of endocytosis, kinesin-2 primarily drives late endosomes and lysosomes. Transient optogenetic inhibition of kinesin-1 or dynein causes both early and late endosomes to move more processively by relieving competition with opposing motors. Kinesin-2 and -3 support long-range transport, and optogenetic inhibition reduces the distances that their cargoes move. These results suggest that the directionality of transport is controlled through regulating kinesin-1 and dynein activity. On vesicles transported by several kinesin and dynein motors, modulating the activity of a single type of motor on the cargo is sufficient to direct motility.

Keywords