6F1U

N terminal region of dynein tail domains in complex with dynactin filament and BICDR-1

Summary for 6F1U

• Entry DOI: 10.2210/pdb6f1u/pdb
• Related: 6F1T
• EMDB information: 4168 4169
• Descriptor: ARP1 actin related protein 1 homolog A, Capping protein (Actin filament) muscle Z-line, alpha 1, F-actin capping protein beta subunit, ... (9 entities in total)
• Functional Keywords: cryo-em, complex, motor protein, cargo adaptor
• Biological source: Homo sapiens (Human); More
• Total number of polymer chains: 13
• Total formula weight: 810936.74

Authors

Urnavicius, L.,Lau, C.K.,Elshenawy, M.M.,Morales-Rios, E.,Motz, C.,Yildiz, A.,Carter, A.P. (deposition date: 2017-11-23, release date: 2018-01-17, Last modification date: 2025-04-09)

Primary citation

Urnavicius, L.,Lau, C.K.,Elshenawy, M.M.,Morales-Rios, E.,Motz, C.,Yildiz, A.,Carter, A.P.
Cryo-EM shows how dynactin recruits two dyneins for faster movement.
Nature, 554:202-206, 2018

PubMed Abstract: Dynein and its cofactor dynactin form a highly processive microtubule motor in the presence of an activating adaptor, such as BICD2. Different adaptors link dynein and dynactin to distinct cargoes. Here we use electron microscopy and single-molecule studies to show that adaptors can recruit a second dynein to dynactin. Whereas BICD2 is biased towards recruiting a single dynein, the adaptors BICDR1 and HOOK3 predominantly recruit two dyneins. We find that the shift towards a double dynein complex increases both the force and speed of the microtubule motor. Our 3.5 Å resolution cryo-electron microscopy reconstruction of a dynein tail-dynactin-BICDR1 complex reveals how dynactin can act as a scaffold to coordinate two dyneins side-by-side. Our work provides a structural basis for understanding how diverse adaptors recruit different numbers of dyneins and regulate the motile properties of the dynein-dynactin transport machine.

PubMed: 29420470
DOI: 10.1038/nature25462

Experimental method

ELECTRON MICROSCOPY (3.4 Å)