Journal
PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA
Volume 118, Issue 23, Pages -Publisher
NATL ACAD SCIENCES
DOI: 10.1073/pnas.2103383118
Keywords
dynein; dynactin; optical trap; supported lipid bilayer; intracellular transport
Categories
Funding
- Wellcome Trust International Senior Research Fellowship [WT079214MA]
- Department of Biotechnology-Wellcome Trust India Alliance Early Career Fellowship [IA/E/15/1/502298]
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Disrupting the interactions between dynactin and dynein or microtubules impacts dynein's behavior on microtubules and its ability to generate force. The dynactin-microtubule link is shown to be crucial for dynein's persistence against load, shedding light on dynein dysfunction.
The dynein-dynactin nanomachine transports cargoes along microtubules in cells. Why dynactin interacts separately with the dynein motor and also with microtubules is hotly debated. Here we disrupted these interactions in a targeted manner on phagosomes extracted from cells, followed by optical trapping to interrogate native dynein- dynactin teams on single phagosomes. Perturbing the dynactin- dynein interaction reduced dynein's on rate to microtubules. In contrast, perturbing the dynactin-microtubule interaction increased dynein's off rate markedly when dynein was generating force against the optical trap. The dynactin-microtubule link is therefore required for persistence against load, a finding of importance because diseaserelevant mutations in dynein-dynactin are known to interfere with high-load functions of dynein in cells. Our findings call attention to a less studied property of dynein-dynactin, namely, its detachment against load, in understanding dynein dysfunction.
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