Microtubule Motors Power Plasma Membrane Tubulation in Clathrin-Independent Endocytosis

Charles A. Day; Nicholas W. Baetz; Courtney A. Copeland; Lewis J. Kraft; Bing Han; Ajit Tiwari; Kimberly R. Drake; Heidi De Luca; Daniel J.F. Chinnapen; Michael W. Davidson; Randall K. Holmes; Michael G. Jobling; Trina A. Schroer; Wayne I. Lencer; Anne K. Kenworthy

doi:10.1111/tra.12269

Microtubule Motors Power Plasma Membrane Tubulation in Clathrin-Independent Endocytosis

Charles A. Day, Nicholas W. Baetz, Courtney A. Copeland, Lewis J. Kraft, Bing Han, Ajit Tiwari, Kimberly R. Drake, Heidi De Luca, Daniel J.F. Chinnapen, Michael W. Davidson, Randall K. Holmes, Michael G. Jobling, Trina A. Schroer, Wayne I. Lencer, Anne K. Kenworthy

Hormel Institute

Research output: Contribution to journal › Article › peer-review

45 Scopus citations

Abstract

How the plasma membrane is bent to accommodate clathrin-independent endocytosis remains uncertain. Recent studies suggest Shiga and cholera toxin induce membrane curvature required for their uptake into clathrin-independent carriers by binding and cross-linking multiple copies of their glycosphingolipid receptors on the plasma membrane. But it remains unclear if toxin-induced sphingolipid crosslinking provides sufficient mechanical force for deforming the plasma membrane, or if host cell factors also contribute to this process. To test this, we imaged the uptake of cholera toxin B-subunit into surface-derived tubular invaginations. We found that cholera toxin mutants that bind to only one glycosphingolipid receptor accumulated in tubules, and that toxin binding was entirely dispensable for membrane tubulations to form. Unexpectedly, the driving force for tubule extension was supplied by the combination of microtubules, dynein and dynactin, thus defining a novel mechanism for generating membrane curvature during clathrin-independent endocytosis.

Original language	English (US)
Pages (from-to)	572-590
Number of pages	19
Journal	Traffic
Volume	16
Issue number	6
DOIs	https://doi.org/10.1111/tra.12269
State	Published - Jun 1 2015

Bibliographical note

Publisher Copyright:
© 2015 The Authors. Traffic published by John Wiley & Sons Ltd.

Keywords

Cholera toxin
Clathrin-independent endocytosis
Dynactin
Dynein
Membrane curvature
Microtubules

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Day, C. A., Baetz, N. W., Copeland, C. A., Kraft, L. J., Han, B., Tiwari, A., Drake, K. R., De Luca, H., Chinnapen, D. J. F., Davidson, M. W., Holmes, R. K., Jobling, M. G., Schroer, T. A., Lencer, W. I., & Kenworthy, A. K. (2015). Microtubule Motors Power Plasma Membrane Tubulation in Clathrin-Independent Endocytosis. Traffic, 16(6), 572-590. https://doi.org/10.1111/tra.12269

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abstract = "How the plasma membrane is bent to accommodate clathrin-independent endocytosis remains uncertain. Recent studies suggest Shiga and cholera toxin induce membrane curvature required for their uptake into clathrin-independent carriers by binding and cross-linking multiple copies of their glycosphingolipid receptors on the plasma membrane. But it remains unclear if toxin-induced sphingolipid crosslinking provides sufficient mechanical force for deforming the plasma membrane, or if host cell factors also contribute to this process. To test this, we imaged the uptake of cholera toxin B-subunit into surface-derived tubular invaginations. We found that cholera toxin mutants that bind to only one glycosphingolipid receptor accumulated in tubules, and that toxin binding was entirely dispensable for membrane tubulations to form. Unexpectedly, the driving force for tubule extension was supplied by the combination of microtubules, dynein and dynactin, thus defining a novel mechanism for generating membrane curvature during clathrin-independent endocytosis.",

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AU - Tiwari, Ajit

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AU - Davidson, Michael W.

AU - Holmes, Randall K.

AU - Jobling, Michael G.

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AU - Kenworthy, Anne K.

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Microtubule Motors Power Plasma Membrane Tubulation in Clathrin-Independent Endocytosis

Abstract

Bibliographical note

Keywords

UN SDGs

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