Microtubule acetylation is implicated in regulating cell motility, yet its physiological role in directional migration and the underlying molecular mechanisms have remained unclear. This knowledge gap has persisted primarily due to a lack of tools capable of rapidly manipulating microtubule acetylation in actively migrating cells. To overcome this limitation and elucidate the causal relationship between microtubule acetylation and cell migration, we developed a novel optogenetic actuator, optoTAT, which enables precise induction of microtubule acetylation within minutes in live cells. Implementing optoTAT in migration assays, we observed striking and rapid responses at both molecular and cellular levels. First, microtubule acetylation triggers release of the RhoA activator GEF-H1 from sequestration on microtubules. This release subsequently enhances actomyosin contractility and drives focal adhesion maturation. These subcellular processes collectively promote sustained directional migration. Our findings position GEF-H1 as a critical molecular responder to microtubule acetylation, enabling a dynamic crosstalk between the actin and microtubule cytoskeletal networks in the coordination of cellular motility.
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March 19 2026
OptoTAT reveals microtubule acetylation as a rapid trigger for GEF-H1–mediated cell migration
Abhijit Deb Roy
,
(Conceptualization, Data curation, Formal analysis, Funding acquisition, Investigation, Methodology, Project administration, Resources, Software, Supervision, Validation, Visualization, Writing - original draft, Writing - review & editing)
1Department of Cell Biology and Center for Cell Dynamics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
3
Center for Cell Analysis and Modeling, University of Connecticut School of Medicine
, Farmington, CT, USA
4Department of Cell Biology,
University of Connecticut School of Medicine
, Farmington, CT, USA
Abhijit Deb Roy: [email protected]
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Cristian Saez Gonzalez
,
Cristian Saez Gonzalez
(Data curation, Formal analysis, Investigation, Methodology, Visualization)
1Department of Cell Biology and Center for Cell Dynamics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
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Milda Stanislauskas
,
Milda Stanislauskas
(Investigation)
3
Center for Cell Analysis and Modeling, University of Connecticut School of Medicine
, Farmington, CT, USA
4Department of Cell Biology,
University of Connecticut School of Medicine
, Farmington, CT, USA
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Farid Shahid
,
Farid Shahid
(Investigation)
2
The Johns Hopkins University
, Baltimore, MD, USA
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Eesha Yadav
,
Eesha Yadav
(Conceptualization, Investigation)
2
The Johns Hopkins University
, Baltimore, MD, USA
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Jalil Rezek
,
Jalil Rezek
(Formal analysis)
2
The Johns Hopkins University
, Baltimore, MD, USA
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Takanari Inoue
(Funding acquisition, Project administration, Supervision, Writing - review & editing)
1Department of Cell Biology and Center for Cell Dynamics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Correspondence to Takanari Inoue: [email protected]
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Abhijit Deb Roy
https://orcid.org/0000-0003-1640-2402
Conceptualization, Data curation, Formal analysis, Funding acquisition, Investigation, Methodology, Project administration, Resources, Software, Supervision, Validation, Visualization, Writing - original draft, Writing - review & editing
1Department of Cell Biology and Center for Cell Dynamics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
3
Center for Cell Analysis and Modeling, University of Connecticut School of Medicine
, Farmington, CT, USA
4Department of Cell Biology,
University of Connecticut School of Medicine
, Farmington, CT, USA
Cristian Saez Gonzalez
https://orcid.org/0000-0003-4846-3680
Data curation, Formal analysis, Investigation, Methodology, Visualization
1Department of Cell Biology and Center for Cell Dynamics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Milda Stanislauskas
https://orcid.org/0009-0005-9029-4798
Investigation
3
Center for Cell Analysis and Modeling, University of Connecticut School of Medicine
, Farmington, CT, USA
4Department of Cell Biology,
University of Connecticut School of Medicine
, Farmington, CT, USA
Farid Shahid
https://orcid.org/0009-0002-2564-1405
Investigation
2
The Johns Hopkins University
, Baltimore, MD, USA
Eesha Yadav
https://orcid.org/0000-0002-6290-5222
Conceptualization, Investigation
2
The Johns Hopkins University
, Baltimore, MD, USA
Jalil Rezek
https://orcid.org/0009-0001-2646-372X
Formal analysis
2
The Johns Hopkins University
, Baltimore, MD, USA
Takanari Inoue
https://orcid.org/0000-0002-7957-7624
Funding acquisition, Project administration, Supervision, Writing - review & editing
1Department of Cell Biology and Center for Cell Dynamics,
Johns Hopkins University School of Medicine
, Baltimore, MD, USA
Correspondence to Takanari Inoue: [email protected]
Abhijit Deb Roy: [email protected]
Disclosures: The authors declare no competing interests exist.
Received:
August 14 2025
Revision Received:
January 08 2026
Accepted:
February 13 2026
Online ISSN: 1540-8140
Print ISSN: 0021-9525
Funding
Funder(s):
National Institutes of Health
- Award Id(s): R35GM149329,T32GM007445,F31GM153141
Funder(s):
American Heart Association
- Award Id(s): 23POST1057352
Funder(s):
D.C. Women’s Board Postdoctoral Fellowship
© 2026 Deb Roy et al.
2026
Deb Roy et al.
This article is distributed under the terms as described at https://rupress.org/pages/terms102024/.
J Cell Biol (2026) 225 (5): e202508095.
Article history
Received:
August 14 2025
Revision Received:
January 08 2026
Accepted:
February 13 2026
Citation
Abhijit Deb Roy, Cristian Saez Gonzalez, Milda Stanislauskas, Farid Shahid, Eesha Yadav, Jalil Rezek, Takanari Inoue; OptoTAT reveals microtubule acetylation as a rapid trigger for GEF-H1–mediated cell migration. J Cell Biol 4 May 2026; 225 (5): e202508095. doi: https://doi.org/10.1083/jcb.202508095
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