Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis

Ewan MacDonald; Alison Forrester; Cesar A. Valades-Cruz; Thomas D. Madsen; Joseph H.R. Hetmanski; Estelle Dransart; Yeap Ng; Rashmi Godbole; Ananthan Akhil Shp; Ludovic Leconte; Valérie Chambon; Debarpan Ghosh; Alexis Pinet; Dhiraj Bhatia; Bérangère Lombard; Damarys Loew; Martin R. Larsen; Hakon Leffler; Dirk J. Lefeber; Henrik Clausen; Anne Blangy; Patrick Caswell; Massiullah Shafaq-Zadah; Satyajit Mayor; Roberto Weigert; Christian Wunder; Ludger Johannes

doi:10.1038/s41556-025-01616-x

Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis

Ewan MacDonald, Alison Forrester, Cesar A. Valades-Cruz, Thomas D. Madsen, Joseph H.R. Hetmanski, Estelle Dransart, Yeap Ng, Rashmi Godbole, Ananthan Akhil Shp, Ludovic Leconte, Valérie Chambon, Debarpan Ghosh, Alexis Pinet, Dhiraj Bhatia, Bérangère Lombard, Damarys Loew, Martin R. Larsen, Hakon Leffler, Dirk J. Lefeber, Henrik ClausenAnne Blangy, Patrick Caswell, Massiullah Shafaq-Zadah, Satyajit Mayor, Roberto Weigert, Christian Wunder, Ludger Johannes^*

^*Corresponding author for this work

Research output: Contribution to journal › Journal article › Research › peer-review

Abstract

Glycolipid-lectin-driven endocytosis controls the formation of clathrin-independent carriers and the internalization of various cargos such as β1 integrin. Whether this process is regulated in a dynamic manner remained unexplored. Here we demonstrate that, within minutes, the epidermal growth factor triggers the galectin-driven endocytosis of cell-surface glycoproteins, such as integrins, that are key regulators of cell adhesion and migration. The onset of this process—mediated by the Na⁺/H⁺ antiporter NHE1 as well as the neuraminidases Neu1 and Neu3—requires the pH-triggered enzymatic removal of sialic acids whose presence otherwise prevents galectin binding. De-sialylated glycoproteins are then retrogradely transported to the Golgi apparatus where their glycan make-up is reset to regulate EGF-dependent invasive-cell migration. Further evidence is provided for a role of neuraminidases and galectin-3 in acidification-dependent bone resorption. Glycosylation at the cell surface thereby emerges as a dynamic and reversible regulatory post-translational modification that controls a highly adaptable trafficking pathway.

Original language	English
Journal	Nature Cell Biology
Volume	27
Pages (from-to)	449–463
ISSN	1465-7392
DOIs	https://doi.org/10.1038/s41556-025-01616-x
Publication status	Published - 2025

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MacDonald, E., Forrester, A., Valades-Cruz, C. A., Madsen, T. D., Hetmanski, J. H. R., Dransart, E., Ng, Y., Godbole, R., Shp, A. A., Leconte, L., Chambon, V., Ghosh, D., Pinet, A., Bhatia, D., Lombard, B., Loew, D., Larsen, M. R., Leffler, H., Lefeber, D. J., ... Johannes, L. (2025). Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis. Nature Cell Biology, 27, 449–463. https://doi.org/10.1038/s41556-025-01616-x

@article{5eb32fef7404458395c4c1f7f0e7c1b5,

title = "Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis",

abstract = "Glycolipid-lectin-driven endocytosis controls the formation of clathrin-independent carriers and the internalization of various cargos such as β1 integrin. Whether this process is regulated in a dynamic manner remained unexplored. Here we demonstrate that, within minutes, the epidermal growth factor triggers the galectin-driven endocytosis of cell-surface glycoproteins, such as integrins, that are key regulators of cell adhesion and migration. The onset of this process—mediated by the Na+/H+ antiporter NHE1 as well as the neuraminidases Neu1 and Neu3—requires the pH-triggered enzymatic removal of sialic acids whose presence otherwise prevents galectin binding. De-sialylated glycoproteins are then retrogradely transported to the Golgi apparatus where their glycan make-up is reset to regulate EGF-dependent invasive-cell migration. Further evidence is provided for a role of neuraminidases and galectin-3 in acidification-dependent bone resorption. Glycosylation at the cell surface thereby emerges as a dynamic and reversible regulatory post-translational modification that controls a highly adaptable trafficking pathway.",

author = "Ewan MacDonald and Alison Forrester and Valades-Cruz, {Cesar A.} and Madsen, {Thomas D.} and Hetmanski, {Joseph H.R.} and Estelle Dransart and Yeap Ng and Rashmi Godbole and Shp, {Ananthan Akhil} and Ludovic Leconte and Val{\'e}rie Chambon and Debarpan Ghosh and Alexis Pinet and Dhiraj Bhatia and B{\'e}rang{\`e}re Lombard and Damarys Loew and Larsen, {Martin R.} and Hakon Leffler and Lefeber, {Dirk J.} and Henrik Clausen and Anne Blangy and Patrick Caswell and Massiullah Shafaq-Zadah and Satyajit Mayor and Roberto Weigert and Christian Wunder and Ludger Johannes",

year = "2025",

doi = "10.1038/s41556-025-01616-x",

language = "English",

volume = "27",

pages = "449–463",

journal = "Nature Cell Biology",

issn = "1465-7392",

publisher = "Nature Research",

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MacDonald, E, Forrester, A, Valades-Cruz, CA, Madsen, TD, Hetmanski, JHR, Dransart, E, Ng, Y, Godbole, R, Shp, AA, Leconte, L, Chambon, V, Ghosh, D, Pinet, A, Bhatia, D, Lombard, B, Loew, D, Larsen, MR, Leffler, H, Lefeber, DJ, Clausen, H, Blangy, A, Caswell, P, Shafaq-Zadah, M, Mayor, S, Weigert, R, Wunder, C & Johannes, L 2025, 'Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis', Nature Cell Biology, vol. 27, pp. 449–463. https://doi.org/10.1038/s41556-025-01616-x

TY - JOUR

T1 - Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis

AU - MacDonald, Ewan

AU - Forrester, Alison

AU - Valades-Cruz, Cesar A.

AU - Madsen, Thomas D.

AU - Hetmanski, Joseph H.R.

AU - Dransart, Estelle

AU - Ng, Yeap

AU - Godbole, Rashmi

AU - Shp, Ananthan Akhil

AU - Leconte, Ludovic

AU - Chambon, Valérie

AU - Ghosh, Debarpan

AU - Pinet, Alexis

AU - Bhatia, Dhiraj

AU - Lombard, Bérangère

AU - Loew, Damarys

AU - Larsen, Martin R.

AU - Leffler, Hakon

AU - Lefeber, Dirk J.

AU - Clausen, Henrik

AU - Blangy, Anne

AU - Caswell, Patrick

AU - Shafaq-Zadah, Massiullah

AU - Mayor, Satyajit

AU - Weigert, Roberto

AU - Wunder, Christian

AU - Johannes, Ludger

PY - 2025

Y1 - 2025

N2 - Glycolipid-lectin-driven endocytosis controls the formation of clathrin-independent carriers and the internalization of various cargos such as β1 integrin. Whether this process is regulated in a dynamic manner remained unexplored. Here we demonstrate that, within minutes, the epidermal growth factor triggers the galectin-driven endocytosis of cell-surface glycoproteins, such as integrins, that are key regulators of cell adhesion and migration. The onset of this process—mediated by the Na+/H+ antiporter NHE1 as well as the neuraminidases Neu1 and Neu3—requires the pH-triggered enzymatic removal of sialic acids whose presence otherwise prevents galectin binding. De-sialylated glycoproteins are then retrogradely transported to the Golgi apparatus where their glycan make-up is reset to regulate EGF-dependent invasive-cell migration. Further evidence is provided for a role of neuraminidases and galectin-3 in acidification-dependent bone resorption. Glycosylation at the cell surface thereby emerges as a dynamic and reversible regulatory post-translational modification that controls a highly adaptable trafficking pathway.

AB - Glycolipid-lectin-driven endocytosis controls the formation of clathrin-independent carriers and the internalization of various cargos such as β1 integrin. Whether this process is regulated in a dynamic manner remained unexplored. Here we demonstrate that, within minutes, the epidermal growth factor triggers the galectin-driven endocytosis of cell-surface glycoproteins, such as integrins, that are key regulators of cell adhesion and migration. The onset of this process—mediated by the Na+/H+ antiporter NHE1 as well as the neuraminidases Neu1 and Neu3—requires the pH-triggered enzymatic removal of sialic acids whose presence otherwise prevents galectin binding. De-sialylated glycoproteins are then retrogradely transported to the Golgi apparatus where their glycan make-up is reset to regulate EGF-dependent invasive-cell migration. Further evidence is provided for a role of neuraminidases and galectin-3 in acidification-dependent bone resorption. Glycosylation at the cell surface thereby emerges as a dynamic and reversible regulatory post-translational modification that controls a highly adaptable trafficking pathway.

UR - https://doi.org/10.1038/s41556-025-01643-8

U2 - 10.1038/s41556-025-01616-x

DO - 10.1038/s41556-025-01616-x

M3 - Journal article

AN - SCOPUS:85218711814

SN - 1465-7392

VL - 27

SP - 449

EP - 463

JO - Nature Cell Biology

JF - Nature Cell Biology

ER -

Growth factor-triggered de-sialylation controls glycolipid-lectin-driven endocytosis

Abstract

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