ISGylation drives basal breast tumour progression by promoting EGFR recycling and Akt signalling

Alfonso Bolado-Carrancio; Martin Lee; Ailith Ewing; Morwenna Muir; Kenneth G. Macleod; William M. Gallagher; Lan K. Nguyen; Neil O. Carragher; Colin A. Semple; Valerie G. Brunton; Patrick T. Caswell; Alex von Kriegsheim

doi:10.1038/s41388-021-02017-8

ISGylation drives basal breast tumour progression by promoting EGFR recycling and Akt signalling

Alfonso Bolado-Carrancio, Martin Lee, Ailith Ewing, Morwenna Muir, Kenneth G. Macleod, William M. Gallagher, Lan K. Nguyen, Neil O. Carragher, Colin A. Semple, Valerie G. Brunton, Patrick T. Caswell, Alex von Kriegsheim

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

20 Citations (Scopus)

Abstract

ISG15 is an ubiquitin-like modifier that is associated with reduced survival rates in breast cancer patients. The mechanism by which ISG15 achieves this however remains elusive. We demonstrate that modification of Rab GDP-Dissociation Inhibitor Beta (GDI2) by ISG15 (ISGylation) alters endocytic recycling of the EGF receptor (EGFR) in non-interferon stimulated cells using CRISPR-knock out models for ISGylation. By regulating EGFR trafficking, ISGylation enhances EGFR recycling and sustains Akt-signalling. We further show that Akt signalling positively correlates with levels of ISG15 and its E2-ligase in basal breast cancer cohorts, confirming the link between ISGylation and Akt signalling in human tumours. Persistent and enhanced Akt activation explains the more aggressive tumour behaviour observed in human breast cancers. We show that ISGylation can act as a driver of tumour progression rather than merely being a bystander.

Original language	English
Pages (from-to)	6235-6247
Number of pages	13
Journal	Oncogene
Volume	40
Issue number	44
DOIs	https://doi.org/10.1038/s41388-021-02017-8
Publication status	Published - 3 Nov 2021

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@article{f5f90a21c9c84adc9ba9589480711ddc,

title = "ISGylation drives basal breast tumour progression by promoting EGFR recycling and Akt signalling",

abstract = "ISG15 is an ubiquitin-like modifier that is associated with reduced survival rates in breast cancer patients. The mechanism by which ISG15 achieves this however remains elusive. We demonstrate that modification of Rab GDP-Dissociation Inhibitor Beta (GDI2) by ISG15 (ISGylation) alters endocytic recycling of the EGF receptor (EGFR) in non-interferon stimulated cells using CRISPR-knock out models for ISGylation. By regulating EGFR trafficking, ISGylation enhances EGFR recycling and sustains Akt-signalling. We further show that Akt signalling positively correlates with levels of ISG15 and its E2-ligase in basal breast cancer cohorts, confirming the link between ISGylation and Akt signalling in human tumours. Persistent and enhanced Akt activation explains the more aggressive tumour behaviour observed in human breast cancers. We show that ISGylation can act as a driver of tumour progression rather than merely being a bystander.",

author = "Alfonso Bolado-Carrancio and Martin Lee and Ailith Ewing and Morwenna Muir and Macleod, {Kenneth G.} and Gallagher, {William M.} and Nguyen, {Lan K.} and Carragher, {Neil O.} and Semple, {Colin A.} and Brunton, {Valerie G.} and Caswell, {Patrick T.} and {von Kriegsheim}, Alex",

note = "Funding Information: We thank Ana Herrero for help with the cellular fractionation method, Breast Cancer NOW (2013NovPR183), Cancer Research UK. Cancer Research UK (CRUK Edinburgh Centre C157/A255140 & C157/A24837), Wellcome Trust (Multiuser Equipment Grant, 208402/Z/17/Z & Centre for Cell-Matrix Research 203128/A/16/Z), MRC (core funding to the MRC Human Genetics Unit MRC grant MC_UU_00007/16 & MR/R009376/1), Worldwide Cancer Research (14–1226), Australia{\textquoteright}s Victorian Cancer Agency (MCRF18026), BREAST-PREDICT (CCRC13GAL) and Science Foundation Ireland (15/ IA/3104) for funding. Publisher Copyright: {\textcopyright} 2021, The Author(s). Copyright: Copyright 2021 Elsevier B.V., All rights reserved.",

year = "2021",

month = nov,

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doi = "10.1038/s41388-021-02017-8",

language = "English",

volume = "40",

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T1 - ISGylation drives basal breast tumour progression by promoting EGFR recycling and Akt signalling

AU - Bolado-Carrancio, Alfonso

AU - Lee, Martin

AU - Ewing, Ailith

AU - Muir, Morwenna

AU - Macleod, Kenneth G.

AU - Gallagher, William M.

AU - Nguyen, Lan K.

AU - Carragher, Neil O.

AU - Semple, Colin A.

AU - Brunton, Valerie G.

AU - Caswell, Patrick T.

AU - von Kriegsheim, Alex

N1 - Funding Information: We thank Ana Herrero for help with the cellular fractionation method, Breast Cancer NOW (2013NovPR183), Cancer Research UK. Cancer Research UK (CRUK Edinburgh Centre C157/A255140 & C157/A24837), Wellcome Trust (Multiuser Equipment Grant, 208402/Z/17/Z & Centre for Cell-Matrix Research 203128/A/16/Z), MRC (core funding to the MRC Human Genetics Unit MRC grant MC_UU_00007/16 & MR/R009376/1), Worldwide Cancer Research (14–1226), Australia’s Victorian Cancer Agency (MCRF18026), BREAST-PREDICT (CCRC13GAL) and Science Foundation Ireland (15/ IA/3104) for funding. Publisher Copyright: © 2021, The Author(s). Copyright: Copyright 2021 Elsevier B.V., All rights reserved.

PY - 2021/11/3

Y1 - 2021/11/3

N2 - ISG15 is an ubiquitin-like modifier that is associated with reduced survival rates in breast cancer patients. The mechanism by which ISG15 achieves this however remains elusive. We demonstrate that modification of Rab GDP-Dissociation Inhibitor Beta (GDI2) by ISG15 (ISGylation) alters endocytic recycling of the EGF receptor (EGFR) in non-interferon stimulated cells using CRISPR-knock out models for ISGylation. By regulating EGFR trafficking, ISGylation enhances EGFR recycling and sustains Akt-signalling. We further show that Akt signalling positively correlates with levels of ISG15 and its E2-ligase in basal breast cancer cohorts, confirming the link between ISGylation and Akt signalling in human tumours. Persistent and enhanced Akt activation explains the more aggressive tumour behaviour observed in human breast cancers. We show that ISGylation can act as a driver of tumour progression rather than merely being a bystander.

AB - ISG15 is an ubiquitin-like modifier that is associated with reduced survival rates in breast cancer patients. The mechanism by which ISG15 achieves this however remains elusive. We demonstrate that modification of Rab GDP-Dissociation Inhibitor Beta (GDI2) by ISG15 (ISGylation) alters endocytic recycling of the EGF receptor (EGFR) in non-interferon stimulated cells using CRISPR-knock out models for ISGylation. By regulating EGFR trafficking, ISGylation enhances EGFR recycling and sustains Akt-signalling. We further show that Akt signalling positively correlates with levels of ISG15 and its E2-ligase in basal breast cancer cohorts, confirming the link between ISGylation and Akt signalling in human tumours. Persistent and enhanced Akt activation explains the more aggressive tumour behaviour observed in human breast cancers. We show that ISGylation can act as a driver of tumour progression rather than merely being a bystander.

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SP - 6235

EP - 6247

JO - Oncogene

JF - Oncogene

IS - 44

ER -

ISGylation drives basal breast tumour progression by promoting EGFR recycling and Akt signalling

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Combating adaptive resistance to tageted therapy in triple-negative breast cancer

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ISGylation drives basal breast tumour progression by promoting EGFR recycling and Akt signalling

Abstract

UN SDGs

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Combating adaptive resistance to tageted therapy in triple-negative breast cancer

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