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A RAC-GEF network critical for early intestinal tumourigenesis

RAC1 activity is critical for intestinal homeostasis, and is required for hyperproliferation driven by loss of the tumour suppressor gene Apc in the murine intestine. To avoid the impact of direct targeting upon homeostasis, we reasoned that indirect targeting of RAC1 via RAC-GEFs might be effective...

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Autores principales: Pickering, K. A., Gilroy, K., Cassidy, J. W., Fey, S. K., Najumudeen, A. K., Zeiger, L. B., Vincent, D. F., Gay, D. M., Johansson, J., Fordham, R. P., Miller, B., Clark, W., Hedley, A., Unal, E. B., Kiel, C., McGhee, E., Machesky, L. M., Nixon, C., Johnsson, A. E., Bain, M., Strathdee, D., van Hoof, S. R., Medema, J. P., Anderson, K. I., Brachmann, S. M., Stucke, V. M., Malliri, A., Drysdale, M., Turner, M., Serrano, L., Myant, K., Campbell, A. D., Sansom, O. J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Nature Publishing Group UK 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7782582/
https://www.ncbi.nlm.nih.gov/pubmed/33397922
http://dx.doi.org/10.1038/s41467-020-20255-4
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author Pickering, K. A.
Gilroy, K.
Cassidy, J. W.
Fey, S. K.
Najumudeen, A. K.
Zeiger, L. B.
Vincent, D. F.
Gay, D. M.
Johansson, J.
Fordham, R. P.
Miller, B.
Clark, W.
Hedley, A.
Unal, E. B.
Kiel, C.
McGhee, E.
Machesky, L. M.
Nixon, C.
Johnsson, A. E.
Bain, M.
Strathdee, D.
van Hoof, S. R.
Medema, J. P.
Anderson, K. I.
Brachmann, S. M.
Stucke, V. M.
Malliri, A.
Drysdale, M.
Turner, M.
Serrano, L.
Myant, K.
Campbell, A. D.
Sansom, O. J.
author_facet Pickering, K. A.
Gilroy, K.
Cassidy, J. W.
Fey, S. K.
Najumudeen, A. K.
Zeiger, L. B.
Vincent, D. F.
Gay, D. M.
Johansson, J.
Fordham, R. P.
Miller, B.
Clark, W.
Hedley, A.
Unal, E. B.
Kiel, C.
McGhee, E.
Machesky, L. M.
Nixon, C.
Johnsson, A. E.
Bain, M.
Strathdee, D.
van Hoof, S. R.
Medema, J. P.
Anderson, K. I.
Brachmann, S. M.
Stucke, V. M.
Malliri, A.
Drysdale, M.
Turner, M.
Serrano, L.
Myant, K.
Campbell, A. D.
Sansom, O. J.
author_sort Pickering, K. A.
collection PubMed
description RAC1 activity is critical for intestinal homeostasis, and is required for hyperproliferation driven by loss of the tumour suppressor gene Apc in the murine intestine. To avoid the impact of direct targeting upon homeostasis, we reasoned that indirect targeting of RAC1 via RAC-GEFs might be effective. Transcriptional profiling of Apc deficient intestinal tissue identified Vav3 and Tiam1 as key targets. Deletion of these indicated that while TIAM1 deficiency could suppress Apc-driven hyperproliferation, it had no impact upon tumourigenesis, while VAV3 deficiency had no effect. Intriguingly, deletion of either gene resulted in upregulation of Vav2, with subsequent targeting of all three (Vav2(−/−) Vav3(−/−) Tiam1(−/−)), profoundly suppressing hyperproliferation, tumourigenesis and RAC1 activity, without impacting normal homeostasis. Critically, the observed RAC-GEF dependency was negated by oncogenic KRAS mutation. Together, these data demonstrate that while targeting RAC-GEF molecules may have therapeutic impact at early stages, this benefit may be lost in late stage disease.
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spelling pubmed-77825822021-01-11 A RAC-GEF network critical for early intestinal tumourigenesis Pickering, K. A. Gilroy, K. Cassidy, J. W. Fey, S. K. Najumudeen, A. K. Zeiger, L. B. Vincent, D. F. Gay, D. M. Johansson, J. Fordham, R. P. Miller, B. Clark, W. Hedley, A. Unal, E. B. Kiel, C. McGhee, E. Machesky, L. M. Nixon, C. Johnsson, A. E. Bain, M. Strathdee, D. van Hoof, S. R. Medema, J. P. Anderson, K. I. Brachmann, S. M. Stucke, V. M. Malliri, A. Drysdale, M. Turner, M. Serrano, L. Myant, K. Campbell, A. D. Sansom, O. J. Nat Commun Article RAC1 activity is critical for intestinal homeostasis, and is required for hyperproliferation driven by loss of the tumour suppressor gene Apc in the murine intestine. To avoid the impact of direct targeting upon homeostasis, we reasoned that indirect targeting of RAC1 via RAC-GEFs might be effective. Transcriptional profiling of Apc deficient intestinal tissue identified Vav3 and Tiam1 as key targets. Deletion of these indicated that while TIAM1 deficiency could suppress Apc-driven hyperproliferation, it had no impact upon tumourigenesis, while VAV3 deficiency had no effect. Intriguingly, deletion of either gene resulted in upregulation of Vav2, with subsequent targeting of all three (Vav2(−/−) Vav3(−/−) Tiam1(−/−)), profoundly suppressing hyperproliferation, tumourigenesis and RAC1 activity, without impacting normal homeostasis. Critically, the observed RAC-GEF dependency was negated by oncogenic KRAS mutation. Together, these data demonstrate that while targeting RAC-GEF molecules may have therapeutic impact at early stages, this benefit may be lost in late stage disease. Nature Publishing Group UK 2021-01-04 /pmc/articles/PMC7782582/ /pubmed/33397922 http://dx.doi.org/10.1038/s41467-020-20255-4 Text en © The Author(s) 2021 Open Access This article is licensed under a Creative Commons Attribution 4.0 International License, which permits use, sharing, adaptation, distribution and reproduction in any medium or format, as long as you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The images or other third party material in this article are included in the article’s Creative Commons license, unless indicated otherwise in a credit line to the material. If material is not included in the article’s Creative Commons license and your intended use is not permitted by statutory regulation or exceeds the permitted use, you will need to obtain permission directly from the copyright holder. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/.
spellingShingle Article
Pickering, K. A.
Gilroy, K.
Cassidy, J. W.
Fey, S. K.
Najumudeen, A. K.
Zeiger, L. B.
Vincent, D. F.
Gay, D. M.
Johansson, J.
Fordham, R. P.
Miller, B.
Clark, W.
Hedley, A.
Unal, E. B.
Kiel, C.
McGhee, E.
Machesky, L. M.
Nixon, C.
Johnsson, A. E.
Bain, M.
Strathdee, D.
van Hoof, S. R.
Medema, J. P.
Anderson, K. I.
Brachmann, S. M.
Stucke, V. M.
Malliri, A.
Drysdale, M.
Turner, M.
Serrano, L.
Myant, K.
Campbell, A. D.
Sansom, O. J.
A RAC-GEF network critical for early intestinal tumourigenesis
title A RAC-GEF network critical for early intestinal tumourigenesis
title_full A RAC-GEF network critical for early intestinal tumourigenesis
title_fullStr A RAC-GEF network critical for early intestinal tumourigenesis
title_full_unstemmed A RAC-GEF network critical for early intestinal tumourigenesis
title_short A RAC-GEF network critical for early intestinal tumourigenesis
title_sort rac-gef network critical for early intestinal tumourigenesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7782582/
https://www.ncbi.nlm.nih.gov/pubmed/33397922
http://dx.doi.org/10.1038/s41467-020-20255-4
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