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The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis

Expression of the initiator methionine tRNA (tRNA(i)(Met)) is deregulated in cancer. Despite this fact, it is not currently known how tRNA(i)(Met) expression levels influence tumor progression. We have found that tRNA(i)(Met) expression is increased in carcinoma-associated fibroblasts, implicating d...

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Autores principales: Clarke, Cassie J., Berg, Tracy J., Birch, Joanna, Ennis, Darren, Mitchell, Louise, Cloix, Catherine, Campbell, Andrew, Sumpton, David, Nixon, Colin, Campbell, Kirsteen, Bridgeman, Victoria L., Vermeulen, Peter B., Foo, Shane, Kostaras, Eleftherios, Jones, J. Louise, Haywood, Linda, Pulleine, Ellie, Yin, Huabing, Strathdee, Douglas, Sansom, Owen, Blyth, Karen, McNeish, Iain, Zanivan, Sara, Reynolds, Andrew R., Norman, Jim C.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Cell Press 2016
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4819511/
https://www.ncbi.nlm.nih.gov/pubmed/26948875
http://dx.doi.org/10.1016/j.cub.2016.01.045
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author Clarke, Cassie J.
Berg, Tracy J.
Birch, Joanna
Ennis, Darren
Mitchell, Louise
Cloix, Catherine
Campbell, Andrew
Sumpton, David
Nixon, Colin
Campbell, Kirsteen
Bridgeman, Victoria L.
Vermeulen, Peter B.
Foo, Shane
Kostaras, Eleftherios
Jones, J. Louise
Haywood, Linda
Pulleine, Ellie
Yin, Huabing
Strathdee, Douglas
Sansom, Owen
Blyth, Karen
McNeish, Iain
Zanivan, Sara
Reynolds, Andrew R.
Norman, Jim C.
author_facet Clarke, Cassie J.
Berg, Tracy J.
Birch, Joanna
Ennis, Darren
Mitchell, Louise
Cloix, Catherine
Campbell, Andrew
Sumpton, David
Nixon, Colin
Campbell, Kirsteen
Bridgeman, Victoria L.
Vermeulen, Peter B.
Foo, Shane
Kostaras, Eleftherios
Jones, J. Louise
Haywood, Linda
Pulleine, Ellie
Yin, Huabing
Strathdee, Douglas
Sansom, Owen
Blyth, Karen
McNeish, Iain
Zanivan, Sara
Reynolds, Andrew R.
Norman, Jim C.
author_sort Clarke, Cassie J.
collection PubMed
description Expression of the initiator methionine tRNA (tRNA(i)(Met)) is deregulated in cancer. Despite this fact, it is not currently known how tRNA(i)(Met) expression levels influence tumor progression. We have found that tRNA(i)(Met) expression is increased in carcinoma-associated fibroblasts, implicating deregulated expression of tRNA(i)(Met) in the tumor stroma as a possible contributor to tumor progression. To investigate how elevated stromal tRNA(i)(Met) contributes to tumor progression, we generated a mouse expressing additional copies of the tRNA(i)(Met) gene (2+tRNA(i)(Met) mouse). Growth and vascularization of subcutaneous tumor allografts was enhanced in 2+tRNA(i)(Met) mice compared with wild-type littermate controls. Extracellular matrix (ECM) deposited by fibroblasts from 2+tRNA(i)(Met) mice supported enhanced endothelial cell and fibroblast migration. SILAC mass spectrometry indicated that elevated expression of tRNA(i)(Met) significantly increased synthesis and secretion of certain types of collagen, in particular type II collagen. Suppression of type II collagen opposed the ability of tRNA(i)(Met)-overexpressing fibroblasts to deposit pro-migratory ECM. We used the prolyl hydroxylase inhibitor ethyl-3,4-dihydroxybenzoate (DHB) to determine whether collagen synthesis contributes to the tRNA(i)(Met)-driven pro-tumorigenic stroma in vivo. DHB had no effect on the growth of syngeneic allografts in wild-type mice but opposed the ability of 2+tRNA(i)(Met) mice to support increased angiogenesis and tumor growth. Finally, collagen II expression predicts poor prognosis in high-grade serous ovarian carcinoma. Taken together, these data indicate that increased tRNA(i)(Met) levels contribute to tumor progression by enhancing the ability of stromal fibroblasts to synthesize and secrete a type II collagen-rich ECM that supports endothelial cell migration and angiogenesis.
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spelling pubmed-48195112016-04-14 The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis Clarke, Cassie J. Berg, Tracy J. Birch, Joanna Ennis, Darren Mitchell, Louise Cloix, Catherine Campbell, Andrew Sumpton, David Nixon, Colin Campbell, Kirsteen Bridgeman, Victoria L. Vermeulen, Peter B. Foo, Shane Kostaras, Eleftherios Jones, J. Louise Haywood, Linda Pulleine, Ellie Yin, Huabing Strathdee, Douglas Sansom, Owen Blyth, Karen McNeish, Iain Zanivan, Sara Reynolds, Andrew R. Norman, Jim C. Curr Biol Article Expression of the initiator methionine tRNA (tRNA(i)(Met)) is deregulated in cancer. Despite this fact, it is not currently known how tRNA(i)(Met) expression levels influence tumor progression. We have found that tRNA(i)(Met) expression is increased in carcinoma-associated fibroblasts, implicating deregulated expression of tRNA(i)(Met) in the tumor stroma as a possible contributor to tumor progression. To investigate how elevated stromal tRNA(i)(Met) contributes to tumor progression, we generated a mouse expressing additional copies of the tRNA(i)(Met) gene (2+tRNA(i)(Met) mouse). Growth and vascularization of subcutaneous tumor allografts was enhanced in 2+tRNA(i)(Met) mice compared with wild-type littermate controls. Extracellular matrix (ECM) deposited by fibroblasts from 2+tRNA(i)(Met) mice supported enhanced endothelial cell and fibroblast migration. SILAC mass spectrometry indicated that elevated expression of tRNA(i)(Met) significantly increased synthesis and secretion of certain types of collagen, in particular type II collagen. Suppression of type II collagen opposed the ability of tRNA(i)(Met)-overexpressing fibroblasts to deposit pro-migratory ECM. We used the prolyl hydroxylase inhibitor ethyl-3,4-dihydroxybenzoate (DHB) to determine whether collagen synthesis contributes to the tRNA(i)(Met)-driven pro-tumorigenic stroma in vivo. DHB had no effect on the growth of syngeneic allografts in wild-type mice but opposed the ability of 2+tRNA(i)(Met) mice to support increased angiogenesis and tumor growth. Finally, collagen II expression predicts poor prognosis in high-grade serous ovarian carcinoma. Taken together, these data indicate that increased tRNA(i)(Met) levels contribute to tumor progression by enhancing the ability of stromal fibroblasts to synthesize and secrete a type II collagen-rich ECM that supports endothelial cell migration and angiogenesis. Cell Press 2016-03-21 /pmc/articles/PMC4819511/ /pubmed/26948875 http://dx.doi.org/10.1016/j.cub.2016.01.045 Text en © 2016 The Authors http://creativecommons.org/licenses/by/4.0/ This is an open access article under the CC BY license (http://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Clarke, Cassie J.
Berg, Tracy J.
Birch, Joanna
Ennis, Darren
Mitchell, Louise
Cloix, Catherine
Campbell, Andrew
Sumpton, David
Nixon, Colin
Campbell, Kirsteen
Bridgeman, Victoria L.
Vermeulen, Peter B.
Foo, Shane
Kostaras, Eleftherios
Jones, J. Louise
Haywood, Linda
Pulleine, Ellie
Yin, Huabing
Strathdee, Douglas
Sansom, Owen
Blyth, Karen
McNeish, Iain
Zanivan, Sara
Reynolds, Andrew R.
Norman, Jim C.
The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis
title The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis
title_full The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis
title_fullStr The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis
title_full_unstemmed The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis
title_short The Initiator Methionine tRNA Drives Secretion of Type II Collagen from Stromal Fibroblasts to Promote Tumor Growth and Angiogenesis
title_sort initiator methionine trna drives secretion of type ii collagen from stromal fibroblasts to promote tumor growth and angiogenesis
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4819511/
https://www.ncbi.nlm.nih.gov/pubmed/26948875
http://dx.doi.org/10.1016/j.cub.2016.01.045
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