Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models

Anti‐angiogenic therapies have shown limited efficacy in the clinical management of metastatic disease, including lung metastases. Moreover, the mechanisms via which tumours resist anti‐angiogenic therapies are poorly understood. Importantly, rather than utilizing angiogenesis, some metastases may i...

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Autores principales: Bridgeman, Victoria L, Vermeulen, Peter B, Foo, Shane, Bilecz, Agnes, Daley, Frances, Kostaras, Eleftherios, Nathan, Mark R, Wan, Elaine, Frentzas, Sophia, Schweiger, Thomas, Hegedus, Balazs, Hoetzenecker, Konrad, Renyi‐Vamos, Ferenc, Kuczynski, Elizabeth A, Vasudev, Naveen S, Larkin, James, Gore, Martin, Dvorak, Harold F, Paku, Sandor, Kerbel, Robert S, Dome, Balazs, Reynolds, Andrew R
Formato: Online Artículo Texto
Lenguaje:English
Publicado: John Wiley & Sons, Ltd 2016
Materias:
Original Papers
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5248628/
https://www.ncbi.nlm.nih.gov/pubmed/27859259
http://dx.doi.org/10.1002/path.4845
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author Bridgeman, Victoria L
Vermeulen, Peter B
Foo, Shane
Bilecz, Agnes
Daley, Frances
Kostaras, Eleftherios
Nathan, Mark R
Wan, Elaine
Frentzas, Sophia
Schweiger, Thomas
Hegedus, Balazs
Hoetzenecker, Konrad
Renyi‐Vamos, Ferenc
Kuczynski, Elizabeth A
Vasudev, Naveen S
Larkin, James
Gore, Martin
Dvorak, Harold F
Paku, Sandor
Kerbel, Robert S
Dome, Balazs
Reynolds, Andrew R
author_facet Bridgeman, Victoria L
Vermeulen, Peter B
Foo, Shane
Bilecz, Agnes
Daley, Frances
Kostaras, Eleftherios
Nathan, Mark R
Wan, Elaine
Frentzas, Sophia
Schweiger, Thomas
Hegedus, Balazs
Hoetzenecker, Konrad
Renyi‐Vamos, Ferenc
Kuczynski, Elizabeth A
Vasudev, Naveen S
Larkin, James
Gore, Martin
Dvorak, Harold F
Paku, Sandor
Kerbel, Robert S
Dome, Balazs
Reynolds, Andrew R
author_sort Bridgeman, Victoria L
collection PubMed
description Anti‐angiogenic therapies have shown limited efficacy in the clinical management of metastatic disease, including lung metastases. Moreover, the mechanisms via which tumours resist anti‐angiogenic therapies are poorly understood. Importantly, rather than utilizing angiogenesis, some metastases may instead incorporate pre‐existing vessels from surrounding tissue (vessel co‐option). As anti‐angiogenic therapies were designed to target only new blood vessel growth, vessel co‐option has been proposed as a mechanism that could drive resistance to anti‐angiogenic therapy. However, vessel co‐option has not been extensively studied in lung metastases, and its potential to mediate resistance to anti‐angiogenic therapy in lung metastases is not established. Here, we examined the mechanism of tumour vascularization in 164 human lung metastasis specimens (composed of breast, colorectal and renal cancer lung metastasis cases). We identified four distinct histopathological growth patterns (HGPs) of lung metastasis (alveolar, interstitial, perivascular cuffing, and pushing), each of which vascularized via a different mechanism. In the alveolar HGP, cancer cells invaded the alveolar air spaces, facilitating the co‐option of alveolar capillaries. In the interstitial HGP, cancer cells invaded the alveolar walls to co‐opt alveolar capillaries. In the perivascular cuffing HGP, cancer cells grew by co‐opting larger vessels of the lung. Only in the pushing HGP did the tumours vascularize by angiogenesis. Importantly, vessel co‐option occurred with high frequency, being present in >80% of the cases examined. Moreover, we provide evidence that vessel co‐option mediates resistance to the anti‐angiogenic drug sunitinib in preclinical lung metastasis models. Assuming that our interpretation of the data is correct, we conclude that vessel co‐option in lung metastases occurs through at least three distinct mechanisms, that vessel co‐option occurs frequently in lung metastases, and that vessel co‐option could mediate resistance to anti‐angiogenic therapy in lung metastases. Novel therapies designed to target both angiogenesis and vessel co‐option are therefore warranted. © 2016 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland.
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spelling pubmed-52486282017-02-03 Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models Bridgeman, Victoria L Vermeulen, Peter B Foo, Shane Bilecz, Agnes Daley, Frances Kostaras, Eleftherios Nathan, Mark R Wan, Elaine Frentzas, Sophia Schweiger, Thomas Hegedus, Balazs Hoetzenecker, Konrad Renyi‐Vamos, Ferenc Kuczynski, Elizabeth A Vasudev, Naveen S Larkin, James Gore, Martin Dvorak, Harold F Paku, Sandor Kerbel, Robert S Dome, Balazs Reynolds, Andrew R J Pathol Original Papers Anti‐angiogenic therapies have shown limited efficacy in the clinical management of metastatic disease, including lung metastases. Moreover, the mechanisms via which tumours resist anti‐angiogenic therapies are poorly understood. Importantly, rather than utilizing angiogenesis, some metastases may instead incorporate pre‐existing vessels from surrounding tissue (vessel co‐option). As anti‐angiogenic therapies were designed to target only new blood vessel growth, vessel co‐option has been proposed as a mechanism that could drive resistance to anti‐angiogenic therapy. However, vessel co‐option has not been extensively studied in lung metastases, and its potential to mediate resistance to anti‐angiogenic therapy in lung metastases is not established. Here, we examined the mechanism of tumour vascularization in 164 human lung metastasis specimens (composed of breast, colorectal and renal cancer lung metastasis cases). We identified four distinct histopathological growth patterns (HGPs) of lung metastasis (alveolar, interstitial, perivascular cuffing, and pushing), each of which vascularized via a different mechanism. In the alveolar HGP, cancer cells invaded the alveolar air spaces, facilitating the co‐option of alveolar capillaries. In the interstitial HGP, cancer cells invaded the alveolar walls to co‐opt alveolar capillaries. In the perivascular cuffing HGP, cancer cells grew by co‐opting larger vessels of the lung. Only in the pushing HGP did the tumours vascularize by angiogenesis. Importantly, vessel co‐option occurred with high frequency, being present in >80% of the cases examined. Moreover, we provide evidence that vessel co‐option mediates resistance to the anti‐angiogenic drug sunitinib in preclinical lung metastasis models. Assuming that our interpretation of the data is correct, we conclude that vessel co‐option in lung metastases occurs through at least three distinct mechanisms, that vessel co‐option occurs frequently in lung metastases, and that vessel co‐option could mediate resistance to anti‐angiogenic therapy in lung metastases. Novel therapies designed to target both angiogenesis and vessel co‐option are therefore warranted. © 2016 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland. John Wiley & Sons, Ltd 2016-12-29 2017-02 /pmc/articles/PMC5248628/ /pubmed/27859259 http://dx.doi.org/10.1002/path.4845 Text en © 2016 The Authors. The Journal of Pathology published by John Wiley & Sons Ltd on behalf of Pathological Society of Great Britain and Ireland. This is an open access article under the terms of the Creative Commons Attribution (http://creativecommons.org/licenses/by/4.0/) License, which permits use, distribution and reproduction in any medium, provided the original work is properly cited.
spellingShingle Original Papers
Bridgeman, Victoria L
Vermeulen, Peter B
Foo, Shane
Bilecz, Agnes
Daley, Frances
Kostaras, Eleftherios
Nathan, Mark R
Wan, Elaine
Frentzas, Sophia
Schweiger, Thomas
Hegedus, Balazs
Hoetzenecker, Konrad
Renyi‐Vamos, Ferenc
Kuczynski, Elizabeth A
Vasudev, Naveen S
Larkin, James
Gore, Martin
Dvorak, Harold F
Paku, Sandor
Kerbel, Robert S
Dome, Balazs
Reynolds, Andrew R
Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
title Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
title_full Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
title_fullStr Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
title_full_unstemmed Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
title_short Vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
title_sort vessel co‐option is common in human lung metastases and mediates resistance to anti‐angiogenic therapy in preclinical lung metastasis models
topic Original Papers
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5248628/
https://www.ncbi.nlm.nih.gov/pubmed/27859259
http://dx.doi.org/10.1002/path.4845
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