Macrophages orchestrate the expansion of a pro-angiogenic perivascular niche during cancer progression

James W. Opzoomer; Joanne E. Anstee; Isaac  Dean; Emily J. Hill; Ihssane Bouybayoune; Jonathan Caron; Tamara Muliaditan; Peter Gordon; Dominika Sosnowska; Rosamond Nuamah; Sarah E. Pinder; Tony Ng; Francesco Dazzi; Shahram Kordasti; David R. Withers; Toby Lawrence; James N. Arnold

Macrophages orchestrate the expansion of a pro-angiogenic perivascular niche during cancer progression

James W. Opzoomer, Joanne E. Anstee, Isaac Dean, Emily J. Hill, Ihssane Bouybayoune, Jonathan Caron, Tamara Muliaditan, Peter Gordon, Dominika Sosnowska, Rosamond Nuamah, Sarah E. Pinder, Tony Ng, Francesco Dazzi, Shahram Kordasti, David R. Withers, Toby Lawrence, James N. Arnold^*

^*Corresponding author for this work

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Abstract

Tumor associated macrophages (TAMs) are a highly plastic stromal cell type which support cancer progression. Using single-cell RNA-sequencing of TAMs from a spontaneous murine model of mammary adenocarcinoma (MMTV-PyMT) we characterize a subset of these cells expressing lymphatic vessel endothelial hyaluronic acid receptor 1 (Lyve-1) which spatially reside proximal to blood vasculature. We demonstrate that Lyve-1+ TAMs support tumor growth and identify a pivotal role for these cells in maintaining a population of perivascular mesenchymal cells which express alpha-smooth muscle actin and phenotypically resemble pericytes. Using photolabeling techniques show that mesenchymal cells maintain their prevalence in the growing tumor through proliferation and uncover a role for Lyve-1+ TAMs in orchestrating a selective platelet-derived growth factor-CC-dependent expansion of the perivascular mesenchymal population, creating a pro-angiogenic niche. This study highlights the inter-reliance of the immune and non-immune stromal network which support cancer progression and provides therapeutic opportunities for tackling the disease.

Original language	English
Journal	Science Advances
Publication status	Published - 3 Nov 2021

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Opzoomer et al 2021Accepted author manuscript, 3.76 MBLicence: CC BY-ND

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@article{3512cd9e8aa246bfa35617bd1310aadf,

title = "Macrophages orchestrate the expansion of a pro-angiogenic perivascular niche during cancer progression",

abstract = "Tumor associated macrophages (TAMs) are a highly plastic stromal cell type which support cancer progression. Using single-cell RNA-sequencing of TAMs from a spontaneous murine model of mammary adenocarcinoma (MMTV-PyMT) we characterize a subset of these cells expressing lymphatic vessel endothelial hyaluronic acid receptor 1 (Lyve-1) which spatially reside proximal to blood vasculature. We demonstrate that Lyve-1+ TAMs support tumor growth and identify a pivotal role for these cells in maintaining a population of perivascular mesenchymal cells which express alpha-smooth muscle actin and phenotypically resemble pericytes. Using photolabeling techniques show that mesenchymal cells maintain their prevalence in the growing tumor through proliferation and uncover a role for Lyve-1+ TAMs in orchestrating a selective platelet-derived growth factor-CC-dependent expansion of the perivascular mesenchymal population, creating a pro-angiogenic niche. This study highlights the inter-reliance of the immune and non-immune stromal network which support cancer progression and provides therapeutic opportunities for tackling the disease. ",

author = "Opzoomer, {James W.} and Anstee, {Joanne E.} and Isaac Dean and Hill, {Emily J.} and Ihssane Bouybayoune and Jonathan Caron and Tamara Muliaditan and Peter Gordon and Dominika Sosnowska and Rosamond Nuamah and Pinder, {Sarah E.} and Tony Ng and Francesco Dazzi and Shahram Kordasti and Withers, {David R.} and Toby Lawrence and Arnold, {James N.}",

year = "2021",

month = nov,

day = "3",

language = "English",

journal = "Science Advances",

issn = "2375-2548",

publisher = "American Association for the Advancement of Science",

}

TY - JOUR

T1 - Macrophages orchestrate the expansion of a pro-angiogenic perivascular niche during cancer progression

AU - Opzoomer, James W.

AU - Anstee, Joanne E.

AU - Dean, Isaac

AU - Hill, Emily J.

AU - Bouybayoune, Ihssane

AU - Caron, Jonathan

AU - Muliaditan, Tamara

AU - Gordon, Peter

AU - Sosnowska, Dominika

AU - Nuamah, Rosamond

AU - Pinder, Sarah E.

AU - Ng, Tony

AU - Dazzi, Francesco

AU - Kordasti, Shahram

AU - Withers, David R.

AU - Lawrence, Toby

AU - Arnold, James N.

PY - 2021/11/3

Y1 - 2021/11/3

N2 - Tumor associated macrophages (TAMs) are a highly plastic stromal cell type which support cancer progression. Using single-cell RNA-sequencing of TAMs from a spontaneous murine model of mammary adenocarcinoma (MMTV-PyMT) we characterize a subset of these cells expressing lymphatic vessel endothelial hyaluronic acid receptor 1 (Lyve-1) which spatially reside proximal to blood vasculature. We demonstrate that Lyve-1+ TAMs support tumor growth and identify a pivotal role for these cells in maintaining a population of perivascular mesenchymal cells which express alpha-smooth muscle actin and phenotypically resemble pericytes. Using photolabeling techniques show that mesenchymal cells maintain their prevalence in the growing tumor through proliferation and uncover a role for Lyve-1+ TAMs in orchestrating a selective platelet-derived growth factor-CC-dependent expansion of the perivascular mesenchymal population, creating a pro-angiogenic niche. This study highlights the inter-reliance of the immune and non-immune stromal network which support cancer progression and provides therapeutic opportunities for tackling the disease.

AB - Tumor associated macrophages (TAMs) are a highly plastic stromal cell type which support cancer progression. Using single-cell RNA-sequencing of TAMs from a spontaneous murine model of mammary adenocarcinoma (MMTV-PyMT) we characterize a subset of these cells expressing lymphatic vessel endothelial hyaluronic acid receptor 1 (Lyve-1) which spatially reside proximal to blood vasculature. We demonstrate that Lyve-1+ TAMs support tumor growth and identify a pivotal role for these cells in maintaining a population of perivascular mesenchymal cells which express alpha-smooth muscle actin and phenotypically resemble pericytes. Using photolabeling techniques show that mesenchymal cells maintain their prevalence in the growing tumor through proliferation and uncover a role for Lyve-1+ TAMs in orchestrating a selective platelet-derived growth factor-CC-dependent expansion of the perivascular mesenchymal population, creating a pro-angiogenic niche. This study highlights the inter-reliance of the immune and non-immune stromal network which support cancer progression and provides therapeutic opportunities for tackling the disease.

M3 - Article

SN - 2375-2548

JO - Science Advances

JF - Science Advances

ER -

Macrophages orchestrate the expansion of a pro-angiogenic perivascular niche during cancer progression

Abstract

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