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Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function

Modulation of immune function at the tumor site could improve patient outcomes. Here, we analyze patient samples of metastatic melanoma, a tumor responsive to T cell-based therapies, and find that tumor-infiltrating T cells are primarily juxtaposed to CD14(+) monocytes/macrophages rather than melano...

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Autores principales: Martinek, Jan, Lin, Jianan, Kim, Kyung In, Wang, Victor G., Wu, Te-Chia, Chiorazzi, Michael, Boruchov, Hannah, Gulati, Ananya, Seeniraj, Shamreethaa, Sun, Lili, Marches, Florentina, Robson, Paul, Rongvaux, Anthony, Flavell, Richard A., George, Joshy, Chuang, Jeffrey H., Banchereau, Jacques, Palucka, Karolina
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9133468/
https://www.ncbi.nlm.nih.gov/pubmed/35584631
http://dx.doi.org/10.1016/j.xcrm.2022.100621
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author Martinek, Jan
Lin, Jianan
Kim, Kyung In
Wang, Victor G.
Wu, Te-Chia
Chiorazzi, Michael
Boruchov, Hannah
Gulati, Ananya
Seeniraj, Shamreethaa
Sun, Lili
Marches, Florentina
Robson, Paul
Rongvaux, Anthony
Flavell, Richard A.
George, Joshy
Chuang, Jeffrey H.
Banchereau, Jacques
Palucka, Karolina
author_facet Martinek, Jan
Lin, Jianan
Kim, Kyung In
Wang, Victor G.
Wu, Te-Chia
Chiorazzi, Michael
Boruchov, Hannah
Gulati, Ananya
Seeniraj, Shamreethaa
Sun, Lili
Marches, Florentina
Robson, Paul
Rongvaux, Anthony
Flavell, Richard A.
George, Joshy
Chuang, Jeffrey H.
Banchereau, Jacques
Palucka, Karolina
author_sort Martinek, Jan
collection PubMed
description Modulation of immune function at the tumor site could improve patient outcomes. Here, we analyze patient samples of metastatic melanoma, a tumor responsive to T cell-based therapies, and find that tumor-infiltrating T cells are primarily juxtaposed to CD14(+) monocytes/macrophages rather than melanoma cells. Using immunofluorescence-guided laser capture microdissection, we analyze transcriptomes of CD3(+) T cells, CD14 (+) monocytes/macrophages, and melanoma cells in non-dissociated tissue. Stromal CD14(+) cells display a specific transcriptional signature distinct from CD14(+) cells within tumor nests. This signature contains LY75, a gene linked with antigen capture and regulation of tolerance and immunity in dendritic cells (DCs). When applied to TCGA cohorts, this gene set can distinguish patients with significantly prolonged survival in metastatic cutaneous melanoma and other cancers. Thus, the stromal CD14(+) cell signature represents a candidate biomarker and suggests that reprogramming of stromal macrophages to acquire DC function may offer a therapeutic opportunity for metastatic cancers.
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spelling pubmed-91334682022-05-27 Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function Martinek, Jan Lin, Jianan Kim, Kyung In Wang, Victor G. Wu, Te-Chia Chiorazzi, Michael Boruchov, Hannah Gulati, Ananya Seeniraj, Shamreethaa Sun, Lili Marches, Florentina Robson, Paul Rongvaux, Anthony Flavell, Richard A. George, Joshy Chuang, Jeffrey H. Banchereau, Jacques Palucka, Karolina Cell Rep Med Article Modulation of immune function at the tumor site could improve patient outcomes. Here, we analyze patient samples of metastatic melanoma, a tumor responsive to T cell-based therapies, and find that tumor-infiltrating T cells are primarily juxtaposed to CD14(+) monocytes/macrophages rather than melanoma cells. Using immunofluorescence-guided laser capture microdissection, we analyze transcriptomes of CD3(+) T cells, CD14 (+) monocytes/macrophages, and melanoma cells in non-dissociated tissue. Stromal CD14(+) cells display a specific transcriptional signature distinct from CD14(+) cells within tumor nests. This signature contains LY75, a gene linked with antigen capture and regulation of tolerance and immunity in dendritic cells (DCs). When applied to TCGA cohorts, this gene set can distinguish patients with significantly prolonged survival in metastatic cutaneous melanoma and other cancers. Thus, the stromal CD14(+) cell signature represents a candidate biomarker and suggests that reprogramming of stromal macrophages to acquire DC function may offer a therapeutic opportunity for metastatic cancers. Elsevier 2022-04-27 /pmc/articles/PMC9133468/ /pubmed/35584631 http://dx.doi.org/10.1016/j.xcrm.2022.100621 Text en © 2022 The Author(s) https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Article
Martinek, Jan
Lin, Jianan
Kim, Kyung In
Wang, Victor G.
Wu, Te-Chia
Chiorazzi, Michael
Boruchov, Hannah
Gulati, Ananya
Seeniraj, Shamreethaa
Sun, Lili
Marches, Florentina
Robson, Paul
Rongvaux, Anthony
Flavell, Richard A.
George, Joshy
Chuang, Jeffrey H.
Banchereau, Jacques
Palucka, Karolina
Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
title Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
title_full Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
title_fullStr Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
title_full_unstemmed Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
title_short Transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
title_sort transcriptional profiling of macrophages in situ in metastatic melanoma reveals localization-dependent phenotypes and function
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9133468/
https://www.ncbi.nlm.nih.gov/pubmed/35584631
http://dx.doi.org/10.1016/j.xcrm.2022.100621
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