OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment

Macrophages represent a highly plastic cell type,indispensable for tissue and organ homeostasis, as well as innate immunity. Basic and translational research attributed tumor-promoting functions to macrophages, and their presence is often associated to poor patient prognosis and therapy resistance....

Descripción completa

Detalles Bibliográficos
Autores principales: Schulz, Michael, Alekseeva, Tijna, Anthes, Julian, Macas, Jandranka, Michels, Birgitta, Möckl, Aylin, Niesel, Katja, Salamero-Boix, Anna, Stein, Stefan, Farin, Henner, Plate, Karl H, Reiss, Yvonne, Rödel, Franz, Sevenich, Lisa
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2021
Materias:
Supplement Abstracts
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8265016/
http://dx.doi.org/10.1093/noajnl/vdab070.057
_version_ 1783719684867096576
author Schulz, Michael
Alekseeva, Tijna
Anthes, Julian
Macas, Jandranka
Michels, Birgitta
Möckl, Aylin
Niesel, Katja
Salamero-Boix, Anna
Stein, Stefan
Farin, Henner
Plate, Karl H
Reiss, Yvonne
Rödel, Franz
Sevenich, Lisa
author_facet Schulz, Michael
Alekseeva, Tijna
Anthes, Julian
Macas, Jandranka
Michels, Birgitta
Möckl, Aylin
Niesel, Katja
Salamero-Boix, Anna
Stein, Stefan
Farin, Henner
Plate, Karl H
Reiss, Yvonne
Rödel, Franz
Sevenich, Lisa
author_sort Schulz, Michael
collection PubMed
description Macrophages represent a highly plastic cell type,indispensable for tissue and organ homeostasis, as well as innate immunity. Basic and translational research attributed tumor-promoting functions to macrophages, and their presence is often associated to poor patient prognosis and therapy resistance. While brain-resident macrophages, the so-called microglia (MG), represent the major immune cell type in the parenchyma under normal conditions, primary and metastatic brain tumors induce the recruitment of different immune cell types from the periphery, including monocyte-derived macrophages (MDM). Controversy remained about the redundancy of disease-associated molecular signatures and functions. The identification of markers that reliably distinguish brain-resident from blood-borne tumor-associated macrophages (TAMs) allowed the interrogation of molecular traits of different TAM populations in mouse and human brain tumors. Using RNA-Seq, we demonstrated that TAMs rapidly acquire disease-associated transcriptional programs upon initial tumor infiltration, while gene expression remained stable during different stages of BrM progression. Across different BrM models, disease-associated transcriptional changes revealed lineage-specific, non-redundant functions of TAM populations, which was further reflected by cell type-specific occupation of different niches within the BrM microenvironment. Furthermore, we observed dose- and cell type-specific immune modulatory effects of whole brain radiotherapy on myeloid cells in BrM leading to a transient loss of disease-associated transcriptional programs predominately in blood-borne myeloid populations. This effect can at least in part be attributed to a replenishment of the recruited macrophage pool. This observation was further supported by scRNA-Seq analyses revealing higher heterogeneity of TAM-MDM compared to TAM-MG under treatment-naïve conditions and in response to radiotherapy. Together, our results point towards the phenotypic plasticity of TAMs, especially MDMs, and the contribution of each compartment in instigating cancer-associated inflammation or the establishment of an immuno-suppressive TME. While TAM-MG exert functions related to pro-inflammatory responses, TAM-MDM are rather involved in tissue repair and regulation of adaptive immune cell functions.
format Online
Article
Text
id pubmed-8265016
institution National Center for Biotechnology Information
language English
publishDate 2021
publisher Oxford University Press
record_format MEDLINE/PubMed
spelling pubmed-82650162021-07-09 OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment Schulz, Michael Alekseeva, Tijna Anthes, Julian Macas, Jandranka Michels, Birgitta Möckl, Aylin Niesel, Katja Salamero-Boix, Anna Stein, Stefan Farin, Henner Plate, Karl H Reiss, Yvonne Rödel, Franz Sevenich, Lisa Neurooncol Adv Supplement Abstracts Macrophages represent a highly plastic cell type,indispensable for tissue and organ homeostasis, as well as innate immunity. Basic and translational research attributed tumor-promoting functions to macrophages, and their presence is often associated to poor patient prognosis and therapy resistance. While brain-resident macrophages, the so-called microglia (MG), represent the major immune cell type in the parenchyma under normal conditions, primary and metastatic brain tumors induce the recruitment of different immune cell types from the periphery, including monocyte-derived macrophages (MDM). Controversy remained about the redundancy of disease-associated molecular signatures and functions. The identification of markers that reliably distinguish brain-resident from blood-borne tumor-associated macrophages (TAMs) allowed the interrogation of molecular traits of different TAM populations in mouse and human brain tumors. Using RNA-Seq, we demonstrated that TAMs rapidly acquire disease-associated transcriptional programs upon initial tumor infiltration, while gene expression remained stable during different stages of BrM progression. Across different BrM models, disease-associated transcriptional changes revealed lineage-specific, non-redundant functions of TAM populations, which was further reflected by cell type-specific occupation of different niches within the BrM microenvironment. Furthermore, we observed dose- and cell type-specific immune modulatory effects of whole brain radiotherapy on myeloid cells in BrM leading to a transient loss of disease-associated transcriptional programs predominately in blood-borne myeloid populations. This effect can at least in part be attributed to a replenishment of the recruited macrophage pool. This observation was further supported by scRNA-Seq analyses revealing higher heterogeneity of TAM-MDM compared to TAM-MG under treatment-naïve conditions and in response to radiotherapy. Together, our results point towards the phenotypic plasticity of TAMs, especially MDMs, and the contribution of each compartment in instigating cancer-associated inflammation or the establishment of an immuno-suppressive TME. While TAM-MG exert functions related to pro-inflammatory responses, TAM-MDM are rather involved in tissue repair and regulation of adaptive immune cell functions. Oxford University Press 2021-07-05 /pmc/articles/PMC8265016/ http://dx.doi.org/10.1093/noajnl/vdab070.057 Text en © The Author(s) 2021. Published by Oxford University Press, the Society for Neuro-Oncology and the European Association of Neuro-Oncology. https://creativecommons.org/licenses/by/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution License (http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) ), which permits unrestricted reuse, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Supplement Abstracts
Schulz, Michael
Alekseeva, Tijna
Anthes, Julian
Macas, Jandranka
Michels, Birgitta
Möckl, Aylin
Niesel, Katja
Salamero-Boix, Anna
Stein, Stefan
Farin, Henner
Plate, Karl H
Reiss, Yvonne
Rödel, Franz
Sevenich, Lisa
OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
title OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
title_full OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
title_fullStr OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
title_full_unstemmed OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
title_short OTME-6. Deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
title_sort otme-6. deep sequencing reveals heterogeneity of brain metastasis-associated macrophages and microglia and uncovers their cell type-specific functions within the tumor microenvironment
topic Supplement Abstracts
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8265016/
http://dx.doi.org/10.1093/noajnl/vdab070.057
work_keys_str_mv AT schulzmichael otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT alekseevatijna otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT anthesjulian otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT macasjandranka otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT michelsbirgitta otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT mocklaylin otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT nieselkatja otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT salameroboixanna otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT steinstefan otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT farinhenner otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT platekarlh otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT reissyvonne otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT rodelfranz otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment
AT sevenichlisa otme6deepsequencingrevealsheterogeneityofbrainmetastasisassociatedmacrophagesandmicrogliaanduncoverstheircelltypespecificfunctionswithinthetumormicroenvironment

Ejemplares similares