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Genetically engineered myeloid cells rebalance the core immune suppression program in metastasis
Author(s) -
Sabina Kaczanowska,
Daniel W. Beury,
Vishaka Gopalan,
Arielle K. Tycko,
Haiying Qin,
Miranda E. Clements,
Justin A. Drake,
Chiadika Nwanze,
Meera Murgai,
Zachary Rae,
Wei Ju,
Katherine A. Alexander,
Jessica Kline,
Cristina F. Contreras,
Kristin M. Wessel,
Shil Patel,
Sridhar Hannenhalli,
Michael C. Kelly,
Rosandra N. Kaplan
Publication year - 2021
Publication title -
cell
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 26.304
H-Index - 776
eISSN - 1097-4172
pISSN - 0092-8674
DOI - 10.1016/j.cell.2021.02.048
Subject(s) - biology , immune system , genetically engineered , myeloid cells , metastasis , myeloid , core (optical fiber) , immunology , cancer research , computational biology , genetics , cancer , gene , materials science , composite material
Metastasis is the leading cause of cancer-related deaths, and greater knowledge of the metastatic microenvironment is necessary to effectively target this process. Microenvironmental changes occur at distant sites prior to clinically detectable metastatic disease; however, the key niche regulatory signals during metastatic progression remain poorly characterized. Here, we identify a core immune suppression gene signature in pre-metastatic niche formation that is expressed predominantly by myeloid cells. We target this immune suppression program by utilizing genetically engineered myeloid cells (GEMys) to deliver IL-12 to modulate the metastatic microenvironment. Our data demonstrate that IL12-GEMy treatment reverses immune suppression in the pre-metastatic niche by activating antigen presentation and T cell activation, resulting in reduced metastatic and primary tumor burden and improved survival of tumor-bearing mice. We demonstrate that IL12-GEMys can functionally modulate the core program of immune suppression in the pre-metastatic niche to successfully rebalance the dysregulated metastatic microenvironment in cancer.

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