Tumor-associated myeloid cells: diversity and therapeutic targeting

被引:0
|
作者
Alberto Mantovani
Federica Marchesi
Sebastien Jaillon
Cecilia Garlanda
Paola Allavena
机构
[1] Humanitas Clinical and Research Center-IRCCS,Department of Immunology and Inflammation
[2] Humanitas University,Department of Biomedical Science
[3] Queen Mary University of London,The William Harvey Research Institute
[4] University of Milan,Department of Biotechnology and Translational Medicine
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关键词
tumor-associated macrophages; tumor microenvironment; macrophage targeting;
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摘要
Myeloid cells in tumor tissues constitute a dynamic immune population characterized by a non-uniform phenotype and diverse functional activities. Both tumor-associated macrophages (TAMs), which are more abundantly represented, and tumor-associated neutrophils (TANs) are known to sustain tumor cell growth and invasion, support neoangiogenesis and suppress anticancer adaptive immune responses. In recent decades, several therapeutic approaches have been implemented in preclinical cancer models to neutralize the tumor-promoting roles of both TAMs and TANs. Some of the most successful strategies have now reached the clinic and are being investigated in clinical trials. In this review, we provide an overview of the recent literature on the ever-growing complexity of the biology of TAMs and TANs and the development of the most promising approaches to target these populations therapeutically in cancer patients.
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页码:566 / 578
页数:12
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