Epigenetic therapy inhibits metastases by disrupting premetastatic niches Journal Articles

abstract

• Cancer recurrence after surgery remains an unresolved clinical problem1-3. Myeloid cells derived from bone marrow contribute to the formation of the premetastatic microenvironment, which is required for disseminating tumour cells to engraft distant sites4-6. There are currently no effective interventions that prevent the formation of the premetastatic microenvironment6,7. Here we show that, after surgical removal of primary lung, breast and oesophageal cancers, low-dose adjuvant epigenetic therapy disrupts the premetastatic microenvironment and inhibits both the formation and growth of lung metastases through its selective effect on myeloid-derived suppressor cells (MDSCs). In mouse models of pulmonary metastases, MDSCs are key factors in the formation of the premetastatic microenvironment after resection of primary tumours. Adjuvant epigenetic therapy that uses low-dose DNA methyltransferase and histone deacetylase inhibitors, 5-azacytidine and entinostat, disrupts the premetastatic niche by inhibiting the trafficking of MDSCs through the downregulation of CCR2 and CXCR2, and by promoting MDSC differentiation into a more-interstitial macrophage-like phenotype. A decreased accumulation of MDSCs in the premetastatic lung produces longer periods of disease-free survival and increased overall survival, compared with chemotherapy. Our data demonstrate that, even after removal of the primary tumour, MDSCs contribute to the development of premetastatic niches and settlement of residual tumour cells. A combination of low-dose adjuvant epigenetic modifiers that disrupts this premetastatic microenvironment and inhibits metastases may permit an adjuvant approach to cancer therapy.

authors

• Lu, Zhihao
• Zou, Jianling
• Li, Shuang
• Topper, Michael J
• Tao, Yong
• Zhang, Hao
• Jiao, Xi
• Xie, Wenbing
• Kong, Xiangqian
• Vaz, Michelle
• Li, Huili
• Cai, Yi
• Xia, Limin
• Huang, Peng
• Rodgers, Kristen
• Lee, Beverly
• Riemer, Joanne B
• Day, Chi-Ping
• Yen, Ray-Whay Chiu
• Cui, Ying
• Wang, Yujiao
• Wang, Yanni
• Zhang, Weiqiang
• Easwaran, Hariharan
• Hulbert, Alicia
• Kim, KiBem
• Juergens, Rosalyn
• Yang, Stephen C
• Battafarano, Richard J
• Bush, Errol L
• Broderick, Stephen R
• Cattaneo, Stephen M
• Brahmer, Julie R
• Rudin, Charles M
• Wrangle, John
• Mei, Yuping
• Kim, Young J
• Zhang, Bin
• Wang, Ken Kang-Hsin
• Forde, Patrick M
• Margolick, Joseph B
• Nelkin, Barry D
• Zahnow, Cynthia A
• Pardoll, Drew M
• Housseau, Franck
• Baylin, Stephen B
• Shen, Lin
• Brock, Malcolm V

status

• published 

publication date

• March 12, 2020

has subject area

• Animals (MeSH)
• Azacitidine (MeSH)
• Benzamides (MeSH)
• Cell Differentiation (MeSH)
• Cell Movement (MeSH)
• Chemotherapy, Adjuvant (MeSH)
• Disease Models, Animal (MeSH)
• Down-Regulation (MeSH)
• Epigenesis, Genetic (MeSH)
• General Science & Technology (Science Metrix)
• Genetic Therapy (MeSH)
• Mice (MeSH)
• Myeloid-Derived Suppressor Cells (MeSH)
• Neoplasm Metastasis (MeSH)
• Neoplasms (MeSH)
• Pyridines (MeSH)
• Receptors, CCR2 (MeSH)
• Receptors, Interleukin-8B (MeSH)
• Tumor Microenvironment (MeSH)

published in

• Nature  Journal

keywords

• Animals
• Azacitidine
• Benzamides
• Cell Differentiation
• Cell Movement
• Chemotherapy, Adjuvant
• Disease Models, Animal
• Down-Regulation
• Epigenesis, Genetic
• Genetic Therapy
• Mice
• Myeloid-Derived Suppressor Cells
• Neoplasm Metastasis
• Neoplasms
• Pyridines
• Receptors, CCR2
• Receptors, Interleukin-8B
• Tumor Microenvironment

Digital Object Identifier (DOI)

• 10.1038/s41586-020-2054-x

start page

• 284

end page

• 290

volume

• 579

issue

• 7798