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Disruption of CCR1-mediated myeloid cell accumulation suppresses colorectal cancer progression in mice

Cancer Lett. 2020-05; 
Yoshiyuki Kiyasu, Kenji Kawada, Hideyo Hirai, Ryotaro Ogawa, Keita Hanada, Hideyuki Masui, Gen Nishikawa, Takamasa Yamamoto, Rei Mizuno, Yoshiro Itatani, Masayuki Kai, Makoto Mark Taketo, Yoshiharu Sakai
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Gene Synthesis … COVID-19 campus closures: see options … conditions can affect the polarization of myeloid cells toward a pro- or anti-tumor state [[17], [18], [19]] … cDNAs encoding human and mouse CCR1 were synthesized (GenScript) and cloned into Tol2 transposon vector Tn-pMug-Hygro [20] … Get A Quote

摘要

Tumor-stromal interaction is implicated in tumor progression. Although CCR1 expression in myeloid cells could be associated with pro-tumor activity, it remains elusive whether disruption of CCR1-mediated myeloid cell accumulation can suppress tumor progression. Here, we investigated the role of CCR1 depletion in myeloid cells in two syngeneic colorectal cancer mouse models: MC38, a transplanted tumor model and CMT93, a liver metastasis model. Both cells induced tumor accumulation of CCR1 myeloid cells that express MMP2, MMP9, iNOS, and VEGF. Lack of the Ccr1 gene in host mice dramatically reduced MC38 tumor growth as well as CMT93 liver metastasis. To delineate the contribution of CCR1 myeloid cells, we perform... More

关键词

CCR1, Colorectal cancer, Myeloid cell, Tumor microenvironment