| Literature DB >> 27872290 |
Yoshitaka Kimura1, Asuka Inoue1,2, Sho Hangai1,3, Shinobu Saijo4, Hideo Negishi1, Junko Nishio1, Sho Yamasaki5, Yoichiro Iwakura6, Hideyuki Yanai1,3, Tadatsugu Taniguchi7,3.
Abstract
Tumor metastasis is the cause of most cancer deaths. Although metastases can form in multiple end organs, the liver is recognized as a highly permissive organ. Nevertheless, there is evidence for immune cell-mediated mechanisms that function to suppress liver metastasis by certain tumors, although the underlying mechanisms for the suppression of metastasis remain elusive. Here, we show that Dectin-2, a C-type lectin receptor (CLR) family of innate receptors, is critical for the suppression of liver metastasis of cancer cells. We provide evidence that Dectin-2 functions in resident macrophages in the liver, known as Kupffer cells, to mediate the uptake and clearance of cancer cells. Interestingly, Kupffer cells are selectively endowed with Dectin-2-dependent phagocytotic activity, with neither bone marrow-derived macrophages nor alveolar macrophages showing this potential. Concordantly, subcutaneous primary tumor growth and lung metastasis are not affected by the absence of Dectin-2. In addition, macrophage C-type lectin, a CLR known to be complex with Dectin-2, also contributes to the suppression of liver metastasis. Collectively, these results highlight the hitherto poorly understood mechanism of Kupffer cell-mediated control of metastasis that is mediated by the CLR innate receptor family, with implications for the development of anticancer therapy targeting CLRs.Entities:
Keywords: C-type lectin receptor; Dectin-2; Kupffer cell; liver metastasis; phagocytosis
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Year: 2016 PMID: 27872290 PMCID: PMC5150405 DOI: 10.1073/pnas.1617903113
Source DB: PubMed Journal: Proc Natl Acad Sci U S A ISSN: 0027-8424 Impact factor: 11.205