| Literature DB >> 28507807 |
Akira Asai1,2, Yusuke Tsuchimoto1, Hideko Ohama1, Shinya Fukunishi1, Yasuhiro Tsuda1, Makiko Kobayashi3, Kazuhide Higuchi1, Fujio Suzuki3.
Abstract
Despite major advances in curative and palliative approaches, hepatocellular carcinoma (HCC) is still the third leading cause of cancer-related death worldwide. M1 macrophages (Mϕ) play a key role in host antitumor defenses in HCC. In our study, CD14+ cells were isolated from the peripheral blood of four groups of HCC patients (group-1, patients with stage 0 HCC; group-2, patients with stage A HCC; group-3, patients with stage B HCC; and group-4, patients with stage C HCC) and characterized phenotypically. Then, CD14+ cells from group-2 and group-3 HCC patients were induced to polarize and tested for their antitumor abilities in a chimera model of HCC patients. Human HCCs (HepG2 solid tumors) grew in a chimera model of group-3 patients (group-3 HCC chimeras) but not in a chimera model of group-2 patients (group-2 HCC chimeras). In response to HCC antigens, the majority of CD14+ cells from group-2 patients (group-2 CD14+ cells) switched to the M1 phenotype (IL-12+IL-10-iNOS+cells), whereas the majority of CD14+ cells from group-3 patients (group-3 CD14+ cells) did not switch to the M1 phenotype and continued to express M2b phenotypic properties (IL-12-IL-10+CCL1+iNOS-cells). Group-3 CD14+ cells showed M1Mϕ polarization after treatment with CCL1 antisense oligodeoxynucleotide (ODN). Therefore, our study indicates that anti-HCC defenses of group-3 HCC chimeras are improved after CCL1 antisense ODN treatment.Entities:
Keywords: Antisense oligodexynuclotide; CCL1; hepatocellular carcinoma; host antitumor resistance; macrophage
Year: 2017 PMID: 28507807 PMCID: PMC5414886 DOI: 10.1080/2162402X.2017.1299301
Source DB: PubMed Journal: Oncoimmunology ISSN: 2162-4011 Impact factor: 8.110