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dc.contributor.authorGunalp, Sinem
dc.contributor.authorHelvaci, Derya Goksu
dc.contributor.authorOner, Aysenur
dc.contributor.authorBursalı, Ahmet
dc.contributor.authorConforte, Alessandra
dc.contributor.authorGüner, Hüseyin
dc.contributor.authorKarakülah, Gökhan
dc.contributor.authorSzegezdi, Eva
dc.contributor.authorSag, Duygu
dc.date.accessioned2024-02-07T08:34:16Z
dc.date.available2024-02-07T08:34:16Z
dc.date.issued2023en_US
dc.identifier.issn1664-3224
dc.identifier.otherWOS:001119319400001
dc.identifier.urihttps://doi.org/10.3389/fimmu.2023.1209249
dc.identifier.urihttps://hdl.handle.net/20.500.12573/1920
dc.description.abstractBackgroundTNF-related apoptosis-inducing ligand (TRAIL) is a member of the TNF superfamily that can either induce cell death or activate survival pathways after binding to death receptors (DRs) DR4 or DR5. TRAIL is investigated as a therapeutic agent in clinical trials due to its selective toxicity to transformed cells. Macrophages can be polarized into pro-inflammatory/tumor-fighting M1 macrophages or anti-inflammatory/tumor-supportive M2 macrophages and an imbalance between M1 and M2 macrophages can promote diseases. Therefore, identifying modulators that regulate macrophage polarization is important to design effective macrophage-targeted immunotherapies. The impact of TRAIL on macrophage polarization is not known.MethodsPrimary human monocyte-derived macrophages were pre-treated with either TRAIL or with DR4 or DR5-specific ligands and then polarized into M1, M2a, or M2c phenotypes in vitro. The expression of M1 and M2 markers in macrophage subtypes was analyzed by RNA sequencing, qPCR, ELISA, and flow cytometry. Furthermore, the cytotoxicity of the macrophages against U937 AML tumor targets was assessed by flow cytometry. TCGA datasets were also analyzed to correlate TRAIL with M1/M2 markers, and the overall survival of cancer patients.ResultsTRAIL increased the expression of M1 markers at both mRNA and protein levels while decreasing the expression of M2 markers at the mRNA level in human macrophages. TRAIL also shifted M2 macrophages towards an M1 phenotype. Our data showed that both DR4 and DR5 death receptors play a role in macrophage polarization. Furthermore, TRAIL enhanced the cytotoxicity of macrophages against the AML cancer cells in vitro. Finally, TRAIL expression was positively correlated with increased expression of M1 markers in the tumors from ovarian and sarcoma cancer patients and longer overall survival in cases with high, but not low, tumor macrophage content.ConclusionsTRAIL promotes the polarization of human macrophages toward a proinflammatory M1 phenotype via both DR4 and DR5. Our study defines TRAIL as a new regulator of macrophage polarization and suggests that targeting DRs can enhance the anti-tumorigenic response of macrophages in the tumor microenvironment by increasing M1 polarization.en_US
dc.description.sponsorshipHORIZON 2020-MSCA-RISE Program 777995en_US
dc.language.isoengen_US
dc.publisherFRONTIERS MEDIA SAen_US
dc.relation.isversionof10.3389/fimmu.2023.1209249en_US
dc.rightsinfo:eu-repo/semantics/openAccessen_US
dc.subjectTRAIL, death receptorsen_US
dc.subjectprimary human macrophagesen_US
dc.subjectmacrophage polarizationen_US
dc.subjectmacrophage cytotoxicityen_US
dc.titleTRAIL promotes the polarization of human macrophages toward a proinflammatory M1 phenotype and is associated with increased survival in cancer patients with high tumor macrophage contenten_US
dc.typearticleen_US
dc.contributor.departmentAGÜ, Yaşam ve Doğa Bilimleri Fakültesi, Moleküler Biyoloji ve Genetik Bölümüen_US
dc.contributor.authorID0000-0002-0220-5224en_US
dc.contributor.institutionauthorHüseyin, Güner
dc.identifier.volume14en_US
dc.identifier.startpage1en_US
dc.identifier.endpage28en_US
dc.relation.journalFRONTIERS IN IMMUNOLOGYen_US
dc.relation.tubitak118Z363
dc.relation.publicationcategoryMakale - Uluslararası Hakemli Dergi - Kurum Öğretim Elemanıen_US


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