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Formyl peptide receptor (FPR) agonists promote immune evasion independent of functional Ncf1 derived ROS
Karolinska Institute (SWE).
Högskolan Väst, Grants and Innovation Office (GIO). Karolinska Institute (SWE).ORCID-id: 0000-0003-4849-8541
Karolinska Institute (SWE).
2020 (Engelska)Ingår i: Journal of Immunology, ISSN 0022-1767, E-ISSN 1550-6606, Vol. 204, nr 1_Supplement, s. 242.46-242.46Artikel i tidskrift (Refereegranskat) Published
Abstract [en]

Previous studies have shown that in both the absence of the Ncf1 gene or in the presence of a loss-of-function SNP, mice have a lower tumor burden when compared to wildtype animals. Here, we investigate a formyl peptide receptor (FPR) agonist in this setting and demonstrate that it promotes tumor immune evasion through an immune-Ncf1/ROS-dependent mechanism. We observed an increased colonization of B16F10 tumor cells in the lungs of FPR-agonist-treated wildtype C57BL6N mice compared to vehicle-control-treated mice. A significant reduction in tumor burden was expectedly seen in the Ncf1*/* mutant strain compared to the wildtype. However, FPR-agonist treatment did not promote tumor growth in Ncf1*/* treated mice when compared to vehicle-control-treated Ncf1*/* mice. These results suggest that FPR agonists can promote tumor evasion by acting through FPRs on immune cells in a NOX2/ROS-independent fashion and in a fashion independent of FPRs on the tumor.
Ort, förlag, år, upplaga, sidor
2020. Vol. 204, nr 1_Supplement, s. 242.46-242.46
Nyckelord [en]
tumors, formyl peptide receptor (FPR), functional Ncf1
Nationell ämneskategori
Cancer och onkologi
Identifikatorer
URN: urn:nbn:se:hv:diva-21404DOI: 10.4049/jimmunol.204.supp.242.46OAI: oai:DiVA.org:hv-21404DiVA, id: diva2:1844288
Tillgänglig från: 2024-03-13 Skapad: 2024-03-13 Senast uppdaterad: 2024-09-19Bibliografiskt granskad

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Olofsson-Sahl, Peter

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Olofsson-Sahl, Peter
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Grants and Innovation Office (GIO)
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Journal of Immunology
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Totalt: 64 träffar
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