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RESEARCH PRODUCT

Time for a “Plan B” in Peritoneal Metastatic Disease

Claudio Tripodo

subject

0301 basic medicineCancer Research03 medical and health sciencesPeritoneal NeoplasmPeritoneal cavity0302 clinical medicineImmune systemImmune privilegeImmunityTumor MicroenvironmentMedicineMacrophagePeritoneal CavityPeritoneal NeoplasmsB-Lymphocyte SubsetTumor microenvironmentbusiness.industryCancermedicine.diseaseImmunity Innate030104 developmental biologymedicine.anatomical_structureOncology030220 oncology & carcinogenesisCancer researchbusinessHuman

description

Abstract Peritoneal involvement in cancer is the harbinger of a particularly unfavorable prognosis. The peritoneal cavity microenvironment is skewed toward immunoregulatory conditions promoted by macrophage populations and innate-like B-1 B cells, which provide immune privilege to malignant cell foci. In this issue of Cancer Research, Haro and colleagues demonstrate that triggering innate IgM-mediated B-1a immune responses via pathogen- or danger-associated molecular pattern recognition exerts antitumor effects on peritoneal metastases by inducing classical complement cascade activation. Exploitation of innate B-1 humoral responses and noncellular immunity is a promising strategy to counter the “castling” of metastatic tumor cells in the peritoneal immunoprivileged site. See related article by Haro et al., p. 159

yearjournalcountryeditionlanguage
2019-01-01Cancer Research
https://doi.org/10.1158/0008-5472.can-18-3553