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γδ T cell dichotomy with opposing cytotoxic and wound healing functions in human solid tumors. | LitMetric

AI Article Synopsis

  • γδ T cells play a crucial role in maintaining tissue health and are linked to better outcomes in various tumors, but their specific characteristics in human cancers are not well understood.
  • In studies of colorectal and endometrial cancer, significant differences were observed in γδ T cell subsets and their functions between tumor and normal tissues; colorectal cancer displayed a specific AREG-producing subset, while endometrial cancer had more cytotoxic γδ cells.
  • A new expansion method was developed to enhance the cytotoxic abilities of γδ T cells for potential use in cell therapy, improving tumor infiltration and clearance while reducing AREG production, thus presenting a promising ‘off-the-shelf’ treatment strategy.

Article Abstract

γδ T cells are important tissue-resident, innate T cells that are critical for tissue homeostasis. γδ cells are associated with positive prognosis in most tumors; however, little is known about their heterogeneity in human cancers. Here, we phenotyped innate and adaptive cells in human colorectal (CRC) and endometrial cancer. We found striking differences in γδ subsets and function in tumors compared to normal tissue, and in the γδ subsets present in tumor types. In CRC, an amphiregulin (AREG)-producing subset emerges, while endometrial cancer is infiltrated by cytotoxic cells. In humanized CRC models, tumors induced this AREG phenotype in Vδ1 cells after adoptive transfer. To exploit the beneficial roles of γδ cells for cell therapy, we developed an expansion method that enhanced cytotoxic function and boosted metabolic flexibility, while eliminating AREG production, achieving greater tumor infiltration and tumor clearance. This method has broad applications in cellular therapy as an 'off-the-shelf' treatment option.

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Source
http://dx.doi.org/10.1038/s43018-023-00589-wDOI Listing

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