Monocyte-derived dendritic cells reflect the immune functional status of a chromophobe renal cell carcinoma patient: Could it be a general phenomenon?
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  • 作者:Maria A. Clavijo-Salomon ; Rodrigo N. Ramos…
  • 关键词:Monocyte ; derived dendritic cells ; T cell anergy ; Foxp3+ T cells ; Chromophobe renal cell carcinoma
  • 刊名:Cancer Immunology, Immunotherapy
  • 出版年:2015
  • 出版时间:February 2015
  • 年:2015
  • 卷:64
  • 期:2
  • 页码:161-171
  • 全文大小:1,462 KB
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  • 刊物类别:Biomedical and Life Sciences
  • 刊物主题:Biomedicine
    Cancer Research
    Immunology
    Oncology
  • 出版者:Springer Berlin / Heidelberg
  • ISSN:1432-0851
文摘
Purpose The chromophobe renal cell carcinoma (ChRCC), though associated with a hereditary cancer syndrome, has a good prognosis after tumor removal. The lack of recurrence could be related to the absence of immune system compromise in patients or to an effective functional recovery of immune functions after tumor removal. Thus, we evaluated monocyte-derived dendritic cells (Mo-DCs) in a 34-year-old male who had a ChRCC, before and after tumor removal. Methods CD14+ monocytes from the patient’s peripheral blood, 1?week before and 3?months after partial nephrectomy, were differentiated in vitro into immature and mature Mo-DCs. These were harvested, analyzed by flow cytometry and used as stimulators of allogeneic T cells. Supernatants from cultures were collected for cytokine analysis. Results Tumor removal was associated with decreased expression of PD-L1, but also, surprisingly, of CD205, HLA-DR, CD80 and CD86 by Mo-DCs. Also, Mo-DC’s ability to stimulate T cell proliferation increased, along with IL-2Rα expression and IFN-γ production. Simultaneously, the patients-Mo-DCs ability to induce Foxp3+ T cells decreased after surgery. One-year postoperative follow-up shows no tumor recurrence. Conclusion The presence of a ChRCC affected Mo-DCs generated in vitro, which recovered their function after tumor removal. This indicates that the favorable outcome observed after ChRCC resection may be due to the restoration of immunocompetence. Furthermore, since functional alterations described for DCs within tumors may be also found in Mo-DCs, their accurate functional analysis—not restricted to the determination of their surface immunophenotype—may provide an indirect “window-to the tumor microenvironment.

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