Immunophenotypic characterization of TCR γδ T cells and MAIT cells in HIV-infected individuals developing Hodgkin’s lymphoma

Christina K.S. Muller; Julian Spagnuolo; Annette Audigé; Andrew Chancellor; Doris Russenberger; Alexandra U. Scherrer; Matthias Hoffmann; Roger Kouyos; Manuel Battegay; Gennaro De Libero; Roberto F. Speck; K. Aebi-Popp; A. Anagnostopoulos; M. Battegay; E. Bernasconi; J. Böni; D. L. Braun; H. C. Bucher; A. Calmy; M. Cavassini; A. Ciuffi; G. Dollenmaier; M. Egger; L. Elzi; J. Fehr; J. Fellay; H. Furrer; C. A. Fux; H. F. Günthard; D. Haerry; B. Hasse; H. H. Hirsch; M. Hoffmann; I. Hösli; M. Huber; C. R. Kahlert; L. Kaiser; O. Keiser; T. Klimkait; R. D. Kouyos; H. Kovari; B. Ledergerber; G. Martinetti; B. Martinez de Tejada; C. Marzolini; K. J. Metzner; N. Müller; D. Nicca; P. Paioni; G. Pantaleo; M. Perreau; A. Rauch; C. Rudin; A. U. Scherrer; P. Schmid; R. Speck; M. Stöckle; P. Tarr; A. Trkola; P. Vernazza; G. Wandeler; R. Weber; S. Yerly

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Immunophenotypic characterization of TCR γδ T cells and MAIT cells in HIV-infected individuals developing Hodgkin’s lymphoma

Infectious Agents and Cancer (2021) 16(1)

DOI: 10.1186/s13027-021-00365-4

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Abstract

Background: Despite successful combined antiretroviral therapy (cART), the risk of non-AIDS defining cancers (NADCs) remains higher for HIV-infected individuals than the general population. The reason for this increase is highly disputed. Here, we hypothesized that T-cell receptor (TCR) γδ cells and/or mucosal-associated invariant T (MAIT) cells might be associated with the increased risk of NADCs. γδ T cells and MAIT cells both serve as a link between the adaptive and the innate immune system, and also to exert direct anti-viral and anti-tumor activity. Methods: We performed a longitudinal phenotypic characterization of TCR γδ cells and MAIT cells in HIV-infected individuals developing Hodgkin’s lymphoma (HL), the most common type of NADCs. Cryopreserved PBMCs of HIV-infected individuals developing HL, matched HIV-infected controls without (w/o) HL and healthy controls were used for immunophenotyping by polychromatic flow cytometry, including markers for activation, exhaustion and chemokine receptors. Results: We identified significant differences in the CD4+ T cell count between HIV-infected individuals developing HL and HIV-infected matched controls within 1 year before cancer diagnosis. We observed substantial differences in the cellular phenotype mainly between healthy controls and HIV infection irrespective of HL. A number of markers tended to be different in Vδ1 and MAIT cells in HIV+HL+ patients vs. HIV+ w/o HL patients; notably, we observed significant differences for the expression of CCR5, CCR6 and CD16 between these two groups of HIV+ patients. Conclusion: TCR Vδ1 and MAIT cells in HIV-infected individuals developing HL show subtle phenotypical differences as compared to the ones in HIV-infected controls, which may go along with functional impairment and thereby may be less efficient in detecting and eliminating malignant cells. Further, our results support the potential of longitudinal CD4+ T cell count analysis for the identification of patients at higher risk to develop HL.

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Muller, C. K. S., Spagnuolo, J., Audigé, A., Chancellor, A., Russenberger, D., Scherrer, A. U., … Yerly, S. (2021). Immunophenotypic characterization of TCR γδ T cells and MAIT cells in HIV-infected individuals developing Hodgkin’s lymphoma. Infectious Agents and Cancer, 16(1). https://doi.org/10.1186/s13027-021-00365-4

Immunophenotypic characterization of TCR γδ T cells and MAIT cells in HIV-infected individuals developing Hodgkin’s lymphoma

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