JCI Insight (Jan 2021)

CD4+CD25+CD127hi cell frequency predicts disease progression in type 1 diabetes

  • Aditi Narsale,
  • Breanna Lam,
  • Rosa Moya,
  • TingTing Lu,
  • Alessandra Mandelli,
  • Irene Gotuzzo,
  • Benedetta Pessina,
  • Gianmaria Giamporcaro,
  • Rhonda Geoffrey,
  • Kerry Buchanan,
  • Mark Harris,
  • Anne-Sophie Bergot,
  • Ranjeny Thomas,
  • Martin J. Hessner,
  • Manuela Battaglia,
  • Elisavet Serti,
  • Joanna D. Davies

Journal volume & issue
Vol. 6, no. 2

Abstract

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Transient partial remission, a period of low insulin requirement experienced by most patients soon after diagnosis, has been associated with mechanisms of immune regulation. A better understanding of such natural mechanisms of immune regulation might identify new targets for immunotherapies that reverse type 1 diabetes (T1D). In this study, using Cox model multivariate analysis, we validated our previous findings that patients with the highest frequency of CD4+CD25+CD127hi (127-hi) cells at diagnosis experience the longest partial remission, and we showed that the 127-hi cell population is a mix of Th1- and Th2-type cells, with a significant bias toward antiinflammatory Th2-type cells. In addition, we extended these findings to show that patients with the highest frequency of 127-hi cells at diagnosis were significantly more likely to maintain β cell function. Moreover, in patients treated with alefacept in the T1DAL clinical trial, the probability of responding favorably to the antiinflammatory drug was significantly higher in those with a higher frequency of 127-hi cells at diagnosis than those with a lower 127-hi cell frequency. These data are consistent with the hypothesis that 127-hi cells maintain an antiinflammatory environment that is permissive for partial remission, β cell survival, and response to antiinflammatory immunotherapy.

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