Frontiers in Immunology (Feb 2020)

Effect of Optimized Immunosuppression (Including Rituximab) on Anti-Donor Alloresponses in Patients With Chronically Rejecting Renal Allografts

  • Kin Yee Shiu,
  • Dominic Stringer,
  • Laura McLaughlin,
  • Olivia Shaw,
  • Paul Brookes,
  • Hannah Burton,
  • Hannah Wilkinson,
  • Harriet Douthwaite,
  • Tjir-Li Tsui,
  • Adam Mclean,
  • Rachel Hilton,
  • Sian Griffin,
  • Colin Geddes,
  • Simon Ball,
  • Richard Baker,
  • Candice Roufosse,
  • Catherine Horsfield,
  • Anthony Dorling

DOI
https://doi.org/10.3389/fimmu.2020.00079
Journal volume & issue
Vol. 11

Abstract

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RituxiCAN-C4 combined an open-labeled randomized controlled trial (RCT) in 7 UK centers to assess whether rituximab could stabilize kidney function in patients with chronic rejection, with an exploratory analysis of how B cell-depletion influenced T cell anti-donor responses relative to outcome. Between January 2007 and March 2015, 59 recruits were enrolled after screening, 23 of whom consented to the embedded RCT. Recruitment was halted when in a pre-specified per protocol interim analysis, the RCT was discovered to be significantly underpowered. This report therefore focuses on the exploratory analysis, in which we confirmed that when B cells promoted CD4+ anti-donor IFNγ production assessed by ELISPOT, this associated with inferior clinical outcome; these patterns were inhibited by optimized immunosuppression but not rituximab. B cell suppression of IFNγ production, which associated with number of transitional B cells and correlated with slower declines in kidney function was abolished by rituximab, which depleted transitional B cells for prolonged periods. We conclude that in this patient population, optimized immunosuppression but not rituximab promotes anti-donor alloresponses associated with favorable outcomes.Clinical Trial Registration: Registered with EudraCT (2006-002330-38) and www.ClinicalTrials.gov, identifier: NCT00476164.

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