open access publication

Article, 2024

FOXP3 full length splice variant is associated with kidney allograft tolerance

Frontiers in Immunology, ISSN 1664-3224, Volume 15, Page 1389105, 10.3389/fimmu.2024.1389105

Contributors

Saleh, Qais Waleed 0000-0001-7705-1269 [1] [2] Mohammadnejad, Afsaneh 0000-0003-4184-7518 [1] Tepel, Martin Ernst 0000-0002-0086-0997 (Corresponding author) [1] [2]

Affiliations

  1. [1] University of Southern Denmark
  2. [NORA names: SDU University of Southern Denmark; University; Denmark; Europe, EU; Nordic; OECD];
  3. [2] Odense University Hospital
  4. [NORA names: Region of Southern Denmark; Hospital; Denmark; Europe, EU; Nordic; OECD]

Abstract

Background: Progressive decline of allograft function leads to premature graft loss. Forkhead box P3 (FOXP3), a characteristic gene of T-regulatory cells, is known to be essential for auto-antigen tolerance. We assessed the hypothesis that low FOXP3 mRNA splice variant levels in peripheral blood cells early after transplantation are associated with progressive allograft injury. Methods: Blood samples were prospectively collected from 333 incident kidney transplant recipients on the first and 29th postoperative day. We used quantitative polymerase chain reaction to determine transcripts of 3 isotypes of FOXP3 splice variants, including pre-mature FOXP3 and full length FOXP3 (FOXP3fl). We investigated the association between FOXP3 splice variant levels and the declines in estimated glomerular filtration rate (eGFR) of more than 5ml/min/1.73m2 within the first-year post-transplant using logistic regression. Results: We observed lower FOXP3fl levels in recipients with declining eGFR (N = 132) than in recipients with stable eGFR (N = 201), (logarithmic value -4.13 [IQR -4.50 to -3.84] vs -4.00 [4.32 to -3.74], p=0.02). In ad hoc analysis pre-transplant FOXP3fl levels were similar in both groups. The association between FOXP3fl and declining eGFR was confirmed by multivariable analysis adjusted for potential confounding factors (Odds Ratio 0.51, 95% confidence interval 0.28 to 0.91: p=0.02). When stratifying FOXP3fl levels into quartiles, recipients with lower day1 FOXP3fl had the highest rate of declining eGFR (p=0.04). Conclusion: Low FOXP3fl splice variant levels at the first postoperative day in kidney transplant recipients were associated with severe decline of eGFR, a well-known surrogate for hard endpoints.

Keywords

FOXP3fl, T regulatory cells, allograft function, allograft injury, allograft tolerance, analysis, associated with severe declines, association, blood, blood cells, blood samples, cells, chain reaction, confounding, confounding factors, day1, days, decline, decline of allograft function, decline of eGFR, declining eGFR, eGFR, endpoint, factors, forkhead, forkhead box P3, full-length splice variants, function, genes, graft loss, group, hypothesis, incidence, incident kidney transplant recipients, injury, isotype, kidney, kidney allograft tolerance, kidney transplant recipients, levels, logistic regression, loss, multivariate analysis, peripheral blood cells, polymerase chain reaction, post-transplant, postoperative day, premature graft loss, progressive allograft injury, progressive decline, quantitative polymerase chain reaction, quartile, rate, reaction, recipients, regression, samples, splice variant levels, splice variants, stable eGFR, surrogate, tolerance, transcription, transplant recipients, transplantation, variant level, variants

Funders

  • Augustinus Foundation

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