Journal of Clinical Medicine (Jan 2022)

Spectrum of Kidney Disorders Associated with T-Cell Immunoclones

  • Alexis Piedrafita,
  • François Vergez,
  • Julie Belliere,
  • Nais Prades,
  • Magali Colombat,
  • Antoine Huart,
  • Jean-Baptiste Rieu,
  • Stéphanie Lagarde,
  • Arnaud Del Bello,
  • Nassim Kamar,
  • Dominique Chauveau,
  • Camille Laurent,
  • Lucie Oberic,
  • Loïc Ysebaert,
  • David Ribes,
  • Stanislas Faguer

DOI
https://doi.org/10.3390/jcm11030604
Journal volume & issue
Vol. 11, no. 3
p. 604

Abstract

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Large granular T-cell leukemia is a clonal hematological condition often associated with autoimmune disorders. Whether small-sized T-cell clones that are otherwise asymptomatic can promote immune kidney disorders remains elusive. In this monocentric retrospective cohort in a tertiary referral center in France, we reviewed characteristics of 29 patients with T-cell clone proliferation and autoimmune kidney disorders. Next-generation sequencing of the T-cell receptor of circulating T-cells was performed in a subset of patients. The T-cell clones were detected owing to systematic screening (mean count 0.32 × 109/L, range 0.13–3.7). Strikingly, a common phenotype of acute interstitial nephropathy was observed in 22 patients (median estimated glomerular filtration rate at presentation of 22 mL/min/1.73 m2 (range 0–56)). Kidney biopsies showed polymorphic inflammatory cell infiltration (predominantly CD3+ T-cells, most of them demonstrating positive phospho-STAT3 staining) and non-necrotic granuloma in six cases. Immune-mediated glomerulopathy only or in combination with acute interstitial nephropathy was identified in eight patients. Next-generation sequencing (n = 13) identified a major T-cell clone representing more than 1% of the T-cell population in all but two patients. None had a mutation of STAT3. Twenty patients (69%) had two or more extra-kidney autoimmune diseases. Acute interstitial nephropathies were controlled with corticosteroids, cyclosporin A, or tofacitinib. Thus, we showed that small-sized T-cell clones (i.e., without lymphocytosis) undetectable without specific screening are associated with various immune kidney disorders, including a previously unrecognized phenotype characterized by severe inflammatory kidney fibrosis and lymphocytic JAK/STAT activation.

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