BMC Immunology (Jan 2009)

Low frequency of CD4<sup>+</sup>CD25<sup>+ </sup>Treg in SLE patients: a heritable trait associated with <it>CTLA4 </it>and <it>TGFβ </it>gene variants

  • Viana João F,
  • Andreia Rita,
  • Martins Berta,
  • Carvalho Cláudia,
  • Alves Miguel,
  • Santos Eugénia,
  • Moraes-Fontes Maria F,
  • Lourenço Lara,
  • Ferreira Ricardo C,
  • Barreto Marta,
  • Vasconcelos Carlos,
  • Mota-Vieira Luísa,
  • Ferreira Carlos,
  • Demengeot Jocelyne,
  • Vicente Astrid M

DOI
https://doi.org/10.1186/1471-2172-10-5
Journal volume & issue
Vol. 10, no. 1
p. 5

Abstract

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Abstract Background CD4+CD25+ regulatory T cells play an essential role in maintaining immune homeostasis and preventing autoimmunity. Therefore, defects in Treg development, maintenance or function have been associated with several human autoimmune diseases including Systemic Lupus Erythematosus (SLE), a systemic autoimmune disease characterized by loss of tolerance to nuclear components and significantly more frequent in females. Results To investigate the involvement of Treg in SLE pathogenesis, we determined the frequency of CD4+CD25+CD45RO+ T cells, which encompass the majority of Treg activity, in the PBMC of 148 SLE patients (76 patients were part of 54 families), 166 relatives and 117 controls. SLE patients and their relatives were recruited in several Portuguese hospitals and through the Portuguese Lupus Association. Control individuals were blood donors recruited from several regional blood donor centers. Treg frequency was significantly lower in SLE patients than healthy controls (z = -6.161, P P bona fide FOXP3+CD4+CD25+ Treg. Treg frequency was negatively correlated with SLE activity index (SLEDAI) and titers of serum anti-dsDNA antibodies. Both Treg frequency and disease activity were modulated by IVIg treatment in a documented SLE case. The segregation of Treg frequency within the SLE families was indicative of a genetic trait. Candidate gene analysis revealed that specific variants of CTLA4 and TGFβ were associated with the decreased frequency of Treg in PBMC, while FOXP3 gene variants were associated with affection status, but not with Treg frequency. Conclusion SLE patients have impaired Treg production or maintenance, a trait strongly associated with SLE disease activity and autoantibody titers, and possibly resulting from the inability to convert FOXP3+CD25- into FOXP3+CD25+ T cells. Treg frequency is highly heritable within SLE families, with specific variants of the CTLA4 and TGFβ genes contributing to this trait, while FOXP3 contributes to SLE through mechanisms not involving a modulation of Treg frequency. These findings establish that the genetic components in SLE pathogenesis include genes related to Treg generation or maintenance.