4.6 Article

Circulating T Cells of Patients with Nijmegen Breakage Syndrome Show Signs of Senescence

Journal

JOURNAL OF CLINICAL IMMUNOLOGY
Volume 37, Issue 2, Pages 133-142

Publisher

SPRINGER/PLENUM PUBLISHERS
DOI: 10.1007/s10875-016-0363-5

Keywords

Tcells; NBS; senescence; CD28null; sjTREC

Categories

Funding

  1. Polish Ministry of Higher Education and Science [2P05A11829]
  2. Dutch Organization for Scientific Research (Veni grant) [916.56.107]

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Purpose The Nijmegen breakage syndrome (NBS) is an inherited genetic disorder characterized by a typical facial appearance, microcephaly, growth retardation, immunodeficiency, and a strong predisposition to malignancies, especially of lymphoid origin. NBS patients have a mutation in the NBN gene which involves the repair of DNA double-strand breaks (DSBs). Here we studied the peripheral T cell compartment of NBS patients with a focus on immunological senescence. Methods The absolute numbers and frequencies of the different T cell subsets were determined in NBS patients from young age till adulthood and compared to age-matched healthy individuals (HI). In addition, we determined the expression of senescent T cell markers and the signal joint T cell receptor excision circles (sjTRECs) content. Results Our results demonstrate that NBS patients have reduced T cell numbers. NBS patients showed lower numbers of alpha beta(+) T cells, but normal gamma delta(+) T cell numbers compared to HI. Concerning the alpha beta(+) Tcells, both CD4(+) as well as CD8(+) T cells were excessively reduced in numbers compared to aged-matched HI. In addition, NBS patients showed higher frequencies of the more differentiated T cells expressing the senescent cell marker CD57 and did not express co-stimulatory molecule CD28. These effects were already present in the youngest age group. Furthermore, NBS patients showed lower sjTREC content in their T cells possibly indicative of a lower thymic output. Conclusions We conclude that circulating T cells from NBS patients show signs of a senescent phenotype which is already present from young age on and which might explain their T cell immune deficiency.

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