4.0 Article

Thymopoiesis in elderly human is associated with systemic inflammatory status

期刊

AGE
卷 31, 期 2, 页码 87-97

出版社

SPRINGER
DOI: 10.1007/s11357-008-9084-x

关键词

Ageing; T cell homeostasis; Human thymus; Immunosenescence; Neutrophil; Systemic inflammation

资金

  1. Fondo de Investigaciones Sanitarias (FIS) [FI06/00176]
  2. Fundacion para la Investigacion y la Prevencion del SIDA en Espana (FIPSE) [12481/05]
  3. Redes Tematicas de Investigacion en SIDA [ISCIII RETIC RD06/0006/0021, ISCIII RECAVA, RD06/0014]
  4. Proyecto de Excelencia, Consejera de Innovacion, Ciencia y Empresa, Junta de Andalucia, Spain [P06-CTS-01579]
  5. Consejer a de Salud, Servicio Andaluz de Salud [156/2006, PI0366/07]

向作者/读者索取更多资源

Immunosenescence studies of age-related immune system damage focused on clinical lymphopenic situations or androgenic blockade have revealed new insights about adult human immune reconstitution. However, as far as we know, the extent of lymphopoiesis in the thymus of elderly humans remains unclear. To this effect, we have analyzed 65 adult human thymuses (from 36 to 81 years; median age 68.6 years) obtained from patients who underwent cardiac surgery. Our results show a correlation between CD4(+)CD8(+) double-positive (DP) cells and both the age (inverse) and percentage (direct) of peripheral naive T cells, indicating that the thymus is still able to affect the peripheral lymphocyte pool even in the elderly. We also found significant correlation between the degree of thymopoiesis and the inflammation markers, as shown by the inverse correlations between DP and the percentage of neutrophils and IL-6 levels and the percentage of peripheral lymphocytes. Furthermore, in a multivariate linear regression the percentage of DP and IL-7 levels, but not age, were independently associated with the percentage of neutrophils. In conclusion, the thymus maintains, even in the elderly, an active thymopoiesis that rejuvenates the peripheral naive T-cell pool. Moreover, age-related thymopoietic decay is associated with the peripheral inflammation markers.

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