Departamento de Biologia Celular e Molecular (FABIO) and Instituto de Pesquisas Biomédicas, PUCRS, Av. Ipiranga, Porto Alegre, RS, Brazil.
Mech Ageing Dev. 2011 Apr;132(4):187-94. doi: 10.1016/j.mad.2011.03.005. Epub 2011 Mar 29.
CD4+ T cells regulate humoral and cell-mediated immune responses, which are progressively impaired in aging, resulting in susceptibility to infections and cancer. Dendritic cells (DCs) are major activators of T cells, providing signals that drive their expansion and differentiation. In this study, we asked if decreased CD4+ T cell responses were influenced by the age of DCs rather than being exclusively due to T cell defects. Old T cells transferred to young recipients expanded and differentiated similarly to young T cells. However, aged recipients were poor stimulators of both old and young T cells, which failed to acquire CD44 expression and produce interferon gamma (IFN-γ). DCs in aged hosts expressed fewer MHC-peptide complexes. The CD86 expression in the DCs of both hosts was similar; however, CD40 levels were reduced in old DCs. Finally, old DCs failed to produce inflammatory cytokines in response to LPS. Our results indicate that the impairment of aged CD4+ T cell function is intimately related to multiple alterations in aged DCs, rather than being caused solely by intrinsic T cell defects, suggesting that the function of aged T cells may be partially rescued in vivo when appropriate stimulation is applied. These findings are relevant to vaccination design for elderly populations.
CD4+ T 细胞调节体液和细胞介导的免疫反应,随着年龄的增长,这些反应逐渐受损,导致易感染和癌症。树突状细胞(DCs)是 T 细胞的主要激活剂,提供驱动其扩增和分化的信号。在这项研究中,我们想知道 CD4+ T 细胞反应的降低是否受到 DC 年龄的影响,而不仅仅是由于 T 细胞缺陷。转移到年轻受者中的老年 T 细胞扩增和分化与年轻 T 细胞相似。然而,老年受者是老年和年轻 T 细胞的不良刺激物,它们无法获得 CD44 表达并产生干扰素 γ(IFN-γ)。老年宿主中的 DCs 表达较少的 MHC-肽复合物。两个宿主的 DC 中 CD86 的表达相似;然而,老年 DC 中的 CD40 水平降低。最后,老年 DCs 未能对 LPS 产生炎症细胞因子。我们的结果表明,老年 CD4+ T 细胞功能的损伤与老年 DC 中的多种改变密切相关,而不仅仅是由于内在的 T 细胞缺陷引起的,这表明在适当的刺激下,老年 T 细胞的功能在体内可能部分得到挽救。这些发现与老年人群的疫苗设计有关。
