唐氏综合症儿童血液中促凋亡活化t细胞:与饮食抗原和肠道改变的关系

M M Corsi, W Ponti, A Venditti, F Ferrara, C Baldo, M Chiappelli, F Licastro
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引用次数: 0

摘要

免疫缺陷、甲状腺异常、感染和乳糜泻通常与唐氏综合征(DS)有关。然而,退行性椎体滑移的免疫缺陷的基础尚不清楚。在本研究中,我们发现DS患儿外周血CD4 t细胞减少,而细胞毒性CD8 t细胞的平均值与健康儿童相当。循环活化的(CD3/HLA-DR阳性)t细胞增加,DS纯化的t细胞中APO-I/FAS (CD95)抗原阳性的比例也很大。为了进一步探讨循环活化t细胞的功能状态,我们将富集的CD3淋巴细胞培养3 h,检测annexin-V (ax - v)和碘化丙啶的阳性。具有早期凋亡表型的t细胞在DS儿童的细胞培养中增加。DS患儿血浆中白细胞介素-6 (IL-6)水平高于健康儿童。乳糜泻的发病率在这组儿童中也有所增加。大多数DS患儿外周血中麦胶蛋白特异性IgG或IgA水平升高,且血浆IL-6水平与抗麦胶蛋白IgG水平相关。伴有乳糜泻的DS患儿CD4循环细胞数极低,血清抗麦胶蛋白抗体组CD4循环细胞数低,无抗麦胶蛋白抗体组CD4循环细胞数正常。由于胃肠道粘膜功能改变而继发的饮食抗原过载和营养吸收受损可能通过诱导CD4 t细胞的程序性细胞死亡来干扰正常的免疫反应。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Proapoptotic activated T-cells in the blood of children with Down's syndrome: relationship with dietary antigens and intestinal alterations.

Immune defects, thyroid abnormalities, infections and coeliac disease are often associated with Down's syndrome (DS). However, the basis of the immune defects is still unclear in DS. In the present study, we show that peripheral CD4 T-cells were decreased in children with DS, while mean values of cytotoxic CD8 T-cells were comparable with those from healthy children. Circulating activated (CD3/HLA-DR positive) T-cells were increased and a large proportion of purified T-cells from DS were also positive for APO-I/FAS (CD95) antigen. To further explore the functional status of circulating activated T-cells, enriched CD3 lymphocytes were cultured for 3 h and were tested for positivity to annexin-V (ANX-V) and propidium iodide. T-cells with the early apoptotic phenotype were increased in cell cultures from DS children. Plasma levels of inteleukin-6 (IL-6) were higher in DS children than in healthy children. The incidence of coeliac disease was also increased in this group of children. Most DS children showed increased levels of circulating IgG or IgA specific for gliadin, and their plasma IL-6 levels correlated with those of antigliadin IgG. The number of CD4 circulating cells was very low in DS children with coeliac disease, was low in those with serum antigliadin antibodies and was normal in DS without antigliadin antibodies. An overload of dietary antigens and impaired nutrient absorption secondary to altered functioning of the gastrointestinal mucosa might interfere with normal immune responses by inducing programmed cell death in CD4 T-cells.

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