INSERM U768, Université Paris Descartes, Hôpital Necker-Enfants Malades, Paris, France.
J Clin Invest. 2011 Jan;121(1):106-12. doi: 10.1172/JCI43752. Epub 2010 Dec 22.
Autoimmune diseases develop in approximately 5% of humans. They can arise when self-tolerance checkpoints of the immune system are bypassed as a consequence of inherited mutations of key genes involved in lymphocyte activation, survival, or death. For example, autoimmune lymphoproliferative syndrome (ALPS) results from defects in self-tolerance checkpoints as a consequence of mutations in the death receptor-encoding gene TNF receptor superfamily, member 6 (TNFRSF6; also known as FAS). However, some mutation carriers remain asymptomatic throughout life. We have now demonstrated in 7 ALPS patients that the disease develops as a consequence of an inherited TNFRSF6 heterozygous mutation combined with a somatic genetic event in the second TNFRSF6 allele. Analysis of the patients' CD4(-)CD8(-) (double negative) T cells--accumulation of which is a hallmark of ALPS--revealed that in these cells, 3 patients had somatic mutations in their second TNFRSF6 allele, while 4 patients had loss of heterozygosity by telomeric uniparental disomy of chromosome 10. This observation provides the molecular bases of a nonmalignant autoimmune disease development in humans and may shed light on the mechanism underlying the occurrence of other autoimmune diseases.
自身免疫性疾病在大约 5%的人类中发展。当参与淋巴细胞激活、存活或死亡的关键基因的遗传突变绕过自身耐受检查点时,它们可能会出现。例如,自身免疫性淋巴增生综合征(ALPS)是由于死亡受体编码基因 TNF 受体超家族成员 6(TNFRSF6;也称为 FAS)的突变导致自身耐受检查点缺陷而引起的。然而,一些突变携带者终生无症状。我们现在在 7 名 ALPS 患者中证明,该疾病是由于遗传的 TNFRSF6 杂合突变与第二个 TNFRSF6 等位基因的体细胞遗传事件共同导致的。对患者的 CD4(-)CD8(-)(双阴性)T 细胞进行分析——这些细胞的积累是 ALPS 的标志——发现其中 3 名患者的第二个 TNFRSF6 等位基因存在体细胞突变,而 4 名患者的第 10 号染色体端粒单亲二体性导致杂合性丧失。这一观察结果为人类非恶性自身免疫性疾病的发展提供了分子基础,并可能阐明其他自身免疫性疾病发生的机制。
