Translational Immunology Research Program, University of Helsinki, Helsinki, Finland.
Department of Neurology, Neurocenter, Helsinki University Hospital, Helsinki, Finland.
PLoS One. 2021 Dec 7;16(12):e0261002. doi: 10.1371/journal.pone.0261002. eCollection 2021.
Somatic mutations have a central role in cancer but their role in other diseases such as common autoimmune disorders is not clear. Previously we and others have demonstrated that especially CD8+ T cells in blood can harbor persistent somatic mutations in some patients with multiple sclerosis (MS) and rheumatoid arthritis. Here we concentrated on CD8+ cells in more detail and tested (i) how commonly somatic mutations are detectable, (ii) does the overall mutation load differ between MS patients and controls, and (iii) do the somatic mutations accumulate non-randomly in certain genes? We separated peripheral blood CD8+ cells from newly diagnosed relapsing MS patients (n = 21) as well as matched controls (n = 21) and performed next-generation sequencing of the CD8+ cells' DNA, limiting our search to a custom panel of 2524 immunity and cancer related genes, which enabled us to obtain a median sequencing depth of over 2000x. We discovered nonsynonymous somatic mutations in all MS patients' and controls' CD8+ cell DNA samples, with no significant difference in number between the groups (p = 0.60), at a median allelic fraction of 0.5% (range 0.2-8.6%). The mutations showed statistically significant clustering especially to the STAT3 gene, and also enrichment to the SMARCA2, DNMT3A, SOCS1 and PPP3CA genes. Known activating STAT3 mutations were found both in MS patients and controls and overall 1/5 of the mutations were previously described cancer mutations. The detected clustering suggests a selection advantage of the mutated CD8+ clones and calls for further research on possible phenotypic effects.
体细胞突变在癌症中起着核心作用,但它们在其他疾病(如常见的自身免疫性疾病)中的作用尚不清楚。此前,我们和其他人已经证明,在多发性硬化症(MS)和类风湿关节炎等一些患者的血液中,特别是 CD8+T 细胞中,可以持续存在体细胞突变。在这里,我们更详细地关注 CD8+细胞,并测试了:(i)体细胞突变是否可检测到,(ii)MS 患者和对照组之间的总体突变负荷是否不同,以及(iii)体细胞突变是否随机积累在某些基因中?我们从新诊断的复发型 MS 患者(n=21)和匹配的对照组(n=21)中分离外周血 CD8+细胞,并对 CD8+细胞的 DNA 进行下一代测序,将我们的搜索范围限制在一个 2524 个免疫和癌症相关基因的定制面板中,这使我们能够获得超过 2000x 的中位数测序深度。我们在所有 MS 患者和对照组的 CD8+细胞 DNA 样本中发现了非同义体细胞突变,两组之间的数量没有显著差异(p=0.60),等位基因分数中位数为 0.5%(范围 0.2-8.6%)。突变显示出统计学上显著的聚类,尤其是 STAT3 基因,并且还富集到 SMARCA2、DNMT3A、SOCS1 和 PPP3CA 基因。在 MS 患者和对照组中都发现了已知的激活 STAT3 突变,并且总体上有 1/5 的突变是以前描述的癌症突变。检测到的聚类表明突变的 CD8+克隆具有选择优势,并呼吁进一步研究可能的表型效应。
