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Quantitative T cell repertoire analysis by deep cDNA sequencing of T cell receptor alpha and beta chains using next-generation sequencing (NGS)

机译:通过使用下一代测序(NGS)对T细胞受体α和β链进行深cDNA测序来对T细胞库进行定量分析

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Immune responses play a critical role in various disease conditions including cancer and autoimmune diseases. However, to date, there has not been a rapid, sensitive, comprehensive, and quantitative analysis method to examine T-cell or B-cell immune responses. Here, we report a new approach to characterize T cell receptor (TCR) repertoire by sequencing millions of cDNA of TCR alpha and beta chains in combination with a newly-developed algorithm. Using samples from lung cancer patients treated with cancer peptide vaccines as a model, we demonstrate that detailed information of the V-(D)-J combination along with complementary determining region 3 (CDR3) sequences can be determined. We identified extensive abnormal splicing of TCR transcripts in lung cancer samples, indicating the dysfunctional splicing machinery in T lymphocytes by prior chemotherapy. In addition, we found three potentially novel TCR exons that have not been described previously in the reference genome. This newly developed TCR NGS platform can be applied to better understand immune responses in many disease areas including immune disorders, allergies, and organ transplantations.
机译:免疫反应在包括癌症和自身免疫性疾病在内的各种疾病中起着至关重要的作用。但是,迄今为止,还没有一种快速,灵敏,全面和定量的分析方法来检查T细胞或B细胞的免疫反应。在这里,我们报告了一种通过结合新开发的算法对数百万个TCRα和β链cDNA进行测序来表征T细胞受体(TCR)库的新方法。使用来自癌症患者的样本进行癌症肽疫苗治疗的模型,我们证明可以确定V-(D)-J组合以及互补决定区3(CDR3)序列的详细信息。我们在肺癌样本中发现了广泛的TCR转录异常剪接,表明先前的化学疗法在T淋巴细胞中的剪接机制功能异常。此外,我们发现了三个潜在的新颖的TCR外显子,之前在参考基因组中没有描述过。这个新开发的TCR NGS平台可用于更好地了解许多疾病领域的免疫反应,包括免疫失调,过敏和器官移植。

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