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RNA Transcription and Splicing Errors as a Source of Cancer Frameshift Neoantigens for Vaccines

机译:RNA转录和剪接误差作为疫苗癌症架构的源头源

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The success of checkpoint inhibitors in cancer therapy is largely attributed to activating the patient's immune response to their tumor's neoantigens arising from DNA mutations. This realization has motivated the interest in personal cancer vaccines based on sequencing the patient's tumor DNA to discover neoantigens. Here we propose an additional, unrecognized source of tumor neoantigens. We show that errors in transcription of microsatellites (MS) and mis-splicing of exons create highly immunogenic frameshift (FS) neoantigens in tumors. The sequence of these FS neoantigens are predictable, allowing creation of a peptide array representing all possible neoantigen FS peptides. This array can be used to detect the antibody response in a patient to the FS peptides. A survey of 5 types of cancers reveals peptides that are personally reactive for each patient. This source of neoantigens and the method to discover them may be useful in developing cancer vaccines.
机译:检查点抑制剂在癌症治疗中的成功主要归因于激活患者对由DNA突变产生的肿瘤的新抗原的免疫应答。基于测序患者的肿瘤DNA来发现新抗原,这种实现促进了对个人癌症疫苗的兴趣。在这里,我们提出了另外,未被识别的肿瘤新抗原来源。我们展示了微卫星(MS)转录的误差和外显子的错误剪接在肿瘤中产生高度免疫原性的架子(FS)新抗原。这些FS NeoAntigens的序列是可预测的,允许产生代表所有可能的新宿老的FS肽的肽阵列。该阵列可用于检测患者对FS肽的抗体应答。 5种类型的癌症的调查显示了对每位患者的亲自反应性的肽。这种新抗原的来源和发现它们的方法可能可用于发展癌症疫苗。

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