Department of Pathology & Immunology, Division of Immunobiology and Bursky Center for Human Immunology and Immunotherapy Programs, Washington University, St. Louis, Missouri, USA.
Proteomics. 2021 Apr;21(7-8):e2000176. doi: 10.1002/pmic.202000176. Epub 2021 Mar 5.
Proteasomal spliced peptides (PSPs) have been identified in the class I major histocompatibility complex (MHC) peptidomes of several tumors and have emerged as novel neoantigens that can stimulate highly specific T cells. Much debate has surrounded the percentage of PSPs in the immunopeptidome; reported numbers have ranged from <1-5% to 12-45%. Recently, our laboratory demonstrated in nonobese diabetic (NOD) mice that hybrid insulin peptides (HIPs), a special class of spliced peptides, are formed during insulin granule degradation in crinosomes of the pancreatic β cells and that modified peptides comprised a significant source of false positive HIP assignments. Herein, this study is extended to crinosomes isolated from other mouse strains and to two recent MHC class I studies, to see if modified peptides explained discrepancies in reported percentages of PSPs. This analysis revealed that both MHC-I peptidomes contained many spectra erroneously assigned as PSPs. While many false positive PSPs did arise from modified peptides, others arose from probable data processing errors. Thus, the reported numbers of PSPs in the literature are likely elevated due to errors associated with data processing and analysis.
蛋白酶体剪接肽 (PSPs) 已在几种肿瘤的 I 类主要组织相容性复合物 (MHC) 肽组中被鉴定出来,并已成为能够刺激高度特异性 T 细胞的新型新抗原。蛋白酶体剪接肽在免疫肽组中的比例存在很大争议;报告的数字范围从 <1-5% 到 12-45%。最近,我们实验室在非肥胖型糖尿病 (NOD) 小鼠中证明,杂种胰岛素肽 (HIPs) 是一种特殊的剪接肽,在胰腺β细胞的颗粒体中胰岛素颗粒降解过程中形成,并且修饰肽构成了假阳性 HIP 分配的重要来源。在此,本研究扩展到从其他小鼠品系中分离的颗粒体,以及最近的两项 MHC 类 I 研究,以了解修饰肽是否解释了报告的 PSP 百分比的差异。该分析表明,两种 MHC-I 肽组都包含许多错误地被分配为 PSP 的光谱。虽然许多假阳性 PSP 确实来自修饰肽,但其他则来自可能的数据处理错误。因此,文献中报告的 PSP 数量可能由于与数据处理和分析相关的错误而升高。
