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整合空间图谱与癌症基因组学以识别免疫浸润的错配修复 proficient 结直肠癌。 注:原文中“proficient”可能有误,根据语境推测可能是“deficient”(缺陷的),若为“deficient”,则译文为:整合空间图谱与癌症基因组学以识别免疫浸润的错配修复缺陷型结直肠癌。

Integrating spatial profiles and cancer genomics to identify immune-infiltrated mismatch repair proficient colorectal cancers.

作者信息

Wala Jeremiah, de Bruijn Ino, Coy Shannon, Gagné Andréanne, Chan Sabrina, Chen Yu-An, Hoffer John, Muhlich Jeremy, Schultz Nikolaus, Santagata Sandro, Sorger Peter K

出版信息

bioRxiv. 2024 Sep 26:2024.09.24.614701. doi: 10.1101/2024.09.24.614701.

DOI:10.1101/2024.09.24.614701
PMID:39386479
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11463659/
Abstract

UNLABELLED

Predicting the progression of solid cancers based solely on genetics is challenging due to the influence of the tumor microenvironment (TME). For colorectal cancer (CRC), tumors deficient in mismatch repair (dMMR) are more immune infiltrated than mismatch repair proficient (pMMR) tumors and have better prognosis following resection. Here we quantify features of the CRC TME by combining spatial profiling with genetic analysis and release our findings via a spatially enhanced version of cBioPortal that facilitates multi-modal data exploration and analysis. We find that ∼20% of pMMR tumors exhibit similar levels of T cell infiltration as dMMR tumors and that this is associated with better survival but not any specific somatic mutation. These T cell-infiltrated pMMR (tipMMR) tumors contain abundant cells expressing PD1 and PDL1 as well as T regulatory cells, consistent with a suppressed immune response. Thus, like dMMR CRC, tipMMR CRC may benefit from immune checkpoint inhibitor therapy.

SIGNIFICANCE

pMMR tumors with high T cell infiltration and active immunosuppression are identifiable with a mid-plex imaging assay whose clinical deployment might double the number of treatment-naïve CRCs eligible for ICIs. Moreover, the low tumor mutational burden in tipMMR CRC shows that MMR status is not the only factor promoting immune infiltration.

摘要

未标记

由于肿瘤微环境(TME)的影响,仅基于遗传学预测实体癌的进展具有挑战性。对于结直肠癌(CRC),错配修复缺陷(dMMR)的肿瘤比错配修复 proficient(pMMR)的肿瘤具有更多的免疫浸润,并且在切除后预后更好。在这里,我们通过将空间分析与基因分析相结合来量化CRC TME的特征,并通过cBioPortal的空间增强版本发布我们的发现,该版本便于多模态数据探索和分析。我们发现约20%的pMMR肿瘤表现出与dMMR肿瘤相似水平的T细胞浸润,并且这与更好的生存率相关,但与任何特定的体细胞突变无关。这些T细胞浸润的pMMR(tipMMR)肿瘤含有大量表达PD1和PDL1的细胞以及调节性T细胞,这与免疫反应受抑制一致。因此,与dMMR CRC一样,tipMMR CRC可能从免疫检查点抑制剂治疗中获益。

意义

具有高T细胞浸润和活跃免疫抑制的pMMR肿瘤可以通过一种中等复杂度的成像检测方法来识别,其临床应用可能会使符合免疫检查点抑制剂治疗条件的初治CRC数量增加一倍。此外,tipMMR CRC中低肿瘤突变负担表明MMR状态不是促进免疫浸润的唯一因素。

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