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从脓毒症患者的结直肠肿瘤转录组谱中揭示了病毒感染风险和脓毒症进展的种族基础。

Transcriptome profiling of colorectal tumors from patients with sepsis reveals an ethnic basis for viral infection risk and sepsis progression.

机构信息

University of Hawai'i Cancer Center, Honolulu, HI, 96813, USA.

Department of Molecular Biosciences and Bioengineering, University of Hawai'i at Mānoa, Honolulu, HI, 96822, USA.

出版信息

Sci Rep. 2022 Nov 30;12(1):20646. doi: 10.1038/s41598-022-24489-8.

Abstract

Mortality from cancer-associated sepsis varies by cancer site and host responses to sepsis are heterogenous. Native Hawaiians have the highest mortality risk from cancer-associated sepsis and colorectal cancer (CRC), even though they demonstrate lower CRC incidence compared to other ethnicities. We conducted a retrospective transcriptomic analysis of CRC tumors and adjacent non-tumor tissue from adult patients of Native Hawaiian and Japanese ethnicity who died from cancer-associated sepsis. We examined differential gene expression in relation to patient survival and sepsis disease etiology. Native Hawaiian CRC patients diagnosed with sepsis had a median survival of 5 (IQR 4-49) months, compared to 117 (IQR 30-146) months for Japanese patients. Transcriptomic analyses identified two distinct sepsis gene signatures classified as early response and late response sepsis genes that were significantly altered in the Native Hawaiian cohort. Analysis of canonical pathways revealed significant up and downregulation in mechanisms of viral exit from host cells (p = 4.52E-04) and epithelial junction remodeling (p = 4.01E-05). Key genes including elongation initiation factor pathway genes, GSK3B, and regulatory associated protein of mTOR (RPTOR) genes that protect cells from infection were significantly downregulated in Native Hawaiians. Genes promoting sepsis progression including CLOCK, PPBP and Rho family GTPASE 2 (RND2) were upregulated in Native Hawaiian patients. Our transcriptomic approach advances understanding of sepsis heterogeneity by revealing a role of genetic background and defining patient subgroups with altered early and late biological responses to sepsis. This study is the first to investigate differential gene expression in CRC-associated sepsis patients in relation to ethnicity. Our findings may lead to personalized approaches in stratifying patient mortality risk for sepsis and in the development of effective targeted therapies for sepsis.

摘要

癌症相关脓毒症的死亡率因癌症部位而异,宿主对脓毒症的反应也存在异质性。尽管与其他种族相比,夏威夷原住民的结直肠癌 (CRC) 发病率较低,但他们的癌症相关脓毒症死亡率最高,尤其是结直肠癌。我们对来自夏威夷原住民和日本裔成年癌症相关脓毒症患者的 CRC 肿瘤和相邻非肿瘤组织进行了回顾性转录组分析。我们研究了与患者生存和脓毒症病因相关的差异基因表达。诊断为脓毒症的夏威夷原住民 CRC 患者的中位生存期为 5(IQR 4-49)个月,而日本患者的中位生存期为 117(IQR 30-146)个月。转录组分析确定了两种不同的脓毒症基因特征,分为早期反应和晚期反应脓毒症基因,在夏威夷原住民队列中明显改变。对经典途径的分析显示,宿主细胞中病毒释放(p = 4.52E-04)和上皮连接重塑(p = 4.01E-05)的机制显著上调和下调。关键基因,包括保护细胞免受感染的延伸起始因子途径基因、GSK3B 和雷帕霉素靶蛋白 (mTOR) 的调节相关蛋白 (RPTOR) 基因,在夏威夷原住民中明显下调。促进脓毒症进展的基因,包括 CLOCK、PPBP 和 Rho 家族 GTPASE 2(RND2),在夏威夷原住民患者中上调。我们的转录组方法通过揭示遗传背景的作用并定义对脓毒症具有早期和晚期生物学反应改变的患者亚组,推进了对脓毒症异质性的理解。这项研究是首次调查与种族相关的 CRC 相关脓毒症患者的差异基因表达。我们的研究结果可能会导致分层脓毒症患者死亡率风险的个体化方法,并为脓毒症开发有效的靶向治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5509/9712675/5ff06ceeb36e/41598_2022_24489_Fig1_HTML.jpg

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