KRAS 基因突变通过下调 SERTAD4 促进核酸镰刀菌在结直肠癌中的定植。

Yizhen Chen, Yuanyuan Zheng, Shaolin Liu
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摘要

本研究探索并验证了 KRAS 突变调控结直肠癌(CRC)中核酸镰刀菌(FN)定殖的潜在分子靶点。这项研究结合了多种生物信息学方法和生物学测定。通过癌症基因组图谱(The Cancer Genome Atlas)、基因表达总库(Gene Expression Omnibus)、人类蛋白质图谱(Human Protein Atlas)、免疫组织化学和共培养试验,我们进一步证实了 SERTAD4 在 CRC 中的差异表达。我们深入研究了 SERTAD4 的表达与免疫细胞浸润的关系以及潜在通路的丰富性。最后,我们通过细菌表型实验验证了 SERTAD4 的功能。作为一种与 KRAS 突变和 FN 感染相关的分子,SERTAD4 在 CRC 中的表达水平被下调。SERTAD4 对 CRC 的诊断效果并不亚于 CEA。SERTAD4 的低表达与较差的 CRC 总生存率相关。相关分析发现,SERTAD4表达的增加与各种免疫细胞浸润和免疫检查点基因有关。最后,细菌粘附和侵袭试验验证了 SERTAD4 可抑制 FN 在 CRC 中的粘附和侵袭能力。这项研究表明,SERTAD4 可通过抑制 FN 的定植对 CRC 发挥保护作用。
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KRAS mutation promotes the colonization of Fusobacterium nucleatum in colorectal cancer by down-regulating SERTAD4

This study explores and verifies potential molecular targets through which KRAS mutations regulate the colonization of Fusobacterium nucleatum (FN) in colorectal cancer (CRC). This study combined multiple bioinformatics methods and biological assays. Through The Cancer Genome Atlas, Gene Expression Omnibus, Human Protein Atlas, immunohistochemistry, and co-culture assays, we further confirmed the differential expression of SERTAD4 in CRC. We delved deeper into examining how expression of SERTAD4 is linked with immune cell infiltration and the enrichment of potential pathways. Lastly, through bacterial phenotypic assays, we validated the function of SERTAD4. As a molecule associated with KRAS mutations and FN infection, the expression levels of SERTAD4 were downregulated in CRC. The diagnostic efficacy of SERTAD4 for CRC is not inferior to that of CEA. Low expression of SERTAD4 is associated with poorer overall survival in CRC. Correlation analysis found that increased expression of SERTAD4 is associated with various immune cell infiltrations and immune checkpoint genes. Finally, bacterial adhesion and invasion assays verify that SERTAD4 inhibits the adhesion and invasion abilities of FN in CRC. This study demonstrates that SERTAD4 exerts a protective role in CRC by inhibiting the colonization of FN.

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期刊介绍: The Journal of Cellular and Molecular Medicine serves as a bridge between physiology and cellular medicine, as well as molecular biology and molecular therapeutics. With a 20-year history, the journal adopts an interdisciplinary approach to showcase innovative discoveries. It publishes research aimed at advancing the collective understanding of the cellular and molecular mechanisms underlying diseases. The journal emphasizes translational studies that translate this knowledge into therapeutic strategies. Being fully open access, the journal is accessible to all readers.
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