Han Jing, Zuo Jing, Zhang Xue, Wang Long, Li Dan, Wang Yudong, Liu Jiayin, Feng Li
Department of Medical Oncology, Hebei Medical University Fourth Affiliated Hospital and Hebei Provincial Tumor Hospital, Shijiazhuang, China.
J Gastrointest Oncol. 2022 Jun;13(3):1132-1151. doi: 10.21037/jgo-22-365.
In colorectal cancer (CRC) patients, different primary tumor locations caused distinct prognosis and clinicopathological features. It is necessary to identify specific tumor markers according tumor site. Our previous work has identified differentially expressed genes between CRC and adjacent normal tissues, in which only TRIM29 was differently expressed between right colon cancer (RCC) and left colon cancer (LCC) patients. Rectal cancer (RECC) was not included in this latter study and the effects of TRIM29 on the survival with RCC and LCC patients were not investigated. This study further verified TRIM29 expression through Gene Expression Omnibus (GEO) database and our retrospective study. The role of TRIM29 on survival according tumor sites was also explored. Furthermore, the molecular mechanisms of TRIM29 were explored.
The GEO dataset was used to confirm the differential expression of TRIM29 in proximal and distal cancers. Moreover, TRIM29 were assess using immunohistochemistry (IHC) in 227 cases to observe the correlation between TRIM29 and tumor site. The relationship between TRIM29 and the clinicopathologic features was investigated according tumor sites. Furthermore, the disease-free survival (DFS) and overall survival (OS) was analyzed using the Kaplan-Meier method to assess the prognostic value of TRIM29. Finally, bioinformatics analysis was used to explore the molecular mechanisms. The Tumor-Immune System Interactions and Drug Bank database (TISIDB) was used to analyze the correlations between TRIM29 expression and tumor immune functions. The correlation of TRIM29 with tumor infiltrating lymphocytes or mismatch-repair-proficient/mismatch-repair-deficient (pMMR/dMMR) status was also investigated.
TRIM29 expression was significantly higher in patients with RCC (P<0.001). RCC patients with high TRIM29 tended to be older, male, in stage III-IV, with N+ staging, and intestinal obstruction (P<0.001, P<0.001, P<0.001, P<0.001, and P=0.010, respectively). High TRIM29 expression was associated with an increased risk of recurrence/metastasis and death, only in RCC patients (P=0.020 and P<0.001). Functional annotations and immune activity analysis showed that TRIM29 is related to tumor infiltrating lymphocytes and immune dysfunction.
TRIM29 plays varying roles in patients with different tumor sites. TRIM29 is correlated with the clinicopathological features and prognosis in RCC patients. Indeed, TRIM29 may serve as a new biomarker for RCC patients.
在结直肠癌(CRC)患者中,不同的原发肿瘤位置导致了不同的预后和临床病理特征。有必要根据肿瘤部位确定特定的肿瘤标志物。我们之前的研究已经确定了CRC与相邻正常组织之间差异表达的基因,其中只有TRIM29在右结肠癌(RCC)和左结肠癌(LCC)患者之间存在差异表达。直肠癌(RECC)未纳入后一项研究,且未研究TRIM29对RCC和LCC患者生存的影响。本研究通过基因表达综合数据库(GEO)和我们的回顾性研究进一步验证了TRIM29的表达。还探讨了TRIM29根据肿瘤部位对生存的作用。此外,还探讨了TRIM29的分子机制。
使用GEO数据集确认TRIM29在近端和远端癌症中的差异表达。此外,对227例患者进行免疫组织化学(IHC)检测TRIM29,以观察TRIM29与肿瘤部位之间的相关性。根据肿瘤部位研究TRIM29与临床病理特征之间的关系。此外,采用Kaplan-Meier法分析无病生存期(DFS)和总生存期(OS),以评估TRIM29的预后价值。最后,利用生物信息学分析探讨分子机制。使用肿瘤-免疫系统相互作用和药物库数据库(TISIDB)分析TRIM29表达与肿瘤免疫功能之间的相关性。还研究了TRIM29与肿瘤浸润淋巴细胞或错配修复 proficient/错配修复缺陷(pMMR/dMMR)状态的相关性。
TRIM29在RCC患者中的表达显著更高(P<0.001)。TRIM29高表达的RCC患者往往年龄较大、为男性、处于III-IV期、N+分期且有肠梗阻(分别为P<0.001、P<0.001、P<0.001、P<0.001和P=0.010)。仅在RCC患者中,高TRIM29表达与复发/转移和死亡风险增加相关(P=0.020和P<0.001)。功能注释和免疫活性分析表明,TRIM29与肿瘤浸润淋巴细胞和免疫功能障碍有关。
TRIM29在不同肿瘤部位的患者中发挥着不同的作用。TRIM29与RCC患者的临床病理特征和预后相关。事实上,TRIM29可能成为RCC患者的一种新的生物标志物。
