Sousa-Squiavinato Annie Cristhine Moraes, Vasconcelos Renata Ivo, Gehren Adriana Sartorio, Fernandes Priscila Valverde, de Oliveira Ivanir Martins, Boroni Mariana, Morgado-Díaz Jose Andrés
Cellular and Molecular Oncobiology Program, Brazilian National Cancer Institute (INCA), 37 André Cavalcanti Street, 3th Floor, Rio de Janeiro, RJ, 20231-050, Brazil.
Pathology Division-DIPAT, Brazilian National Cancer Institute (INCA), Rio de Janeiro, Brazil.
Cancer Cell Int. 2021 Jan 22;21(1):69. doi: 10.1186/s12935-021-01770-w.
Colorectal cancer (CRC) is among the deadliest cancers, wherein early dissemination of tumor cells, and consequently, metastasis formation, are the main causes of mortality and poor prognosis. Cofilin-1 (CFL-1) and its modulators, LIMK1/SSH1, play key roles in mediating the invasiveness by driving actin cytoskeleton reorganization in various cancer types. However, their clinical significance and prognostic value in CRC has not been fully explored. Here, we evaluated the clinical contribution of these actin regulators according to TNM and consensus molecular subtypes (CMSs) classification.
CFL-1, LIMK1 and SSH1 mRNA/protein levels were assessed by real-time PCR and immunohistochemical analyses using normal adjacent and tumor tissues obtained from a clinical cohort of CRC patients. The expression levels of these proteins were associated with clinicopathological features by using the chi square test. In addition, using RNA-Seq data of CRC patients from The Cancer Genome Atlas (TCGA) database, we determine how these actin regulators are expressed and distributed according to TNM and CMSs classification. Based on gene expression profiling, Kaplan-Meier survival analysis was used to evaluated overall survival.
Bioinformatic analysis revealed that LIMK1 expression was upregulated in all tumor stages. Patients with high levels of LIMK1 demonstrated significantly lower overall survival rates and exhibited greater lymph node metastatic potential in a clinical cohort. In contrast, CFL-1 and SSH1 have expression downregulated in all tumor stages. However, immunohistochemical analyses showed that patients with high protein levels of CFL-1 and SSH1 exhibited greater lymph node metastatic potential and greater depth of local invasion. In addition, using the CMSs classification to evaluate different biological phenotypes of CRC, we observed that LIMK1 and SSH1 genes are upregulated in immune (CMS1) and mesenchymal (CMS4) subtypes. However, patients with high levels of LIMK1 also demonstrated significantly lower overall survival rates in canonical (CMS2), and metabolic (CMS3) subtypes.
We demonstrated that CFL-1 and its modulators, LIMK1/SSH1, are differentially expressed and associated with lymph node metastasis in CRC. Finally, this expression profile may be useful to predict patients with aggressive signatures, particularly, the immune and mesenchymal subtypes of CRC.
结直肠癌(CRC)是最致命的癌症之一,肿瘤细胞的早期播散以及由此形成的转移是导致死亡和预后不良的主要原因。丝切蛋白-1(CFL-1)及其调节剂LIMK1/SSH1在多种癌症类型中通过驱动肌动蛋白细胞骨架重组介导侵袭性方面发挥关键作用。然而,它们在结直肠癌中的临床意义和预后价值尚未得到充分探索。在此,我们根据TNM和共识分子亚型(CMSs)分类评估了这些肌动蛋白调节剂的临床作用。
通过实时PCR和免疫组织化学分析,使用从CRC患者临床队列中获取的正常相邻组织和肿瘤组织,评估CFL-1、LIMK1和SSH1的mRNA/蛋白水平。使用卡方检验将这些蛋白质的表达水平与临床病理特征相关联。此外,利用来自癌症基因组图谱(TCGA)数据库的CRC患者的RNA-Seq数据,我们确定这些肌动蛋白调节剂如何根据TNM和CMSs分类进行表达和分布。基于基因表达谱,使用Kaplan-Meier生存分析来评估总生存期。
生物信息学分析显示,LIMK1在所有肿瘤阶段的表达均上调。在临床队列中,LIMK1水平高的患者总生存率显著降低,并且表现出更大的淋巴结转移潜能。相反,CFL-1和SSH1在所有肿瘤阶段的表达均下调。然而,免疫组织化学分析表明,CFL-1和SSH1蛋白水平高的患者表现出更大的淋巴结转移潜能和更深的局部浸润深度。此外,使用CMSs分类评估CRC的不同生物学表型,我们观察到LIMK1和SSH1基因在免疫(CMS1)和间充质(CMS4)亚型中上调。然而,LIMK1水平高的患者在经典(CMS2)和代谢(CMS3)亚型中的总生存率也显著降低。
我们证明了CFL-1及其调节剂LIMK1/SSH1在结直肠癌中差异表达,并与淋巴结转移相关。最后,这种表达谱可能有助于预测具有侵袭性特征的患者,特别是结直肠癌的免疫和间充质亚型患者。
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