Oncogenic tuftelin 1 as a potential molecular-targeted for inhibiting hepatocellular carcinoma growth

BACKGROUND Abnormal tuftelin 1(TUFT1)has been reported in multiple cancers and exhibits oncogenic roles in tumor progression.However,limited data are available on the relationship between TUFT1 and hepatocellular carcinoma(HCC),and the exact biological mechanism of TUFT1 is still poorly understood in HCC.AIM To investigate TUFT1 expression in HCC and how interfering TUFT1 transcription affects HCC growth.METHODS TUFT1 in HCC and non-HCC tissues based on databases of the Cancer Genome Atlas and Oncomine were analyzed,and TUFT1 in human HCC tissues on microarray were detected by immunohistochemistry for clinicopathological features,overall survival,and disease-free survival.HCC cells were transfected with constructed vectors of TUFT1 that interfere or over-express TUFT1 for analyzing the biological behaviors of HCC cells.Proliferation,invasion,migration,and apoptosis of cells were detected by cell counting kit-8,scratch assay,transwell tests,and flow cytometry and confirmed by Western blotting,respectively.RESULTS Abnormal TUFT1 levels in databases expressed in HCC at messenger RNA(mRNA)level and HCC tissues were mainly located in cytoplasm and membrane.The level of TUFT1 expression in the HCC group was significantly higher(χ2=18.563,P<0.001)than that in the non-cancerous group,closely related to clinical staging,size,vascular invasion of tumor,hepatitis B e-antigen positive,and ascites(P<0.01)of HCC patients,and negatively to HCC patients’overall survival and disease-free survival(P<0.001).After interfering with TUFT1 transcription at mRNA level in the MHCC-97H cells by the specific TUFT1-short hairpin RNA,cell proliferation,invasion,and metastasis were significantly inhibited with increasing apoptosis rate.In contrast,proliferation,invasion,and migration were significantly enhanced after over-expression of TUFT1 mRNA in Hep3B cells in vitro.CONCLUSION Oncogenic TUFT1 was associated with the progression of HCC and could be a potential molecular-target for inhibiting HCC growth.

TUFT1在直肠癌组织中表达及其临床诊断和预后价值

目的探究釉丛蛋白1(TUFT1)在直肠癌组织中的表达水平及其对直肠癌的诊断和预后价值。方法利用Ualcan数据库分析TUFT1 mRNA在正常直肠组织及直肠癌组织中的表达水平;选取2014年12月~2018年4月新乡市第一人民医院诊治的77例直肠癌患者为研究对象,实时荧光定量PCR(qRT-PCR)法测定直肠癌组织、癌旁正常组织TUFT1 mRNA表达水平;分析直肠癌组织TUFT1 mRNA表达水平与直肠癌患者临床病理特征的关系;受试者工作特征曲线(ROC曲线)评价直肠组织TUFT1 mRNA表达水平对直肠癌的诊断价值;Kaplan-Meier生存曲线分析直肠癌组织TUFT1 mRNA表达水平与直肠癌患者预后的关系;COX回归分析影响直肠癌患者预后的因素。结果Ualcan数据库分析显示,直肠癌组织TUFT1 mRNA表达水平高于正常直肠组织(P<0.05);qRT-PCR法检测显示,直肠癌组织TUFT1 mRNA表达水平高于癌旁正常组织(P<0.05);直肠癌组织TUFT1 mRNA表达水平与直肠癌患者淋巴结转移、TNM分期、分化程度相关(P<0.05);直肠组织TUFT1 mRNA表达水平诊断直肠癌的曲线下面积(AUC)为0.889,其截断值为1.59,此时敏感度为83.1%,特异性为87.0%;TUFT1 mRNA低表达组直肠癌患者总生存率高于TUFT1 mRNA高表达组(P<0.05);淋巴结转移、TNM分期、TUFT1 mRNA是影响直肠癌不良预后的独立危险因素(P<0.05)。结论直肠癌患者癌组织中TUFT1 mRNA表达水平较高,均与淋巴结转移、TNM分期、分化程度及预后相关,TUFT1 mRNA可作为诊断直肠癌、评估患者预后的潜在指标。

肝癌组织TPX2、TUFT1、Vimentin表达与癌细胞恶性生物学行为的关系及预测远处转移的价值研究

目的:探讨肝癌组织爪蟾驱动蛋白样蛋白2靶蛋白(TPX2)、釉丛蛋白1(TUFT1)、波形蛋白(Vimentin)表达与癌细胞恶性生物学行为的关系及预测远处转移的价值。方法:选取2018年1月~2020年4月收治的51例肝癌远处转移患者为观察组,51例肝癌无远处转移患者为对照组,比较两组患者一般资料、TPX2 mRNA、TUFT1和Vimentin蛋白、癌细胞恶性生物学行为指标[B淋巴细胞瘤-2(Bcl-2)mRNA、survivin mRNA、Bax mRNA、半胱氨酸天冬氨酸蛋白酶-3(caspase-3)mRNA],分析TPX2 mRNA、TUFT1和Vimentin蛋白之间及与癌细胞恶性生物学行为指标、病理特征的相关性,并分析TPX2 mRNA、TUFT1和Vimentin蛋白预测远处转移的价值。结果:观察组患者TPX2 mRNA、TUFT1和Vimentin蛋白表达高于对照组患者(P<0.05)。TPX2 mRNA与TUFT1、Vimentin蛋白呈正相关,TUFT1蛋白与Vimentin蛋白呈正相关(P<0.05)。TPX2 mRNA、TUFT1蛋白、Vimentin蛋白与Bcl-2 mRNA、survivin mRNA均呈正相关,与Bax mRNA、caspase-3 mRNA均呈负相关(P<0.05)。TPX2 mRNA、TUFT1蛋白、Vimentin蛋白与肿瘤T、N分期呈正相关,与分化程度呈负相关(P<0.05)。TPX2 mRNA、TUFT1、Vimentin联合预测肝癌远处转移的AUC最大,为0.932。结论:肝癌组织TPX2、TUFT1、Vimentin表达与癌细胞恶性生物学行为存在一定相关性,早期采用三者联合检测方式,有望成为临床预测肝癌远处转移、制定恰当治疗方案的新途径。

TUFT1在恶性肿瘤中的研究进展

釉丛蛋白1(TUFT1)作为一种多功能的牙釉质相关蛋白质,最早发现其在牙釉质的结构形成和矿化过程中起主要作用,随后发现其也参与体内多种生理和病理过程。其中,TUFT1在多种恶性肿瘤中表达上调,能作为一种癌基因促进恶性肿瘤增殖和转移、抑制细胞凋亡,在恶性肿瘤的发生发展过程发挥重要作用。靶向TUFT1可抑制恶性肿瘤进展以及逆转化疗耐药性。此外,TUFT1在恶性肿瘤预后评估中也显示出潜在的应用价值,有望成为新的潜在治疗靶点以及预后评估的分子标志物。

TUTF1表达对肝癌细胞增殖凋亡及预后的影响

目的研究Tuftelin 1(TUFT1)的表达与肝细胞肝癌临床病理特征关系及其对肝癌细胞增殖凋亡的影响,探讨TUFT1与肝癌发生发展的关系。方法应用免疫组织化学检测98例肝细胞肝癌及30例癌旁正常组织中TUFT1的表达,应用qRT-PCR的方法检测肝癌细胞系中TUFT1的表达,通过慢病毒载体介导敲减SMMC-7221细胞系中TUFT1的表达,采用细胞增殖检测、平板克隆形成试验、细胞凋亡实验、细胞周期检测检测下调TUFT1后肝癌细胞的增殖、凋亡能力及细胞周期的变化。统计学采用X?检验及/检验。结果98例肝细胞癌组织中TUFT1阳性表达65例(66.33%),30例癌旁正常组织中阳性表达6例(16.67%),差异有统计学意义(X^2=19.956,P<0.05)。肝癌组织中TUFT1表达与肿瘤大小、肿瘤分期及复发转移有关(x^2值分别为6.214、8.066,14.400,P值均<0.05)。慢病毒载体介导敲减SMMC-7221细胞中TUFT1的表达后,与肝癌细胞SMMC-7221对照组比较,SMMC-7221细胞增殖率减少[(18.62%±0.15%)对比(67.91%±0.62%)],克隆形成能力下降[(8.10%±0.80%)对比(50.80%±1.60%)],G1期细胞明显减少[(36.71%±0.69%)对比(44.65%±0.73%)],G2期细胞增加[(22.31%±0.20%)对比(15.44%±0.53%)],细胞凋匸增加[(3.45%±0.18%)对比(5.45%±0.06%)],P值均<0.05,差异均有统计学意义。结论肝癌组织中TUFT1高表达,TUFT1的表达促进肝癌细胞增殖、抑制细胞凋亡,是肝癌预后不良的因素。