趋化因子CCL15在肝细胞肝癌组织中的表达及其临床意义

目的:研究趋化因子CCL15在肝细胞肝癌(HCC)组织中的表达及其临床意义,并对CCL15与肝癌的恶性行为之间关系进行研究。方法:80例HCC、80例癌旁组织和50例正常肝组织标本常规制作石蜡包埋切片,CCL15染色为SP免疫组化法。结果:HCC组织中的CCL15表达阳性率及其评分明显高于癌旁组织和正常肝组织(P<0.05),在癌旁组织和正常肝组织之间没有差异;CCL15的蛋白表达与患者的性别、年龄、肝硬化、病理学分级、术前AFP浓度无明显关系(P>0.05),而与肿瘤的大小、癌栓、有无包膜以及TNM分期等有显著关系。结论:CCL15的表达与HCC的一些恶性临床病理特征密切相关,提示CCL15可能是反映HCC发生发展、侵袭、转移的一个重要的生物学指标。

CCL15在脓毒症免疫病理过程中的作用及机制研究

目的:检测脓毒症中CCL15的含量,探究CCL15在脓毒症免疫病理中的作用和机制。方法:选取健康对照者和脓毒症患者各30例,通过盲肠结扎穿刺建立动物模型(CLP),ELISA检测患者和小鼠血清中CCL15含量;给脓毒症小鼠补充重组人CCL15蛋白或PBS,探究CCL15对生存率的影响;通过HE染色和生化指标检测评估器官损伤;通过流式细胞术检测吞噬细胞变化,探究CCL15对细胞吞噬杀伤的影响。结果:脓毒症患者和脓毒症小鼠的CCL15水平显著升高;在实验性脓毒症中,补充CCL15蛋白可以显著提高生存率,改善器官损伤,促进细菌清除。CCL15处理可以促进腹腔灌洗液(PLF)中巨噬细胞募集。结论:CCL15促进细菌清除,改善器官损伤,在脓毒症中发挥免疫保护作用,并改善生存率。

Analysis of the HNF4A isoform-regulated transcriptome identifies CCL15 as a downstream target in gastric carcinogenesis

Objective:Hepatocyte nuclear factor 4α(HNF4 A)has been demonstrated to be an oncogene in gastric cancer(GC).However,the roles of different HNF4 A isoforms derived from the 2 different promoters(P1 and P2)and the underlying mechanisms remain obscure.Methods:The expression and prognostic values of P1-and P2-HNF4 A were evaluated in The Cancer Genome Atlas(TCGA)databases and GC tissues.Then,functional assays of P1-and P2-HNF4 A were conducted both in vivo and in vitro.High-throughput RNA-seq was employed to profile downstream pathways in P1-and P2-HNF4 A-overexpressing GC cells.The expression and gene regulation network of the candidate target genes identified by RNA-seq were characterized based on data mining and functional assays.Results:HNF4 A amplification was a key characteristic of GC in TCGA databases,especially for the intestinal type and early stage.Moreover,P1-HNF4 A expression was significantly higher in tumor tissues than in adjacent non-tumor tissues(P<0.05),but no significant differences were found in P2-HNF4 A expression(P>0.05).High P1-HNF4 A expression indicated poor prognoses in GC patients(P<0.01).Furthermore,P1-HNF4 A overexpression significantly promoted SGC7901 and BGC823 cell proliferation,invasion and migration in vitro(P<0.01).Murine xenograft experiments showed that P1-HNF4 A overexpression promoted tumor growth(P<0.05).Mechanistically,RNA-seq showed that the cytokine-cytokine receptor interactions pathway was mostly enriched in P1-HNF4 A-overexpressing GC cells.Finally,chemokine(C-C motif)ligand 15 was identified as a direct target of P1-HNF4 A in GC tissues.Conclusions:P1-HNF4 A was the main oncogene during GC progression.The cytokine-cytokine receptor interaction pathway played a pivotal role and may be a promising therapeutic target.

趋化因子CCL15调控肝脏肿瘤微环境的作用机制研究进展

肝脏中肿瘤细胞生长存活所处的生理环境被称为肝脏肿瘤微环境。肝细胞癌(HCC)是一种典型的炎症相关性肿瘤,肿瘤微环境的改变被认为是HCC发生的关键性始动因素。趋化因子是一组具有趋化作用的细胞因子,在调节肿瘤微环境中起关键作用。CCL15是HCC中表达最丰富的趋化因子之一,在HCC进展过程中通过招募免疫细胞引起免疫抑制、促进血管生成、诱导上皮间质转化以及与乙肝病毒X蛋白协同作用,对肝脏肿瘤微环境产生影响。CCL15有望作为HCC的血清检查标志物以及临床诊断治疗HCC的新靶点,为更多的HCC患者带来希望。

CCL15在不同转移潜能人肝癌细胞株中的功能分析

目的解析CeL15的生物学功能，验证其是否在肝癌侵袭、转移和复发中发挥作用。方法用RT-PCR、Westemblot分别检测CCL15在不同转移潜能人肝癌细胞株中的基因和蛋白表达水平并进行比较。用CCL15特异性的小干扰RNA质粒转染高转移潜能人肝癌细胞株HCCML3，得到CeL15低表达的细胞株HccML3-SiCCL15，通过划痕实验和Matrigel体外侵袭实验观察CeL15表达降低后对HCCML3细胞生物学行为的影响。数据用均数±标准差伍±s）表示，用SPSS11．0统计软件包进行t检验。结果CeL15在有转移潜能人肝癌细胞株HCCML3和MHCC97-L中高表达。划痕实验结果显示，HCCML3组和HCCML3siCCLl5组划痕两侧边缘之间的距离分别是（0．35士0．02）mm和（0．82±0．03）mm（t=15．67，P〈0．05）。Matrigel侵袭实验结果显示，HCCML3组和HCCML3-siCCLl5组平均每视野侵袭细胞分别为（657．9±22．9）个和（148．4±10．2）个（t=19．34，P〈0．05）。HccML3-SiccL15组细胞内基质金属蛋白酶（MMP-9表达水平明显低于HCCML3组。结论降低CCLl5表达后HCCML3细胞迁移和侵袭能力均明显降低，细胞内MMP-9表达水平降低。提示CCL15通过增强肝癌细胞的运动侵袭能力和上调MMP-9的分泌参与肝癌细胞的侵袭、转移过程。