血清AFP水平和组织GPC3、VEGF蛋白表达在丙肝相关肝癌中的意义

目的探讨在慢性丙型肝炎病毒(hepatitis C virus,HCV)感染患者中检测血清甲胎蛋白(alpha fetoprotein,AFP)水平和组织中磷脂酰肌醇蛋白聚糖-3(glypican-3,GPC3)、血管内皮生长因子(vascular endothelial growth factor,VEGF)蛋白表达在丙肝相关肝癌(HCV-related hepatocellular carcinoma,HCV-HCC)中的临床应用价值。方法采用电化学发光分析技术和免疫组化染色技术检测30例慢性丙型肝炎(chromc hepatitis C,CHC)、35例丙肝相关肝硬化(HCV-related liver cirrhosis,HCV-Cirr)、30例HCV-HCC患者和30例对照组血清AFP水平和组织中GPC3、VEGF蛋白的表达,分析评价在慢性HCV感染患者肝脏病变的不同阶段中血清AFP水平变化和组织中GPC3、VEGF蛋白的表达情况。结果血清AFP水平在HCV-HCC组和HCV-Cirr组均显著高于CHC组和对照组(P <0. 05),但HCV-HCC组与HCV-Cirr组之间血清AFP水平差异无统计学意义(P> 0. 05)。GPC3、VEGF蛋白在对照组无阳性表达,在HCV-HCC组的阳性表达率分别为86. 7%(26/30)、76. 7%(23/30),显著高于HCV-Cirr组的31. 4%(11/35)和40. 0%(14/35)(χ~2=20. 10、P <0. 001;χ~2=8. 86、P <0. 05)和CHC组的10. 0%(3/30)、16. 7%(5/30)(χ~2=35. 31、P <0. 001,χ~2=21. 69、P <0. 001),且HCV-Cirr组显著高于CHC组(χ~2=4. 39、P <0. 05,χ~2=4. 25、P <0. 05)。GPC3蛋白在中、低分化肝癌组中的阳性率显著高于高分化组(P <0. 05);而VEGF在高分化组与中、低分化组之间差异无统计学意义(P=0. 120)。HCV-HCC组中10例血清AFP阴性者组织中GPC3、VEGF蛋白阳性表达分别为6例和5例,且两者联合检测的阳性率为70. 0%(7/10); HCV-HCC组中GPC3与VEGF蛋白表达呈正相关(r=0. 479、P=0. 03)。结论 GPC3和VEGF蛋白在HCV-HCC组织中高表达与HCV-HCC的发生、发展有关。在HCV-Cirr患者的持续监测中联合检测血清AFP和组织中GCP3、VEGF蛋白有助于提高临床对HCV-HCC的鉴别水平。

云南地区丙型肝炎病毒基因亚型及RNA载量在丙型肝炎进展中的变化

目的检测云南地区慢性丙型肝炎、丙肝相关性肝硬化、丙肝相关性肝癌患者中丙肝病毒(HCV)的基因亚型及RNA载量在疾病进展过程中的变化.方法通过收集2016年1月至2017年4月昆明医科大学第一附属医院及云南省传染病医院收治的患者241例,其中丙型肝炎组患者169例,丙肝相关性肝硬化组56例,丙肝相关的肝癌组16例作为研究对象.采用PCR荧光探针法检测血清中丙肝病毒基因亚型以及HCV RNA载量.结果在丙型肝炎患者中3b型最多(27.81%);在丙肝相关性肝硬化患者中1b型最多(30.36%);在丙肝相关性肝癌中3 b型最多(31.25%).3组患者基因亚型比例无显著差别(P>0.05).慢性丙型肝炎、丙肝相关性肝硬化、丙肝相关性肝癌组患者的HCV RNA载量分别为(332±114)Copies/m L、(189±73)Copies/m L、(152±56)Copies/m L.3组患者HCV RNA载量的差异显著(P<0.01),慢性丙型肝炎组高于其他2组(P<0.01),但丙肝相关性肝硬化组与丙肝相关性肝癌组患者HCV RNA载量没有明显差别(P>0.05).结论云南地区丙型肝炎中以3b型为主,丙肝相关性肝硬化中以1b型为主,丙肝相关性肝癌中3b型为主.在慢性丙型肝炎进展过程中HCV RNA载量减低.

Estrogen receptor expression in chronic hepatitis C and hepatocellular carcinoma pathogenesis

AIM To investigate gender-specific liver estrogen receptor(ER) expression in normal subjects and patients with hepatitis C virus(HCV)-related cirrhosis and hepatocellular carcinoma(HCC).METHODS Liver tissues from normal donors and patients diagnosed with HCV-related cirrhosis and HCV-related HCC were obtained from the NIH Liver Tissue and Cell Distribution System. The expression of ER subtypes, ERα and ERβ, were evaluated by Western blotting and real-time RT-PCR. The subcellular distribution of ERα and ERβ was further determined in nuclear and cytoplasmic tissue lysates along with the expression ofinflammatory [activated NF-κB and IκB-kinase(IKK)] and oncogenic(cyclin D1) markers by Western blotting and immunohistochemistry. The expression of ERα and ERβ was correlated with the expression of activated NF-κB, activated IKK and cyclin D1 by Spearman's correlation. RESULTS Both ER subtypes were expressed in normal livers but male livers showed significantly higher expression of ERα than females(P < 0.05). We observed significantly higher m RNA expression of ERα in HCV-related HCC liver tissues as compared to normals(P < 0.05) and ERβ in livers of HCV-related cirrhosis and HCV-related HCC subjects(P < 0.05). At the protein level, there was a significantly higher expression of nuclear ERα in livers of HCV-related HCC patients and nuclear ERβ in HCV-related cirrhosis patients as compared to normals(P < 0.05). Furthermore, we observed a significantly higher expression of phosphorylated NF-κB and cyclin D1 in diseased livers(P < 0.05). There was a positive correlation between the expression of nuclear ER subtypes and nuclear cyclin D1 and a negative correlation between cytoplasmic ER subtypes and cytoplasmic phosphorylated IKK in HCV-related HCC livers. These findings suggest that dysregulated expression of ER subtypes following chronic HCVinfection may contribute to the progression of HCVrelated cirrhosis to HCV-related HCC.CONCLUSION Gender differences were observed in ERα expression in normal livers. Alterations in ER subtype expression observed in diseased livers may influence genderrelated disparity in HCV-related pathogenesis.