肝细胞癌变过程中cyclin D_1的异常表达与端粒酶活性的相关分析及意义

目的:探讨肝细胞癌变过程中 cyclin D_1的异常表达与端粒酶活性之间的关系及其意义.方法:用0.5g/L 的2-AAF 诱导 Wistar 大鼠建立肝癌动物模型,应用原位杂交法和 PCR-TRAP-ELISA 法检测大鼠肝脏在癌变过程中 cyclin D_1的异常表达和端粒酶的活性.结果:正常组8例中 cyclin D_1表达均正常,端粒酶均阴性肝硬化组16例中有12例 cyclin D_1过表达,有4例 cyclinD_1表达正常;有9例端粒酶阳性,有7例端粒酶阴性.肝癌组11例中有4例 cyclin D_1过表达,有7例 cyclin D_1表达正常;有10例端粒酶阳性,有1例端粒酶阴性.结论:肝硬化组和肝癌组的 cyclin D_1异常表达、端粒酶活性均高于正常组,而且肝硬化组的 cyclin D_1异常表达与端粒酶活性呈正相关,肝癌组的 cyclin D_1异常表达与端粒酶活性呈负相关.

Ras蛋白与肝细胞癌变过程中的信号转导

细胞信号转导(signal transduction)是指胞间通讯的激素以及外界环境因子作用于细胞表面(或胞内受体),跨膜形成胞内第二信使,通过信息分子级联传递,诱导基因表达和引起生理反应的过程。细胞信号转导在应答环境因素和调节基因表达、生理反应的同时,不仅维持着细胞的正常代谢,而且最终决定了细胞增殖、生长、分化、衰老和死亡等生命的基本现象。 肝细胞癌变的主要特征是肝细胞异常增殖,癌基因的激活和抑癌基因失活是引起肝细胞癌变的原因,而癌基因和抑癌基因的变异引起细胞内信号转导途径异常激活则是肝细胞癌变的主要机制之一。 RasP21是肝细胞增殖信号传导的关键因子。

腺苷脱氨酶在鼠肝细胞癌变过程中的表达与动态改变

本文以化学致癌剂2-FAA喂饲SD大鼠，对鼠肝细胞在癌变过程中的组织学改变、腺苷脱氨酶(ADA)的表达和动态变化进行了研究。结果表明：当肝细胞轻度损伤时，肝组织ADA的释放就可以引起血ADA的显著增加，第2周时血清ADA活性明显高了对照组（P<0．001)，且出现异常时较谷丙转氨酶(ALT)早；当肝细胞表现为癌前病变时，血及肝组织中ADA活性仍然明显异常；在肝细胞完全癌变时，肝中ADA比活性仍较高，而血中ADA和ALT活性巳都降至较低水平；在诱癌过程中ADA的动力学常数术发生改变。研究资料提示，血清ADA为反映肝细胞损伤很灵敏的标志酶。

肝细胞癌变过程中Wnt3a过表达及其早期监测价值

目的以肝癌发生模型探讨癌胚型Wnt3a动态表达规律及其早期监测价值。方法Sprague-Dawley(SD)鼠48只,以含2-乙酰氨基芴(2-FAA,0.05%)颗粒饲料喂养,诱发肝癌发生,对照鼠以颗粒饲料喂养,每隔2周留取肝组织和血液;肝组织经HE染色病理学检查并分组。以全基因组芯片分析基因和Wnt3a mRNA表达情况,以免疫组织化学分析Wnt3a在肝组织的表达分布情况,以酶联免疫吸附法定量肝组织和血清Wnt3a浓度。采用χ2检验、Mann-Whitney检验和方差分析等统计学方法分析组间差异。结果依据病理学检查,将鼠肝分为对照、肝细胞变性、癌前病变和肝癌形成4组。全基因表达谱分析并与对照组比较,在信号对数比率(SLR)>8 log2cy5/cy3时,癌前组和癌变组分别有268个、312个基因上调,57个、201个基因下调,这些显著改变的基因主要涉及细胞增殖、信号转导、肿瘤转移、细胞凋亡等。诱癌各阶段Wnt3a在mRNA水平表达增加,变性组(1.15±0.24,q=8.227)、癌前组(1.85±0.18,q=12.361)和肝癌组(2.59±0.55,q=18.082)均显著高于对照组(0.25±0.11,F=121.103,P<0.001),变性组、癌前组和肝癌组分别上调4.6倍、7.4倍和10.4倍。免疫组织化学显示Wnt3a表达与对照组比较,变性组阳性率为66.7%(12/18,χ2=10.701,P=0.001)。癌前组和肝癌组均全数阳性(9/9,χ2=17.115,P<0.001)。癌变过程中肝及血中Wnt3a呈进行表达增加,组间差异有统计学意义(F肝=176.711,P<0.001);癌变肝组织表达的Wnt3a分泌入血,血与肝Wnt3a水平呈直线相关(r=0.732,P<0.001)。结论Wnt3a过表达与肝细胞癌变密切相关,有望成为监测肝细胞癌变新标志物。

超声造影对非肝细胞癌肝脏局灶性病变的诊断价值

目的探讨超声造影(CEUS)对非肝细胞癌肝脏局灶性病变的诊断价值。方法对1753例行CEUS的非肝细胞癌肝脏局灶性病变患者的超声造影进行回顾分析,将超声造影结果与诊断金标准对比,评价CEUS对非肝细胞癌肝脏局灶性病变良恶性及病灶类型区分的诊断价值。结果 1753病例中,良性病灶1318个、CEUS正确诊断92.94%(1225/1318);恶性病灶435个,CEUS正确诊断88.74%(386/435);CEUS对非肝细胞癌肝脏局灶性恶性病变诊断的敏感度为88.74%(386/435),特异度为92.94%(1225/1318),准确率为91.90%(1611/1753),阳性预测值为80.58.7%(386/479),阴性预测值为96.15%(1225/1274)。CEUS对不同病灶病理类型诊断的准确率:血管瘤97.41%(640/657)、局灶性脂肪变96.43%(216/224)、MLC 84.81%(268/316)、FNH85.55%(225/263)、炎性病变(包括肝脓肿)58.82%(40/68)、RN 57.14%(28/49)、DN 12.50%(2/16)。结论 CEUS对非肝细胞癌肝脏局灶性病变的良恶性鉴别诊断有较高的价值,但对病种类型的定性诊断准确率有待提高。

人肝癌细胞诱导分化的体外研究

事实证明:去分化的恶性肿瘤细胞可以在分化诱导剂的作用下向正常方向逆转而成为分化细胞。这一发现开辟了肿瘤治疗的新纪元,因过去的手术、化疗、放疗和一部分生物治疗都要损伤正常细胞,而用分化诱导剂来治疗肿瘤则是一种“

肥胖通过不同机制导致脂肪性肝炎和肝细胞癌

非酒精性脂肪性肝病(NAFLD)是肥胖和代谢综合征累及肝脏的病理表现,疾病谱包括单纯性脂肪肝(NAFL)、非酒精性脂肪性肝炎(NASH)及其相关肝纤维化、肝硬化和肝细胞癌(HCC)。随着肥胖在全球的流行,NAFLD已成为全球第一大慢性肝脏疾病,普通成人和肥胖患者NAFLD患病率分别高达25%和50%,肥胖症显著增加NAFLD患者肝硬化和HCC发病风险[1-2]。临床上,90%以上的丙型肝炎相关HCC和酒精性肝病相关HCC发生在肝硬化的基础上,肝炎、肝硬化、HCC是慢性肝病患者经典的三步曲。在NAFLD的漫长病程中慢性炎症(NASH)引起肝组织损伤并随之启动肝脏的修复反应,从而形成肝细胞死亡、再生与星状细胞活化增殖、肝纤维化肝硬化发生的恶性循环,进而发生HCC前体细胞的恶性转化及肝细胞癌变。NASH现已成为美国成人失代偿期肝硬化和HCC愈来愈重要的原因[1-2]。然而,NASH及其相关肝纤维化肝硬化并不是NAFLD患者发生HCC的前提条件,相当比例的HCC发生在没有肝硬化甚至没有明显肝纤维化或NASH的NAFLD患者。最近一项包括19项研究的荟萃分析显示,HCC在非肝硬化NAFLD患者中的检出率高达38.0%以上[3]。肥胖群体在并无NASH和(或)明显肝纤维化肝硬化的情况下发生HCC的机制至今尚未完全阐明[4]。

年轻成年慢性乙型肝炎病毒感染患者无肝硬化的肝细胞性肝癌

Background. The aims of this study were to define the clinical characteristics of hepatitis B virus (HBV)-related hepatocellular carcinoma (HCC) in young adult patients without cirrhosis and to evaluate the efficacy of interferon (IFN) therapy on HCC recurrence. Methods. Of 187 patients with HBV-related HCC treated at our hospital, 4 had no liver cirrhosis and were less than 30 years of age (10, 22, 23, and 26 years). Results. At the time of diagnosis of HCC, all cases had antibody to hepatitis Be antigen (anti-HBe) and histological staging of nontumorous liver was F0 or F1, i.e., low-grade hepatitis. The mothers of all 4 young adult patients with HCC had HBV-related liver disease. Three cases developed recurrence of HCC. In these patients, long-term intermittent IFN therapy after reresection of HCC resulted in long-term survival without recurrence for more than 3 years of follow-up. Conclusions. (1) Young adult patients with HCC are positive for anti-HBe, lack cirrhosis,and the route of infection seems to be mother-to-infant transmission.Transplacental transmission of HBV and HBV DNA integration into the cellular genomic DNA during fetal life is a possible explanation of HBV-related hepatocarcinogenesis in young adults; and (2) long-term IFN therapy seems to be useful for prevention of tumor recurrence after radical operation for HBV-related HCC.

肝细胞性肝癌细胞因子信号1抑制因子基因的甲基化状态

Background. Silencing of the suppressor of cytokine signaling(SOCS-1) by aberrant methylation at the CpG island in the coding region gene has been reported in hepatocellular carcinoma(HCC). However, principally, it is methylation in the 5-noncoding region but not that in the coding region which determines the regulation of gene expression. Methods. Methylation-specific PCR was performed for the analysis of methylation status both in the 5-noncoding region and the CpG island of SOCS-1 from 22 HCC tissue samples with adjacent non-HCC tissue samples and from two cell lines. Results. Using primers in the CpG island, 9 of 22 HCC samples exhibited aberrant methylation of SOCS-1, while only 1 of 22 adjacent non-HCC samples did so.The unmethylation pattern was detected in 1 of 22 HCC and in 5 of 22 non-HCC samples. Thus, aberrant methylation of SOCS-1 was significantly associated with HCC (P = 0.0076 by Fisher s exact test). Using primers in the 5-noncoding region,aberrant methylation was observed in 12 of 22 HCC and in 2 non-HCC samples. The unmethylated pattern was observed in 5 of 22 HCC and in 10 of 22 non-HCC samples (P = 0.0042). There was no significant correlation between the methylation status of SOCS-1 and clinicopathological findings, such as the presence or absence of cirrhosis or the histological grade of HCC. Conclusions. Aberrant methylation of the SOCS-1 had a significant correlation with HCC. The rate of aberrant methylation was similar in the 5-noncoding region and in the CpG island. Aberrant methylation of SOCS-1 may be associated with hepatocarcinogenesis, although further studies are necessary.

慢性肝炎、肝硬化及肝细胞性肝癌中间隙连接蛋白Cx32的表达

Background. The gap junction (GJ) plays important roles in the maintenance of tissue homeostasis, the control of cell growth and differentiation, and the prevention of experimental hepatocarcinogenesis. In this study, we examined the relationship between the expression of the GJ protein connexin (Cx) 32 in 24 human hepatocellular carcinomas (HCCs) and 29 non carcinomatous liver specimens (NCLs) of 31 patients. Methods. An immunohistochemical study of Cx32 was done in 24 HCCs and 29 NCLs from 31 patients who had undergone hepatic resection. Results. The Cx32 expression decreased gradually as the disease progressed to cirrhosis and HCC. In all Cx32 positive HCCs, the expression was mostly recognized in cytoplasm, not only on the cell membrane. This internalization of Cx32 was also recognized in liver specimens showing hepatitis and cirrhosis, although it was less frequent than in the HCCs. Conclusions. These findings suggest the possibility that changes in both the amount and the distribution of Cx32 may be implicated in human hepatocarcinogenesis.

二乙基亚硝胺对大白鼠肝脏的影响——肝癌模型的建立及癌变过程

本实验采用口喂二乙基亚硝胺(DEN)诱发大白鼠肝癌,在肝癌模型建立过程中观察其癌变过程和肝癌组织的结构特点。1.口喂DEN诱发肝癌,在总剂量达96.1±1.61毫克至185±0毫克;致癌日期90±1.73天至195±0天时可使体重146±25.8克雄性大白鼠全部获得肝细胞肝癌。2.口喂DEN总剂量达96.1±1.61毫克,致癌日期90±1.73天可获得A型(嗜酸性)肝癌组织;总剂量达123±2.35毫克,致癌日数123±3.81天起可获得B型(嗜硷性)、A型和M型(混合型)三型肝癌组织与肝癌的转移材料。3.采用PAS反应法,在显微镜下很易鉴别增生结节和肝癌结节,因前者呈强阳性而后者呈阴性。在某些增生结节与肝癌结节中均存在一些PAS反应呈弱阳性的肝细胞(或肝癌细胞)。4.肝细胞癌变过程中的特点是糖原下降最后消失,嗜硷性物质(核糖核酸)和去氧核糖核酸增加。

TGF-β_1及其Ⅱ型受体在原发性肝癌中表达的研究

目的 探讨原发性肝癌中转化生长因子β1 (TGF β1 )与其Ⅱ型受体的表达及其价值。方法 采用免疫组化技术对50例原发性肝癌、50例癌旁组织、20 例正常肝组织TGF β1 及其Ⅱ型受体表达进行检测,结合临床资料进行分析。结果 TGF β1 在癌旁组织的表达要高于癌组织,TGF β1RⅡ在肝癌组织的表达明显低于正常组织;TGF β1 在有转移的肝癌组织中的表达明显增高(P<0.01),而TGF β1RⅡ的表达在分化高、肿瘤小、转移少、复发间隔时间长的肝癌组织均较高(P<0.05)。结论 TGF β1 在原发性肝癌中表达异常增高,其高表达有利于肿瘤细胞的浸润转移;TGF β1RⅡ在肝癌组织表达降低,导致肝癌细胞负性调控障碍,这可能是肝细胞癌变的重要因素之一;TGF β1RⅡ的表达与肝癌的恶性进展成负相关,有潜在的治疗肝癌意义。

中医药与自杀基因疗法结合治疗肝癌的思路

肝癌的发生和演进是典型的多因素（肝炎病毒慢性感染％黄曲霉素AFB1暴露，过量饮酒和遗传性肝病肝硬化等）多基因和多阶段、多途径（Rb、p53和Wnt途径等）的复杂过程，是遗传与环境因素相互作用的结果，其中因遗传学、表遗传学改变引起的原癌基因的活化和抑癌基因的灭活，是癌变的中心生物学过程。肝细胞癌变到形成肝肿瘤的发生是一个多阶段、多步骤、

肝癌疫苗的研究现状和进展

近些年来,肝癌疫苗备受关注,已成为肝癌免疫治疗的研究热点之一。运用肝癌细胞、肝癌抗原、树突状细胞及核酸等为基础构建的肝癌疫苗,通过激发机体的免疫系统,诱导机体产生针对肝癌特异性抗原的免疫应答,达到杀灭表达肝癌抗原的肿瘤细胞而产生抗肿瘤效应的目的。通过临床试验发现,肝癌疫苗可减少肝癌的复发转移、改善患者生存质量以及延长存活时间,已成为肝癌综合治疗的重要部分。