树Qu实验性肝癌发生过程p53基因的变化

目的探讨由人乙型肝炎病毒(HBV)和黄曲霉毒素B1(AFB1)诱发的树鼩肝细胞癌变过程,p53基因的表达及变化.方法将树鼩分为四组A组HBV+AFB1,B组只感染HBV;C组只摄入AFB1;D组作空白对照.定期肝活检,用免疫组织化学、分子生物学等技术对实验树鼩肝及肿瘤组织进行检测.结果 (1)接受HBV及AFB1双因素的A组,肝细胞癌(HCC)发生率(66.7%)明显高于只接受HBV的B组或AFB1的C组(30%),而且HCC的平均发生时间也明显早于C组,(120.0±16.6)周与(153.3±5.8)周,t=3.336,P＜0.01.(2)在第75周前各组动物肝均未检出突变的p53蛋白.(3)105周时,A组p53蛋白表达率为78.6%,B组为60%,C组为71.4%,D组为10%(x2≥5.03,P＜0.05).在A、C组检出p53基因异常带.(4)树鼩肝癌p53基因突变点分别位于2 7 5、7 8及1 3密码子;其野生型p 5 3基因的核苷酸及氨基酸序列与人的p 5 3基因的核苷酸及氨基酸序列的同源性分别为91.7%、93.4%.结论再次证实HBV和AFB1有协同致肝癌作用;突变的p53蛋白出现于肝细胞发生癌变之前,p 5 3基因的突变促进了肝癌的发生和演进.HBV可能协同AFB1致p 5 3基因突变.     

Expression of IGF- II, p53, p21 and HBxAg in precancerous events of hepatocarcinogenesis induced by AFB1 and/or HBV in tree shrews

INTRODUCTION In order to study the relationship between oncogene expression and HCC generation, we observed the precancerous hepatic GGT foci, IGF-Ⅱ, p53 and p21 expression during hepatocarcinogenesis of tree shrew induced by hepatitis B virus (HBV) and/or aflatoxin B1 (AFB1).     

用树鼩cDNA芯片研究树鼩肝癌中参与信号传导的部分基因变化情况

目的利用树鼩cDNA芯片研究黄曲霉毒素B1（AFBl）和（或）乙型肝炎病毒（HBV）引起的树鼩肝细胞癌（HCC）发生过程中参与信号传导的部分基因表达变化情况，从而进一步探讨HCC发生的分子机制。方法实验树鼩分3组：A组（AFB1组）、B组（AFB1＋HBV组）、C组（正常对照组）。所有动物在实验过程中定期接受剖腹手术取肝组织检查，至肝癌形成时处死动物取肝癌和癌旁组织。用树鼩cDNA芯片检测实验第30、60、90周肝活检组织、肝癌组织及其癌旁组织中各基因的表达情况，并用实时逆转录聚合酶链反应（Real time RT-PCR）法验证cDNA芯片结果。结果在A组和B组从癌前到癌变过程中胰岛素样生长因子-Ⅱ（IGF-Ⅱ）、C-rel、核因子-κB2（NF—κB2）均显示有差异表达，同时bcl-2、细胞周期素A（cyclin A）、睫状神经营养因子（CNTF）仅在B组显示有差异表达。而C组这几个基因无差异表达。实验组与对照组比较，在诱癌的早、中期（30、60周）均出现CNTF及cyclin A的差异表达。realtime RT PCR结果与cDNA芯片检测结果基本一致。A组IGF-Ⅱ、C—rel基因及B组IGF-Ⅱ基因，在肝癌组织表达水平明显低于癌旁及实验30、60周组织，而癌旁与实验30、60周相比较则无明显差异；B组CNTF基因在癌旁、肝癌及60周之间比较无明显改变，但均明显高于30周；A组CNTF基因表达水平在癌旁、肝癌组织高于癌前组织，但差异无统计学意义；C组这3个基因不同时期比较亦无明显差异。结论树目自部分信号传导通路相关cDNA芯片应用于检测树目目HCC发生过程中信号传导通路中各基因表达的变化，对进一步了解树鼠甸HCC发生的机制有重要实用价值。IGF-Ⅱ、NF-κB2、C-rel、Bcl-2、cyclin A及CNTF这几个基因与树HCC的发生发展密切相关。     

Aflatoxin sufferer and p53 gene mutation in hepatocellular carcinoma

Ａｆｌａｔｏｘｉｎｓｕｆｅｒｅｒａｎｄｐ５３ｇｅｎｅｍｕｔａｔｉｏｎｉｎｈｅｐａｔｏｃｅｌｕｌａｒｃａｒｃｉｎｏｍａＤＥＮＧＺｈｕｏＬｉｎａｎｄＭＡＹｕｎＳｕｂｊｅｃｔｈｅａｄｉｎｇｓＡｆｌａｔｏｘｉｎＢ１;ｇｅｎｅｓ,ｐ５３;ｍｕｔａｔｉｏｎ;...     

肝细胞癌肿瘤抑制基因p53过度表达及点突变的研究

目的检测重庆地区肝细胞癌 p53突变发生率,并进一步探讨 p53突变与肝细胞癌临床病理及相关危险因素的关系.方法应用一种敏感的 ARF 免疫组化和 PCR、银染 PCR-SSCP 方法检测本地区38例肝细胞癌(HCC)组织中肿瘤抑制基因p53的过度表达及点突变.结果 16例有P53蛋白过度表达(41.2%),7例有 p53基因249位密码子点突变(18.4%),2例249位密码子外第7外显子点突变.9例 p53基因有突变的肝癌中8例 P53蛋白阳性,两者符合率为88.9%.p53基因蛋白过度表达和点突变与 HCC 分化和转移有关.本组 HCC p53基因突变率与该地区黄曲霉素(AFB1)含量及乙型肝炎病毒(HBV)感染分布一致.结论该结果提示 p53基因突变与 AFB1和 HBV 等环境因素的协同作用有关,其中 AFB1主要与 p53基因249位密码子特异型突变有关,而 HBV 可能在散发型突变中发挥重要作用.     

Geographic characterization of hepatitis virus infections,genotyping of hepatitis B virus,and p53 mutation in hepatocellular carcinoma analyzed by in situ detection of viral genomes from carcinoma tissues: comparison among six different countries

We investigated the relationship of infection with hepatitis B virus (HBV) and hepatitis C virus (HCV) to p53 mutation in hepatocellular carcinomas (HCC) from six countries, including Japan, China, Korea, Vietnam, Spain, and the Unites States. For this purpose, we used formalin-fixed, paraffin-embedded liver tissues obtained from 449 patients with HCC to detect the viral and p53 genes by polymerase chain reaction (PCR). HBV was the most prevalent in Korea (69.1%), China (66.1%), Vietnam (60.5%), and Spain (38.6%). In contrast, HCV was the most prevalent in Japan (59.8%) and in the United States (41.5%). Type C of HBV was the most common genotype (78.6%) encountered in HCC in these countries. Importantly, among 125 intrahepatic HBV DNA-positive patients, 44 (35.2%) were serologically negative for HBsAg (occult hepatitis B). Based on PCR, immunohistochemical, serological, and clinical findings, 4.8% of HCC patients were diagnosed with non-B, non-C. A point mutation at exon 7 of p53 was detected in 20 of the 239 HCC samples examined, including those from 9 Chinese, 5 American, 2 Japanese, 2 Korean, and 2 Spanish patients, respectively. Interestingly, a point mutation with an amino acid substitution at codon 251 (Ile-->Asn) was detected frequently in 11 of 20 (55%) cases. A specific mutation induced by Aflatoxin B1 at codon 249 was seen in two patients, both Chinese. Our results suggest that genotype C of HBV may play an important role in hepatocarcinogenesis in different geographic regions, and that in situ detection of HBV genomes could be important for clarifying the agent(s) of unknown etiology related to HCC.     

Human hepatitis B virus and hepatocellular carcinoma II. Experimental induction of hepatocellular carcinoma in tree shrews exposed to hepatitis B virus and aflatoxin B1

On the basis of the successful establishment of an animal model in tree shrews experimentally infected with human hepatitis B virus (HBV), a study on the hepatocarcinogenic effects of HBV and/or aflatoxin B1 (AFB1) was conducted. The results showed that the incidence of hepatocellular carcinoma (HCC) was significantly higher in the animals both infected with HBV and exposed to AFB1 (52.94%) than in those solely infected with HBV (11.11%) or exposed to AFB1 (12.50%). No HCC of precancerous lesions were found in the controls that were neither HBV-infected nor AFB1-exposed. Precancerous lesions, including liver cell dysplasia and enzyme-altered hyperplastic hepatocyte foci, were observed before the occurrence of HCC, and the frequency of their appearance correlated well with the incidence of HCC. HBV DNA and the protein it encodes were detected in the cancer cells and/or the surrounding hepatocytes. Integration of HBV DNA inot the host liver genome was found during hepatocarcinogenesis among the animals infected by HBV. These results suggest that exposure to HBV and AFB1 may play a synergistic role in the development of HCC, and support the viewpoint of an aetiological relationship between HBV and HCC.Abbreviations HCC hepatocellular carcinoma - HBV human hepatitis B virus - AFB1 aflatoxin B1 - GGT foci hyperplastic hepatocyte foci positive for -glutamyltranspeptidase - LCD liver cell dysplasia     

Aflatoxin B1 induces the transversion of G-->T in codon 249 of the p53 tumor suppressor gene in human hepatocytes.

Approximately half of hepatocellular carcinoma (HCC) from regions in the world with high contamination of food with the mycotoxin aflatoxin B1 (AFB1) contain a mutation in codon 249 of the p53 tumor suppressor gene. The mutation almost exclusively consists of a G-->T transversion in the third position of this codon, resulting in the insertion of serine at position 249 in the mutant protein. To gain insight into the mechanism of formation of this striking mutational hot spot in hepatocarcinogenesis, we studied the mutagenesis of codons 247-250 of p53 by rat liver microsome-activated AFB1 in human HCC cells HepG2 by restriction fragment length polymorphism/polymerase chain reaction genotypic analysis. AFB1 preferentially induced the transversion of G-->T in the third position of codon 249. However, AFB1 also induced G-->T and C-->A transversions into adjacent codons, albeit at lower frequencies. Since the latter mutations are not observed in HCC it follows that both mutability on the DNA level and altered function of the mutant serine 249 p53 protein are responsible for the observed mutational hot spot in p53 in HCC from AFB1-contaminated areas. Our results are in agreement with an etiological role of AFB1 in hepatocarcinogenesis in regions of the world with AFB1-contaminated food.     

肝细胞癌抑癌基因p53突变

目的分析重庆地区肝细胞癌ｐ５３基因突变谱．方法住院肝细胞癌患者２０例，皆经病理证实，长期在重庆地区居住，其中早期小肝癌４例，中期６例，晚期１０例．采用ＰＣＲ－ＳＳＣＰ，ＰＣＲ直接测序技术分析ｐ５３基因５，６，７和８外显子突变．结果ｐ５３基因总的突变率为４０％．其中外显子５和６各占１０％，外显子７占２０％，未发现外显子８的突变；测序证实外显子７为第２４９位密码子Ｇ→Ｔ的颠换突变．突变病例多为晚期肿瘤．结论重庆地区肝细胞癌存在明显的ｐ５３基因突变，反映了该地区肝癌与黄曲霉毒素和ＨＢＶ或ＨＣＶ病毒有关     

Hepatitis B Virus Gene in Liver Tissue Promotes Hepatocellular Carcinoma Development in Chronic Hepatitis C Patients

The hepatitis B virus (HBV) gene has been detected in hepatocellular carcinoma (HCC) tissue negative for the hepatitis B surface antigen and positive for the hepatitis C virus (HCV) antibody, but the precise role of the HBV gene in hepatocarcinogenesis has yet to be clarified. We studied the HBV gene in liver tissue several years before the emergence of HCC. Eleven patients diagnosed with HCV-positive chronic liver disease and who developed HCC were assigned to group A. HBV DNA was detected in 8 of the 11 patients (73%). Twenty-five patients, who did not develop HCC, were selected as group B. Six of the group B patients were classified as DNA-positive (24%). The HBV DNA in liver tissue was found to be significantly related to HCC development (P < 0.01). Thus, the presence of the HBV gene in patients with chronic HCV associated-liver injury appears to promote hepatocarcinogenesis, although prospective studies are needed to confirm this result.     

肝细胞癌基因P53异常的研究

目的：分析我国重庆地区肝细胞癌Ｐ５３基因失活机制及突变谱。方法：采用ＰＣＲ—ＲＦＬＰＰＣＲＳＳＣＰ和ＰＣＲ直接测序技术对来自我国重庆地区２８例肝细胞癌Ｐ５３抑癌基因结构异常进行了分析。结果：６１．５１％的肝癌存在ｐ５３的杂合缺失：５０％肝癌伴有ｐ５３基因突变，其突变模式为突普通散在于５６７和８外显子，其中第７外显子２４９们密友情子突弯率最高（２１％）；具有突变的肝癌多同时伴夺缺失。伴有ｐ５３基因结构异常的肝癌均属进展期。结论：我国重庆地区肝癌存在Ｐ５３基因结构异常，Ｐ５３基因结构异常，ｐ５３基因突变模式反映了该地区肝癌发生可能与肝炎病互和黄贡互素两种因素及其相互作用有关；ｐ５３基因结构异常属肝癌晚期事件，可能参加与肝癌的进展过程。     

Codon 249 mutations of p53 gene in development of hepatocellular carcinoma

Ｃｏｄｏｎ２４９ｍｕｔａｔｉｏｎｓｏｆｐ５３ｇｅｎｅｉｎｄｅｖｅｌｏｐｍｅｎｔｏｆｈｅｐａｔｏｃｅｌｕｌａｒｃａｒｃｉｎｏｍａＰＥＮＧＸｉａｏＭｏｕ,ＰＥＮＧＷｅｎＷｅｉａｎｄＹＡＯＪｉＬｕＳｕｂｊｅｃｔｈｅａｄｉｎｇｓｌｉｖｅｒｎｅｏｐｌａ...     

Hepatic aflatoxin B1‐DNA adducts and TP53 mutations in patients with hepatocellular carcinoma despite low exposure to aflatoxin B1 in southern Japan

Background & aims: Hepatitis B or C virus infection is considered to be the main cause of hepatocellular carcinoma (HCC) in Japan. Aflatoxin B1 (AFB1) is a carcinogen associated with HCC in regions with high exposure. Mutations in codon 249, exon 7 are a hallmark of AFB1 exposure. Therefore, to clarify the role of AFB1 in hepatocarcinogenesis, we examined AFB1‐DNA in liver tissue and sequenced TP53 in Japanese patients with HCC. Methods: Hepatocyte AFB1‐DNA adducts were determined immunohistochemically and direct sequencing of TP53 was done to determine mutations in 188 of 279 patients who underwent hepatic resection for HCC. We assessed hepatitis C virus antibodies (HCV Ab) and HBSAg expression; patients without either were defined as having non‐B non‐C hepatocellular carcinoma (NBNC HCC). Results: AFB1‐DNA adducts were detected in hepatocyte nuclei in 18/279 patients (6%), including13/83 patients (16%) with NBNC HCC and 5/51 patients (10%) expressing hepatitis B surface antigen. None of the patients with HCV Ab (n=136) were positive for AFB1‐DNA. The incidence of the G–T transversion and mutations in exon 7 of TP53 in patients with AFB1‐DNA adducts were significantly higher in patients with than in patients without AFB1‐DNA adducts. All three patients with the codon 249 AGG–AGT mutation had AFB1‐DNA adducts. Conclusion: Although exposure to AFB1 is thought to be low in Japan, it is still associated with hepatocarcinogenesis, particularly in NBNC HCC and hepatitis B individuals.     

原发性肝细胞癌中HBV各基因片段整合与癌基因,抑癌基因表达？…

目的 研究肝细胞癌中ＨＢＶ各基因整合与癌基因、抑制基因表达的关系。方法 以随机引物法制备ＨＢＶ全基因及各基因探针,用Ｓｏｕｔｈｅｒｎ杂交测定ＨＢＶ ＤＮＡ的整合状态,以斑点杂交检查整合型ＨＣＣ中ＨＢＶ各基因的整合,以免疫组织细胞化学方法检查癌基因、抑癌基因的表达。结果 ３２例纯整合型ＨＣ中ＨＢＶ Ｘ．Ｓ．Ｐｅｒ－Ｓ和Ｃ的整合率分别为８７．５％（２８／３２）,６２．５％（２０／３２）,６２．５％（２     

用cDNA阵列技术研究黄曲霉毒素B1诱发树鼩肝癌形成过程中的基因变化

目的 对树鼩肝癌形成过程中的基因表达差异进行动态分析,探讨肝癌发生的分子机制。 方法用cDNA阵列技术,将2例黄曲霉毒素B1诱发的树鼩肝癌组织分别与其癌旁组织和其肝癌形成前的活检肝组织、实验前对照和同期对照肝组织进行基因表达水平的6种比较分析。结果 不同的比较方式所显示的差异表达的基因谱不同,可归为4类:癌组织表达高于癌旁组织、癌旁组织表达高于癌发生前肝的组织;癌与癌旁表达水平相仿,但高于癌发生前的肝组织;癌组织下调,低于癌旁组织;癌发生前表达上调,在癌发生后表达下调。 结论 对肝癌形成过程中不同时期的肝组织基因表达水平进行动态对比分析,有助于阐明肝癌发生的分子机制并最终筛选出与肝癌发生有关的关键基因。     

HBsAg and HBx knocked into the p21 locus causes hepatocellular carcinoma in mice

Hepatocellular carcinoma (HCC) affects males in a significantly higher proportion than females and is one of the human cancers etiologically related to viral factors. Many studies provide strong evidence of the direct role that hepatitis B virus (HBV) plays in hepatic carcinogenesis, but the functions of HBV surface antigen (HBsAg) and X protein (HBx) in hepatocarcinogenesis through direct or indirect mechanisms are still being debated. We generated two HBV gene knock-in transgenic mouse lines by homologous recombination. HBsAg and HBx genes were integrated into the mouse p21 locus. Both male and female p21-HBx transgenic mice developed HCC after the age of 18 months; however, male p21-HBsAg transgenic mice began to develop HCC 3 months earlier. The expression of a number of genes related to metabolism and genomic instability largely resembled the molecular changes during the development of HCC in humans. ER-beta (estrogen receptor-beta) was extremely up-regulated only in tumor tissues of male p21-HBsAg mice, providing genetic evidence that HBsAg might be the major risk factor affecting the gender difference in the causes of HCC. In conclusion, these mice might serve as good models for studying the different roles of HBsAg and HBx in early events of HBV-related hepatocarcinogenesis.     

PeroxiredoxinⅡ基因在肝癌组织中的表达及意义

目的观察peroxiredoxinⅡ（PrxⅡ）mRNA和蛋白在黄曲霉毒素B1（AFB1）诱发树鼩HCC形成过程中的表达变化,并在人肝癌癌旁组织和正常肝组织中进行验证,以探讨PrxⅡ在肝癌形成过程中的作用。方法应用RT-PCR和Western blot方法,检测6例AFB1诱发的树鼩肝癌、癌旁组织和这些动物肝癌发生前的活检肝组织,以及6例对照组动物相应时期的肝活检组织PrxⅡ在mRNA水平和蛋白水平的表达情况,并在18例人肝癌及其相应癌旁组织以及17名正常人肝组织进行验证。结果PrxⅡ在树鼩肝癌组织中的mRNA和蛋白质表达水平均明显高于相应的癌旁和癌前组织,也高于对照组同期活检肝组织（P〈0．05）;人肝癌组织中PrxⅡ的mRNA和蛋白表达改变和树鼩相符,即肝癌中的表达高于癌旁组织和正常肝组织（P〈0．05）。结论PrxⅡ基因可能与肝癌的发生发展有关,并有可能成为防治肝癌的分子靶标。     

Hepatic expression of the proliferative marker Ki-67 and p53 protein in HBV or HCV cirrhosis in relation to dysplastic liver cell changes and hepatocellular carcinoma

To evaluate hepatic expression of the nuclear proliferative marker Ki-67 and the p53 oncoprotein in hepatitis B virus (HBV)/HCV cirrhosis in relation to dysplastic liver cell changes and hepatocellular carcinoma (HCC). We studied needle liver biopsies from 107 patients with cirrhosis and no HCC (52 HBV, 55 HCV) who had been assessed for protocol studies, and 57 cirrhotic patients with HCC (40 HBV, 17 HCV). We evaluated small and large cell dysplastic changes along with the expression of Ki-67 and p53 by immunohistochemistry. The labelling index (LI) was defined as the proportion (%) of positive-stained nuclei of the 500 measured. Large and small cell dysplastic changes were observed in 12 and 9% of specimens respectively. Only small cell changes were associated with Ki-67 expression. Ki-67 LI was 5.50 +/- 5.7 in cirrhosis (13.90 +/- 3.84 in those with small cell dysplastic changes vs 4.64 +/- 4.98 in those without, P < 0.01), 10.2 +/- 5.95 in cirrhosis with HCC (P < 0.05) and 18.56 +/- 10 in HCC (P < 0.01). Neither the presence of small cell dysplastic changes nor the expression of Ki-67 was related to severity or aetiology of cirrhosis. Expression of p53 was observed in 30% of the non-tumorous and in 53% of the neoplastic tissue obtained from patients with HCC, with no differences between HCV and HBV. Ki-67 and p53 expression was associated with the tumour grade (P < 0.001). Our observations clearly demonstrate the association between the proliferation activity and the morphological changes in the cirrhotic liver from the non-dysplastic to dysplastic lesion to HCC. They also support the hypothesis that p53 alterations are a rather late event in carcinogenesis and related to HCC grade. And finally, they suggest that the final steps of hepatocarcinogenesis are common and independent of the aetiology of the chronic viral infection.