Biological impacts of 'hot-spot' mutations of hepatitis B virus X proteins are genotype B and C differentiated.

Lin X; Xu X; Huang QL; Liu YQ; Zheng DL; Chen WN; Lin JY

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Biological impacts of 'hot-spot' mutations of hepatitis B virus X proteins are genotype B and C differentiated.

机译：乙型肝炎病毒X蛋白的“热点”突变的生物影响是B型和C型基因区分的。

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AIM: To investigate the biological impacts of "hot-spot" mutations on genotype B and C HBV X proteins (HBx). METHODS: Five types of "hot-spot" mutations of genotype B or C HBV X genes, which sequentially lead to the amino acid substitutions of HBx as I127T, F132Y, K130M+V131I, I127T+K130M+V131I, or K130M+V131I+F132Y, respectively, were generated by means of site-directed mutagenesis. To evaluate the anti-proliferative effects, HBx or related mutants' expression vectors were transfected separately to the Chang cells by lipofectamine, and the cells were cultured in hygromycin selective medium for 14 d, drug-resistant colonies were fixed with cold methanol, stained with Giemsa dyes and scored (increase of the colonies indicated the reduction of the anti-proliferation activity, and vice versa). Different types of HBx expression vectors were co-transfected separately with the reporter plasmid pCMVbeta to Chang cells, which were lysed 48 h post-transfection and the intra-cellular beta-galactosidase activities were monitored (increase of the beta-galactosidase activities indicated the reduction of the transactivation activity, and vice versa). All data obtained were calculated by paired-samples t-test. RESULTS: As compared to standard genotype B HBx, mutants of I127T and I127T+K130M+V131I showed higher transactivation and anti-proliferative activities, while the mutants of F132Y, K130M+V131I, and K130M+V131I+F132Y showed lower activities. As compared to standard genotype C HBx, I127T mutant showed higher transactivation activity, while the other four types of mutants showed no differences. With regard to anti-proliferative activity, compared to standard genotype C HBx, F132Y and K130M+ V131I mutants showed lower activities, and K130M+V131I +F132Y mutant, on the other hand, showed higher activity, while the mutants of I127T and I127T+K130M+V131I showed no differences. CONCLUSION: "Hot-spot" mutations affect the anti-proliferation and transactivation activities of genotype B and/or C HBx, and the biological impacts of most "hot-spot" mutations on HBx are genotype B and C differentiated.

机译：目的：研究“热点”突变对基因型B和C HBV X蛋白（HBx）的生物学影响。方法：基因型B或C HBV X基因的五种“热点”突变，依次导致HBx的氨基酸替换为I127T，F132Y，K130M + V131I，I127T + K130M + V131I或K130M + V131I + F132Y分别通过定点诱变产生。为了评估其抗增殖作用，用lipofectamine将HBx或相关突变体的表达载体分别转染到Chang细胞中，并将细胞在潮霉素选择培养基中培养14 d，用冷甲醇固定耐药菌落，并用Giemsa染色并记分（菌落增加表明抗增殖活性降低，反之亦然）。将不同类型的HBx表达载体与报道质粒pCMVbeta分别共转染到Chang细胞，转染后48 h将其裂解，并监测细胞内β-半乳糖苷酶的活性（β-半乳糖苷酶活性的增加表明其减少了反式激活活性，反之亦然）。通过配对样本t检验计算获得的所有数据。结果：与标准基因型HBx相比，I127T和I127T + K130M + V131I突变体显示更高的反式激活和抗增殖活性，而F132Y，K130M + V131I和K130M + V131I + F132Y突变体显示较低的活性。与标准基因型C HBx相比，I127T突变体显示出更高的反式激活活性，而其他四种类型的突变体则没有差异。关于抗增殖活性，与标准基因型C HBx相比，F132Y和K130M + V131I突变体显示较低的活性，而K130M + V131I + F132Y突变体显示较高的活性，而I127T和I127T + K130M的突变体+ V131I没有显示任何差异。结论：“热点”突变影响基因型B和/或C HBx的抗增殖和反式激活活性，并且大多数“热点”突变对HBx的生物学影响是基因型B和C区分的。

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来源
《World Journal of Gastroenterology》 |2005年第30期|P.4703-4708|共6页
作者
Lin X; Xu X; Huang QL; Liu YQ; Zheng DL; Chen WN; Lin JY;
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作者单位

Research Center of Molecular Medicine, Fujian Medical University, Fuzhou 350004, Fujian Province, China. linxu70@hotmail.com.;

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收录信息美国《科学引文索引》(SCI);美国《工程索引》(EI);美国《生物学医学文摘》(MEDLINE);美国《化学文摘》(CA);
原文格式 PDF
正文语种 eng
中图分类消化系及腹部疾病;
关键词
Genotype; Carbon ion; vice; 基因型;

机译：Genotype;Carbon ion;vice;基因型;

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1. Hepatitis B virus core protein with hot-spot mutations inhibit MxA gene transcription but has no effect on inhibition of virus replication by interferon α [J] . Yu Zhijian, Huang Zhen, Zhang Fan, Virology Journal . 2010,第1期

机译：具有热点突变的乙型肝炎病毒核心蛋白抑制MxA基因转录，但对干扰素α抑制病毒复制没有影响
2. Hepatitis B virus genotypes and hepatitis B surface antigen mutations in family contacts of hepatitis B virus infected patients with occult hepatitis B virus infection. [J] . Kumar GT, Kazim SN, Kumar M, Journal of gastroenterology and hepatology . 2009,第4期

机译：隐性乙型肝炎病毒感染患者的家庭接触中的乙型肝炎病毒基因型和乙型肝炎表面抗原突变。
3. Mutations on S Gene Region of Hepatitis B Virus Genotype D and Biological Significant Analyses of These Mutations [J] . Mehmet Ozaslan, Canan Can, Arzu Barsgan Journal of Medical Sciences . 2006,第1期

机译：乙型肝炎病毒D基因型S基因区域的突变及其生物学意义分析
4. Influence of hepatitis C virus genotypes and F protein on outcome of HCV infection among injection drug users [C] . Yun Zhang, Jingjing Yang, Haopeng Wang, International symposium on pharmacogenomics and the regulation of drug metabolism enzymes and genes. . 2010

机译：丙型肝炎病毒基因型和F蛋白对注射吸毒者HCV感染结局的影响
5. Characterization of structural and functional liver changes in a transgenic mouse model expressing genotype 1a hepatitis C virus core and envelope proteins 1 and 2 [D] . Naas, Turaya 2007

机译：在表达基因型1a丙型肝炎病毒核心和包膜蛋白1和2的转基因小鼠模型中表征结构和功能性肝脏变化
6. Biological impacts of hot-spot mutations of hepatitis B virus X proteins are genotype B and C differentiated [O] . Xu Lin, Xiao Xu, Qing-Ling Huang, 2005

机译：乙型肝炎病毒X蛋白热点突变的生物影响是基因型B和C的区分
7. Biological impacts of 'hot-spot' mutations of hepatitis B virus X proteins are genotype B and C differentiated [O] . Xu X, Lin JY, Chen WN, 2005

机译：乙型肝炎病毒X蛋白“热点”突变的生物学影响是基因型B和C分化

Biological impacts of 'hot-spot' mutations of hepatitis B virus X proteins are genotype B and C differentiated.

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