Q-T和Q-P工艺对Fe-C-B合金组织与性能的影响

为了获得综合性能好、成本低的耐磨钢,分别采用淬火-回火(Q-T)和淬火-分配(Q-P)工艺对Fe-C-B合金进行热处理。结果表明,相较于Q-T工艺,Q-P工艺处理后的试样综合性能更加优异。采用Q-T工艺处理后合金的冲击韧性提升了18.9%,而采用Q-P工艺处理后的合金,获得了板条马氏体和薄片状残余奥氏体组成的基体,薄片状的残余奥氏体对于提升Fe-C-B合金的冲击性能产生了重要效果,使该合金的冲击性能提升了50.9%。

血清CysC、hs-cTnT、BNP水平变化与慢性心力衰竭患者NYHA分级的关系及临床意义

目的:探讨血清CysC、hs-cTnT、BNP水平变化与慢性心力衰竭患者NYHA分级的关系及临床意义。方法:选取2020年3月-2022年3月我院收治的慢性心力衰竭患者145例作为观察组,根据NYHA心功能分级将其分为Ⅱ级36例、Ⅲ级71例、IV级38例;并选择同期健康体检志愿者95例作为对照组。检测并比较观察组、对照组及不同心功能分级患者血清CysC、hs-cTnT、BNP水平,并分析血清CysC、hs-cTnT、BNP水平与NYHA分级的相关性。结果:与对照组相比,观察组血清CysC、hs-cTnT、BNP水平较高;血清CysC、hs-cTnT、BNP水平与慢性心力衰竭患者NYHA分级呈正相关关系;心功能ⅡI级、Ⅲ级、IV级患者血清CysC、hs-cTnT、BNP水平呈依次升高趋势,且任意两组间经比较,差异有统计学意义(P<0.05)。结论:血清CysC、hs-cTnT、BNP水平升高可增加慢性心力衰竭的发病风险,其水平变化与慢性心力衰竭患者的NYHA分级存在显著的相关性,可反映患者病情的严重程度和心功能的改善情况,为临床诊断及后续治疗提供一定的参考依据。

C-B样条曲线与T-B样条曲线的G^1拼接

在对T-B样条基函数及曲线端点特性分析的基础上提出了n+1阶T-B样条基函数表达式及求解方法.给出了C-B样条曲线与T-B样条曲线的G1拼接条件.在这种条件下,当C-B样条曲线和T-B样条曲线拼接时,可增加控制顶点使C-B样条曲线通过控制多边形的首末顶点,并与首末边相切.并给出应用实例,即利用T-B样条曲线能精确表示半椭圆弧(半圆弧)的特点,与C-B样条曲线进行G1拼接,从而解决了C-B样条曲面造型中无法精确表示半椭圆弧(半圆弧)的问题.

HIV合并HBV/HCV感染患者外周血T细胞亚群的变迁

目的了解HIV合并HBV、HCV感染患者外周血T细胞亚群的变化特征,探讨HIV合并HBV和HCV感染后患者的免疫功能。方法采用三色流式细胞学检测技术,对26例HIV合并HBV和HCV感染患者(合并感染组)、35例单纯HIV感染患者(单纯感染组)和194例健康人群(健康对照组)外周血总T细胞、T4细胞、T8细胞含量进行测定并计算T4/T8比值。结果单纯感染组患者外周血总T细胞、T4细胞、T8细胞的百分含量和T4/T8比值分别为66.42±4.11、27.74±2.34、47.72±3.86和0.74±0.19,合并感染组分别为54.76±3.42、22.31±1.87、58.23±4.62和0.33±0.12,健康对照组值分别为69.98±5.79、35.25±5.16、25.08±4.34和1.45±0.28单纯感染组患者T4细胞和T4/T8比值明显低于健康对照组(P<0.05,P<0.01),T8细胞较对照组明显升高(P<0.05);合并感染组总T细胞、T4细胞和T4/T8比值明显低于健康对照组和单纯感染组(P<0.05,P<0.01),T8细胞较健康对照组和单纯感染组明显升高(P<0.05,P<0.01)。结论 HIV感染患者合并HBV和HCV感染将进一步加重体内免疫功能的紊乱;检测外周血T细胞亚群有利于HIV、HBV和HCV多重感染患者的鉴别诊断、病情监测以及预后判断,是一项十分有效的客观依据。

不同猪种背肌中Cst B基因的表达研究

[目的]研究Cst B基因在大白猪、野猪及野家杂交猪背肌组织中表达情况。[方法]采用RT-PCR技术对试验猪只进行检测,探索Cst B基因在大白猪、野猪及野家杂交猪背肌组织中表达情况。[结果]背肌中Cst B基因的表达在90日龄的野家杂种猪表达量最高,其他个体相对较均衡。[结论]从蛋白酶水解的角度来说,90日龄的野家杂种猪利用背肌制作的火腿品质高于大白猪。

人类免疫缺陷病毒-1B和C亚型Nef蛋白特异性CD8^+ T细胞交叉应答反应的研究

目的:探讨中国人群人类免疫缺陷病毒-1B(H IV-1B亚型)Nef蛋白特异性CD8+T细胞应答在B、C亚型间的交叉反应性。方法:选取51例H IV-1B亚型感染者,采取外周血单个核细胞(PBMC),用合成的54个H IV-1B、C亚型Nef全基因序列肽库作为抗原,酶联免疫斑点吸附试验(ELISpot)方法检测H IV-1B亚型Nef蛋白特异性CD8+T细胞对B、C亚型抗原的应答反应。结果:在产生特异性应答效应的个体中,82.9%(29/35)感染个体同时识别B和C亚型肽段。感染个体在对两个亚型肽段的识别数量及应答强度上无显著差异(P=0.529和P=0.754)。H IV-1B亚型特异性CD8+T细胞能针对70.4%无论B还是C亚型的Nef肽段产生应答反应。被特异性CD8+T细胞同时识别的B、C亚型Nef肽段间氨基酸序列的同源性显著高于仅能被识别的B亚型或C亚型肽段的氨基酸序列(P=0.01)。结论:H IV-1B亚型Nef蛋白特异性CD8+T细胞应答在B、C亚型间具有良好的交叉反应性,能产生交叉反应的氨基酸序列具有较高的亚型间同源性。

联合检测肌钙蛋白T、高敏C反应蛋白和B型钠尿肽对非ST段抬高的急性冠状动脉综合征预后诊断的价值

目的探讨联合检测肌钙蛋白T、高敏C反应蛋白、B型钠尿肽对非ST段抬高的急性冠状动脉综合征预后诊断的价值。方法检测145例经冠状动脉造影证实的非ST段抬高的急性冠状动脉综合征患者肌钙蛋白T、高敏C反应蛋白、B型钠尿肽的水平。随访急性冠状动脉综合征患者12个月,观察终点为心肌梗死新发或再发和心源性死亡。结果多因素Logistic回归分析发现肌钙蛋白T、高敏C反应蛋白、B型钠尿肽可独立预测非ST段抬高急性冠状动脉综合征患者远期预后。经过已知的临床危险因素校正后,心脏生化标志物异常的数目仍然是其心血管事件重要危险因子。结论联合检测肌钙蛋白T、高敏C反应蛋白、B型钠尿肽对急性冠状动脉综合征患者长期预后有重要的临床价值。

两类G_t^s(a,b;c,d)图的着色

在综述国内外关于广义多边形树Gst(a,b;c,d)着色研究的基础上,对一些广义多边形树Gst(a,b;c,d)(s+t=2)组成的图类2ξ(a,b;c,d)的着色、色唯一和色等价类等相关问题进行了研究,得到了两类特殊图2ξ(m,m;m,m)(m≥2)和2ξ(a,a;b,b)(a≠b)且min{a,b}≥2是两个色等价类的结论.

肝癌组织、癌旁组织中HBsAg、HCV抗原表达与T细胞亚群及NK活性的相关性研究

研究肝癌组织、癌旁组织中HBsAg、HCV抗原表达与T细胞亚群及NK活性的相关性。采用免疫组织化学方法(SP法)对肝癌组织及癌旁组织中的HBsAg、HCV抗原表达进行了标记和分析,同时对外周血T细胞亚群及 NK活性进行检测。肝癌患者中,CD4+细胞减少,CD8+细胞升高,CD4+／CD8+比值及NK细胞的活性均比正常对照组明显降低,且HBsAg阳性、HCV抗原阳性者比阴性者下降更显著。肝癌组织、癌旁组织中HBsAg、HCV抗原表达与外周血T细胞亚群及NK活性Spearman相关性分析,与NK细胞、CD4+细胞、CD8+细胞、CD4+／CD8+相关系数分别为-0．67,-0．28,0．35,-0．50(P<0．001)。肝癌患者出现免疫紊乱与乙肝、丙肝病毒感染有关,且混合感染者免疫功能紊乱较显著,提示抗病毒治疗可能改善肝癌患者的免疫功能。

HIV/AIDS合并HBV/HCV感染病毒载量水平及与T淋巴细胞相关性的探讨

目的探讨人类免疫缺陷病毒(HIV)/艾滋病(AIDS)合并乙型肝炎病毒(HBV)/丙型肝炎病毒(HCV)感染后病毒载量水平变化及对机体T淋巴细胞免疫机制的影响。方法分别测定HIV/AIDS单纯感染组,HIV/HBV合并感染组,HIV/HCV合并感染组3组的HIV RNA、HBV DNA、HCV RNA、CD4+T淋巴细胞频数、CD8+T淋巴细胞频数、CD4/CD8比值,并分析各组T淋巴细胞与HIV RNA的关系,HBV DNA/HCV RNA与HIV RNA、CD4+T淋巴细胞、CD8+T淋巴细胞、CD4/CD8比值的相关性。结果 HIV/AIDS单纯感染组、HIV/HBV合并感染组及HIV/HCV合并感染组的CD4+T淋巴细胞与各自组的HIV RNA呈负相关,差异有统计学意义(P<0.05);HIV/AIDS单纯感染组、HIV/HBV合并感染组的CD8+T淋巴细胞与各自组的HIV RNA呈负相关,差异有统计学意义(P<0.05);HIV/AIDS单纯感染组、HIV/HBV合并感染组及HIV/HCV合并感染组的CD4/CD8与各自组的HIV RNA呈负相关,差异有统计学意义(P<0.05)。结论合并感染HBV后,HIV/AIDS患者T细胞的数量下降更明显,致HIV RNA、HBV DNA高载量,加速了HIV病情进展;感染HBV后CD4+T细胞的数量下降比感染HCV更明显。

血清hs-cTnT和BNP在维持性血液透析患者左室舒张功能障碍中的预测价值

目的探讨维持性血液透析(MHD)患者血清超敏肌钙蛋白T(hs-c TnT)和B型脑钠肽(BNP)与左室舒张功能参数E/e’的相关性,以期评价血清hs-c TnT与BNP预测左室舒张功能障碍(LVDD)的敏感性和特异性。方法收集2017年10月—2018年9月在上海交通大学医学院附属同仁医院血液净化中心维持性血液透析且年龄≥55岁的124例患者临床资料、心脏超声参数,包括左室质量指数(LVMI)、左室射血分数(LVEF)和E/e’。E/e’>15作为评价LVDD的标准。电化学法检测周中透析前血清hs-c TnT和BNP水平。Spearman相关分析评估血清hs-c TnT和BNP与超声心动图各参数间的相关性;多因素Logistic回归分析评估血清hs-c TnT和BNP与LVDD的相关性;受试者工作特征曲线(ROC)评价血清hs-c TnT和BNP用于预测LVDD的敏感性和特异性。结果 124例患者,LVDD组(E/e’>15)54例(43.5%),非LVDD组(E/e’≤15)70例(56.5%)。LVDD组血清hs-c TnT和BNP水平高于非LVDD组(P<0.001);Spearman相关分析显示血清hs-c TnT(r=0.756,P<0.001)及BNP(r=0.638,P<0.001)与E/e’正相关;而与LVEF无关(hs-c TnT:r=-0.048,P=0.459;BNP:r=-0.073,P=0.392);多因素回归分析显示,血清hs-c TnT和BNP均与LVDD独立相关,校正透析龄、血压、合并症及LVMI等因素后,hs-c TnT每升高1 ln pg/mL,LVDD风险增加5.5倍(P <0.001),BNP每升高1 ln pg/mL,LVDD风险增加2.1倍(P<0.001);血清hs-c TnT预测LVDD的ROC曲线下面积(AUC)为0.876,最佳临界值为47.4 pg/mL(敏感性为82.8%,特异性为76.7%),血清BNP预测LVDD的ROC曲线下面积为0.732,最佳临界值为392 pg/mL(敏感性为73.5%,特异性为62.4%)。结论血清hs-c TnT和BNP均与MHD患者LVDD独立相关;且血清hs-c TnT对MHD患者LVDD的预测价值优于血清BNP。

Clinical characteristics and current management of hepatitis B and C in China

AIM: To describe a population of outpatients in China infected by hepatitis B virus (HBV) and/or hepatitis C virus (HCV), and assess their current management status. METHODS: A multicenter, cross-sectional study of HBV- and/or HCV-infected patients was conducted from August to November, 2011 in western China. Patients >= 18 years of age with HBV and/or HCV infections who visited outpatient departments at 10 hospitals were evaluated, whether treated or not. Data were collected on the day of visit from medical records and patient interviews. RESULTS: A total 4010 outpatients were analyzed, including 2562 HBV- infected and 1406 HCV-infected and 42 HBV/HCV co-infected patients. The median duration of documented infection was 7.5 years in HBV- infected and 1.8 years in HCV-infected patients. Cirrhosis was the most frequent hepatic complication (12.2%), appearing in one-third of patients within 3 years prior to or at diagnosis. The HCV genotype was determined in only 10% of HCV-infected patients. Biopsy data were only available for 54 patients (1.3%). Antiviral medications had been received by 58.2% of patients with HBV infection and 66.6% with HCV infection. Nucleos(t) ide analogs were the major antiviral medications prescribed for HBV- infected patients (most commonly adefovir dipivoxil and lamivudine). Ribavirin + pegylated interferon was prescribed for two-thirds of HCV-infected patients. In the previous 12 mo, around one-fifth patients had been hospitalized due to HBV or HCV infection. CONCLUSION: This observational, real-life study has identified some gaps between clinical practice and guideline recommendations in China. To achieve better health outcomes, several improvements, such as disease monitoring and optimizing antiviral regimens, should be made to improve disease management. (C) 2014 Baishideng Publishing Group Inc. All rights reserved.

C.B.T.三菌混合发酵益生菌酸奶发酵基本特性研究

利用酪乳杆菌干酪亚种,德氏乳杆菌保加利亚种和嗜热链球菌三菌混合发酵制作风味独特的酸奶。实验结果表明,在干酪乳杆菌接种量为10%,种子酸度为1000T,混合发酵温度为38℃,发酵4.5-5h后能获得风味自然独特,口感良好,后酸不强的益生菌酸牛奶。

CD4^+CXCR5^+ T cells activate CD27^+IgG^+ B cells via IL-21 in patients with hepatitis C virus infection

BACKGROUND： Chronic hepatitis C virus （HCV） infection causes the skewing and activation of B cell subsets, but the characteristics of IgG＋ B cells in patients with chronic hepa- titis C （CHC） infection have not been thoroughly elucidated. CD4＋CXCR5＋ follicular helper T （Tfh） cells, via interleukin （IL）-21 secretion, activate B cells. However, the role of CD4＋CXCR5＋ T cells in the activation ofIgG＋ B cells in CHC patients is not clear. METHODS： The frequency of IgG＋ B cells, including CD27-IgG＋ B and CD27＋IgG＋ B cells, the expression of the activation markers （CD86 and CD95） in IgG＋ B cells, and the percentage of circu- lating CD4＋CXCR5＋ T cells were detected by flow cytometry in CHC patients （n=70） and healthy controls （n=25）. The con- centrations of serum IL-21 were analyzed using ELISA. The role of CD4＋CXCR5＋ T cells in the activation of IgG＋ B cells was investigated using a co-culture system. RESULTS： A significantly lower proportion of CD27＋IgG＋ B cells with increased expression of CD86 and CD95 was observed in CHC patients. The expression of CD95 was negatively correlated with the percentage of CD27＋IgG＋ B cells, and it contributed to CD27＋IgG＋ B cell apoptosis. Circulating CD4＋CXCR5＋ T cells and serum IL-21 were significantly increased in CHC patients. Moreover, circulating CD4＋CXCR5＋ T cells from CHC patients induced higher expressions of CD86 and CD95 in CD27＋IgG＋ B cells in a co-culture system; the blockade of the IL-21 decreased the expression levels of CD86 and CD95 in CD27＋IgG＋ B cells.CONCLUSIONS： HCV infection increased the frequency of CD4＋CXCR5＋ T cells and decreased the frequency of CD27＋IgG＋ B cells. CD4＋CXCR5＋ T cells activated CD27＋IgG＋ B cells via the secretion of IL-21.

应用CBCT观察三种镍钛预备系统对根管成形能力的影响

目的:利用牙科锥束CT(以下简称CBCT)探究三种不同机用镍钛根管锉对根管的成形能力。方法:选取近期拔除的上颌或下颌前磨牙(至少带有一个弯曲根管)开髓,用Kodak Dental Imaging Software 3D module v2.4软件确定根管的弯曲度和弯曲半径。被选的根管通畅,弯曲度范围应约为10°~25°的离体牙30颗,分三个实验组(n=10)。实验组分别为Protaper Universal,M3-Pro,S3三种镍钛根管锉预备根管,根管预备过程完成后每组分别拍摄CBCT记录,测定实验根管的根尖偏移、轴中心率。将每组10个样本截断冠部后,三等分截取根部样本,将每等分牙根颊舌(腭)向劈裂,在扫描电子显微镜(以下简称SEM)下观察根管内牙本质小管的开放率、牙本质的玷污层及牙本质碎屑评价。结果:实验组中镍钛根管预备系统S3系列组在根上1/3和根中1/3的牙本质碎屑、玷污层的清理及牙本质小管的开放率高于Protaper Universal系列组和M3-Pro系列组,存在显著差异(P<0.05),而Protaper Universal系列组和M3-Pro系列组没有明显差异(P>0.05)。根管预备前后对比,三种镍钛器械对根尖偏移量及轴中心率方面改变不明显(P>0.05)。结论:S3镍钛器械系列组清理根管能力较好,而三种镍钛器械产生微小的根尖偏移,且能基本维持根管形态。

Associations of IFN-γ rs2430561 T/A,IL28B rs12979860 C/T and ERα rs2077647 T/C polymorphisms with outcomes of hepatitis B virus infection:a meta-analysis

Several studies investigated associations of IFN-γ rs2430561 T/A,IL28 B rs12979860 C/T and ERα rs2077647 T/C gene polymorphisms with outcomes of hepatitis B virus（HBV） infection,but the results were controversial.Therefore,we performed a meta-analysis of all published observational studies to address this inconsistency.Literature was searched in online database and a systematic review was conducted based on the search results.A total of 24 studies were included and dichotomous data were presented as odds ratio（OR） with a 95%confidence interval（CI）.The rs2430561 T allele was associated with reduced persistent HBV infection risk（T vs.A：OR,0.690;95%CI,[0.490,0.971]）,while the rs2077647 T allele significantly increased the risk of persistent HBV infection（T vs.C：OR.1.678;95%CI,[1.212,2.3231）.Rs 2077647 CC might play a role in protecting individuals against HBV persistence（TT vs.CC：OR,4.109;95%CI,[2.609,6.473]）.Furthermore,carriers of the rs2430561 TT genotype were more likely to clear HBV spontaneously compared with those of the AA genotype（TT vs.AA：OR,0.555;95%CI,[0.359,0.856]）.For rs12979860 C/T polymorphism,no significant correlation with HBV infection outcomes was found.In subgroup analyses,the results were similar to those of overall analysis.However,for rs2077647 TT vs.TC＋CC,significantly increased risks were observed in the Asian and hospital-based population,but not in the overall analysis.IFN-γrs2430561 T/A and ERα rs2077647 T/C genetic polymorphisms were associated with outcomes of HBV infection,but no association was found between IL28 B rs12979860 C/T and HBV infection.

BNP、CRP水平和T淋巴细胞亚群百分比变化在慢性阻塞性肺疾病合并肺动脉高压中的意义

目的探讨B型钠尿肽(BNP)、C-反应蛋白(CRP)水平和T淋巴细胞亚群百分比变化在慢性阻塞性肺疾病合并肺动脉高压(COPD-PH)中的意义,同时了解BNP、CRP对COPD-PH的预测价值。方法选择于奉贤区中心医院住院治疗的COPD患者170例,以第1秒用力呼气容积(FEV_(1))占预计值百分比(FEV_(1)%)、FEV_(1)/用力肺活量百分比(FEV_(1)/FVC%)评价患者的肺功能,根据肺动脉压是否正常分为COPD-PH组(n=80)和COPD组(n=90),比较两组患者BNP、CRP水平和T淋巴细胞亚群百分比。应用Logistic回归模型分析影响COPD患者发生PH的危险因素。应用受试者工作特征(ROC)曲线评价BNP、CRP水平用于COPD-PH诊断的价值。结果COPD-PH组入院时的BNP、CRP水平高于COPD组(P<0.05);COPD-PH组CD8+T淋巴细胞百分比低于COPD组(P<0.05)。单因素和多因素回归分析显示:BNP、CRP升高和CD8+T淋巴细胞百分比降低是COPD患者发生PH的危险因素(P<0.05);用于COPD-HP诊断的ROC曲线分析显示:血清BNP水平的曲线下面积为0.727,灵敏度为0.65,特异度为0.68;血清CRP水平的曲线下面积为0.669,灵敏度为0.63,特异度为0.63。结论BNP、CRP升高和CD8+T淋巴细胞百分比降低是COPD患者发生PH的危险因素,与肺动脉压呈正相关,同时BNP、CRP可作为预测COPD患者发生PH的参考指标。

T helper cell dysregulation with hepatitis B and rebalance with glucocorticoids

AIM: To investigate T helper 17/regulatory T cell alterations in early severe hepatitis B and the effect of glucocorticoids.

BALB/c小鼠腹腔接种HBV表面S抗原疫苗引起的CTL反应(英文)

目的研究BALB/c小鼠免疫接种HBV表面S抗原疫苗(HBV small surface vaccine,S-HBsAg)能否引起特异性细胞毒T淋巴细胞(CTL)反应.方法分别给BALB/c小鼠腹腔内接种0～6μg S-HBsAg,两周后加强一次,4周后分离小鼠脾细胞,体外用S-HBsAg特异性CTL表位多肽刺激;用特异性多肽、51Cr标记的P815细胞作为靶细胞;4 h51Cr释放实验检测CTL反应.结果分别接种0、0.65、1.25、2.5、5μg S-HBsAg的小鼠,其脾淋巴细胞CTL特异性释放率分别为31.21%±9.23%、42.36%±19.32%、91.21%±22.97%、69.25%±24.13%、51.49%±21.661%;只接受一次免疫接种的小鼠,其脾淋巴细胞CTL特异性释放率分别为27.34%±14.25%、32.27%±15.35%、56.28%±24.35%、44.34%±18.65%、40.76%±56%.结论BALB/c(H-2d)小鼠腹腔内接种S-HBsAg引起剂量依赖性特异性CTL反应,加强免疫能够提高CTL反应.

Antiviral treatment to prevent chronic hepatitis B or C-related hepatocellular carcinoma

Antiviral treatment is the only option to prevent or defer the occurrence of hepatocellular carcinoma(HCC) in patients chronically infected with hepatitis B virus(HBV) or hepatitis C virus(HCV). The approved medication for the treatment of chronic HBV infection is interferon-α(IFNα) and nucleos(t)ide analogues(NAs), including lamivudine, adefovir dipivoxil, telbivudine, entecavir and tenofovir disoproxil fumarate. IFNα is the most suitable for young patients with less advanced liver diseases and those infected with HBV genotype A. IFNα treatment significantly decreases the overall incidence of HBV-related HCC in sustained responders. However, side effects may limit its long-term clinical application. Orally administered NAs are typically implemented for patients with more advanced liver diseases. NA treatment significantly reduces disease progression of cirrhosis and therefore HCC incidence, especially in HBV e antigen-positive patients. NA-resistance due to the mutations in HBV polymerase is a major limiting factor. Of the NA resistance-associated mutants, A181 T mutant significantly increases the risk of HCC development during the subsequent course of NA therapy. It is important to initiate treatment with NAs that have a high genetic barrier to resistance, to counsel patients on medication adherence and to monitor virological breakthroughs. The recommended treatment for patients with chronic HCV infection is peg-IFN plus ribavirin that can decrease the occurrence of HCC in those who achieve a sustained virological response and have not yet progressed to cirrhosis. IFN-based treatment is reserved for patients with decompensated cirrhosis who are under evaluation of liver transplantation to reduce post-transplant recurrence of HCV. More effective therapeutic options such as direct acting antiviral agents will hopefully increase the response rate in difficult-totreat patients with HCV genotype 1. However, the risk of HCC remains in cirrhotic patients(both chronic HBV and HCV infection) if treatment is initiated after cirrhosis is established. Future research should focus on investigating new agents, especially for those patients with hepatic decompensation or post-transplantation.