IFIT1 polymorphisms predict interferon-α treatment efficiency for hepatitis B virus infection

AIM To investigate the association between interferoninduced protein with tetratricopeptide repeats 1(IFIT1) polymorphisms and interferon-α(IFNα) treatment efficiency among Chinese hepatitis B virus(HBV) infection patients.METHODS Two hundred and twenty five newly diagnosed chronichepatitis B(CHB) patients were enrolled in the study. All of these patients received IFNα treatment for a course of 48 wk, and were followed up for 24 wk after the treatment was end. Clinical information about virological response, hepatitis B e antigen(HBe Ag) seroconversion rate and combined response at the end of the treatment, as well as the sustained response by the time of following up 24 wk after the treatment, was collected. Four tag-single nucleotide polymorphisms(SNPs) of IFIT1 were selected and assessed for their association with these clinical outcomes.RESULTS At the end of the treatment, HBe Ag seroconversion was observed in 27.1% patients. Thirty-six point nine percent patients achieved virological response, and 15.6% patients exhibited combined response. Sustained response was obtained in 26.2% patients. The main HBV genotype of the study was genotype B. Patients who infected with HBV genotype B or C showed better treatment efficiency, no matter which clinical outcome was considered. Among the four SNPs assessed, rs303218(A > G) was found to be significantly associated with the end point virological response when assuming additive model [OR = 0.64(95%CI: 0.42-0.96), P = 0.032]. Patients who carried rs303218 GG genotype had a rather higher rate of achieving virological response(response rate: 52%, OR = 0.40, 95%CI: 0.18-0.91; P = 0.028) when compared to those had AA genotype(response rate: 27%). The most significant interaction was observed in patients who had relative lower baseline aspartate transaminase. No association between SNPs and HBe Ag seroconversion, combined response or sustained response was observed.CONCLUSION IFIT1 involves in the regulation of IFNα treatment for CHB and its polymorphism rs303218 can predict the end point virological response. The finding requires further validation.

Twenty four-week peginterferon plus ribavirin after interferon-β induction for genotype 1b chronic hepatitis C

AIM:To investigate the possibility of shortening the duration of peginterferon(Peg-IFN)plus ribavirin(RBV) combination therapy by incorporating interferon-β (IFN-β)induction therapy. METHODS:A one treatment arm,cohort prospective study was conducted on seventy one patients.The patients were Japanese adults with genotype 1b chronic hepatitis C,HCV-RNA levels of≥5.0 Log IU/mL or 100 KIU/mL,and platelet counts of≥90 000/μL.The treatment regimen consisted of a 2 wk course of twicedaily administration of IFN-βfollowed by 24 wk PegIFN plus RBV combination therapy.We prolonged the duration of the Peg-IFN plus RBV therapy to 48 wk if the patient requested it. RESULTS:The patients,including 44%males,were characterized by an median age of 63 years(range: 32-78 years),an median platelet count of 13.9(range: 9.1-30.6)×10 4 /μL,62%IFN-na?ve,and median HCV- RNA of 6.1(range:5.1-7.2)Log IU/mL.The sustained virologic response(SVR)rates were 34%(Peg-IFN:1-24 wk,n=61,95%confidence interval(CI): 24%-47%)and 55%(Peg-IFN:20-24 wk,n=31,95% CI:38%-71%,P<0.001;vs Peg-IFN:1-19 wk).TheSVR rate when the administration was discontinued early was 13%(Peg-IFN:1-19 wk,n=30,95%CI: 5%-30%),and that when the administration was prolonged was 50%(Peg-IFN:25-48 wk,n=10,95% CI:24%-76%,P<0.05;vs Peg-IFN:1-19 wk).In the patients who received 20-24 wk of Peg-IFN plus RBV,only the higher platelet count(≥130 000/μL) was significantly correlated with the SVR(odds ratio: 11.680,95%CI:2.3064-79.474,P=0.0024).In 45% (14/31)of the patients with a higher platelet count (≥130000/μL)before therapy,the HCV-RNA level decreased to below 3.3 Log IU/mL at the completion of IFN-β,and their SVR rate was 93%(13/14)after 20-24 wk administration of Peg-IFN plus RBV. CONCLUSION:These results suggest the possibilities of shortening the duration of Peg-IFN plus RBV combination therapy by actively reducing HCV-RNA levels using the IFN-βinduction regimen.

干扰素α-1b和拉米夫定序贯治疗慢性乙型肝炎的高水平HBV清除动力学观察

目的观察干扰素α-1b(IFNα-1b)和拉米夫定序贯治疗对慢性乙型肝炎的高水平复制HBV清除动力学的影响。方法76例HBeAg阳性且HBV DNA>1×107copies/ml慢性乙型肝炎患者随机分为治疗组和对照组。治疗组40例,先用拉米夫定治疗4周,再加用IFNα-1b治疗8周,然后单用IFNα-1b治疗16周,对照组36例单用IFNα-1b治疗24周。分别于治疗前后定期检测肝功能、血常规、乙肝标志物及HBV DNA。结果治疗结束时,治疗组的ALT复常率、HBV DNA阴转率、HBeAg阴转率及抗-HBe阳转率均明显高于对照组(P<0.05,P<0.01),治疗组有效率(72.5%)明显高于对照组(50.0%)(P<0.05)。治疗期间两组的副反应无明显的差异(P>0.05)。随访6个月治疗组的上述指标仍高于对照组(P<0.05),仅两组间的抗-HBe阳转率差异无显著性(P>0.05)。结论IFNα-1b和拉米夫定序贯治疗对HBV高水平复制的慢性乙型肝炎有较好的效果,优于单用IFNα-1b治疗。

Genetic biomarkers for hepatocellular cancer risk in a caucasian population

AIM To uncover novel genetic markers that could contribute to predicting hepatocellular carcinoma(HCC)susceptibility in Caucasians. METHODS The present retrospective case-control study compared genotype frequencies between a cohort of HCC cases and two,independent,HCC-free,age/sex-matched control groups.The HCC cohort comprised 192 homogeneous patients that had undergone orthotopic liver transplantation.The first control group comprised167 patients that were matched to the HCC cohort for the percentage of hepatitis B(HBV)and/or hepatitis C(HCV)infections.A second control group included192 virus-free,healthy individuals that were used to evaluate the generalizability of the identified predictive markers.All cases and controls were Caucasian.The three study populations were characterized with a panel of 31 markers derived from 21 genes that encoded key proteins involved in hepatocarcinogenesis-related pathways.The study end-point was to assess the association between genetic variants and HCC onset. RESULTS Five genetic markers were identified as risk factors for HCC in high-risk patients infected with HBV/HCV.According to a dominant model,reduced HCC risk was associated with three polymorphisms:ERCC1rs3212986(OR=0.46,95%CI:0.30-0.71,P=0.0005),GST-P1 rs1138272(OR=0.41,95%CI:0.21-0.81,P=0.0097),and CYP17A1 rs743572(OR=0.50,95%CI:0.31-0.79,P=0.0032).Conversely,according to a recessive model,increased HCC risk was associated with two polymorphisms:XRCC3 rs1799794(OR=3.70,95%CI:1.02-13.39,P=0.0461)and ABCB1 rs1128503(OR=2.06,95%CI:1.18-3.61,P=0.0111).These associations remained significant in a subgroup analysis,where patients were stratified according to viral status(HBV-or HCV-positive serology).Two variants exhibited a serology-specific effect:ABCB1 rs1128503(OR=4.18,95%CI:1.55-11.29,P=0.0048)showed an effect in the HBV-positive subgroup;and ERCC1 rs3212986(OR=0.33,95%CI:0.18-0.60,P=0.0003)showed an effect in the HCV-positive subgroup.Among the five markers identified,ERCC1 rs3212986(OR=0.43,P<0.0001)and CYP17A1 rs743572(OR=0.73,P=0.0310)had a different distribution in patients with HCC compared to healthy individuals.With a recursive partitioning approach,we also demonstrated that significant gene-gene interactions between ERCC1rs3212986,CYP17A1 rs743572,GST-P1 rs1138272,and the previously described UGT1A7*3 predictive marker,played a role in the complex trait of HCC susceptibility.CONCLUSION We identified five polymorphisms and interactions that contributed crucially to predicting HCC risk.These findings represented an important step towards improving HCC diagnosis and management.

Hepatitis C virus infection and insulin resistance

Approximately 170 million people worldwide are chronically infected with hepatitis C virus(HCV).Chronic HCV infection is the leading cause for the development of liver fibrosis,cirrhosis,hepatocellular carcinoma(HCC)and is the primary cause for liver transplantation in the western world.Insulin resistance is one of the pathological features in patients with HCV infection and often leads to development of typeⅡdiabetes.Insulin resistance plays an important role in the development of various complications associated with HCV infection.Recent evidence indicates that HCV associated insulin resistance may result in hepatic fibrosis,steatosis,HCC and resistance to anti-viral treatment.Thus,HCV associated insulin resistance is a therapeutic target at any stage of HCV infection.HCV modulates normal cellular gene expression and interferes with the insulin signaling pathway.Various mechanisms have been proposed in regard to HCV mediated insulin resistance,involving up regulation of inflammatory cytokines,like tumor necrosis factor-α,phosphorylation of insulin-receptor substrate-1,Akt,up-regulation of gluconeogenic genes like glucose 6 phosphatase,phosphoenolpyruvate carboxykinase 2,and accumulation of lipid droplets.In this review,we summarize the available information on how HCV infection interferes with insulin signaling pathways resulting in insulin resistance.

Correlation between constitution of Yin deficiency syndrome and polymorphism of HLADQA1 / treatment response of Peg-IFNα therapy in HBeAg positive chronic hepatitis B patients

Objective To observe the correlation between constitution of yin deficiency syndrome(YDS)and polymorphism of HLA-DQA1/treatment response of Peg-IFNαtherapy in HBe Ag positive chronic hepatitis B(CHB)patients,and to explore constitution of Chinese medicine(CM)in response to interferon therapy.Methods Totally 120 HBe Ag positive CHB patients who were

外周血T细胞表面PD-1在慢性乙型肝炎患者干扰素治疗期间的表达

目的:观察慢性HBV感染(CHB)免疫清除期PD-1的表达状态以及干扰素抗病毒治疗期间T细胞PD-1的表达,明确免疫清除期CHB患者PD-1表达的临床意义.方法:伴有长期ALT反复升高的CHB患者20例被纳入本研究,所有病例均接受为期6mo的Peg干扰素(1.5μg/kg)抗病毒治疗,每周1次.应用流式细胞术对所有患者抗病毒治疗不同时间点(0、12、24wk)的外周血总CD8+T细胞和CD4+T细胞PD-1表达百分比和表达强度进行检测.结果:免疫清除期CHB患者外周血总CD8+T细胞和CD4+T细胞PD-1阳性率和PD-1表达荧光强度均明显高于健康对照组(P<0.05);PEG干扰素治疗早期CD8+T细胞PD-1阳性率呈现明显下降,且CD8+T细胞PD-1表达阳性率同ALT水平和病毒水平均呈现明显正相关(R2=0.22,0.357,P=0.001,0.002).结论:CHB患者外周血T细胞PD-1呈高表达;干扰素治疗诱导的病毒水平下降可导致CD8+T细胞PD-1表达明显下降.

补肾解毒方阻断程序性死亡受体1/程序性死亡配体1信号通路对辅助慢性乙型肝炎树突状细胞疫苗抗乙型肝炎病毒的免疫效果与机制研究

目的研究补肾解毒方阻断程序性死亡受体1(PD-1)/程序性死亡配体1(PD-L1)信号通路对辅助慢性乙型肝炎(以下简称乙肝)树突状细胞(DC)疫苗抗乙肝病毒(HBV)的免疫效果与机制。方法将40只BALB/c HBV转基因小鼠按照随机数字表法分为补肾解毒方组、PD-L1抗体组、磷酸缓冲液(PBS)组及联合组4组,每组10只。4组分别予补肾解毒方、PD-L1单克隆抗体、PBS溶液及补肾解毒方联合PD-L1单克隆抗体,持续给药2周后处死小鼠,观察小鼠脾脏组织γ干扰素(IFN-γ)水平、CD8^+T淋巴细胞的PD-1表达情况及乙肝表面抗原(HBsAg)特异性细胞毒性T淋巴细胞(CTL)的杀伤活性。结果联合组小鼠脾脏组织IFN-γ水平高于补肾解毒方组、PD-L1抗体组、PBS组(P<0.05);补肾解毒方组、PD-L1抗体组小鼠脾脏组织IFN-γ水平高于PBS组(P<0.05);补肾解毒方组与PD-L1抗体组小鼠脾脏组织IFN-γ水平比较差异无统计学意义(P>0.05)。联合组小鼠脾脏组织CD8^+T淋巴细胞PD-1表达均低于补肾解毒方组、PD-L1抗体组、PBS组(P<0.05);补肾解毒方组、PD-L1抗体组CD8^+T淋巴细胞PD-1表达均低于PBS组(P<0.05);PD-L1抗体组CD8^+T淋巴细胞PD-1表达低于补肾解毒方组(P<0.05)。当效靶比为100∶1、50∶1时,联合组小鼠脾脏组织HBsAg特异性CTL杀伤活性均高于补肾解毒方组、PD-L1抗体组、PBS组(P<0.05);PD-L1抗体组HBsAg特异性CTL杀伤活性均高于补肾解毒方组、PBS组(P<0.05);补肾解毒方组与PBS组HBsAg特异性CTL杀伤活性比较差异无统计学意义(P>0.05)。当效靶比为25∶1时,补肾解毒方组、PD-L1抗体组、联合组小鼠脾脏HBsAg特异性CTL杀伤活性均高于PBS组(P<0.05);补肾解毒方组、PD-L1抗体组、联合组小鼠脾脏HBsAg特异性CTL杀伤活性两两比较差异均无统计学意义(P>0.05)。结论 HBV感染时阻断PD-1/PD-L1信号通路可起到恢复特异性T淋巴细胞功能的作用,补肾解毒方能有效发挥对HBV感染时的T淋巴细胞免疫功能的调整作用,补肾解毒方联合PD-L1抗体更具明显协同作用。

慢性乙型肝炎患者抗病毒治疗与免疫细胞上PD-1/PD-L1表达的关系

在我国,乙型肝炎病毒(hepatitis B virus,HBV)在体内不断复制并由此导致的肝细胞免疫病理损伤是H B V感染后慢性化及病情加重的原因,因此,抗病毒是阻止病情进展的有效手段.在多种与宿主免疫调控异常有关的发病机制中,程序性死亡分子1(programmed death 1,PD-1)/程序性死亡分子1配体1(PD-1 ligand 1,PD-L1)通路被认为与HBV感染后结局相关,本文就慢性乙型肝炎(chronic hepatitis B,CHB)患者抗病毒治疗与免疫细胞上PD-1/PD-L1表达间关系进行综述.

恩替卡韦对慢性乙型肝炎患者外周血单核细胞表面PD-1和PD-L1表达的影响

目的探讨恩替卡韦对慢性乙型肝炎(CHB)患者外周血单核细胞(PBMCs)表面PD-1、PD-L1的影响及其与血清HBV-DNA载量、谷丙转氨酶(ALT)之间的关系。方法收集CHB患者40例,其中2×ULN≤ALT<5×ULN 20例(A组),ALT≥5×ULN 20例(B组),健康献血者20例(C组)。A组、B组均给予恩替卡韦口服抗病毒治疗,疗程为24周。采用流式细胞术检测治疗前及治疗24周时患者PBMCs表面PD-1及其配体PDL1表达,以实时荧光定量PCR检测血清HBV-DNA,同时检测血清ALT。结果 A组、B组2组患者PBMCs表面PD-1、PD-L1表达显著高于C组(P<0.05),A组与B组比较PBMCs表面PD-1、PD-L1表达水平差异无统计学意义(P>0.05)。恩替卡韦抗病毒治疗24周时,A组、B组2组患者PBMCs表面PD-1、PD-L1表达水平均明显下降,差异有统计学意义(P<0.05),且B组较A组下降更为显著,差异有统计学意义(P<0.05);但2组患者治疗后PBMCs表面PD-1、PD-L1表达水平仍高于C组,差异有统计学意义(P<0.05)。治疗24周时A组、B组2组患者血清HBV-DNA、ALT水平均明显下降,差异有统计学意义(P<0.05),A组、B组2组患者治疗后比较,HBV-DNA及ALT水平差异无统计学意义(P>0.05)。结论恩替卡韦不但能抑制HBV-DNA合成,还可以降低CHB患者PBMCs表面PD-1、PD-L1表达水平,且在肝脏炎症损伤重的CHB患者中下降幅度更为明显。

长期抗病毒治疗的慢性乙型肝炎患者血清TIMP-1和M-CSF水平变化

目的 探讨长期抗病毒治疗的慢性乙型肝炎(CHB)患者血清组织基质金属蛋白酶抑制物-1(TIMP-1)和巨噬细胞集落刺激因子(M-CSF)水平变化。方法 纳入2017年4月—2019年2月合肥市第三人民医院收治的CHB患者148例为研究对象,连续抗病毒治疗2年。观察治疗前后血清TIMP-1和M-CSF水平变化。统计CHB患者肝硬化发生情况,并依据是否发生肝硬化分为发生组和未发生组。对比发生组和未发生组患者的临床资料。logistic多因素回归分析影响CHB患者肝硬化发生的因素。制作受试者工作特征曲线(ROC),以曲线下面积(AUC)评价血清TIMP-1、M-CSF变化对CHB患者肝硬化发生的预测效能。结果 与治疗前1 d相比,治疗6个月后CHB患者血清TIMP-1和M-CSF均降低(P<0.05),ΔTIMP-1、ΔM-CSF分别为(56.6±8.3)μg/L、(62.5±9.2)ng/L。治疗2年后肝硬化发生率为24.32%。发生组丙氨酸氨基转移酶(ALT)、肝门静脉内径、肝脏弹性值(LSM)、TIMP-1,治疗6个月后TIMP-1、M-CSF均高于未发生组(P<0.05),ΔTIMP-1、ΔM-CSF则低于未发生组(P<0.05)。logistic回归分析结果显示,LSM、ΔTIMP-1及ΔM-CSF均为影响CHB患者肝硬化发生的危险因素(OR=2.732、3.040、3.330,P<0.05)。ROC分析显示,血清ΔTIMP-1、ΔM-CSF预测CHB患者肝硬化发生的最佳截断点分别为50.9μg/L、61.4 ng/L,灵敏度分别为80.6%、72.2%;特异度分别为75.9%、80.4%,AUC分别为0.848、0.809。结论 血清TIMP-1、M-CSF水平变化预测CHB患者肝硬化发生的效能较高,可作为临床评估CHB患者是否发生肝硬化的重要参考指标。

替比夫定联合胸腺肽α-1治疗慢性乙型肝炎患者80例疗效分析

目的观察替比夫定联合胸腺肽α-1治疗慢性乙型肝炎患者的早期疗效。方法将80例慢性乙型肝炎患者随机分为替比夫定联合胸腺肽α-1治疗组40例和拉米夫定联合胸腺肽α-1治疗组40例。采用ELISA法检测血清HBV标志物,采用荧光定量PCR法检测血清HBV DNA。观察两组治疗12 w的疗效。结果在治疗8 w末,替比夫定治疗患者血清HBV DNA阴转率和HBe Ag阴转率分别为32.5%和20.0%,与拉米夫定治疗患者比,无显著性相差(分别为17.5%和5.0%,P>0.05),在治疗12w末,替比夫定治疗患者血清HBV DNA阴转率显著高于拉米夫定治疗患者(95.0%对62.5%,P<0.05);在治疗12 w末,替比夫定治疗患者完全应答、部分应答和无应答率分别为57.5%、40.0%和2.5%,而拉米夫定治疗患者则分别为37.5%、45.0%和17.5%,其中完全应答率显著高于拉米夫定组(P<0.05)。结论替比夫定联合胸腺肽α-1治疗慢性乙型肝炎患者早期疗效更优。

国产人α＿1型基因工程干扰素治疗慢性肝炎Ⅲ期临床试验

３９例慢性肝炎患者，其中乙型肝炎１２例，丙型肝炎２７例，接受人α＿１型基因工程干扰素治疗（ｒＨＩＦＮα＿１）。１０例丙型肝炎病人ｒＨＩＦＮα＿１每日肌注１×１０￣６Ｕ，连用９０天，１７例丙型肝炎病人和乙型肝炎ｒＨＩＦＮα＿１每日肌注３×１０￣６Ｕ，连用９０天。治疗后乙型肝炎组ＨＢｅＡｇ和ＨＢＶＤＮＡ的阴转率均为４１．６７％；丙型肝炎用１×１０￣６Ｕ／ｄ和３×１０￣６Ｕ／ｄ组ＨＣＶＲＮＡ阴转率分别为５０％和６４．７％，两个剂量组阴转率比较差异无显著性（Ｐ＞０．０５），治疗期间不良反应发生率较低，远期疗效尚待观察。

CK1α upregulates the IFNAR1 expression to prompt the anti-HBV effect of type Ⅰ IFN in hepatoma carcinoma cells

Casein kinase 1α(CK1α) mediates the phosphorylation and degradation of interferon-α/β receptor 1(IFNAR1) in response to viral infection. However, how CK1α regulates hepatitis B virus(HBV) replication and the anti-HBV effects of IFN-α are less reported. Here we show that CK1α can interact with IFNAR1 in hepatoma carcinoma cells and increased the abundance of IFNAR1 by reducing the ubiquitination levels in the presence of HBV.Furthermore, CK1α promotes the IFN-α triggered JAK-STAT signaling pathway and consequently enhances the antiviral effects of IFN-α against HBV replication. Our results collectively provide evidence that CK1α positively regulates the anti-HBV activity of IFN-α in hepatoma carcinoma cells, which would be a promising therapeutic target to improve the effectiveness of IFN-α therapy to cure CHB.

胸腺肽α_1单用治疗慢性乙型肝炎的临床荟萃分析

目的研究单用胸腺肽α_1(thymosin alpha-1,Tα_1,zadaxin)对慢性乙型肝炎(CHB)的治疗作用。方法通过MEDLINE、PUBMED、Blackwell等电子数据库搜寻有关Tα_1治疗慢性乙型肝炎的相关资料,加以统计学上的比较、分析、观察及评价其对CHB的治疗效果。结果对7个研究胸腺肽α_1(zadaxin)单用治疗慢性乙型肝炎的随机对照实验进行临床荟萃分析发现,Tα_1单用的疗效(38%)几乎是对照组(13%)的3倍,在统计学上差异有显著性意义。结论胸腺肽α_1单用治疗CHB能取得较好的临床治疗效果,与干扰素相比不仅表现在能有效地减少乙肝病毒(HBV)复制,较少不良反应,为机体较好地耐受,而且诱导了持续的、递增的血清丙氨酸转氨酶(ALT)复常和HBV-DNA的清除。

乙肝Ⅰ号治疗慢性乙型肝炎的临床研究

用自拟中药乙肝Ⅰ号冲剂治疗慢性乙型肝炎100例,并与服用焦三仙的对照组100例相比较,结果治疗组在降低转氨酶、抑制乙肝病毒复制及改善白球蛋白比例方面均优于对照组,动物实验亦证实了以上作用。

干扰素治疗慢性乙型肝炎预后与降钙素基因相关肽及受体活性蛋白1基因多态性的关联研究

目的探讨降钙素基因相关肽(CGRP)rs155209和受体活性蛋白1(RAMP1)rs3754701两个基因位点突变是否与干扰素治疗慢性乙型肝炎(乙肝)预后有关。方法采用调查问卷的方法收集317例研究对象的一般资料,收集其抗凝血,提取DNA,用基质辅助激光解吸电离飞行时间质谱实验平台进行SNPs分型,使用单因素及多因素logistic回归方法分析CGRP及RAMP1基因多态性与干扰素治疗慢性乙肝预后的关系。结果携带RAMP1基因rs3754701T者更容易出现DNA应答和ALT应答(OR=2.277,95%CI:1.386~3.741,P=0.001;OR=1.694,95%CI:1.073~2.675,P=0.024),而携带CGRP基因rs155209C者更不易出现DNA应答和ALT应答(OR=0.150,95%CI:0.083~0.271,P<0.001;OR=0.583,95%CI:0.367~0.925,P=0.022)。结论在中国北方汉族人群中,CGRP基因的rs155209和RAMP1基因的rs3754701位点与干扰素治疗慢性乙肝预后有关,rs3754701T在干扰素治疗后的DNA应答和ALT应答中起保护作用,而rs155209C携带者不易出现DNA应答和ALT应答。