HLA-DQA1*0501、HLA-DQB1*02基因多态性与抗Ro/SSA抗体阳性pSS易感性的关系分析

目的基于数据库相关数据分析人类白细胞抗原(HLA)-DQA1*0501和HLA-DQB1*02基因多态性与抗Ro/SSA抗体阳性的原发性干燥综合征(pSS)易感性的关系。方法使用计算机检索相关数据库,筛选并收集pSS患者、抗Ro/SSA抗体阳性的pSS患者、抗Ro/SSA抗体阴性的pSS患者以及健康对照人群的HLA-DQA1*0501、HLA-DQB1*02基因多态性资料。使用STATA 16.0(USA)统计软件分析抗Ro/SSA抗体阳性的pSS患者中HLA-DQA1*0501和HLA-DQB1*02基因多态性与pSS发生的关系。结果纳入文献5篇,涉及420例pSS患者、250例抗Ro/SSA抗体阳性pSS患者、120例抗Ro/SSA抗体阴性的pSS患者和733例健康对照者。在pSS患者中,HLA-DQA1*0501和HLA-DQB1*02基因阳性分别为159、246例;在健康对照者中,HLA-DQA1*0501和HLA-DQB1*02基因阳性分别为196、282例;在抗SSA抗体阳性pSS患者中,HLA-DQA1*0501和HLA-DQB1*02基因阳性分别为129、158例;在抗SSA抗体阴性pSS患者中,HLA-DQA1*0501和HLA-DQB1*02基因阳性分别为30、46例。HLA-DQA1*0501和HLA-DQB1*02基因多态性与pSS的易感性有关(I2分别为62.99%、40.75%,合计OR值分别为2.60、2.43,95%CI分别为1.49~4.55、1.88~3.14,P均<0.05)。HLA-DQA1*0501和HLA-DQB1*02基因多态性也与抗Ro/SSA抗体阳性pSS的易感性有关(I2分别为0.00%、9.41%,合计OR值分别为3.85、2.61,95%CI分别为1.81~8.21、1.52~4.48,P均<0.05)。结论HLA-DQA1*0501和HLA-DQB1*02基因多态性与抗Ro/SSA抗体阳性的pSS患者的易感性相关。具有HLA-DQA1*0501和HLA-DQB1*02基因阳性的抗Ro/SSA抗体阳性患者更容易患pSS。

Carrier frequency of HLA-DQB1*02 allele in patients affected with celiac disease:A systematic review assessing the potential rationale of a targeted allelic genotyping as a first-line screening

BACKGROUND Celiac Disease(CD)is an immune-mediated disorder,in which the HLA immunogenetic background(DQ2 and DQ8 heterodimers)and environmental trigger(gluten)are well established.Indeed,both factors are necessary–but not sufficient–to develop CD.However,it is very likely that CD is underdiagnosed in both developing and developed countries,due to several aspects,including the fact that a lot of patients present mild and/or atypical symptoms,without the presence of any recognized risk factors.Therefore,the possibility and feasibility of widened screening strategies to identify CD patients are debated.AIM To provide further evidence of the main epidemiological importance of HLADQB1*02 allele in the population of CD patients.METHODS We performed a systematic search in PubMed,EMBASE,Cochrane,Web of Science and Scopus databases,in order to produce a systematic review assessing the carrier frequency of HLA-DQB1*02 allele in the celiac population.Following the PRISMA guidelines,we retrieved all the original articles describing CD patients’HLA-DQB1 genotype in such a way that could allow to assess the HLADQB1*02 carrier frequency among CD patients,along with the evidence of the appropriate diagnostic work-up to achieve a correct and final diagnosis of CD.RESULTS The final output of this systematic search in the medical literature consisted of 38 studies providing the appropriate HLA-DQB1 genotype information of the respective CD population.According to this systematic review,including a pool of 4945 HLA-DQ genotyped CD patients,the HLA-DQB1*02 carrier frequency was 94.94%,meaning that only 5.06%of CD patients were completely lacking this allelic variant.Interestingly,if we consider only the studies whereby the prevalence of CD patients affected with type 1 diabetes mellitus was supposed or clearly established to be very low,the frequency of non-HLA-DQB1*02 carriers among CD patients dropped to 3.65%.CONCLUSION Such a high carrier frequency of the HLA-DQB1*02 allelic variant(which is>95%-96%in CD patients without risk factors,like type 1 diabetes mellitus comorbidity)might be exploited to consider a cost-effective and widened screening approach.If a sustainable strategy could be implemented through a low-cost targeted genetic test to detect the individual presence of HLA-DQB1*02 allele,an appropriate algorithm for serological screening in individuals resulting to be genetically predisposed to CD,might be considered.

乙肝疫苗无、弱应答与HLA-DRB1*07、DQB1*02相关性的研究

目的探讨HLA-DRB1＊07、DQB1＊02基因与无、弱应答之间的关系。方法选取1 342名接种乙肝疫苗后无、弱应答者128人作为病例组,在有应答者中按性别匹配随机抽取128人作为对照组进行研究,应用PCR-SSP技术检测研究对象的HLA-DRB1＊07、DQB1＊02基因。采用SPSS13.0软件进行分析。结果携带HLA-DRB1＊07基因发生无、弱应答的风险为不携带此基因的4.83倍（1.76~13.24）,携带HLA-DQB1＊02基因发生无、弱应答的风险为不携带此基因的2.58倍（1.38~4.83）;同时携带HLA-DRB1＊07基因和HLA-DQB1＊02基因者发生无、弱应答的风险比不携带这两个基因者大（OR=5.64,95%CI1.84~17.27）。结论 HLA-DRB1＊07、DQB1＊02基因均与无、弱应答的发生有关;两种基因联合作用可提高无、弱应答的危险性。

HLA-DQB1~*02、03基因及IFN-γ、IL-4与广西壮、瑶族肝癌家族聚集性的相关性

本研究探讨HLA-DQB1~*02、03等位基因及细胞因子IFN-γ和IL-4与广西壮、瑶族肝癌家庭聚集性的相关性。将来自肝癌高发区,民族为瑶族的肝癌高发家族成员、无癌家族成员各40例及民族为壮族的肝癌高发家族成员、无癌家族成员各48例作为研究对象(采用相同性别,年龄(±5岁)配对方法),采集研究对象外周血并提取全血DNA,采用PCR-SSP技术检测受试者的HLA-DQB1~*02和HLA-DQB1~*03等位基因,IFN-γ及IL-4细胞因子表达水平采用ELISA法检测。结果发现,HLA-DQB1~*02、03基因在壮族肝癌高发家族成员组的表达频率均低于无癌家族成员组(p<0.05);HLA-DQB1~*02基因在瑶族肝癌高发家族成员组的表达频率高于无癌家族组(p=0.002),HLA-DQB1~*03在两组间的表达频率无明显差异(p>0.05)。广西壮、瑶族人群HLA-DQB1~*02、03基因在乙肝病毒感染组及非感染组中的表达频率比较无显著性差异(p>0.05)。壮、瑶族肝癌高发家族成员组IL-4平均表达水平均高于无癌家族成员组,肝癌高发家族成员组IFN-γ平均表达水平均低于无癌家族成员组,差异具有统计学意义(p<0.05)。广西壮、瑶族人群中HLA-DQB1~*02基因阳性和阴性成员的IL-4平均表达水平无明显差异(p>0.05)。广西壮族人群中HLA-DQB1~*03基因阳性成员的IFN-γ平均表达水平高于HLA-DQB1~*03阴性成员(p=0.011),HLA-DQB1~*03阳性和阴性成员的IL-4平均表达水平无明显差异(p<0.05)。本课题得出结论,HLA-DQB1~*02、03基因与广西壮、瑶族肝癌家庭聚集性有关,但存在较大的民族差异;细胞因子IFN-γ及IL-4的表达水平失衡可能是广西壮、瑶族肝癌家族聚集性的危险因素。HLA-DQB1~*03基因导致广西壮族肝癌家族聚集性的发生可能是通过影响IFN-γ的表达水平来实现的。

发作性睡病研究进展

发作性睡病是一种慢性睡眠障碍性疾病。近年来经过不断研究,发作性睡病被认为是一种免疫介导性疾病,该病与HLA-DQB1*06:02基因和下丘脑分泌素密切相关,同时2个新的易患基因也已明确。诊断标准的制订更利于该病的早期诊断,一些新药的研制成功和给药方式的改进也提高了发作性睡病的疗效。在今后的工作中,通过对发作性睡病免疫机制的深入研究,将为临床治疗该病提供更好的实验依据。

创伤性脑损伤后继发性1型发作性睡病1例

1型发作性睡病是一种罕见的中枢神经系统疾病,一般认为是环境因素和遗传因素相互作用的结果。创伤性脑损伤(TBI)是继发性发作性睡病最常见的病因之一。目前国内外关于TBI后发作性睡病的报道非常少见。本例是国内报道的首例HLA-DQB1*06:02阳性的TBI后1型发作性睡病患者。现将我院收治的这例患者的临床资料进行回顾性分析,旨在提高临床医师对该疾病诊断及其发病机制的认识。