汉族人IL-12b和IL-10启动子区基因多态性与HBV感染的相关性

目的:我国是一个乙型肝炎大国,乙型肝炎感染及其转归显然有人种、人群差异。本研究对我国汉族人群中乙型肝炎病毒(hepatitis virus B,HBV)感染和发病与白介素-12p40(interleukin-12p40,IL-12b)、白介素-10(interleukin-10,IL-10)启动子区基因多态性之间的关系进行了探讨。方法:利用聚合酶链反应-限制性内切酶片段长度多态性分析(restricted enzyme-fragment length polymorphisms,PCR-RFLP)的方法对非相关人群的健康人群与HBV感染患者(轻、中度慢性肝炎、重度慢性肝炎)和HBV感染家系中的HBV携带者、既往HBV感染者、健康人群的IL-12b,IL-10启动子区-540C、-592A(IL10-5’A,IL12-5’C)单碱基多态性(SNP)进行了分析,并且对两个突变位点进行了基因测序。使用SAS统计软件进行统计分析。结果:IL10-5’A、IL12-5’C在非相关人群中的分布符合Hardy-Weinberg平衡。非相关人群IL10-5’A、IL12-5’C突变等位基因在HBV患者中的频率近似于健康人群(IL10-5’A,HBV患者42.08％,健康人41.9％,P>0.05;IL12-5’C,HBV患者55.8％,健康人64.6％,P>0.05)。IL10-5’A与IL12-5’C基因分布在慢性肝炎(轻中)和慢性肝炎(重)两组无显著性差异(P>0.05)。提示IL10-5’A,IL12-5’C单碱基多态性(SNP)对乙型肝炎病情轻中无影响;HBV感染家系中IL10-5’A,IL12-5’C单碱基多态性在携带者、健康人群以及既往感染者三组间均匀分布,IL12-5’C突变频率与非相关人群相似(非相关人群-540T 55.3％,相关人群-540T 55.9％);IL10-5’A 突变频率与非相关人群有显著性差异(非相关人群-592C42.0％,相关人群-592C 19.5％,P<0.01)。结论:IL10-5’A突变比IL12-5’C突变在HBV感染家系中可能起到更重要的作用,或影响相关人群对HBV的易感性。

IL-12B基因rs3212227位点多态性与川崎病及其并发冠状动脉损伤的关联性研究

目的:探讨IL-12B基因rs3212227位点多态性与川崎病(KD)及其并发冠状动脉损伤(CAL)的关联性。方法:收集2004年至2014年间83例KD患儿及86例健康儿童外周血标本,提取DNA,应用基因扩增-聚合酶链限制性长片段法(PCR-RFLP)检测IL-12B基因rs3212227位点多态性,并用直接测序法进行验证;χ~2检验分析该位点多态性与KD及其并发CAL之间是否存在关联性,P<0. 05代表差异有统计学意义。结果:KD组AA、AC、CC基因型分布和A、C等位基因分布与对照组比较差异无统计学意义(χ~2=4. 095、3. 31,P> 0. 05)。KD组中合并CAL组基因型和等位基因分布与冠状动脉正常组(NCAL组)比较差异亦无统计学意义(χ~2=1. 586、1. 254,P>0. 05)。结论:IL-12B基因rs3212227位点多态性与川崎病及其并发冠状动脉损伤有关联。

IL-12B和TTC1基因交互作用与中国汉族人银屑病的相关性研究

目的研究IL-12B和TTC1基因交互作用对中国汉族人银屑病发病的影响。方法从前期银屑病GWAS中选取1 139个病例和1 132个对照,经过性别和年龄匹配。使用PLINK软件的SNP×SNP计算两SNPs之间的交互作用,Logistic回归分析每个SNP的最佳关联模型。结果 IL-12B和TTC1在中国汉族人银屑病发病中存在交互作用(P=3.74×10-4)。IL-12B的最佳关联模型为累加模型(OR=1.42,P=6.04×10-3);GG和AG为风险基因型。结论 IL-12B和TTC1在中国汉族人银屑病发病过程中存在交互作用。

IL-12B基因多态性与肝硬化易感性的关联研究

目的探讨白细胞介素12B(IL-12B)基因多态性与肝硬化易感性的关联。方法收集肝硬化患者173例作为研究组,其生物学父母作为对照组。运用聚合酶链反应扩增及单核苷酸多态性的分子生物学技术,检测IL-12B基因rs15677380、rs14050311基因多态性,进行肝硬化与IL-12B基因多态性的关联分析和单体型相对风险率分析。结果 IL-12B基因单核苷酸多态性(SNP)位点rs15677380与肝硬化相关联(P=0.009),其中等位基因A为危险因素(Z=2.36),G是保护因素(Z=-2.36);rs14050311等位基因多态性与肝硬化相关联(P=0.013),其中等位基因C是保护因素(Z=-2.24),T为危险因素(Z=2.24)。rs15677380、rs14050311单体型的G/T、A/C与肝硬化有关联(P=0.021、0.015,Z=-1.85、2.16)。结论 IL-12B基因多态性与肝硬化的发生存在关联。

IL-12B基因多态性及单倍型与克罗恩病的关系研究

目的 探讨IL-12B基因多态性及单倍型与克罗恩病(CD)的关系。方法 选取94例CD患者(CD组)和106例健康体检者(对照组),采用改良多重高温连接酶检测反应技术检测IL-12B基因2个功能性单核苷酸多态性(SNP)位点rs3212227和rs6887695的等位基因及基因型,用Haploview 4.2软件进行连锁不平衡和单倍型分析,并分析IL-12B基因多态性及单倍型与CD的关系。结果 CD组与对照组比较,该2个IL-12B基因SNP位点的突变等位基因和基因型频率均无统计学差异(均P>0.05)。进一步亚组分析发现回肠型CD组患者rs6887695位点的突变C等位基因和GC+CC基因型频率均明显低于与对照组(28.75%vs 44.34%,P<0.05,OR=0.507,95%CI:0.291~0.882;50.00%vs 71.70%,P<0.05,OR=0.395,95%CI:0.186~0.836);而上述2个位点的等位基因及基因型频率分布在结肠病变(结肠型+回结肠型)CD组患者与对照组间比较均无统计学差异(均P>0.05)。此外,CD患者组内分层比较发现,与结肠病变CD组比较,回肠型CD组患者rs6887695位点的突变C等位基因、GC+CC基因型以及CC基因型频率亦均明显降低(28.75%vs 50.00%,P<0.05,OR=0.404,95%CI:0.218~0.745;50.00%vs 72.22%,P<0.05,OR=0.385,95%CI:0.163~0.908;7.50%vs27.78%,P<0.05,OR=0.150,95%CI:0.037~0.613)。经Haploview 4.2软件分析发现rs3212227和rs6887695 2个SNP位点之间存在中等强度连锁不平衡关系(D′=0.545,r2=0.235),但CD组与对照组比较,各单倍型的频率均无统计学差异(均P>0.05)。结论 IL-12B基因rs6887695位点多态性与CD的临床表型相关,该位点基因突变后可能降低回肠型CD的发病风险。

Association of IFNGR2 and IL-12B gene polymorphisms with susceptibility to hand,foot and mouth disease infected by EV71

Objective:To study the relationship between the single nucleotide polymorphisms(SNPs)of IFNGR2genes(rs9808753,rs11910627 and rs1532) and IL-12 B gene(rs2288831)and the susceptibility to hand,foot and mouth disease(HFMD)caused by enterovirus 71(EV71).Methods:Blood samples were collected from 145 HFMD children infected by EV71,104 children with EV71 covert infection,and 89 normal control children,followed by DNA extraction.IFNGR2 and IL-12 Bpolymorphisms were detected by imLDRTM.Results:Compared with the control group,IFNGR2rs9808753 genotype and allele distributions of EV71-infected group and EV71 covert infection group showed significant differences(P<0.05).A allele frequency in EV71-infected patients and covert EV71-infected patients was higher than that in the control group(P <0.05).While the genotype and allele frequencies of rs2288831 in IL-12 B did not show significant difference between EV71-infected groups and healthy controls.Conclusion:These findings suggested that the single nucleotide polymorphism of IFNGR2 gene site rs9808753(A/G)was associated with the susceptibility to EV71-infection,and A allele of rs9808753 might be one potential genetic susceptibility factor of EV71-infection.While the rs2288831(C/T)polymorphism of IL-12 Bdid not correlate with the susceptibility of EV71-infection.

IL-12B启动子序列多态性在Adamantiades-Behet病易感性中的作用:涉及Th1对血链球菌抗原的免疫反应性

Adamantiades-Behcet’s disease(ABD)is a chronic inflammatory multisystem disorder.Although the precise etiology is unclear,high prevalence of human leukocyte antigen(HLA)-B51 predisposition and predominantly involved T-helper type 1 cells(Th1)-type proinflammatory cytokines and extrinsic Streptococcal infection suggest a substantial association with an immunogenetic basis and strengthens the hypothesis that IL-12,a potent inducer of Th-1 immune reaction,is a putative candidate in its pathogenesis.These clinicopathological findings led us to examine interleukin 12 p40(IL-12B)promoter polymorphism,for which the 4-base pair(bp)heterozygous insertion has been shown to affect the gene transcription and subsequent protein production.We analyzed IL-12B promoter genotypes in 194 Japanese subjects(92 with ABD and 102 normal controls)-by PCR-based restriction enzyme digestion.The frequency of the insertion heterozygosity was significantly higher in patients than in controls(49/92,53.3%vs 39/102,38.2%,respectively)-Comparing these with HLA haplotype data,this trend was more significant in HLA-B51-negative patients(29/42,69.0%vs 20/50,40.0%;P=0.005).As assessed by semiquantitative reverse transcription-PCR and ELISA,stimulation with Streptococcal antigens specifically increased expression of IL-12 p40 mRNA and protein,in conjunction with IL-12 p70 induction,in peripheral blood mononuclear cells from heterozygous patients.Our results provide evidence for anti-bacterial host response toward Th1-immunity mediated by IL-12 in patients with ABD,and the possible insight into the genetic susceptibility that is independent of HLA background.

广西肝细胞癌与TGF-β1及IL-12B基因多态性关系

目的探讨广西地区肝细胞癌遗传易感性与人群转化生长因子β1(TGF-β1)基因和白细胞介素12B(IL-12B)基因单核苷酸多态性关系。方法采用以医院为基础的病例对照研究,选取广西户籍的新发肝细胞癌患者608例,选取相同户籍地、年龄、性别和民族频数匹配的非肿瘤患者612例作为对照,采用TaqMan MGB实时荧光定量PCR方法检测TGF-β1 rs1800469(-509 C>T)位点和IL-12B rs3212227(3’UTR+1188A>C)位点基因单核苷酸多态性,比较不同基因型与肝细胞癌患病风险的关系。结果对照组IL-12B基因rs3212227位点的C突变等位基因频率为43.5%,病例组为48.9%,差异有统计学意义(P<0.05);与IL-12B基因rs3212227位点AA基因型相比,携带rs3212227 AC杂合子及携带rs3212227 CC突变基因型的个体发生原发性肝细胞癌的风险明显升高(分别校正OR=1.271,95%CI=0.976～1.655;校正OR=1.515,95%CI=1.092～2.102);IL-12B基因rs3212227位点AC+CC基因型可增加女性和<55岁者罹患肝细胞癌的风险(分别校正OR=2.036,95%CI=1.169-3.548;校正OR=1.529,95%CI=1.129～2.071);肝细胞癌患病风险与TGF-β1基因rs1800469位点多态性无明显关联。结论 IL-12B基因rs3212227位点与广西地区人群原发性肝细胞肝癌发病风险明显关联。

儿童激素敏感性肾病综合征的临床过程与功能性IL-12B启动子基因多态性相关

激素敏感性肾病综合征是儿童最常见的肾小球疾病。临床学者根据患儿对激素治疗的反应类型及过程而确定其临床分型，激素依赖患儿其临床过程更复杂，更需要强化免疫抑制治疗。虽然有文献报道可能细胞因子介导了激素依赖的过程，但其确切的临床过程尚不十分清楚。白细胞介素12（IL-12）是决定免疫反应类型的重要因子。

白介素-12B基因多态性与原因不明复发性流产的易感性研究

目的:探讨IL-12B基因启动子区多态性与山东潍坊地区汉族育龄期妇女原因不明复发性流产(URSA)的相关性。方法:采用直接测序法检测83例原因不明复发性流产孕妇和90例正常孕妇IL-12B基因的启动子区的多态位点,并分析IL-12B基因多态性与原因不明复发性流产的关系。结果:IL-12B的启动子区检测到2个单核苷酸多态性(SNPs)(-671G/T和-405G/T)。2个SNPs紧密连锁,多态性分布符合Hardy-Weinberg平衡。URSA组和对照组的基因型和等位基因频率分布比较,差异无统计学意义(P>0.05)。单体型分析显示,-671T/-405G频率在URSA组和正常对照组分别为0.65和0.41,URSA组显著高于正常对照组,差异有统计学意义(P<0.05)。结论:正常孕妇IL-12B基因启动子区存在多态性变异,其中-671G/T和-405G/T构成的单体型-671T/-405G可能与URSA的易感性有关。

膀胱癌组织中白细胞介素-12B基因启动子区甲基化的变化及其意义

目的研究膀胱癌组织中白细胞介素-12B基因(IL-12B)启动子区甲基化的变化及其临床意义.方法应用甲基化特异性聚合酶链反应、Western-blot检测膀胱癌及癌旁组织78例,比较IL-12B基因启动子区甲基化及其蛋白质与膀胱癌发生发展的关系.结果 (1)膀胱癌组织IL-12B启动子区甲基化产物明显多于癌旁组织,差异有统计学意义(χ2=14.8,P=0.001);(2)膀胱癌组织和癌旁组织IL-12B启动子区甲基化产物的PMR水平差异有统计学意义(t=3.42,P=0.001);(3)膀胱癌组织IL-12B蛋白的表达水平显著低于癌旁组织(t=2.832,P=0.012).结论 IL-12B基因启动子区甲基化及其编码蛋白质的失活与膀胱癌的发生相关.

Genetic associations of inflammatory bowel disease in a South Asian population

AIM To estimate prevalence and phenotypic associations of selected inflammatory bowel disease(IBD)-associated genetic variants among Sri Lankan patients. METHODS A case study of histologically confirmed ulcerative colitis(UC) or Crohn's disease(CD) patients with ≥ 1 year disease duration, who were compared to unrelated, gender-matched, healthy individuals as controls, was conducted at four major centers in Sri Lanka. Phenotypic data of the cases were obtained and all participants were genotyped for 16 selected genetic variants: IL12 B :rs1045431, IL23 R :rs11805303, ARPC2 :rs12612347, IRGM :rs13361189, IL26/IL22 :rs1558744, CDH1 :rs1728785, IL10 :rs3024505, FCGR2 A :rs3737240, PTGER4 :rs4613763, IL17 REL/PIM3 :rs5771069, HNF4 a :rs6017342, STAT3 :rs744166, SMURF1 :rs7809799, LAMB1 :rs886774, HLA-DRB5, DQA1, DRB1, DRA :rs9268853, MST1, UBA7, and APEH :rs9822268. The genotypes of all variants were in Hardy-Weinberg Equilibrium(P > 10^(-3)). To account for multiple hypothesis testing, P-values < 0.003 were considered significant.RESULTS A total of 415 patients and 465 controls were recruited. Out of the single nucleotide polymorphisms(SNPs) tested, the majority were not associated with IBD in Sri Lankans. Significant positive associations were noted between rs886774(LAMB1-gene) and UC(odds ratio(OR) = 1.42, P = 0.001). UC patients with rs886774 had mild disease(OR = 1.66, P < 0.001) and remained in remission(OR = 1.48, P < 0.001). A positive association was noted between rs10045431(IL 12 B gene) and upper gastrointestinal involvement in CD(OR = 4.76, P = 0.002). CONCLUSION This confirms the heterogeneity of allelic mutations in South Asians compared to Caucasians. Most SNPs and disease associations reported here have not been described in South Asians.

促吞噬肽衍生物TP对树突状细胞功能的影响

目的:探讨促吞噬肽衍生物TP对树突状细胞(DC)功能的影响。方法:分离、提纯小鼠骨髓来源DC,培养至第3 d弃上清,去除悬浮细胞,加入新鲜培养液,补充细胞因子,之后隔天半量换液,至第7 d获得DC;分别用TP和LPS刺激DC,Wright-Gimsa染色,用倒置显微镜观察细胞生长情况;流式细胞分析细胞表面分子CD80、CD83、CD86及CD11c的表达,鉴定细胞成熟度;q RT-PCR分析TP对DC分泌白细胞介素12b(IL-12b)的影响。结果:光镜及Wright-Gimsa染色的细胞形态学结果都显示TP可促进DC增殖及成熟,流式分析证明了这一结果,同时TP还促进DC大量分泌IL-12b。结论:TP不仅能促进DC增殖及成熟,还能影响DC的IL-12b表达;DC有可能是TP发挥抗癌作用的靶细胞之一。