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作 者:钱小兵[1,2] 程腊梅[2,3] 谢毓滨[4] 周佳[2] 金文静[2] 卢光琇[2,3]
机构地区:[1]中国科学院研究生院,北京100049 [2]人类干细胞国家工程研究中心,长沙410078 [3]中南大学生殖与干细胞工程研究所,长沙410078 [4]长沙血液中心,长沙410001
出 处:《现代免疫学》2009年第6期497-500,共4页Current Immunology
基 金:国家重点基础研究发展计划资助项目(2007CB948103)
摘 要:探讨HLA-A、-B和-DRB1位点等位基因多态性与原因不明习惯性流产的相关性。应用PCR-SSP方法对175对(350例)湖南汉族原因不明习惯性流产(URSA)患者夫妇进行HLA-A、-B、-DRB1基因分型,并以2 000例(男女各1 000例)湖南无关健康汉族个体造血干细胞分型资料作为对照,分析HLA等位基因频率在两组中的分布差异。结果是HLA-A、-B及-DRB1位点各等位基因频率在对照组男女中均无显著差异(P>0.05);URSA患者组A*31(2.86%)、B*08(0.86%)、B*39(4.14%)和B*56(1.86%)的等位基因频率显著高于对照组(RR值分别为2.07、2.99、1.56和2.19;P值分别为0.0059、0.0276、0.0404和0.0172);在URSA妻子组中,B*39(4.57%)显著高于对照组(RR=1.75;P=0.0474),A*33(3.71%)、B*58(3.14%)和DRB1*03(2.29%)的等位基因频率明显低于对照组(RR值分别为0.57、0.51和0.50;P值分别为0.0339、0.0182和0.0383);A*31(3.14%)、B*08(1.43%)、B*52(2.29%)及B*56(2.29%)在URSA丈夫组中的等位基因频率均高于对照组(RR值分别为2.32、5.08、2.31和2.77;P值分别为0.013、0.0012、0.0374及0.0105)。结果表明湖南汉族人群中A*31、B*08、B*39、B*52和B*56可能是URSA的易感等位基因,而A*33、B*58和DRB1*03可能对URSA的发生有保护作用。To investigate the association between the HLA-A, B and -DRB1 polymorphism and the unexplained recurrent spon taneous abortions (URSA), the HLA-A, -13 and - DR131 genotyping of 175 couples (350 individuals) with URSA were inves tigated by polymerase chain reaction sequence specific primers (PCR SSP) method. The allele frequencies (AFs) of HLA-A,B and -DRB1 of the patients were calculated and compared with the control group (2 000 normal health individuals, 1 000 male and 1 000 female) using a chisquare test. h was found that there was no significantly difference between the male and female AFs in the control group. The AFs of A * 31(2.86%), B * 08(0.86 %), B * 39(4.14%) and B * 56(1.86%) were significant ly higher in the URSA patients than those in controls (RR=2.07, 2.99, 1.56, 2. 19; P=0. 0059, 0. 0276, 0. 0404, 0. 0172 respectively). When the patients group was divided into wife group and husband group, B * 39 (AF= 4.57%, RR= 1.75,P= 0. 0474 ) was significantly increased in the URSA wife group, while A * 33 (3.71 % ), B * 58 (3.14% ) and DRB1 * 03 (2.29 % ) were significantly decreased (RR=0.57, 0. 51, 0. 50; P = 0. 0339, 0. 0182, 0. 0383 respectively). The AFs of A * 31 (3. 14 % ), B * 08 (1.43 % ), B * 52 (2.29 % ) and B * 56 (2.29 % ) in the URSA husband group were strikingly higher than those in controls (RR=2.32, 5.08, 2.31, 2.77;P=0. 013, 0. 0012, 0. 0374, 0. 0105 respectively). Our data suggest that HLA-A 31, B * 08, B* 39, B* 52 and B* 56 may contribute to the genetic susceptibility to URSA, while A* 33, B* 58 and DRB1 *03 may play the protective role.
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