凝血因子XII 46 C/T多态性的基因分型分析及因子XII活性在复发性流产患者中的作用
Genotyping analysis for the 46 C/T polymorphism of coagulation factor XII and the involvement of factor XII activity in patients with recurrent pregnancy loss.
作者信息
Asano Eriko, Ebara Takeshi, Yamada-Namikawa Chisato, Kitaori Tamao, Suzumori Nobuhiro, Katano Kinue, Ozaki Yasuhiko, Nakanishi Makoto, Sugiura-Ogasawara Mayumi
机构信息
Department of Obstetrics and Gynecology, Nagoya City University, Graduate School of Medical Sciences, Nagoya, Japan.
Occupational and Environmental Health, Nagoya City University, Graduate School of Medical Sciences, Nagoya, Japan.
出版信息
PLoS One. 2014 Dec 9;9(12):e114452. doi: 10.1371/journal.pone.0114452. eCollection 2014.
BACKGROUND
Established causes of recurrent pregnancy loss (RPL) include antiphospholipid syndrome, uterine anomalies, parental chromosomal abnormalities, particularly translocations and abnormal embryonic karyotype. A systematic review concluded that coagulation factor XII (FXII) deficiency was associated with RPL. However, it could not be established whether the 46 C/T SNP of FXII or low activity of FXII was a risk factor for RPL, because of the small sample size.
METHODS AND FINDINGS
We conducted a cross-sectional and cohort study in 279 patients with two or more unexplained consecutive pregnancy losses and 100 fertile women. The association between the lupus anticoagulant (LA) activity and FXII activity was examined. The frequency of the CC, CT and TT genotypes and the FXII activity were also compared between the patients and controls. Subsequent miscarriage rates among the CC, CT, TT genotypes and according to the FXII activity was examined. LA was associated with reduced FXII activity. The CT, but not the TT, genotype was confirmed to be a risk factor for RPL in the cross-sectional study using multivariate logistic regression analysis (OR, 2.8; 95% CI, 1.37-5.85). The plasma FXII activity in the patients was similar to that in the controls. Neither low FXII activity nor the CT genotype predicted the subsequent pregnancy outcome in the cohort study. On the other hand, and intermediate FXII activity level of 85-101% was predictive of subsequent miscarriage.
CONCLUSIONS
Low FXII activity was not associated with RPL. The FXII gene was found to be one of the significant susceptibility genes for RPL, similar to the FV Leiden mutation. However, the clinical influence of the CT genotype might be relatively small, because the presence/absence of this genotype did not have any predictive value for the subsequent pregnancy outcome. This was the first study indicating the influence of FXII 46C/T on further pregnancy outcomes.
背景
复发性流产(RPL)的既定病因包括抗磷脂综合征、子宫异常、父母染色体异常,尤其是易位和胚胎核型异常。一项系统评价得出结论,凝血因子XII(FXII)缺乏与RPL有关。然而,由于样本量小,无法确定FXII的46 C/T单核苷酸多态性(SNP)或FXII低活性是否为RPL的危险因素。
方法与结果
我们对279例有两次或更多次不明原因连续流产的患者和100例有生育能力的妇女进行了横断面和队列研究。检测了狼疮抗凝物(LA)活性与FXII活性之间的关联。还比较了患者和对照组中CC、CT和TT基因型的频率以及FXII活性。研究了CC、CT、TT基因型以及根据FXII活性的后续流产率。LA与FXII活性降低有关。在横断面研究中,使用多因素逻辑回归分析(比值比[OR],2.8;95%置信区间[CI],1.37 - 5.85)证实CT基因型而非TT基因型是RPL的危险因素。患者的血浆FXII活性与对照组相似。在队列研究中,低FXII活性和CT基因型均不能预测后续妊娠结局。另一方面,FXII活性水平为85%至101%的中间值可预测后续流产。
结论
FXII低活性与RPL无关。发现FXII基因是RPL的重要易感基因之一,类似于凝血因子V莱顿突变。然而,CT基因型对临床的影响可能相对较小,因为该基因型的有无对后续妊娠结局没有任何预测价值。这是第一项表明FXII 46C/T对进一步妊娠结局有影响的研究。
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