In a previous study it was shown that lower factor XI (FXI) levels in women with heavy menstrual bleeding (HMB). Our aim was to determine the single-nucleotide variants (SNVs) in the F11 gene in women with HMB. In addition, an extensive literature search was performed to determine the clinical significance of each SNV. Patients referred for HMB (PBAC-score >100) were included. With direct sequencing analysis of all 15 exons and flanking introns of the F11 gene, 29 different non-structural SNVs were detected in 49 patients with HMB. Interestingly, most of these SNVs have previously been associated with venous thrombosis instead of bleeding. These findings have not helped to elucidate the molecular basis of HMB. They also question the specificity of previously reported F11 variations in patients with thrombosis. More studies are needed to explain the lower FXI levels seen in patients with HMB. IMPACT STATEMENT Women with mild deficiencies of factor XI (FXI) (< 70%) are prone to excessive bleeding during menstruation. Bleeding manifestations are not well correlated with plasma FXI levels and bleeding episodes can vary widely among patients with similar low FXI levels. In a previous study we showed that women with heavy menstrual bleeding (HMB) had normal, but on average, lower levels of FXI than controls. In light of these findings, we performed F11 gene analysis to determine the single-nucleotide variants (SNVs) in women with HMB and performed an extensive literature search to determine the clinical significance of each SNV. By direct sequencing analysis of the F11 gene we found 29 different non-structural SNVs in 49 women with heavy menstrual bleeding. Remarkably, a number of these SNVs have previously been implicated in thrombosis. These findings have not helped to elucidate the molecular basis of lower FXI levels in HMB. They also question the specificity of previously reported F11 variations in patients with thrombosis. More studies are needed to explain the lower FXI levels seen in patients with HMB.

译文

在先前的研究中,显示月经大量出血 (HMB) 女性的因子XI (FXI) 水平较低。我们的目的是确定HMB女性F11基因中的单核苷酸变体 (snv)。此外,还进行了广泛的文献检索,以确定每种SNV的临床意义。纳入HMB转诊的患者 (PBAC评分> 100)。通过对F11基因的所有15个外显子和侧翼内含子的直接测序分析,在49例HMB患者中检测到29种不同的非结构性snv。有趣的是,这些snv中的大多数以前都与静脉血栓形成有关,而不是出血。这些发现无助于阐明HMB的分子基础。他们还质疑先前报道的血栓形成患者F11变异的特异性。需要更多的研究来解释HMB患者中较低的FXI水平。影响声明轻度缺乏因子XI (FXI) (<  70%) 的女性在月经期间容易出血过多。出血表现与血浆FXI水平没有很好的相关性,在FXI水平相似的患者中,出血发作可能有很大差异。在先前的研究中,我们表明,月经大量出血 (HMB) 的女性FXI水平正常,但平均而言,低于对照组。根据这些发现,我们进行了F11基因分析以确定HMB女性的单核苷酸变异体 (SNV),并进行了广泛的文献检索以确定每种SNV的临床意义。通过对F11基因的直接测序分析,我们在49名月经大量出血的女性中发现了29种不同的非结构性snv。值得注意的是,这些snv中的许多以前都与血栓形成有关。这些发现无助于阐明HMB中FXI水平较低的分子基础。他们还质疑先前报道的血栓形成患者F11变异的特异性。需要更多的研究来解释HMB患者中较低的FXI水平。

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