Tissue factor (F3) gene variants and thrombotic risk among middle-aged and older adults: A population-based cohort study

Q4 Medicine Thrombosis Update Pub Date : 2024-09-28 DOI:10.1016/j.tru.2024.100190

Eric Manderstedt , Christina Lind-Halldén , Christer Halldén , Johan Elf , Peter J. Svensson , Gunnar Engström , Olle Melander , Aris Baras , Luca A. Lotta , Bengt Zöller , for the Regeneron Genetics Center

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Abstract

Background

Tissue factor (TF), encoded by the F3 gene, is the main initiator of blood coagulation. The molecular epidemiology of the F3 gene and the relation to venous thromboembolism (VTE) remains to be determined.

Objectives

The aim was to determine the molecular epidemiology and the importance of F3 variants for incident VTE by analysis of the population-based MDC study (Malmö Diet and Cancer), consisting of unselected middle-aged and older individuals.

Methods

The exons of F3 were analyzed in a total of 28,794 individuals from the MDC cohort, and of these, 2584 (9 %) were affected by VTE during follow‐up (1991–2018). Qualifying variants used in gene-collapsing analysis were defined as loss-of-function or non-benign (PolyPhen-2) missense variants with minor allele frequency less than 0.1 %.

Results

Exon sequencing of the F3 gene identified 61 different variants, 3′ UTR variants (n = 5), 5′ UTR variants (n = 9) synonymous (n = 10), in frame insertion (n = 1), splice region variants (n = 2), missense (n = 33) or loss-of-function variants (n = 1). No associations between common F3 gene variants and incident VTE were found. Seventeen rare variants were classified as qualifying and included in collapsing analysis (16 non-benign missense and 1 loss-of-function variants). The prevalence of F3 qualifying variants was 0.14 %. Seven individuals with F3 qualifying variants had VTE, while 34 individuals had no VTE. The adjusted VTE model was significant (hazard ratio = 2.1 [95 % confidence interval, 1.02–4.48], P-value = 0.045).

Conclusions

Qualifying F3 gene variants are very rare, indicating a constrained gene. Rare but not common variation in the F3 gene may be involved in VTE.

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组织因子 (F3) 基因变异与中老年人血栓风险：基于人群的队列研究

背景F3基因编码的组织因子（TF）是血液凝固的主要启动因子。目的通过分析以人口为基础的 MDC 研究（马尔默饮食与癌症研究），确定分子流行病学以及 F3 变体对 VTE 事件的重要性，该研究由未经筛选的中老年人组成。方法分析了MDC队列中28794人的F3外显子，其中2584人（9%）在随访期间（1991-2018年）受到VTE影响。用于基因重组分析的合格变异被定义为功能缺失或非良性（PolyPhen-2）错义变异，其小等位基因频率低于 0.1%。结果 F3 基因的外显子测序发现了 61 个不同的变异，包括 3′ UTR 变异（n = 5）、5′ UTR 变异（n = 9）、同义变异（n = 10）、框内插入变异（n = 1）、剪接区变异（n = 2）、错义变异（n = 33）或功能缺失变异（n = 1）。未发现常见的F3基因变异与VTE事件之间存在关联。17个罕见变异被归类为合格变异并纳入折叠分析（16个非良性错义变异和1个功能缺失变异）。F3合格变异的发生率为0.14%。7名F3合格变异体患者出现了VTE，34名患者未出现VTE。调整后的 VTE 模型具有显著性（危险比 = 2.1 [95 % 置信区间，1.02-4.48]，P 值 = 0.045）。F3 基因中罕见但不常见的变异可能与 VTE 有关。

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