Abstract

Thrombophilia refers to a group of conditions where the blood clots more easily than normal. These blood clots can cause problems such as deep vein thrombosis or pulmonary embolism. Most kinds of mutated coagulation factors II (F2) exhibit lower procoagulant activity, but in some cases, a higher coagulation rate has been observed. The underlying mechanism is that those variations can prevent F2s from being inhibited by antithrombin, leading to a contiguous activation of procoagulation, and causing recurrent thromboembolism. In this study, a patient was admitted to our hospital due to repeated chest pain for 2 days and aggravated for 4 h. A medical history investigation showed that he had three deep venous thromboses in the lower limbs and one portal vein thrombosis events during the past 10 years. The electrocardiogram showed Q wave elevation and slight ST segment elevation in lead V2, and coronary angiogram showed a total occlusion of the left anterior descending artery. Laboratory testing found that troponin I was obviously elevated. Family history also indicated that both his father (II-3) and grandfather (I-1) died from pulmonary thromboembolism. Whole-exome sequencing was performed to detect the genetic lesion of the patient, and a novel mutation (c.1621 C>T/p.R541W) of F2 was identified in the patient. This novel mutation resulted in a substitution of arginine by tryptophan, leading to antithrombin resistance (ATR). Our study is consistent with previously published papers. In conclusion, this study not only identifies a novel mutation of F2 and will contribute to the genetic diagnosis and counseling of families with thrombosis but also suggests that the site p.R541 of F2 may play a crucial role in thrombosis.

Highlights

  • Thrombophilia is an increased tendency to form abnormal blood clots in blood vessels (Lim and Moll, 2015; Stevens et al, 2016; Skelley et al, 2017)

  • In the The Human Gene Mutation Database (HGMD) database, 70 mutations of coagulation factor II (F2) have been identified in patients

  • The mutation Belgrade (p.R596Q) of F2 can lead to pulmonary embolism, acute mesenteric vein thrombosis and myocardial infarction

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Summary

INTRODUCTION

Thrombophilia is an increased tendency to form abnormal blood clots in blood vessels (Lim and Moll, 2015; Stevens et al, 2016; Skelley et al, 2017). A medical history investigation showed that he had had three deep venous thromboses in the lower limbs and one portal vein thrombosis events during the past 10 years His electrocardiogram showed Q wave elevation and slight ST segment elevation in lead V2 (Figure 1B). The mutation identified in the proband was absent in all available healthy relatives included in this study, but it was not tested in the two deceased symptomatic relatives (father and paternal grandfather) This new mutation (p.R541W), resulting in a substitution of arginine by tryptophan, was located in a highly evolutionarily conserved site (Figure 1F) and was absent in our 200 local control subjects (Fan et al, 2018). A previous in vitro study proved that this mutation (p.R541W) may substantially impaire inactivation by antithrombin, resulting in a prolonged clotting function and leading to an ATR phenotype, which further proved that the mutation may be a high risk factor for thrombosis (Tamura et al, 2017)

DISCUSSION
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