Homozygous factor Ⅴ Leiden mutation in type Ⅳ Ehlers-Danlos patient

Ehlers-Danlos syndrome(EDS) is a group of inherited connective tissue disorders caused by collagen synthesis defects. Several hemostatic abnormalities have been described in EDS patients that increase the bleeding tendencies of these patients. This case report illustrates a patient with an unusual presentation of a patient with type Ⅳ EDS, platelet δ-storage pool disease and factor Ⅴ Leiden mutation. Young woman having previous bilateral deep vein thrombosis and pulmonary emboli coexisting with ruptured splenic aneurysm and multiple other aneurysms now presented with myocardial infarction. Presence of factor Ⅴ Leiden mutation raises the possibility that the infarct was due to acute coronary thrombosis, although coronary artery aneurysm and dissection with myocardial infarction is known to occur in vascular type EDS. This is the first report in the medical literature of factor Ⅴ Leiden mutation in an EDS patient which made the management of our patient challenging with propensity to both bleeding and clotting.

Mesenteric vein thrombosis in a patient heterozygous for factor Ⅴ Leiden and G20210A prothrombin genotypes

Mesenteric venous thrombosis(MVT)is a rare but life threatening form of bowel ischemia.It is implicated in 6%-9% of all cases of acute mesenteric ischemia.The proportion of patients with primary(or idiopathic)MVT varies from 0% to 49%,with a decrease in frequency secondary to more recent availability of newer investigations for hypercoagulability.The presence of factor Ⅴ Leiden(FVL)and prothrombin G20210A mutations(PGM)have been well documented in these cases.However,there have been scarce case reports describing MVT in heterozygotes of both these mutations occurring simultaneously and its implications on long term management.Our case describes acute MVT in a previously asymptomatic young patient with no prior history of venous thromboembolism.The patient was found to be heterozygous for FVL and PGM and treated with lifelong anticoagulation with warfarin(goal international normalized ratio:2-3)and avoidance of hormonal contraceptives.

Prevention of thromboembolic events after radical prostatectomy in patients with hereditary thrombophilia due to a factor V Leiden mutation by multidisciplinary coagulation management

Objective:To examine the perioperative impact of factor V Leiden mutation on thromboembolic events'risk in radical prostatectomy(RP)patients.With an incidence of about 5%,factor V Leiden mutation is the most common hereditary hypercoagulability among Caucasians and rarer in Asia.The increased risk of thromboembolic events is three-to seven-fold in heterozygous and to 80-fold in homozygous patients.Methods:Within our prospectively collected database,we analysed 33006 prostate cancer patients treated with RP between December 2001 and December 2020.Of those,patients with factor V Leiden mutation were identified.All patients received individualised recommendation of haemostaseologists for perioperative anticoagulation.Thromboembolic complications(deep vein thrombosis and pulmonary embolism)were assessed during hospital stay,as well as according to patient reported outcomes within the first 3 months after RP.Results:Overall,85(0.3%)patients with known factor V Leiden mutation were identified.Median age was 65(interquartile range:61-68)years.There was at least one thrombosis in 53(62.4%)patients and 31(36.5%)patients had at least one embolic event in their medical history before RP.Within all 85 patients with factor V Leiden mutation,we experienced no thromboembolic complications within the first 3 months after surgery.Conclusion:In our cohort of patients with factor V Leiden mutation,no thromboembolic events were observed after RP with an individualised perioperative coagulation management concept.This may reassure patients with this hereditary condition who are counselled for RP.

Frequency of the C677T Polymorphism of MTHFR, G20210A of Prothrombin and R506Q of Factor V Leiden in Type 2 Diabetics in Abidjan

In Africa, the prevalence of diabetes is escalating and remains a concern due to the numerous complications it causes. Vascular damage associated with diabetes leads to a prothrombotic state observed in diabetic individuals. Diabetes is a complex and multifactorial disease involving genetic components. With the aim of preventing complications and contributing to an efficient management of diabetes, we investigated genes likely to lead to a risk of thrombosis, in particular the C677T of MTHFR, G20210A of prothrombin, and R506Q of factor V Leiden in type 2 diabetics in Abidjan receiving ambulatory care. A descriptive cross-sectional study was carried out on consenting type 2 diabetic patients. Mutation detection was carried out using the PCR-RFLP method employing restriction enzymes. Hemostasis tests (fibrinogen, D-dimers, fibrin monomers, and von Willebrand factor) were performed using citrate tubes on the Stage? Star Max automated system. Plasminogen activator inhibitor was assayed by ELISA method, and biochemical parameters were determined using the COBAS C311. The study population consisted of 45 diabetic patients, 51.1% of whom presented vascular complications, mainly neuropathy. Disturbances in hemostasis parameters were observed, with 15.5% of patients showing an increase in fibrin monomers. Mutation analysis revealed an absence of factor V mutation (factor V Leiden) and of G20210A mutation of the prothrombin gene. However, 15.6% of subjects had a heterozygous C677T mutation of MTHFR, with 57% of them being anemic. The exploration of biological and genetic factors associated with thrombotic risk is of significant interest in the optimal management of African type 2 diabetics.

凝血因子Ⅴ Leiden突变检测对肺血栓栓塞症的预测价值

目的探讨我国东北地区肺血栓栓塞症(PTE)患者中凝血因子ⅤLeiden突变(FVL)的发生频率。方法病例组是81例经螺旋CT肺动脉造影(CTPA)或核素肺灌注显像结合临床症状确诊的PTE患者,对照组是81例年龄、性别相匹配,来自相同地区的健康人群。采用聚合酶链式反应(PCR)对实验组及对照组抽提出的DNA片段进行扩增,对确认扩增成功的PCR产物,用HindⅢ限制酶进行酶切,酶切产物行琼脂糖凝胶电泳检测FⅤL基因突变情况。结果两组凝血因子Ⅴ基因经HindⅢ酶切后,均仅出现241 bp一条带,FⅤL发生频率为0%,病例组与对照组相比无显著差异(P>0.05),病例组及对照组均未发现凝血因子V基因杂合子及纯合子突变。结论凝血因子ⅤLeiden突变在我国东北地区发生率低,可能对我国东北地区人群PTE诊断没有预测价值。

国人布-加综合征与FⅤ Leiden突变的相关研究

目的 :探讨国人布 -加综合征 (BCS)与凝血第 因子 L eiden(F L)突变的相关性。方法 :收集 2 9例国人BCS(其中 2 5例为散发 BCS、4例为家族性 BCS)和 2 9名健康对照者 ,并对其血样进行 PCR- RFL P的 F L 突变分析。结果 :2 9例 BCS中 ,共有 3例 F L 突变阳性 ,均为家族性 BCS病例。其中家系 A姐妹均有 F L 突变 ,家系 B妹妹突变阳性 ,均为杂合性突变。散发病例无 1例阳性。对照组无 1例阳性。 2 9例国人 BCS中 ,F L 突变频率为0 .0 5 17,而 4例家族性 BCS的 F L 突变频率则为 0 .375 0。2 9例 BCS病例组与 2 9例对照组间 F L 突变频率无统计学差别 ,但家族性 BCS病例组与对照组间 F L 突变频率有显著统计学差别。结论 :国人家族性 BCS与 F L 突变相关 ,国人散发性 BCS与 F L

FⅤ Leiden突变与缺血性卒中

F Ⅴ Leiden突变可导致活化蛋白C抵抗现象,是引起白种人静脉血栓栓塞的最常见遗传因素。但对这一突变与缺血性卒中的关系尚存有争议。文章综述了F Ⅴ Leiden突变的分子机制及近年来在缺血性卒中方面的研究情况。

凝血因子ⅤLeiden突变的群体遗传学研究

凝血因子 { Factor ,F ) L eiden突变是引起遗传性静脉血栓病的病因之一。近年的研究表明 F L eiden突变的发生率在不同种族人群中存在明显差异 ,引起了各国学者的广泛关注和兴趣。本文就 F L eiden突变的世界群体分布、起源。

Mesenteric and portal vein thrombosis associated with hyperhomocysteinemia and heterozygosity for factor V Leiden mutation

A 79-year-old man was hospitalized because of worsening upper abdominal pain which started two days before admission and was continuously present. His personal and family historywas uneventful, he did not smoke and denied toxic habits or using any medications, including overthe-counter medications, herbal remedies or any vitamin supplements.

Down Regulated Protein C Plasma Levels in the Absence of Factor V Leiden Mutation in HIV Patients: An Observational Study in Maiduguri, North-Eastern Nigeria

Background: As life expectancy of HIV-infected patients increases with use of highly active antiretroviral therapy (HAART), protean haematologic manifestation including decreased activity of natural anticoagulants such as protein C may occur in the absence of genetic risk factors. Based on this preposition, we assessed the plasma level of protein C, and prevalence of factor V Leiden mutation among HIV-infected individuals. Our cohort consisted of 499 HIV-infected patients, of which 250 had AIDS, while 249 were either asymptomatic or had minor mucocutaneous infection consistent with WHO clinical stages I and II without features of AIDS. We also evaluated 251 healthy, HIV-negative subjects as controls. All participants were tested for plasma protein C levels and factor V Leiden (FVL) mutation (Arg 506 Gln) by automation and amplification created restriction enzyme site (ACRES) polymerase chain reaction, respectively. The prevalence of reduced protein C plasma levels among HIV positive patients was 20%;it was more prevalent among those that had AIDS compared with those without features of AIDS, but within WHO clinical stage I and II, (93.3% vs 6.7%) respectively. None of the control patients had either reduced protein C nor FVL mutation. All participants that demonstrated reduced protein C plasma levels demonstrated normal FVL genotype (1691G/G). Conclusion: Decreased protein C plasma levels can occur in HIV-infected patients in the absence of factor V Leiden mutation. The risk increases with severity of the disease. Deranged protein C plasma level increases the risk of hypercoagulable state in patients with advanced HIV disease;it should be considered among the causes of thrombo embolism in this group of patients.

Prevalence of factor V Leiden and prothrombin G20210A in patients with gastric cancer

AIM： To analyze the prevalence of the two commonest thrombophilic mutations, factor V Leiden and prothrombin G20210A, in patients with gastric cancer. METHODS： One hundred and twenty-one patients with primary gastric carcinoma and 130 healthy subjects, comparable for age and sex, were investigated. Factor V Leiden was detected by using polymerase chain reaction and restriction enzyme digestion, and prothrombin G20210A gene mutation by allele-specific PCR. RESULTS： Among the 121 cancer patients, factor V Leiden was found in 4 cases （GA genotype： 3.3%） and prothrombin G20210A in 10 cases （GA genotype： 8.3%）. Of the 130 control subjects, factor V Leiden was detected in 6 cases （GA genotype： 4.6%） and prothrombin G20210A in 8 cases （GA genotype： 6.1%）. No double heterozygous carriers of both mutations were found in either group. The prevalence of both factor V Leiden and prothrombin G20210A variant was not statistically different between the cancer patients and the healthy subjects. CONCLUSION： Our study suggests that, in gastric cancer, the risk factors of thrombophilic cancer state are on acquired rather than on a genetic basis and that prothrombin G20210A does not seem to be a cofactor in gastric cancer pathogenesis.

Effect of Factor V Leiden on Thrombosis in Childhood Leukemia

Thromboembolism is an important complication in children undergoing therapy for ALL as it has the potential to impact adversely on both their survival and quality of life. The incidence of thrombosis in children with ALL varies between 1.1% and 36.7% and the actual mean is 3.2%. The aim of our study is to review the available reported data on the effect of FVL on thrombotic risk in pediatric patients with acute leukemia.

口服避孕药与凝血因子的变化及因子Ⅴ基因突变的关系

目的 探讨国产复方口服避孕药 (COC)与凝血因子的变化及因子V基因突变的关系。方法 测定 14 1例健康妇女凝血因子Ⅱ、Ⅴ、Ⅶ、Ⅷ、Ⅹ活性 ;分析女性脑卒中患者因子Ⅴ基因多态性。结果 炔诺酮组和炔诺孕酮组凝血因子X活性均数均显著高于对照组 (97 0 8± 14 78,P <0 0 5 ;98 5 8± 13 2 8,P <0 0 1) ;炔诺酮组凝血因子Ⅷ活性均显著高于对照组 (15 0 96± 5 7 11,P <0 0 5 ) ;二服药组凝血因子Ⅱ、Ⅴ、Ⅶ活性均数与对照组相似 ,差异无显著性 ;女性脑卒中患者中服避孕药者和非服避孕药者均未发现因子Ⅴ基因多态性。结论 长期服用国产低剂量COC对妇女的凝血因子有一些负面影响 ,不同避孕药的影响略有不同 ;COC不会引起中国妇女凝血因子ⅤLeiden突变。

Thrombosis and inflammatory bowel disease-the role of genetic risk factors

Thromboembolism is a significant cause of morbidity and mortality in patients with inflammatory bowel disease （IBD）. Recent data suggest thromboembolism as a disease-specific extraintestinal manifestation of IBD, which is developed as the result of multiple interactions between acquired and genetic risk factors. There is evidence indicating an imbalance of procoagulant, anticoagulant and fibrinolitic factors predisposing in thrombosis in patients with IBD. The genetic factors that have been suggested to interfere in the thrombotic manifestations of IBD include factor V Leiden, factor Ⅱ （prothrombin, G20210A）, methylenetetrahydrofolate reductase gene mutation （MTHFR, 6777T, plasminogen activator inhibitor type 1 （PAI-1） gene mutation and factor X Ⅲ （val34leu）. In this article we review the current data and future prospects on the role of genetic risk factors in the development of thromboembolism in TBD.

汉族人深静脉血栓形成患者FV Leiden突变检测

目的 ;探讨汉族人FV基因 16 91位点多态分布情况及FVLeiden突变与深静脉血栓形成的关系。方法 :利用聚合酶链反应和限制性片段长度多态性 (PCR RFLP)方法 ,检测 10 3例深静脉血栓形成 (DVT)患者与 10 6例正常对照的FVLeiden突变 ,并进行对比分析。结果 :2组FV基因第 16 91位点的基因型为G/G ,全部为野生型 ,未见突变类型。结论

FVLeiden和FIIG20210A与中国人群肺血栓栓塞症的相关性

目的:探讨凝血因子V基因突变(FVLeiden)和凝血酶原G20210A基因突变(FIIG20210A)与中国人群肺血栓栓塞症的关系。方法:选取45例经过核素肺灌注显像和(或)螺旋CT肺动脉造影(CTPA)确诊的肺血栓栓塞症患者为实验组,85例正常健康人群为对照组。对实验组和对照组分别进行凝血因子V基因突变和凝血酶原G20210A基因突变检测。结果:FVL和凝血酶原G20210A基因杂合子及纯合子突变在PTE患者组及对照组中基因型频率均为0,提示病例组及对照组上述基因型变异频率及突变等位基因频率均为0。结论:凝血因子V基因G1691A突变和凝血因子G20210A基因突变可能与中国人群肺血栓栓塞症无关。

利用标准回归方程建立分析因子氢化物发生-原子荧光光谱法直接测定As(Ⅲ)和As(Ⅴ)

根据As(Ⅲ)和As(Ⅴ)在HG-AFS仪器上的响应差别,利用As(Ⅲ)、As(Ⅴ)标准回归方程建立的分析因子,通过测定溶液中预还原前的荧光强度和预还原后的砷量,建立了一种高灵敏度、干扰少、快速、操作简便的HG-AFS法直接测定As(Ⅲ)和As(Ⅴ)的分析方法.对影响分析因子的各种仪器条件和共存离子干扰进行了试验,考察了样品中不同浓度As(Ⅲ)和As(Ⅴ)的测定精密度.方法的检出限As(Ⅲ)为0.050ng.ml-1,As(Ⅴ)为0.087ng.ml-1,相对误差为0.31%—19.2%,相对标准偏差为1.18%—20.96%.方法对水中As(Ⅲ)和As(Ⅴ)的测定相对标准偏差为7.55%—24.97%,回收率为89.5%—110.2%,对土壤中酸提取和磷酸盐交换性As(Ⅲ)和As(Ⅴ)的回收率为91.2%—104.8%.

慢性重型肝炎凝血因子Ⅴ、Ⅶ、Ⅹ的动态变化及临床意义

探讨慢性重型肝炎患者血清中凝血因子Ⅴ、Ⅶ、Ⅹ水平的动态变化及临床意义。方法:78例慢性重型肝炎患者分为死亡组和存活组,前者分为早期、中期、晚期,后者分为早期、恢复期,采用血凝法动态检测两组各期及对照组中患者凝血因子Ⅴ、Ⅵ、Ⅹ的水平,并比较它们之间的差异。结果:慢性重型肝炎患者死亡组早期凝血因子Ⅴ、Ⅶ、Ⅹ水平分别为34.64±2.89、20.96±2.23、42.62±3.28,中期分别为22.81±2.28、14.40±1.63、32.67±2.70,晚期分别为14.25±1.76、9.90±1.48、25.76±2.44,均显著低于正常对照组,且随肝功能受损程度加剧而呈进行性降低,其中19因子下降最明显。存活组早期3种因子水平分别为45.58±8.69、21.96±6.61、42.27±12.25,均显著低地正常对照组。恢复期中Ⅶ因子为68.85±31.74,Ⅹ因子为64.12±11.65,仍低于正常对照组(P<0.05),但Ⅴ因子与对照组相比差异无显著性(P>0.05)。在存活组与死亡组的早期Ⅴ因子的活性有显著性差异(t=2.44,P<0.05),而Ⅶ因子、Ⅹ因子差异无显著性(t值分别为0.38、0.09,P>0.05)。结论:动态观察凝血因子Ⅴ、Ⅶ、Ⅹ水平的变化,对慢性重型肝炎的早期诊断和判断预后有一定价值。Ⅶ因子是较灵敏的指标,Ⅴ因子是判断预后的最好指标,由于凝血酶原时间(PT)和凝血酶原活动度(PTA)

载钠硅碳羟基磷灰石的制备及其对水中As(Ⅴ)的吸附特性

由于自然和人为活动导致自然水体和土壤被As(砷)污染,严重危及生态环境并已受到广泛关注.为实现更大程度地去除含As废水的新型吸附材料,以废弃蛋壳为原材料,采用超声波法制备多孔状且较大比表面积的Na-Si-CHAP[Ca10-xNax(PO4)6-y-z(Si O4)z(CO3)y(OH)2-α,载钠硅碳羟基磷灰石],深入分析去除含As(Ⅴ)废水的吸附特性.通过BET比表面积、扫描电镜(SEM)、EDX(能量色散X射线光谱)、X-射线衍射(XRD)等手段对样品进行表征,并进一步探讨了pH、吸附时间、初始ρ[As(Ⅴ)]以及反应温度等因素对吸附效果的影响.结果表明:在pH为6. 0、作用时间为60 min、反应温度为313 K等优化条件下,0. 2 g Na-Si-CHAP对100 mL 30 mg/L含As(Ⅴ)废水的去除率和平衡吸附容量分别为96. 53%和14. 48 mg/g. Langmuir等温吸附模型较好地拟合了吸附试验数据,313 K下相关系数(r2)高达0. 998 0,饱和吸附容量达46. 73 mg/g,明显高于其他同类材料;准二级动力学模型可较好地描述该吸附行为,相关系数高达0. 999 9;热力学参数ΔG(吉布斯自由能变)、ΔH(焓变)和ΔS(熵变)的计算值显示,该吸附过程为自发吸热过程.研究显示,Na-Si-CHAP作为一种吸附剂,对含As(Ⅴ)的去除效果明显优于同类材料.

凝血因子Ⅴ和凝血酶原基因型与血栓形成

凝血因子的基因多态性对凝血系统中生化成分的改变及血栓形成有重要意义。本文对凝血酶原和凝血因子 (F )基因型及表现型与血栓形成的相关性作一综述 ,重点讨论这两种凝血因子基因突变可能对人类身体健康产生的严重损害 ;并认为单基因变化在疾病中作用甚小 ,但这种变化与特殊的环境因素和 (或 )多个基因突变共同作用时 。