Severe factor X deficiency and successful pregnancy

Konje, Justin C.; Murphy, Philip; Chazal, R. de; Davidson, Allan M.; Taylor, David O.

doi:10.1111/j.1471-0528.1994.tb13557.x

Cited by 29 publications

(40 citation statements)

References 3 publications

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“…The coagulation parameters in our patient had improved during pregnancy when compared to non-pregnant levels. Konje et al 8 reported a case of FX deficiency which was complicated by recurrent retro placental bleeding in the antenatal period which was managed conservatively by the use of BPL factor IXA (composition per unit: 500 IU factor X, 500 IU ant thrombin III, 550 IU factor IXA, 600 IU factor II and 5000 IU Heparin). Kumar & Mehta 9 reported four pregnancies in one woman with FX deficiency, theorizing that prophylactic clotting factor replacement was instrumental in the favorable pregnancy outcome.…”

Section: Discussionmentioning

confidence: 99%

Severe Factor X Deficiency in Pregnancy-An Obstetric Challenge

Venkatesh¹,

Ross²,

Vani³

2017

IPCB

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Abbreviations: FX, factor X; FX,C, factor X coagulant; FFP, fresh frozen plasma; PCC, prothrombin complex concentrate Case reportA 23year old lady with one previous abortion, presented to the antenatal outpatient department of St. John s Hospital, for the first time at 20weeks of gestation. She gave a history of prolonged bleeding following trivial trauma since childhood which stopped on compression. She also had hemarthrosis and spontaneous gum bleeds since childhood. At puberty, she gave history of menorrhagia which responded to oral Tranexamic acid. At 17years of age, patient had a severe episode of menorrhagia leading to hemorrhagic shock. She received multiple blood products and eventually required bilateral uterine artery ligation and a few haemostatic sutures on the uterus (exact details of which are not known and have not been documented). Soon after marriage, at 21years of age, she was diagnosed to have blighted ovum and presented later with incomplete abortion, for which she received Misoprostol. She had heavy bleeding leading to severe anemia and a provisional diagnosis of disseminated intravascular coagulation was made. Her investigations at that time were Prothrombin time 102s, Activated thromboplastin time 65.5 s, INR 8.5, Factor X levels were <1% with normal platelet count and morphology. Thus, a diagnosis of severe factor X deficiency was made. During the present pregnancy, she was referred to the antenatal outpatient department. She had developed gestational diabetes mellitus which was controlled with diet. The antenatal period was uneventful. As there was no significant bleeding in this pregnancy, the coagulation parameters were not repeated until term. Ultrasound done at 37weeks confirmed a flexed breech presentation. At 37weeks of gestation, patient received FFPs at 1 bag/10kg body weight to assess her laboratory haemostatic parameters and her investigations were as shown in Table 1. Elective cesarean delivery was planned at 38weeks of gestation and external cephalic version was not considered due to the previous scar on the uterus (i.e. haemostatic sutures on the uterus following an episode of menorrhagia at 17years of age). Patient underwent emergency cesarean delivery at 37weeks of gestation, as a spontaneous retro placental bleed of about 50ml was seen on ultrasound. Patient again received the same dose of FFP and 2g of intravenous Tranexamic acid preoperatively. A healthy baby boy of weight 2.5kg was delivered as flexed breech. A previous scar was noted on the uterus. Both ovaries were normal. Intraoperatively, a peritoneal drain was left in situ. Patient developed hematuria which cleared after 12hours. Postoperatively, patient received 3units of FFP and 1g intravenous Tranexamic acid 8 hourly for 48hours and then followed by 2units of FFP and 1g intravenous Tranexamic acid 12hourly till the seventh postoperative day. Sutures were removed on the seventh postoperative day. Postoperative period was uneventful. Patient has come for follow-up and has had no signs of postpartum hemorrhage til...

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Section: Discussionmentioning

confidence: 99%

Severe Factor X Deficiency in Pregnancy-An Obstetric Challenge

Venkatesh¹,

Ross²,

Vani³

2017

IPCB

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“…The haematoma remained stable during the follow‐up, and the patient was delivered by c‐section at 34 weeks due to preterm labour . The third case (FX 0.02 IU/mL) presented with a retroplacental haematoma diagnosed on ultrasound scan at 22 and 34 weeks, and the patient had a successful delivery by c‐section at 39 weeks for foetal distress . The fourth case (FX 0.1 IU/mL) presented with vaginal bleeding at 6 and 13 weeks.…”

Section: Antenatal Complicationsmentioning

confidence: 99%

Congenital Factor X deficiency in women: A systematic review of the literature

Spiliopoulos

Kadir

2019

Haemophilia

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Factor X deficiency (FXD) is a rare autosomal recessive bleeding disorder with a variable phenotypic severity. In women, heavy menstrual bleeding (HMB), recurrent ovulation bleeding with haemoperitoneum and bleeding complications in pregnancy such as retroplacental haematoma and postpartum haemorrhage have been reported. The aim of this review was to examine gynaecological problems and obstetric complications in women with congenital FXD. A total number of 49 relevant articles were identified, including 332 women, dating from 1960 to 2018. Heavy menstrual bleeding was reported in 72/284 (25%) women in total, 14/30 (47%) in case reports and 58/254 (23%) in 11 case series, 64% and 10% required blood products and blood transfusion, respectively. Haemoperitoneum from ovulation bleeding or ruptured haemorrhagic ovarian cyst requiring blood transfusion occurred in 8/322 (2.4%) women, six required surgical intervention, including oophorectomy in two. 31 pregnancies were reported in 19 women. There were four miscarriages (including a late miscarriage at 21 weeks). There was a high rate of preterm birth and neonatal death occurring in eight (30%) and three (11%) of pregnancies reaching viability stage. Postpartum haemorrhage (PPH) occurred in six (22%) of deliveries, one requiring hysterectomy. In conclusion, women with FXD are at an increased risk of heavy bleeding during menstruation and ovulation as well as adverse pregnancy outcome and postpartum haemorrhage. Collaboration in a multidisciplinary team including an obstetrician/gynaecologist, a perinatologist and a haematologist is necessary for the prevention and management of these complications.

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“…Because treatment with high doses or prolonged administration of prothrombin complex concentrates rich in FX increases the risk of thromboembolism and disseminated intravascular coagulation, it is not recommended that the FX activity is raised more than 50% [2]. However, there are specific prothrombin complex concentrates containing antithrombin III and heparin as prophylaxis against thromboembolism [7].…”

Section: Discussionmentioning

confidence: 99%

“…The patient should receive an initial dose of 15-20 ml/kg body weight, followed by 3-6 ml/kg every 24 h. The rationale for such therapy is that the biological half-life of FX is 40 h. Also, prothrombin complex concentrates rich in FX have been used [2]. These concentrates are now the preferred therapy because they are virally inactivated, and the risk of volume overload during treatment is less compared with FFP [7]. Because treatment with high doses or prolonged administration of prothrombin complex concentrates rich in FX increases the risk of thromboembolism and disseminated intravascular coagulation, it is not recommended that the FX activity is raised more than 50% [2].…”

Section: Discussionmentioning

confidence: 99%

Two Episodes of Hemoperitoneum from Luteal Cysts Rupture in a Patient with Congenital Factor X Deficiency

Dafopoulos¹,

Γαλάζιος²,

Georgadakis³

et al. 2003

Gynecol Obstet Invest

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The clinical manifestation of two episodes of hemoperitoneum from ruptured corpus luteum cysts, during the luteal phase of the cycle in a young patient with the rare congenital factor X deficiency, is reported for the first time in literature. The correct diagnosis of the underlying disorder, the gynecological management and the regular follow-up can minimize the risks of this potentially life-threatening hematological disorder.

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Severe factor X deficiency and successful pregnancy

Cited by 29 publications

References 3 publications

Severe Factor X Deficiency in Pregnancy-An Obstetric Challenge

Severe Factor X Deficiency in Pregnancy-An Obstetric Challenge

Congenital Factor X deficiency in women: A systematic review of the literature

Two Episodes of Hemoperitoneum from Luteal Cysts Rupture in a Patient with Congenital Factor X Deficiency

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