Novel Insights into Heterozygous Factor XIII Deficiency

Dorgalaleh, Akbar

doi:10.1055/s-0043-1764471

Cited by 3 publications

(3 citation statements)

References 86 publications

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“…FXIIID may be congenital or acquired, and congenital FXIIID is a rare autosomal recessive bleeding disorder [ 9 ]. FXIII activity in patients with severe congenital FXIIID is undetectable [ 9 ], while in heterozygous FXIIID, FXIII activity is typically between 30% and 70% [ 10 ]. The FXIII activity level required to prevent spontaneous major bleeding is 15% [ 11 ], and the requirement for FXIII increases during surgery and bleeding because of hyperconsumption.…”

Section: Discussionmentioning

confidence: 99%

“…Postoperative/tooth extraction bleeding has been reported in patients with heterozygous FXIIID who had FXIII activity between 23% and 71% [ 10 ]. The bleeding risk after surgical procedures is higher in heterozygotes with FXIIID than in healthy individuals because the baseline levels of FXIII are lower [ 10 ]. By contrast, acquired FXIIID is caused by the generation of antibodies, hyperconsumption, or hyposynthesis due to an underlying comorbidity [ 9 ].…”

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Post-renal Biopsy Retroperitoneal Haematoma Accompanied by Decreased Coagulation Factor XIII Levels in Immunoglobulin A Nephropathy

Hirano,

Kanda,

Hidaka

et al. 2024

Cureus

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Post-biopsy bleeding is the primary complication of renal biopsy. Retroperitoneal haematoma is a rare but severe bleeding complication; it commonly occurs among patients who have risk factors or vascular lesions. The bleeding risks in patients with immunoglobulin A (IgA) nephropathy (IgAN) have been discussed in the literature, but clinical data are lacking. Here, we report a case of a post-biopsy retroperitoneal haematoma accompanied by decreased coagulation factor XIII (FXIII) in a patient with IgAN. A 14-year-old male patient with haematuria and proteinuria but no bleeding or family history of bleeding underwent pre-renal biopsy evaluation that showed no coagulation abnormalities. He underwent percutaneous renal biopsy, and the histopathological diagnosis was IgAN. Five days after the biopsy, he presented with delayed bleeding from a retroperitoneal haematoma. During the workup for undiagnosed haemorrhagic diatheses, a mildly decreased FXIII level was discovered. This result suggested the possibility of bleeding complications associated with decreased FXIII. Some bleeding diatheses, including FXIII deficiency, cannot be evaluated in routine pre-biopsy coagulation tests. Mild FXIII deficiency can increase the risk of post-biopsy bleeding complications. Therefore, physicians should consider unevaluated haemorrhagic diatheses when a patient presents with major bleeding complications or delayed bleeding following renal biopsy without any known risk factors or vascular lesions.

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Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

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Post-renal Biopsy Retroperitoneal Haematoma Accompanied by Decreased Coagulation Factor XIII Levels in Immunoglobulin A Nephropathy

Hirano,

Kanda,

Hidaka

et al. 2024

Cureus

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Editorial Compilation XIV

Favaloro,

Pasalic,

Lippi

2023

Semin Thromb Hemost

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Factor XIII Deficiency: Laboratory, Molecular, and Clinical Aspects

Dorgalaleh,

Jozdani,

Zadeh

2024

Semin Thromb Hemost

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Factor XIII-A (FXIII-A) deficiency is an ultra-rare bleeding disorder characterized by high rates of morbidity and mortality, primarily resulting from intracranial hemorrhage, umbilical cord bleeding, and miscarriage, whereas patients with severe FXIII-B deficiency present with a milder phenotype. Although the estimated incidence of severe FXIII-A deficiency is one per 2 million, a high prevalence ranging from 0.8 to 3.5% has been observed for heterozygous FXIII-A deficiency. Unlike most bleeding disorders, individuals with heterozygous FXIII-A deficiency, particularly women, are more likely to experience hemorrhagic complications during hemostatic challenges. About 200 Mutations have been observed in F13A and F13B genes, with most being missense mutations, while large deletions are the rarest. There is no correlation between genotype and phenotype, but a moderate to strong correlation between factor activity and clinical severity in FXIII-A deficiency difficult. Primary prophylaxis is mandatory for all patients with severe FXIII-A deficiency, while those with heterozygous deficiency are generally asymptomatic and may require on-demand therapy during hemostatic challenges, most commonly in women. On the other hand, patients with severe FXIII-B deficiency may only require on-demand therapy, while heterozygotes are generally asymptomatic. Although there are general recommended therapeutic regimens for prophylaxis or on-demand therapy in different situations, personalized pharmacokinetic-based replacement therapy represents the optimal approach that can optimize intervention efficacy. In such an approach, several factors may affect the effectiveness of treatment and determine the dose and type of intervention, including the classification of FXIII deficiency, residual plasma levels of FXIII, clinical situation requiring intervention, age, weight, and also gender.

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Novel Insights into Heterozygous Factor XIII Deficiency

Cited by 3 publications

References 86 publications

Post-renal Biopsy Retroperitoneal Haematoma Accompanied by Decreased Coagulation Factor XIII Levels in Immunoglobulin A Nephropathy

Post-renal Biopsy Retroperitoneal Haematoma Accompanied by Decreased Coagulation Factor XIII Levels in Immunoglobulin A Nephropathy

Editorial Compilation XIV

Factor XIII Deficiency: Laboratory, Molecular, and Clinical Aspects

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