Molecular Pathology of Rare Bleeding Disorders (RBDs) in India: A Systematic Review

Kulkarni, Bipin; Nair, Sona; Vijapurkar, Manasi; Mota, Leenam; Shanbhag, S.; Ali, Shehnaz; Shetty, Shrimati; Ghosh, Kanjaksha

doi:10.1371/journal.pone.0108683

Cited by 14 publications

(11 citation statements)

References 29 publications

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“…29,[63][64][65] This common mutation was also observed in India. 66 Arg326Gln FXIII-A gene mutation has been detected in patients from Germany and the Netherlands. 58,67 Thus, in patients with European origin, these three mutations can be selected as the first step in molecular diagnosis of FXIIID.…”

Section: Molecular Diagnosis Of Fxiiidmentioning

confidence: 99%

Diagnosis of factor XIII deficiency

et al. 2016

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Section: Molecular Diagnosis Of Fxiiidmentioning

confidence: 99%

Diagnosis of factor XIII deficiency

et al. 2016

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“…Our literature review identified a large number of novel mutations accounting for congenital fibrinogen disorders, both quantitative [49][50][51][52][53][54][55][56][57][58][59][60][61][62][63][64] and qualitative. [65][66][67][68][69][70][71][72][73][74][75][76] The majority of dysfibrinogenemias, inherited as a dominant trait, are caused by heterozygous missense mutations in one of the three fibrinogen genes.…”

Section: Genetic Diagnosis Of Congenital Fibrinogen Disordersmentioning

confidence: 99%

Laboratory and Genetic Investigation of Mutations Accounting for Congenital Fibrinogen Disorders

Neerman-Arbez

Moerloose

Casini

2016

Semin Thromb Hemost

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Congenital fibrinogen disorders are classified into two types of plasma fibrinogen defects: type I (quantitative fibrinogen deficiencies), that is, hypofibrinogenemia or afibrinogenemia, in which there are low or absent plasma fibrinogen antigen levels, respectively, and type II (qualitative fibrinogen deficiencies), that is, dysfibrinogenemia or hypodysfibrinogenemia, in which there are normal or reduced antigen levels associated with disproportionately low functional activity. These disorders are caused by mutations in the three fibrinogen-encoding genes FGA, FGB, and FGG. Afibrinogenemia is associated with mild to severe bleeding, whereas hypofibrinogenemia is often asymptomatic. For these quantitative disorders, the majority of mutations prevent protein production. However, in some cases, missense or late-truncating nonsense mutations allow synthesis of the mutant fibrinogen chain, but intracellular fibrinogen assembly and/or secretion are impaired. Qualitative fibrinogen disorders are associated with bleeding, thrombosis, or both thrombosis and bleeding, but many dysfibrinogenemias are asymptomatic. The majority of cases are caused by heterozygous missense mutations. Here, we review the laboratory and genetic diagnosis of fibrinogen gene anomalies with an updated discussion of causative mutations identified.

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“…Glanzmann's Thrombasthenia (GT) is a rare (1: 1 000 000) congenital bleeding disorder caused by dysfunctional or absent platelet integrin aIIbb3, because of mutations in the ITGA2B and ITGB3 genes located on chromosome 17q21-23 [1]. The clinical manifestations are highly heterogenous, which include mucocutaneous bleeding such as epistaxis, gum bleeding, haematuria, menorrhagia and gastrointestinal bleed resulting in major morbidity and mortality in affected families.…”

mentioning

confidence: 99%

“…The mutations which cause GT are spread all over the ITGA2B and ITGB3 genes. More than 200 mutations have been reported from across the world, which mainly comprise of deletions, point mutations, inversions, insertions and splice site variations, along with large number of polymorphisms [1]. The data published from Indian studies shows 47 unique mutations in 102 GT patients, while in 27 patients, mutation could not be detected despite scanning the entire coding, splice site and the regulatory regions of both the genes [1,3,4].…”

mentioning

confidence: 99%

“…More than 200 mutations have been reported from across the world, which mainly comprise of deletions, point mutations, inversions, insertions and splice site variations, along with large number of polymorphisms [1]. The data published from Indian studies shows 47 unique mutations in 102 GT patients, while in 27 patients, mutation could not be detected despite scanning the entire coding, splice site and the regulatory regions of both the genes [1,3,4]. This along with widespread molecular heterogeneity of mutations pose a major hurdle in offering first trimester prenatal diagnosis to the affected families, though it is a safer method over second trimester diagnosis, where the risk of bleeding through cord puncture site could be higher [5].…”

mentioning

confidence: 99%

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