Determinação das bases moleculares da deficiência hereditária de fator VII da coagulação

Detalhes bibliográficos
Ano de defesa: 2011
Autor(a) principal: Flavia Yankous Rabelo
Orientador(a): Não Informado pela instituição
Banca de defesa: Não Informado pela instituição
Tipo de documento: Dissertação
Tipo de acesso: Acesso aberto
Idioma: por
Instituição de defesa: Universidade Federal de Minas Gerais
UFMG
Programa de Pós-Graduação: Não Informado pela instituição
Departamento: Não Informado pela instituição
País: Não Informado pela instituição
Palavras-chave em Português:
Brasil
Gene
Mutação
Fator VII
Hemorragia
Polimorfismo
Sangramento
Deficiência do fator VII 
Aberrações cromossômicas
Polimorfismo (Genética)
Fatores de coagulação sanguínea
Polimorfismo genético
Variação genética
Link de acesso: http://hdl.handle.net/1843/BUOS-98SHHF
Resumo: Introduction: The inherited deficiency of coagulation factor VII (FVII) is the most frequent among rare coagulopathies, with an estimated prevalence of 1: 500,000 inhabitants. It is transmitted as an autosomal recessive inheritance, due to mutations in the gene coding FVII (F7). It presents variable clinical manifestations, from asymptomatic forms to severe bleedings. Molecular studies are rare in non-Caucasian populations. Thus, we studied, at molecular level, a cohort of patients with FVII deficiency, registered at Hemocentro de Belo Horizonte (HBH), Belo Horizonte, Brazil. Methods: All patients diagnosed with FVII deficiency were invited to participate in the study through an invitation letter. We collected clinical data and blood samples between November 2003 and February 2004. Thirty-one (82%) out of 38 patients accepted the invitation; 26 of them (84%) had FVII activity (FVII:C) lower than 50% and 4 patients (13%) had FVII:C slightly over than 50% (included as they presented a hemorrhagic manifestation). FVII:C was not assessed in 1 patient (3%). Patients were clinically evaluated and submitted to laboratory tests, among these, prothrombin time and FVII:C, with different thromboplastins. All exons and intron/exon borders of F7 were amplified and sequenced. Results: Thirteen gene variants were identified. Six (46%) are known genetic variants (Arg304Gln; Thr324Met, c.-323_-313insCCTATATCCT; Glu95Glu; His175His and Arg353Gln) and seven (54%) are new ones (Arg43Lys, Phe84Phe; Gln116Gln; Arg139Arg, Glu142Glu, c.745_747delGTG and Gln281Gln). Conclusion: Most patients with moderate to mild FVII deficiency have polymorphisms or genetic alterations in homozygosis. No association was seen between phenotype and genotype of the patients studied, which corroborates data from the literature.

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