Luz Karime Yunis Hazbun scite author profile

BackgroundHemophilia B (HB) is a coagulation disorder with an X‐linked recessive inheritance pattern, caused by plasma FIX deficiency. In Colombia, HB is considered a rare and high‐cost disease, with 362 males reported in 2017.MethodsHere, we characterized 20 HB apparently unrelated families by PCR amplification and Sanger sequencing.ResultsFourteen unique variants were identified: seven missense, three nonsense, one variant in the 3′ UTR region, two large deletions >50 bp, and one intronic substitution that affects splicing c.520+13A>G that was present in 7/20 patients (35%). All these variants have been previously reported in the literature, except for exons 3 and 4, deletions, present in one patient. The genotype‐phenotype association correlates with the reported in the literature, with the exception of one patient.ConclusionThis molecular analysis allowed us to establish the causal variant of HB in 100% of patients, to provide the appropriate genetic counseling to each of the families, and to propose a more cost‐effective carrier analysis. Here, we reported the first variants in Colombian population with Hemophilia B, finding a new variant and one intron recurrent variant present in 35% of patients.

Programa para diagnóstico molecular de hemofilia A y B en Colombia.

Hazbun¹,

Jara²,

Ballesteros³

et al. 2018

Mutaciones en el gen NPM1 en leucemia mieloide aguda (LMA) en una muestra de población colombiana : implicaciones en el diagnóstico, estratificación del riesgo y tratamiento.

Hazbun¹,

Díaz²,

Gavilanes³

et al. 2018

Dos casos con hallazgo citogenético de inversión del brazo largo del cromosoma 3 –inv(3q)– : reporte de casos y revisión de la literatura.

Hazbun¹,

Cuéllar²,

Vásquez³

et al. 2018

Mutaciones en el gen FLT3 en leucemia mieloide aguda (LMA) en una muestra de población colombiana : implicaciones en el diagnóstico, estratificación del riesgo y tratamiento.

Hazbun¹,

Díaz²,

Gavilanes³

et al. 2018