Variant "HBB:p.Glu6Lys"
Search results: 2 records
Variant information
Gene:
HBB 
Variant:
HBB:p.Glu6Lys 
dbSNP ID:
no data 
GWAS trait:
no data 
Modifier statisitcs
Record:
Disorder:
Reference:
Effect type:
Expressivity(2)  
Modifier effect:
Altered hemoglobin level(2)  
Details:
  • Target disease:
    Beta Thalassemia (DOID_12241)
    Effect type:
    Expressivity 
    Modifier effect:
    Altered hemoglobin level 
    Evidence:
    From review article 
    Effect:
    Modify HbF production
    Reference:
    PMID29127676
    Title:
    Genetic Basis and Genetic Modifiers of β-Thalassemia and Sickle Cell Disease.
    Species studied:
    Human
    Abstract:
    β-thalassemia and sickle cell disease (SCD) are prototypical Mendelian single gene disorders, both caused by mutations affecting the adult β-globin gene. Despite the apparent genetic simplicity, both disorders display a remarkable spectrum of phenotypic severity and share two major genetic modifiers-α-globin genotype and innate ability to produce fetal hemoglobin (HbF, α2γ2).This article provides an overview of the genetic basis for SCD and β-thalassemia, and genetic modifiers identified through phenotype correlation studies. Identification of the genetic variants modifying HbF production in combination with α-globin genotype provide some prediction of disease severity for β-thalassemia and SCD but generation of a personalized genetic risk score to inform prognosis and guide management requires a larger panel of genetic modifiers yet to be discovered.Nonetheless, genetic studies have been successful in characterizing some of the key variants and pathways involved in HbF regulation, providing new therapeutic targets for HbF reactivation.
  • Target disease:
    Sickle Cell Anemia (DOID_10923)
    Effect type:
    Expressivity 
    Modifier effect:
    Altered hemoglobin level 
    Evidence:
    From review article 
    Effect:
    Modify HbF production
    Reference:
    PMID29127676
    Title:
    Genetic Basis and Genetic Modifiers of β-Thalassemia and Sickle Cell Disease.
    Species studied:
    Human
    Abstract:
    β-thalassemia and sickle cell disease (SCD) are prototypical Mendelian single gene disorders, both caused by mutations affecting the adult β-globin gene. Despite the apparent genetic simplicity, both disorders display a remarkable spectrum of phenotypic severity and share two major genetic modifiers-α-globin genotype and innate ability to produce fetal hemoglobin (HbF, α2γ2).This article provides an overview of the genetic basis for SCD and β-thalassemia, and genetic modifiers identified through phenotype correlation studies. Identification of the genetic variants modifying HbF production in combination with α-globin genotype provide some prediction of disease severity for β-thalassemia and SCD but generation of a personalized genetic risk score to inform prognosis and guide management requires a larger panel of genetic modifiers yet to be discovered.Nonetheless, genetic studies have been successful in characterizing some of the key variants and pathways involved in HbF regulation, providing new therapeutic targets for HbF reactivation.