1. L-Ferritin: One Gene, Five Diseases; from Hereditary Hyperferritinemia to Hypoferritinemia—Report of New Cases
- Author
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Cadenas, Beatriz, Fita-Torró, J., Bermúdez-Cortés, M., Hernandez-Rodriguez, Inés, Fuster, J.L., Llinares, M.E., Galera, A.M., Romero, J.L., Pérez-Montero, S., Tornador, C., Sánchez-Fernández, Mayka, and Universitat Autònoma de Barcelona
- Subjects
Metabolismo del hierro ,Enfermedad neurodegenerativa ,Neurodegeneration with brain iron accumulation ,Síndrome de cataratas ,lcsh:Medicine ,lcsh:RS1-441 ,Pharmaceutical Science ,Neuroferritinopathy ,Biology ,Neurodegenerative disease ,Genetic analysis ,Article ,Cataract syndrome ,lcsh:Pharmacy and materia medica ,Hiperferritinèmia hereditària ,neurodegenerative disease ,Drug Discovery ,Gene expression ,medicine ,Hereditary hyperferritinemia ,iron metabolism ,hereditary hyperferritinemia ,Gene ,cataracts syndrome ,Metabolisme del ferro ,Hereditary hypoferritinemia ,Genetics ,Ferritin ,hereditary hypoferritinemia ,Ferritina ,lcsh:R ,ferritin ,Iron metabolism ,medicine.disease ,Síndrome de cataractes ,Phenotype ,Malaltia neurodegenerativa ,Hiperferritinemia hereditaria ,Hereditary Diseases ,biology.protein ,Molecular Medicine ,Cataracts syndrome - Abstract
Ferritin is a multimeric protein composed of light (L-ferritin) and heavy (H-ferritin) subunits that binds and stores iron inside the cell. A variety of mutations have been reported in the L-ferritin subunit gene (FTL gene) that cause the following five diseases: (1) hereditary hyperferritinemia with cataract syndrome (HHCS), (2) neuroferritinopathy, a subtype of neurodegeneration with brain iron accumulation (NBIA), (3) benign hyperferritinemia, (4) L-ferritin deficiency with autosomal dominant inheritance, and (5) L-ferritin deficiency with autosomal recessive inheritance. Defects in the FTL gene lead to abnormally high levels of serum ferritin (hyperferritinemia) in HHCS and benign hyperferritinemia, while low levels (hypoferritinemia) are present in neuroferritinopathy and in autosomal dominant and recessive L-ferritin deficiency. Iron disturbances as well as neuromuscular and cognitive deficits are present in some, but not all, of these diseases. Here, we identified two novel FTL variants that cause dominant L-ferritin deficiency and HHCS (c.375+2T > A and 36_42delCAACAGT, respectively), and one previously reported variant (Met1Val) that causes dominant L-ferritin deficiency. Globally, genetic changes in the FTL gene are responsible for multiple phenotypes and an accurate diagnosis is useful for appropriate treatment. To help in this goal, we included a diagnostic algorithm for the detection of diseases caused by defects in FTL gene. info:eu-repo/semantics/publishedVersion
- Published
- 2019