Ítem
Acceso Abierto
Next generation sequencing in women affected by nonsyndromic premature ovarian failure displays new potential causative genes and mutations
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Fonseca Mendoza, Dora Janeth
Patiño, Liliana Catherine
Suárez, Yohjana Carolina
de Jesús Rodríguez, Asid
Mateus, Heidi Eliana
Jiménez, Karen Marcela
Ortega-Recalde, Oscar
Díaz-Yamal, Ivonne
Laissue, Paul
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Fecha
2015
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Elsevier Inc.
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Resumen
Abstract
Objective To identify new molecular actors involved in nonsyndromic premature ovarian failure (POF) etiology. Design This is a retrospective case-control cohort study. Setting University research group and IVF medical center. Patient(s) Twelve women affected by nonsyndromic POF. The control group included 176 women whose menopause had occurred after age 50 and had no antecedents regarding gynecological disease. A further 345 women from the same ethnic origin (general population group) were also recruited to assess allele frequency for potentially deleterious sequence variants. Intervention(s) Next generation sequencing (NGS), Sanger sequencing, and bioinformatics analysis. Main Outcome Measure(s) The complete coding regions of 70 candidate genes were massively sequenced, via NGS, in POF patients. Bioinformatics and genetics were used to confirm NGS results and to identify potential sequence variants related to the disease pathogenesis. Result(s) We have identified mutations in two novel genes, ADAMTS19 and BMPR2, that are potentially related to POF origin. LHCGR mutations, which might have contributed to the phenotype, were also detected. Conclusion(s) We thus recommend NGS as a powerful tool for identifying new molecular actors in POF and for future diagnostic/prognostic purposes. © 2015 American Society for Reproductive Medicine.
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Keywords
Adamts19 gene , human , Article , Bioinformatics , Bmpr2 gene , Case control study , Cohort analysis , Computer model , Female , Gene , Gene mutation , Gene sequence , Human , Lhcgr gene , Major clinical study , Menopause , Next generation sequencing , Phenotype , Premature ovarian failure , Priority journal , Retrospective study , Sanger sequencing , Genetics , High throughput sequencing , Mutation , Primary ovarian insufficiency , Procedures , Sequence analysis , Adam protein , Adamts19 protein , Bmpr2 protein , Bone morphogenetic protein receptor 2 , Adam proteins , Adult , Bone morphogenetic protein receptors , Case-control studies , Cohort studies , Female , High-throughput nucleotide sequencing , Humans , Mutation , Primary ovarian insufficiency , Retrospective studies , Sequence analysis , Adamts19 , Bmpr2 , Next generation sequencing , Pof , Premature ovarian failure
