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Review
. 2018 Nov;61(11):664-673.
doi: 10.1016/j.ejmg.2017.10.017. Epub 2017 Oct 26.

Molecular approaches to diagnose Diamond-Blackfan anemia: The EuroDBA experience

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Free article
Review

Molecular approaches to diagnose Diamond-Blackfan anemia: The EuroDBA experience

Lydie Da Costa et al. Eur J Med Genet. 2018 Nov.
Free article

Abstract

Diamond-Blackfan anemia (DBA) is a rare congenital erythroblastopenia and inherited bone marrow failure syndrome that affects approximately seven individuals in every million live births. In addition to anemia, about 50% of all DBA patients suffer from various physical malformations of the face, hands, heart, or urogenital region. The disorder is almost exclusively driven by haploinsufficient mutations in one of several ribosomal protein (RP) genes, although for ∼30% of diagnosed patients no mutation is found in any of the known DBA-linked genes. Because DBA is such a rare disease with a particularly wide range of clinical phenotypes and molecular signatures, the development of collaborative efforts such as the ERARE-funded European DBA consortium (EuroDBA) has become imperative for DBA research. EuroDBA was founded in 2012 and brings together dedicated clinical and biological researchers of DBA from France, Italy, the Netherlands, Germany, Israel, Poland, and Turkey to achieve a number of goals including the consolidation of data in patient registries, establishment of minimal diagnostic criteria, and projects aimed at more fully describing the different mutations linked to DBA. This review will cover the history of the EuroDBA registries, the methods used by EuroDBA in the diagnosis of DBA, and how the consortium has successfully worked together towards the discovery of new DBA-linked genes and the better understanding their pathophysiological effects.

Keywords: Diamond-Blackfan anemia; Polysome profiling; Pre-rRNA processing; Ribosomal protein genes; Ribosome biogenesis.

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