TY - JOUR
T1 - Congenital imprinting disorders
T2 - Application of multilocus and high throughput methods to decipher new pathomechanisms and improve their management
AU - Soellner, Lucas
AU - Monk, David
AU - Rezwan, Faisal I.
AU - Begemann, Matthias
AU - Mackay, Duncan H.
AU - Eggermann, Thomas
N1 - Funding Information:
The authors are members of the COST Action BM1208 and EUCID.net (European congenital imprinting disorders network; www.imprinting-disorders.eu ). The group in Aachen is supported by the Bundesministerium für Bildung und Forschung (Network “Imprinting Diseases”, 01GM1513B ).
Publisher Copyright:
© 2015 Elsevier Ltd.
PY - 2015/10
Y1 - 2015/10
N2 - Imprinting disorders (IDs) are a group of congenital diseases affecting growth, development and metabolism. They are caused by changes in the allele-specific regulation ("epigenetic mutation") or in the genomic sequence ("genetic mutation") of imprinted genes. Currently molecular tests in ID patients are generally restricted to single loci classically associated with the disease, but this approach limits diagnostic yield, because of the molecular and clinical heterogeneity between IDs. From the technical point of view, these limitations are aggravated by the lack of standardization in testing methodology, in the DNA sequences tested, and in clinical inclusion criteria prompting testing. However, an increasing number of new studies show that these problems can be addressed by the use of new tests targeting multiple loci and/or a total exome and genome analysis. The rapid development of efficient and high-throughput molecular techniques and their applications in research and diagnostics in the last decade have led to an impressive increase of knowledge on IDs and their basic pathomechanisms. In combination with the improvement of data recording and documentation, the diagnostic strategies are increasingly based on standardized protocols, and thereby provide the backbone for directed counseling, more personalized management, and new therapeutic approaches.
AB - Imprinting disorders (IDs) are a group of congenital diseases affecting growth, development and metabolism. They are caused by changes in the allele-specific regulation ("epigenetic mutation") or in the genomic sequence ("genetic mutation") of imprinted genes. Currently molecular tests in ID patients are generally restricted to single loci classically associated with the disease, but this approach limits diagnostic yield, because of the molecular and clinical heterogeneity between IDs. From the technical point of view, these limitations are aggravated by the lack of standardization in testing methodology, in the DNA sequences tested, and in clinical inclusion criteria prompting testing. However, an increasing number of new studies show that these problems can be addressed by the use of new tests targeting multiple loci and/or a total exome and genome analysis. The rapid development of efficient and high-throughput molecular techniques and their applications in research and diagnostics in the last decade have led to an impressive increase of knowledge on IDs and their basic pathomechanisms. In combination with the improvement of data recording and documentation, the diagnostic strategies are increasingly based on standardized protocols, and thereby provide the backbone for directed counseling, more personalized management, and new therapeutic approaches.
KW - High throughput techniques
KW - Imprinting disorders
KW - Methylation-specific assay
KW - Multilocus imprinting analysis
UR - http://www.scopus.com/inward/record.url?scp=84946498197&partnerID=8YFLogxK
U2 - 10.1016/j.mcp.2015.05.003
DO - 10.1016/j.mcp.2015.05.003
M3 - Review Article
SN - 0890-8508
VL - 29
SP - 282
EP - 290
JO - Molecular and Cellular Probes
JF - Molecular and Cellular Probes
IS - 5
ER -