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Characterization of multi-locus imprinting disturbances and underlying genetic defects in patients with chromosome 11p15.5 related imprinting disorders

Authors :
L. Fontana
M. F. Bedeschi
S. Maitz
A. Cereda
C. Faré
S. Motta
A. Seresini
P. D’Ursi
A. Orro
V. Pecile
M. Calvello
A. Selicorni
F. Lalatta
D. Milani
S. M. Sirchia
M. Miozzo
S. Tabano
Source :
Epigenetics, Vol 13, Iss 9, Pp 897-909 (2018)
Publication Year :
2018
Publisher :
Taylor & Francis Group, 2018.

Abstract

The identification of multilocus imprinting disturbances (MLID) appears fundamental to uncover molecular pathways underlying imprinting disorders (IDs) and to complete clinical diagnosis of patients. However, MLID genetic associated mechanisms remain largely unknown. To characterize MLID in Beckwith-Wiedemann (BWS) and Silver-Russell (SRS) syndromes, we profiled by MassARRAY the methylation of 12 imprinted differentially methylated regions (iDMRs) in 21 BWS and 7 SRS patients with chromosome 11p15.5 epimutations. MLID was identified in 50% of BWS and 29% of SRS patients as a maternal hypomethylation syndrome. By next-generation sequencing, we searched for putative MLID-causative mutations in genes involved in methylation establishment/maintenance and found two novel missense mutations possibly causative of MLID: one in NLRP2, affecting ADP binding and protein activity, and one in ZFP42, likely leading to loss of DNA binding specificity. Both variants were paternally inherited. In silico protein modelling allowed to define the functional effect of these mutations. We found that MLID is very frequent in BWS/SRS. In addition, since MLID-BWS patients in our cohort show a peculiar pattern of BWS-associated clinical signs, MLID test could be important for a comprehensive clinical assessment. Finally, we highlighted the possible involvement of ZFP42 variants in MLID development and confirmed NLRP2 as causative locus in BWS-MLID.

Details

Language :
English
ISSN :
15592294 and 15592308
Volume :
13
Issue :
9
Database :
Directory of Open Access Journals
Journal :
Epigenetics
Publication Type :
Academic Journal
Accession number :
edsdoj.636a1de7037f49c083e24d8c49ec7ca6
Document Type :
article
Full Text :
https://doi.org/10.1080/15592294.2018.1514230