| Literature DB >> 28489339 |
Kaori Yamoto1, Hirotomo Saitsu2, Norio Nakagawa3, Hisakazu Nakajima3, Tatsuji Hasegawa4, Yasuko Fujisawa1, Masayo Kagami5, Maki Fukami5, Tsutomu Ogata1,5.
Abstract
Although paternally expressed IGF2 is known to play a critical role in placental and body growth, only a single mutation has been found in IGF2. We identified, through whole-exome sequencing, a de novo IGF2 indel mutation leading to frameshift (NM_000612.5:c.110_117delinsAGGTAA, p.(Leu37Glnfs*31)) in a patient with Silver-Russell syndrome, ectrodactyly, undermasculinized genitalia, developmental delay, and placental hypoplasia. Furthermore, we demonstrated that the mutation resided on the paternal allele by sequencing the long PCR product harboring the mutation- and methylation-sensitive SmaI and SalI sites before and after SmaI/SalI digestion. The results, together with the previous findings in four cases from a single family with a paternally inherited IGF2 nonsense mutation and those in patients with variable H19 differentially methylated region epimutations leading to compromised IGF2 expression, suggest that the whole phenotype of this patient is explainable by the IGF2 mutation, and that phenotypic severity is primarily determined by the IGF2 expression level in target tissues.Entities:
Keywords: IGF2; Silver-Russell syndrome; ectrodactyly; frameshift mutation; imprinting
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Year: 2017 PMID: 28489339 DOI: 10.1002/humu.23253
Source DB: PubMed Journal: Hum Mutat ISSN: 1059-7794 Impact factor: 4.878