Abstract
X-linked intellectual deficiency (XLID) is a widely heterogeneous group of genetic disorders that involves more than 100 genes. The mediator of RNA polymerase II subunit 12 (MED12) is involved in the regulation of the majority of RNA polymerase II-dependent genes and has been shown to cause several forms of XLID, including Opitz-Kaveggia syndrome also known as FG syndrome (MIM #305450), Lujan-Fryns syndrome (MIM #309520) and the X-linked Ohdo syndrome (MIM #300895). Here, we report on two first cousins with X-linked Ohdo syndrome with a missense mutation in MED12 gene, identified through whole exome sequencing. The probands had facial features typical of X-linked Ohdo syndrome, including blepharophimosis, ptosis, a round face with a characteristic nose and a narrow mouth. Nextera DNA Exome kit (Illumina Inc., San Diego, CA, USA) was used for exome capture. The variant identified was a c.887G > A substitution in exon 7 of the MED12 gene leading to the substitution of a glutamine for a highly conserved arginine (p. Arg296Gln). Although the variant described has been previously reported in the literature, our study contributes to the expanding phenotypic spectrum of MED12-related disorders and above all, it demonstrates the phenotypic variability among different affected patients despite harboring identical mutations.
Highlights
X-linked intellectual deficiency (XLID) is a widely heterogeneous group of genetic disorders that involves more than one hundred genes [1]
Mutations in mediator of RNA polymerase II subunit 12 (MED12) have been shown to cause several forms of XLID, including Opitz-Kaveggia syndrome known as FG syndrome (MIM #305450), LujanFryns syndrome (MIM #309520) and the X-linked Ohdo syndrome (OSMKB subtype)
Using whole exome sequencing (WES), we discovered that both carry the MED12 missense variant c.887G > A
Summary
X-linked intellectual deficiency (XLID) is a widely heterogeneous group of genetic disorders that involves more than one hundred genes [1]. Mutations in MED12 have been shown to cause several forms of XLID, including Opitz-Kaveggia syndrome known as FG syndrome (MIM #305450), LujanFryns syndrome (MIM #309520) and the X-linked Ohdo syndrome (OSMKB subtype). (MIM #300895) [3,4,5,6,7,8,9,10] These syndromes are allelic disorders that share clinical symptoms including ID, hypotonia and some physical features, such as tall prominent forehead, open mouth or high narrow palate. Other variants have been described to cause syndromic, but not falling exactly in the three syndromes, or non-syndromic
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