Homozygous SHOX gene deletion detected by array CGH in a girl with langer mesomelic dysplasia
Author
Toksoy, Güven
Satkın, N
Altunoğlu, Umut
Kayserili Karabay, Hülya
Başaran, Seher
Karaman, Birsen
Uyguner, Zehra Oya
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Langer mesomelic dysplasia (LMD) is characterized by hypomelia with severehypoplasia of ulnae and ibulae, and bowed, thickened radii and tibiae,causing deformities of the hands and feet. LMD is caused by homozygousmutations in the SHOX/SHOXY (short stature homoebox) gene, of whichheterozygous mutations or deletions cause Leri-Weil Dysplasia (LWD).Phenotype of LWD can be incomplete between and within families. We presenta 13 year old female with LMD, the second child of healthy irst cousinparents. She had micrognathia, disproportionate short stature with variousmusculoskeletal indings (absence of the distal lexion creases of the 3rd,4th, 5th ingers on the right, camptodactyly of the 3rd, 4th, 5th ingers onthe left, tibial bowing). X-rays revealed hypoplasia of ulnae, ibulae and themandible. Chromosome analysis and FISH investigation by using SHOX geneprobe revealed normal results. Sequence analysis failed due to unsuccessfulPCR ampliications. Array comparative genomic hybridization (a-CGH) studyshowed a 174 kb homozygous deletion, encompassing the SHOX gene.Proband‘s parents were heterozygous for the same deletion by a-CGH. FISHwas uninformative, because there was no difference between the intensityof the signals on both chromosomes. Since the primers used were locatedwithin the deleted region, molecular studies could not be performed. A-CGHproved to be the most powerful diagnostic tool in this case.
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