Prenatal diagnosis and genetic analysis of a fetus with 6q27 microdeletion.

Dong WU; Weili Shi; Hongdan Wang; Qiaofang Hou; Hui Zhang; Tao LI; Chaoyang Zhang; Yanli Yang; Shixiu Liao

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Prenatal diagnosis and genetic analysis of a fetus with 6q27 microdeletion.

VernacularTitle:一例6q27微缺失的产前诊断及遗传学分析
Author: Dong WU ¹ ; Weili SHI ; Hongdan WANG ; Qiaofang HOU ; Hui ZHANG ; Tao LI ; Chaoyang ZHANG ; Yanli YANG ; Shixiu LIAO
Author Information

1. Henan Provincial People's Hospital, Medical Genetic Institute of Henan Province, People's Hospital of Zhengzhou University, Zhengzhou, Henan 450003, China. ychslshx@126.com.
Publication Type:Case Reports
MeSH: Adult; Chromosome Deletion; Chromosomes, Human, Pair 6; Comparative Genomic Hybridization; Female; Genetic Testing; Humans; Pregnancy; Prenatal Diagnosis
From: Chinese Journal of Medical Genetics 2017;34(5):718-721
CountryChina
Language:Chinese
Abstract:
OBJECTIVETo determine the origin and pathogenicity of a chromosomal aberration for a fetus and analyze the possible mechanism.
METHODSThe karotypes of the fetus and its parents were analyzed with routine G-banding. Their genomic DNA was also analyzed with array comparative genomic hybridization (aCGH).
RESULTSNo karyotypic abnormality was detected at cytogenetic level for the fetus and its parents. aCGH has identified a de novo 2.04 Mb deletion at 6q27 in the fetus. The region involves candidate genes responsible for structural brain abnormalities. The area flanking the chromosomal breakpoint contains a 2410 bp sequence rich in palindromes which can form stable secondary structures.
CONCLUSIONThe de novo 6q27 deletion is pathogenic. The 6q27 deletion may be responsible for the structural brain abnormalities in the fetus. The palindrome sequence flanking the chromosomal breakpoint may be involved the formation of the 6q27 deletion.