Kowalczyk M, Tomaszewska A, Podbioł-Palenta A, Constantinou M, Wawrzkiewicz-Witkowska A, Kowalski J, Kałużewski B, Zajączek S, Srebniak M I
Department of Medical Genetics, Medical University of Silesia, Sosnowiec, Poland.
Cytogenet Genome Res. 2013;139(1):9-16. doi: 10.1159/000342165. Epub 2012 Sep 5.
Trisomy 9p is the fourth most common chromosome abnormality found in liveborns. We report on a rare case of partial trisomy 9p complicated by partial monosomy 9p. Clinical manifestation included craniofacial abnormalities typical for trisomy 9p syndrome, developmental delay, mental retardation and brain anomaly in the form of Dandy-Walker malformation. The cytogenetic abnormality was investigated with FISH and array-CGH to characterize the breakpoints of the complex rearrangement. The patient's karyotype was 46,XX,der(9)del(9)(p24)dup(9)(p21p24)dn.arr 9p24.3p24.2 (1-2,414,485)×1,9p24.2p21.3(2,414,485-24,101,280)×3. The cytogenetic rearrangement led to a 2.4-Mb deletion of 9p24.2pter and a 21.6-Mb duplication of 9p24.2p21.3. The clinical and cytogenetic findings in our and other similar patients are compared.
9号染色体短臂三体是活产儿中第四常见的染色体异常。我们报告了一例罕见的9号染色体短臂部分三体合并9号染色体短臂部分单体的病例。临床表现包括9号染色体短臂三体综合征典型的颅面异常、发育迟缓、智力障碍以及丹迪-沃克畸形形式的脑异常。采用荧光原位杂交(FISH)和阵列比较基因组杂交(array-CGH)研究细胞遗传学异常,以确定复杂重排的断点。患者的核型为46,XX,der(9)del(9)(p24)dup(9)(p21p24)dn.arr 9p24.3p24.2 (1-2,414,485)×1,9p24.2p21.3(2,414,485-24,101,280)×3。细胞遗传学重排导致9号染色体短臂24.2至末端2.4兆碱基的缺失以及9号染色体短臂24.2至21.3区域21.6兆碱基的重复。我们将本病例及其他类似患者的临床和细胞遗传学发现进行了比较。
