伊朗一名小头畸形、癫痫发作和发育迟缓儿童的 基因复合杂合突变。
Compound Heterozygous Mutations in Gene in an Iranian Child with Microcephaly, Seizures, and Developmental Delay.
机构信息
Department of Cellular and Molecular Biology, North Tehran Branch, Islamic Azad University, Tehran, Iran.
Department of Medical Genetics, DeNA Laboratory, Tehran, Iran.
出版信息
Fetal Pediatr Pathol. 2021 Apr;40(2):174-180. doi: 10.1080/15513815.2019.1686784. Epub 2019 Nov 9.
BACKGROUND
Pathogenic variants within polynucleotide kinase 3'phosphatase () gene cause microcephaly, seizures, and developmental delay (MCSZ) and ataxia-oculomotor apraxia type 4 (AOA4) disorders due to unrepaired DNA lesions.
METHODS
Whole exome sequencing was performed on a child with microcephaly, seizures, developmental delay, callosal dysgenesis on MRI, intellectual disability, speech disorder, hyperactivity, and ataxic gait.
RESULTS
Two heterozygous mutations in the gene, a novel intronic frameshift variant c.1298 + 33_1299-24del and a previously reported duplication, c.1253_1269dup; p.Thr424Glyfs*49 in exon 14 were identified. Both of these mutations affect the DNA kinase domain of PKNP.
CONCLUSIONS
Our finding along with previous studies provide more evidence of the clinical heterogeneity of diseases caused by mutations in which makes its clinical diagnosis difficult and highlights the importance of genetic testing to unravel the cause of these diseases.
背景
多核苷酸激酶 3'磷酸酶()基因内的致病性变异导致未修复的 DNA 损伤,从而引起小头畸形、癫痫和发育迟缓(MCSZ)以及共济失调-眼动运动不能症 4 型(AOA4)疾病。
方法
对一名患有小头畸形、癫痫、发育迟缓、MRI 上胼胝体发育不良、智力残疾、言语障碍、多动和共济失调步态的儿童进行了全外显子组测序。
结果
在基因中发现了两个杂合突变,一个新的内含子移码变异 c.1298 + 33_1299-24del 和一个先前报道的重复,c.1253_1269dup; p.Thr424Glyfs*49 在第 14 外显子中。这两种突变都影响了 PKNP 的 DNA 激酶结构域。
结论
我们的发现以及以前的研究提供了更多由基因突变引起的疾病的临床异质性的证据,这使得其临床诊断变得困难,并强调了遗传检测对于揭示这些疾病病因的重要性。
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