CHD1基因变异导致发育落后1例患儿的临床特征及遗传学分析

doi:10.12372/jcp.2025.24e0015

Abstract

Abstract:

Objective To explore the clinical features and genetic mutation characteristics of a case of global developmental delay caused by a novel variant in the CHD1 gene, and to investigate its relationship with Pilarowski- Bjornsson syndrome (PILBOS, OMIM# 617682). Method Trio whole-exome sequencing (trio-WES) was performed to identify the pathogenic gene within the pedigree, and the clinical data of the patient were summarized to analyze both clinical and genetic characteristics. Result The patient was an 8-month-old male and presented to the Department of Pediatric Neurology at our hospital with the main complaint of " developmental delay for more than six months". Trio-WES detection revealed a missense mutation in exon 1 of the CHD1 gene on chromosome 5q15-q21, with a c.13A>G (p.Ser5Gly) mutation (transcript number NM_001270), which represented a novel (de novo) variation consistent with an autosomal dominant inheritance pattern. The final diagnosis was" Comprehensive developmental delay caused by CHD1 gene deficiency". Conclusion There are currently few reports on cases of CHD1 gene mutations, and the identified mutations in this case has not been previously documented. Expanding the genotype phenotype spectrum of CHD1 gene defects also provides data for further understanding of PILBOS disease. Accurate diagnosis relies on molecular genetic testing, and additional cases need to be accumulated for further analysis of genotype phenotype relationships and prognosis evaluation.

Key words: CHD1 gene, Pilarowski-Bjornsson syndrome, trio whole-exome sequencing

CHEN Hao, LI Xiao, LI Lin, GUAN Jing, DONG Yan, ZHANG Xiaoli, DU Kaixian. Clinical characteristics and genetic analysis of a case of developmental delay caused by CHD1 gene variation[J].Journal of Clinical Pediatrics, 2025, 43(1): 45-49.

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References 14

[1]	Pilarowski GO, Vernon HJ, Applegate CD, et al. Missense variants in the chromatin remodeler CHD1 are associated with neurodevelopmental disability[J]. J Med Genet, 2018, 55(8): 561-566. doi: 10.1136/jmedgenet-2017-104759 pmid: 28866611
[2]	Zepeda-Mendoza C, Goodenberger ML, Kuhl A, et al. Familial segregation of a 5q15-q21.2 deletion associated with facial dysmorphism and speech delay[J]. Clin Case Rep, 2019, 7(6): 1154-1160.
[3]	Lusser A, Urwin DL, Kadonaga JT. Distinct activities of CHD1 and ACF in ATP-dependent chromatin assembly[J]. Nat Struct Mol Biol, 2005, 12(2): 160-166.
[4]	Kim MS, Chung NG, Kang MR, et al. Genetic and expressional alterations of CHD genes in gastric and colorectal cancers[J]. Histopathology, 2011, 58(5): 660-668. doi: 10.1111/j.1365-2559.2011.03819.x pmid: 21447119
[5]	Flanagan JF, Mi LZ, Chruszcz M, et al. Double chromodomains cooperate to recognize the methylated histone H3 tail[J]. Nature, 2005, 438(7071): 1181-1185.
[6]	Woodage T, Basrai MA, Baxevanis AD, et al. Characterization of the CHD family of proteins[J]. Proc Natl Acad Sci U S A, 1997, 94(21): 11472-11477.
[7]	Konev AY, Tribus M, Park SY, et al. CHD1 motor protein is required for deposition of histone variant H3.3 into chromatin in vivo[J]. Science, 2007, 317(5841): 1087-1090.
[8]	Simic R, Lindstrom DL, Tran HG, et al. Chromatin remodeling protein Chd1 interacts with transcription elongation factors and localizes to transcribed genes[J]. EMBO J, 2003, 22(8): 1846-1856.
[9]	Lin JJ, Lehmann LW, Bonora G, et al. Mediator coordinates PIC assembly with recruitment of CHD1[J]. Genes Dev, 2011, 25(20): 2198-2209.
[10]	Sims RJ 3rd, Millhouse S, Chen CF, et al. Recognition of trimethylated histone H3 lysine 4 facilitates the recruitment of transcription postinitiation factors and pre-mRNA splicing[J]. Mol Cell, 2007, 28(4): 665-676. doi: 10.1016/j.molcel.2007.11.010 pmid: 18042460
[11]	Al-Aamri M, Alshaqaq M, Al-Abdi SY. A Saudi girl with co-occurring CHD1 (Pilarowski-Bjornsson syndrome) and ASH1L gene variants[J]. Cureus, 2023, 15(12): e49905
[12]	Sunwoo Y, Seo S H, Kim HJ, et al. Variant of CHD1 gene resulting in a Korean case of Pilarowski-Bjornsson syndrome[J]. Journal of Genetic Medicine, 2022, 19(2): 111-114.
[13]	赵少志, 段红芳, 杜囡, 等. 应用CNV-seq鉴定染色体新发不平衡易位一例[J]. 中华医学遗传学杂志, 2020, 37(9): 1053-1054.
	Zhao SZ, Duan HF, Du N, et al. Application of CNV-seq to identify a new case of chromosomal imbalanced translocation[J]. Zhonghua Yixue Yichuan Zazhi, 2020, 37 (9): 1053-1054.
[14]	Wyatt BH, Raymond TO, Lansdon LA, et al. Using an aquatic model, Xenopus laevis, to uncover the role of chromodomain 1 in craniofacial disorders[J]. Genesis, 2021, 59(1-2): e23394.

CHD1变异	例1^[1]	例2^[1]	例3^[1]	例4^[1]	例5^[1]	例6^[12]	本例
CHD1变异	c.1853G>A；p.Arg618Gln (NM_001270)	c.5123G>A；p.Arg1708Gln (NM_001270)	c.5123G>A；p.Arg1708Gln (NM_001270)	c.1379G>A；p.Arg460Lys (NM_001270)	c.421A>G；p.Arg141Gly (NM_001270)	c.862A>G； p.Thr288Ala (NM_001270)	c.13A>G；p.Ser5Gly (NM_001270)
新发变异	+	未知	未知	+	未知	+	+
性别，末次体检年龄	女，5岁	女，6岁	女，10岁	女，7月龄	女，4岁	男，17岁	男，4岁9月龄
身高/cm	103.1(P₁₀~P₂₅)	99.1(<P₃)	128(<P₃)	66.4(P_63.1)	104(P₇₅)	133(<P₃)	105（P₁₀~P₂₅）
体重/kg	18.4(P₅₀)	18.2(P₂₅)	23.4(<P₃)	7.5(P_59.7)	17.7(P₇₅)	19.2(<P₃)	17（P₂₅~P₅₀）
发育落后	+	+	-	+	+	+	+
言语失用	+	+	+		+	+	+
自闭症	+	+	+	-	-	-	-
刻板印象	+	+	+	-	-	-	-
低肌张力	+	+	+/运动障碍	+/运动障碍	+	+	+
智力低下	-	+	+	临界	临界	+	+
大头畸形	+	+	-	-	-	-	-
免疫异常	+	-	+	-	-	-	-
面部凹陷	+	+	+	-	-	+	+
生长迟缓	-	+	+	-	-	+	+
皮肤白皙	+	+	+	-	-	-	-
惊厥发作	失神发作	应用抗发作药物	脑电图异常	+	-	-	-
杏仁眼	+	+/长睫毛	-	-	-	+	+
眉毛下垂	+	+	-	-	-	+	-
眼裂下斜	+	+	+	-	-	+	+
眼周饱满		+	-	+	-	+	-

Clinical characteristics and genetic analysis of a case of developmental delay caused by CHD1 gene variation

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