<i>ADNP</i>基因变异所致Helsmoortel-Van der Aa综合征一例报道并文献复习

doi:10.3877/cma.j.issn.2095-123X.2022.06.012

Helsmoortel-van der Aa综合征又称ADNP综合征，是由ADNP基因变异引起的一种神经发育障碍疾病，多为常染色体显性遗传。临床表现主要为全面发育迟缓（global developmental delay，GDD）、孤独症谱系障碍（autism spectrum disorder，ASD）表现、特殊面容，也可有行为问题、肌张力减退、癫痫发作、喂养困难、睡眠障碍、先天性心脏病、眼科疾病、皮肤问题、乳牙早萌及头颅MR异常等表现。ADNP基因编码的蛋白由几个功能重要的结构域组成，包括9个锌指基序、1个部分谷胱甘肽还蛋白活性位点、1个二部分核定位信号和1个DNA结合同源盒结构域，该结构域包含1个从N端到C端富含亮氨酸的核输出序列。ADNP基因编码活性依赖的神经保护蛋白广泛表达，参与染色质重塑、转录和微管/自噬调控，与细胞的生长和分化有关，影响大脑发育和认知能力，而且与癌症发生风险存在一定相关性^[1-2]。本文总结1例以"全面发育迟缓"就诊的Helsmoortel-van der Aa综合征患儿的临床资料、基因检测结果及3年的康复治疗效果，现报道如下。

关键词: ADNP基因, Helsmoortel-van der Aa综合征, 错义突变, 康复治疗

图1 先证者及先证者父母一代测序验证图

表1 国内ADNP基因变异所致Helsmoortel-van der Aa综合征的临床特征

项目	病例1^[24]	病例2^[25]	病例3^[26]	本例
性别	男	男	男	男
初诊年龄	18个月	6岁4个月	3岁	2岁
突变位点	c.190dupA（p T64Nfs*35）	c.1222_1223del	c.568C>T（p.Q190X）	c.68T>G（p.L23R）
发育迟缓	1	1	1	1
智力障碍	1	1	1	1
孤独症谱系障碍	1	1	1	0
行为问题	1	1	1	1
癫痫发作	0	1	0	0
头影像学异常	0	1	1	1
乳牙早萌	1	1	1	1
肌张力低下	0	0	0	1
胃肠道问题	1	0	0	0
反复感染	1	0	0	0
视力异常	0	0	1	0
先心	0	0	0	0
前额突出	1	0	1	1
发际线高	1	0	0	0
宽鼻梁	0	1	1	1
鼻短小	0	0	0	1
鼻孔前倾	0	0	0	1
上唇薄	1	1	1	1
耳畸形	0	0	1	0
手畸形	1	0	0	1
外生殖器异常	1	0	0	1

表1 国内ADNP基因变异所致Helsmoortel-van der Aa综合征的临床特征

项目	病例1^[24]	病例2^[25]	病例3^[26]	本例
性别	男	男	男	男
初诊年龄	18个月	6岁4个月	3岁	2岁
突变位点	c.190dupA（p T64Nfs*35）	c.1222_1223del	c.568C>T（p.Q190X）	c.68T>G（p.L23R）
发育迟缓	1	1	1	1
智力障碍	1	1	1	1
孤独症谱系障碍	1	1	1	0
行为问题	1	1	1	1
癫痫发作	0	1	0	0
头影像学异常	0	1	1	1
乳牙早萌	1	1	1	1
肌张力低下	0	0	0	1
胃肠道问题	1	0	0	0
反复感染	1	0	0	0
视力异常	0	0	1	0
先心	0	0	0	0
前额突出	1	0	1	1
发际线高	1	0	0	0
宽鼻梁	0	1	1	1
鼻短小	0	0	0	1
鼻孔前倾	0	0	0	1
上唇薄	1	1	1	1
耳畸形	0	0	1	0
手畸形	1	0	0	1
外生殖器异常	1	0	0	1

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Helsmoortel-van der Aa syndrome caused by ADNP gene variation was followed up for 3 years of rehabilitation: a case report and literature review

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Helsmoortel-van der Aa syndrome caused by ADNP gene variation was followed up for 3 years of rehabilitation: a case report and literature review