DHTKD1基因复合杂合变异致α-酮己二酸尿症1例报告

doi:10.12372/jcp.2023.22e0486

摘要/Abstract

摘要：

α-酮己二酸尿症为赖氨酸、羟赖氨酸和色氨酸降解代谢紊乱所致的遗传代谢病，临床表现轻重不一，受累系统广泛，主要临床表现有生长发育迟缓、肌张力减退、癫痫、共济失调、小头畸形、行为异常等。本例患儿2岁8月龄，表现为抽搐和行为异常，尿有机酸分析示α-酮己二酸明显增高，基因遗传学检测发现DHTKD1基因存在致病复合杂合变异，结合患儿临床特征和遗传学特点，确诊为α-酮己二酸尿症。经低赖氨酸、低蛋白饮食和康复治疗等对症处理后，患儿病情有所改善。该病临床罕见，为国内医学数据库首例报道。本病例报道扩充了α-酮己二酸尿症基因谱，也为临床上该病的诊治提供借鉴与参考。

关键词: α-酮己二酸尿症, DHTKD1基因, 复合杂合变异, 儿童

Abstract:

Alpha-ketoadipic aciduria is a genetic metabolic disease caused by the disorder of lysine, hydroxylysine and tryptophan degradation metabolism. The clinical manifestations of the disease vary in severity and affect a wide range of systems. The main clinical manifestations include growth retardation, hypotonia, epilepsy, ataxia, microcephaly and abnormal behavior. The patient was 2 years and 8 months old and presented with convulsions and behavioral abnor malities. Urine organic acid analysis showed that α-ketoadipic acid was significantly increased. Genetic testing revealed that DHTKD1 gene had pathogenic compound heterozygous variation. Combined with the clinical and genetic characteristics of the child, the diagnosis of α-ketoadipic aciduria was confirmed. The patient's condition improved after symptomatic treatment with a low lysine and protein diet and rehabilitation. This is the first report of α-ketoadipic aciduria in Chinese medical database, which expands the genetic spectrum of α-ketoadipic aciduria and provides reference for clinical diagnosis and treatment of the disease.

Key words: α-ketoadipic aciduria, DHTKD1 gene, compound heterozygous variation, child

王红霞, 潘翔, 逯军. DHTKD1基因复合杂合变异致α-酮己二酸尿症1例报告[J]. 临床儿科杂志, 2023, 41(8): 624-628.

WANG Hongxia, PAN Xiang, LU Jun. Report a case of α-ketoadipic aciduria caused by compound heterozygous variant of DHTKD1 gene[J]. Journal of Clinical Pediatrics, 2023, 41(8): 624-628.

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参考文献 11

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扩增子	对照（男性）	对照（女性）	受检者
SG9800	2.00	1.76	1.68
SG9795	2.00	2.04	1.08
SG9796	2.00	1.93	1.05
SG9797	2.00	2.03	1.18
SG9801	2.00	2.08	2.28
S7	2.00	2.25	2.07
XP60	1.00	1.87	1.10

病例	性别	发病年龄	诊断年龄	基因型	临床表型
1^[6]	男	N/A	N/A	c.2185G>A (p.G729R; c.2318C>T (p.P773L)	自闭症，癫痫，智力低下
2^[6]	女	N/A	新生儿期	c.2185G>A(p.G729R); c.1309G>T (p.E437X)	无异常（疾病筛查发现）
3^[6]	男	2岁	2岁	c.2185G>A (p.G729R)	生长发育迟缓，癫痫
4^[6]	男	16岁	17岁	c.1364G>A (p.R455Q); c.2329 T>C (p.S777P)	行为去抑，智力低下
5^[6]	男	N/A	N/A	c.1364G>A (p.R455Q); c.1159+5G>A	运动、语言发育落后，轻度智力低下，强迫症，睡眠障碍
6^[6]	男	N/A	24岁	c.1671+1G>A; c.1671+1G>A	巨结肠，小脑发育异常，多指畸形，面容异常，行为异常
7^[6]	男	新生儿期	2岁6月	c.700_701delinsGG(p.L234G); c.700_701delinsGG (p.L234G)	肝脏增大，黄疸，生长发育迟缓
8^[6]	男	1岁	9岁	c.2185G>A (p.G729R); c.86dup (p.Y63IfsX3)	严重精神运动性迟滞，癫痫，反复感染
9^[6]	女	8月	1岁2月	c.1364G>A (p.R455Q)	智力低下，癫痫，肌张力低下，面容异常
10^[6]	女	新生儿期	1岁2月	c.2134C>T (p.R712X); c.2134C>T (p.R712X)	运动发育落后，肌张力低下，代谢性酸中毒，纤维母细胞缺乏
11^[2]	女	1岁3月	2岁	c.2143C>T(p.R715C); c.2185G>A(p.G729R)	运动、语言发育落后，多动症，小头畸形
12^[2]	女	N/A	1月15天	c.915G>C(p.Q305H); c.915G>C( p.Q305H)	无异常（疾病筛查发现）
13^[2]	女	10月	2岁	c.1A>G(p.M1?); c.2185G>A(p.G729R)	精神运动发育迟缓，多动症
14^[2]	女	9月	2岁	c.1228C>T(p.R410X); c.2185G>A(p.G729R)	精神运动发育迟缓，语言发育落后，肌张力低下

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