PSAT1基因变异致轻型丝氨酸缺乏症：以鱼鳞病合并周围神经病为表型的临床特征与遗传学分析

doi:10.12372/jcp.2026.25e1598

临床儿科杂志 ›› 2026, Vol. 44 ›› Issue (5): 424-430.doi: 10.12372/jcp.2026.25e1598

PSAT1基因变异致轻型丝氨酸缺乏症：以鱼鳞病合并周围神经病为表型的临床特征与遗传学分析

黄海生¹^,², 赵安琪², 曾琴², 王雨蒙², 何伟², 李明¹^,²()

1.安徽理工大学第一附属医院（安徽淮南 232001）
2.复旦大学附属儿童医院皮肤科（上海 201102）

收稿日期:2025-12-16 录用日期:2026-03-30 出版日期:2026-05-15 发布日期:2026-05-08
通讯作者: 李明电子邮箱：mingli@fudan.edu.cn
作者简介:作者贡献（Authors’ Contributions）
黄海生负责论文构思，撰写论文；赵安琪负责整理与收集资料；曾琴负责收集资料；王雨蒙负责分析、解释数据；何伟负责查阅文献；李明负责指导论文撰写，论文审核。
基金资助:
国家自然科学基金资助项目(82273504);国家自然科学基金资助项目(82473509)

PSAT1 gene variant causes mild serine deficiency: clinical and genetic analysis of ichthyosis combined with peripheral neuropathy

HUANG Haisheng¹^,², ZHAO Anqi², ZENG Qin², WANG Yumeng², HE Wei², LI Ming¹^,²()

1. Anhui University of Science and Technology First Affiliated Hospital, Huainan 232001, Anhui, China
2. Department of Dermatology, Children’s Hospital of Fudan University, Shanghai 201102, China

Received:2025-12-16 Accepted:2026-03-30 Published:2026-05-15 Online:2026-05-08

摘要/Abstract

摘要：

目的探讨PSAT1基因变异丝氨酸缺乏症的临床分型、遗传学基础及诊疗策略，提升临床对该病的识别能力。方法回顾性收集1例以鱼鳞病合并周围神经病为表现的患儿临床资料，通过家系全外显子组测序、Sanger验证及蛋白质结构预测研究其遗传学病理机制，并随访其治疗结果。系统检索数据进行文献复习，总结其临床表型、基因变异特征、治疗反应及预后特点。结果患儿女，12岁，2岁起出现全身皮肤干燥脱屑，7岁起进行性双下肢无力、足下垂，伴水平眼震。既往检查示血浆丝氨酸水平正常（233.29μmol/L、319.19μmol/L），家系全外显子组测序检出PSAT1基因新纯合变异c.697C>A（p.Q233K），ACMG评级为意义未明变异，Sanger验证显示父母均为携带者。予以患者口服L-丝氨酸（300 mg·kg^-1·d^-1）和甘氨酸（200 mg·kg^-1·d^-1）补充治疗，1周后皮肤干燥脱屑明显好转，13周后行走步态显著改善，可自主下蹲站起。文献复习共纳入5例轻型丝氨酸缺乏症，结合本例共6例，均为PSAT1基因变异。结论丝氨酸缺乏症表型谱广泛，轻型以儿童期鱼鳞病合并青少年期周围神经病为核心表现，因血浆丝氨酸水平多正常或轻度降低极易漏诊。早期诊断与及时补充L-丝氨酸对改善预后至关重要，可避免不可逆神经损伤。对原因不明的鱼鳞病伴周围神经病变患者，应尽早行基因检测以明确诊断。

关键词: PSAT1基因, 轻型丝氨酸缺乏症, 鱼鳞病合并周围神经病

Abstract:

Objective To investigate the clinical classification, genetic basis, and diagnostic and treatment strategies for serine deficiency caused by PSAT1 gene variants, in order to improve clinical recognition of this disorder. Methods Clinical data were retrospectively collected from a pediatric patient presenting with ichthyosis complicated by peripheral neuropathy. Family-based whole exome sequencing, Sanger validation, and protein structure prediction were performed. Following identification of the causative gene, treatment and follow-up were conducted. A systematic literature review was also carried out to summarize the clinical phenotypes, genetic variant characteristics, treatment responses, and prognostic features. Results The patient was a 12-year-old female who developed dry, scaly skin across the body at 2 years of age. Since the age of 7 years, she experienced progressive weakness in both lower limbs, foot drop, and horizontal nystagmus. Previous examinations revealed normal plasma serine levels (233.29 μmol/L and 319.19 μmol/L). Family-based whole exome sequencing identified a novel homozygous PSAT1 gene variant, c.697C>A (p.Q233K), which was classified as a variant of uncertain significance according to ACMG guidelines. Sanger sequencing confirmed that both parents were carriers. The patient received oral supplementation with L-serine （300 mg·kg^-1·d^-1） and glycine （200 mg·kg^-1·d^-1）. After one week of treatment, the dry skin and desquamation improved significantly. After 13 weeks, gait showed marked improvement, and the patient was able to squat and stand up independently. A literature review identified five additional cases of mild serine deficiency. Including the present case, a total of six cases were identified, all of which carried PSAT1 gene variants. Conclusion The phenotypic spectrum of serine deficiency is broad, with the mild form characterized by childhood-onset ichthyosis and adolescent-onset peripheral neuropathy as core manifestations. Affected individuals often have normal or only mildly reduced plasma serine levels, making this condition highly prone to being missed. Early diagnosis and timely supplementation with L-serine are critical for improving prognosis and can prevent irreversible neurological damage. For patients presenting with unexplained ichthyosis accompanied by peripheral neuropathy, genetic testing should be pursued as early as possible to establish a definitive diagnosis.

Key words: PSAT1 gene, mild serine deficiency disorders, ichthyosis combined with peripheral neuropathy

中图分类号:

黄海生, 赵安琪, 曾琴, 王雨蒙, 何伟, 李明. PSAT1基因变异致轻型丝氨酸缺乏症：以鱼鳞病合并周围神经病为表型的临床特征与遗传学分析[J]. 临床儿科杂志, 2026, 44(5): 424-430.

HUANG Haisheng, ZHAO Anqi, ZENG Qin, WANG Yumeng, HE Wei, LI Ming. PSAT1 gene variant causes mild serine deficiency: clinical and genetic analysis of ichthyosis combined with peripheral neuropathy[J]. Journal of Clinical Pediatrics, 2026, 44(5): 424-430.

图/表 4

图1

图2

图3

表1

6例轻型丝氨酸缺乏症临床资料"

患者	性别	确诊年龄/岁	PSAT1基因变异位点	临床表现	治疗方案	治疗效果
1^[2]	男	19	纯合变异：c. 43G>C（p. A15P）	皮肤（婴儿期起病鱼鳞病），神经（16岁起病足下垂，下肢无力、远端麻木，双手拇指伸直困难，水平+垂直眼震，低频感音神经性耳聋）	口服L-丝氨酸300 mg·kg^-1·d^-1+甘氨酸300 mg·kg^-1·d^-1	皮肤3个月后完全缓解；肌力改善，但深感觉障碍无缓解（未提及改善时间）
2^[2]	男	17	纯合变异：c. 43G>C（p. A15P）	皮肤（4岁起病鱼鳞病，16岁时面部、四肢远端红肿脱屑伴溃疡）；神经（6岁起病下肢无力、无法踮脚、足部麻木，水平+垂直眼震，视盘轻度萎缩1）	口服L-丝氨酸300 mg·kg^-1·d^-1+甘氨酸300 mg·kg^-1·d^-1	皮肤5个月后完全恢复；下肢肌力提升，痛温觉减退范围缩小
3^[3]	男	16	纯合变异：c. 43G>C（p. A15P）	皮肤（4岁起病鱼鳞病）；神经（16岁起病下肢无力、上楼梯需搀扶，足底麻木，水平+垂直眼震）	口服L-丝氨酸300 mg·kg^-1·d^-1+甘氨酸300 mg·kg^-1·d^-1	皮肤1年后完全恢复正常；2年后下肢麻木好转、肌力改善（可快走、上下楼梯，仍无法跑步）
4^[4]	男	17	纯合变异：c. 43G>C（p. A15P）	皮肤（出生即鱼鳞病），神经（13岁起病足下垂、下肢无力，17岁丧失行走能力，水平眼震，低频感音神经性耳聋）	口服L-丝氨酸初始3 g·d^-1，1年内逐渐增至100 mg·kg^-1·d^-1	丝氨酸补充治疗前通过对症治疗皮损已显著改善；1 年后下肢感觉改善，足跖屈、背屈肌力提升
5^[4]	女	14	复合杂合变异： c.43G>C （p.A15P）； c.112A>C （p.S38R）	皮肤（5岁起病鱼鳞病），神经（12岁起病无法踮脚，14岁足下垂）	口服L-丝氨酸初始3 g·d^-1，10个月内逐渐增至100 mg·kg^-1·d^-1	10天后皮损显著改善；10个月后四肢肌力恢复至5/5
本文	女	12	纯合变异：c. 697C>A p.Q233K）	皮肤（生后2年起病鱼鳞病），神经（7岁起病足下垂，下肢无力，水平眼震）	口服L-丝氨酸300 mg·kg^-1·d^-1+甘氨酸200 mg·kg^-1·d^-1	1周后皮损显著改善；3个月后肌力部分恢复，可自主下蹲站起

表1

参考文献 12

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PSAT1基因变异致轻型丝氨酸缺乏症：以鱼鳞病合并周围神经病为表型的临床特征与遗传学分析

PSAT1 gene variant causes mild serine deficiency: clinical and genetic analysis of ichthyosis combined with peripheral neuropathy

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