Department of Rehabilitation, The Children's Hospital, Zhejiang University School of Medicine, Zhejiang, 310052, China.
Cipher Gene, LLC, Beijing, 100080, China.
BMC Med Genet. 2020 Mar 14;21(1):51. doi: 10.1186/s12881-020-0988-3.
The AP4B1 gene encodes a subunit of adaptor protein complex-4 (AP4), a component of intracellular transportation of proteins which plays important roles in neurons. Bi-allelic mutations in AP4B1 cause autosomal recessive spastic paraplegia-47(SPG47).
Here we present a Chinese patient with spastic tetraplegia, moderate psychomotor development delay and febrile seizures plus. Brain MRIs showed dilated supratentorial ventricle, thin posterior and splenium part of corpus callosum. The patient had little progress through medical treatments and rehabilitating regimens. Whole exome sequencing identified novel compound heterozygous truncating variants c.1207C > T (p.Gln403*) and c.52_53delAC (p.Cys18Glnfs*7) in AP4B1 gene. Causal mutations in AP4B1 have been reported in 29 individuals from 22 families so far, most of which are homozygous mutations.
Our study enriched the genetic and phenotypic spectrum of SPG47. Early discovery, diagnosis and proper treatment on the conditions generally increase chances of improvement on the quality of life for patients.
AP4B1 基因编码衔接蛋白复合物-4(AP4)的一个亚基,该复合物是蛋白质细胞内运输的组成部分,在神经元中发挥重要作用。AP4B1 的双等位基因突变导致常染色体隐性痉挛性截瘫 47(SPG47)。
本研究介绍了一名痉挛性四肢瘫痪、中度精神运动发育迟缓、热性惊厥伴热性惊厥附加症的中国患者。脑 MRI 显示扩张性幕上脑室,胼胝体后部和压部变薄。患者经过药物治疗和康复方案治疗后进展甚微。全外显子组测序在 AP4B1 基因中发现了新的复合杂合截断变异 c.1207C>T(p.Gln403*)和 c.52_53delAC(p.Cys18Glnfs*7)。迄今为止,已有 29 名来自 22 个家族的个体报道了 AP4B1 中的致病突变,其中大多数为纯合突变。
本研究丰富了 SPG47 的遗传和表型谱。早期发现、诊断和适当的治疗通常会增加改善患者生活质量的机会。
