Neurology Department, Centro Hospitalar de Vila Nova de Gaia/Espinho, Vila Nova de Gaia, Portugal.
Neuroradiology Unit, Imagiology Department, Centro Hospitalar de Vila Nova de Gaia/Espinho, Vila Nova de Gaia, Portugal.
Neurol Sci. 2021 Jul;42(7):2955-2959. doi: 10.1007/s10072-021-05096-3. Epub 2021 Jan 31.
Adult polyglucosan body disease (APBD) is an autosomal recessive leukodystrophy characterized by neurogenic bladder starting after 40 years old, spastic paraparesis and peripheral neuropathy. It is mainly resultant from the GBE1 homozygous p.Tyr329Ser (c.986A>C) mutation, especially in Ashkenazi-Jewish patients, although some cases of compound heterozygous have been reported. A genotype-phenotype correlation is not established, but atypical phenotypes have been described mainly in non-p.Tyr329Ser pathogenic variants.
We describe an atypical case in a 62-year-old Portuguese woman, presenting the typical clinical triad of APBD plus prominent autonomic dysfunction, suggested by orthostatic hypotension and thermoregulatory dysfunction; she has compound heterozygous GBE1 mutations, namely, p.Asn541Asp (c.1621A>G) and p.Arg515Gly (c.1543C>G), the last one not yet reported in literature and whose pathogenicity was suggested by bioinformatics analysis and confirmed by sural nerve biopsy that showed intra-axonal polyglucosan bodies.
Besides the report of a novel GBE1 mutation, this case also expands the phenotypic spectrum of this disorder, reinforcing autonomic dysfunction as a possible and prominent manifestation of APBD, mimicking autosomal dominant leukodystrophy with autonomic disease in some way. Therefore, we questioned a possible relationship between this genotype and the phenotype marked by dysautonomia. Additionally, we review previously reported cases of APBD in non-homozygous p.Tyr329Ser patients with atypical phenotypes.
成人多聚糖体病(APBD)是一种常染色体隐性遗传性脑白质病,其特征为 40 岁以后出现神经性膀胱、痉挛性截瘫和周围神经病。它主要是由于 GBE1 纯合 p.Tyr329Ser(c.986A>C)突变引起的,尤其是在阿什肯纳兹犹太人患者中,尽管已经报道了一些复合杂合突变的病例。基因型-表型相关性尚未建立,但已描述了一些非 p.Tyr329Ser 致病性变异的不典型表型。
我们描述了一个 62 岁葡萄牙女性的不典型病例,该患者表现为 APBD 的典型临床三联征,外加明显的自主神经功能障碍,表现为直立性低血压和体温调节功能障碍;她携带 GBE1 的复合杂合突变,即 p.Asn541Asp(c.1621A>G)和 p.Arg515Gly(c.1543C>G),后者尚未在文献中报道,其致病性通过生物信息学分析和腓肠神经活检证实存在轴内多聚糖体得到提示。
除了报告一种新的 GBE1 突变外,本病例还扩展了该疾病的表型谱,强化了自主神经功能障碍作为 APBD 的一种可能且突出的表现,在某种程度上类似于具有自主神经疾病的常染色体显性遗传性脑白质病。因此,我们质疑这种基因型与以自主神经功能障碍为特征的表型之间是否存在关联。此外,我们还回顾了以前报道的非 p.Tyr329Ser 杂合突变的不典型表型的 APBD 病例。
