Lysosomal sialidase NEU1, its intracellular properties, deficiency, and use as a therapeutic agent.

IF 2.7 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Glycoconjugate Journal Pub Date : 2023-12-01 Epub Date: 2023-12-26 DOI:10.1007/s10719-023-10135-6
Kohji Itoh, Jun Tsukimoto
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Abstract

Neuraminidase 1 (NEU1) is a lysosomal sialidase that cleaves terminal α-linked sialic acid residues from sialylglycans. NEU1 is biosynthesized in the rough endoplasmic reticulum (RER) lumen as an N-glycosylated protein to associate with its protective protein/cathepsin A (CTSA) and then form a lysosomal multienzyme complex (LMC) also containing β-galactosidase 1 (GLB1). Unlike other mammalian sialidases, including NEU2 to NEU4, NEU1 transport to lysosomes requires association of NEU1 with CTSA, binding of the CTSA carrying terminal mannose 6-phosphate (M6P)-type N-glycan with M6P receptor (M6PR), and intralysosomal NEU1 activation at acidic pH. In contrast, overexpression of the single NEU1 gene in mammalian cells causes intracellular NEU1 protein crystallization in the RER due to self-aggregation when intracellular CTSA is reduced to a relatively low level. Sialidosis (SiD) and galactosialidosis (GS) are autosomal recessive lysosomal storage diseases caused by the gene mutations of NEU1 and CTSA, respectively. These incurable diseases associate with the NEU1 deficiency, excessive accumulation of sialylglycans in neurovisceral organs, and systemic manifestations. We established a novel GS model mouse carrying homozygotic Ctsa IVS6 + 1 g/a mutation causing partial exon 6 skipping with simultaneous deficiency of Ctsa and Neu1. Symptoms developed in the GS mice like those in juvenile/adult GS patients, such as myoclonic seizures, suppressed behavior, gargoyle-like face, edema, proctoptosis due to Neu1 deficiency, and sialylglycan accumulation associated with neurovisceral inflammation. We developed a modified NEU1 (modNEU1), which does not form protein crystals but is transported to lysosomes by co-expressed CTSA. In vivo gene therapy for GS and SiD utilizing a single adeno-associated virus (AAV) carrying modNEU1 and CTSA genes under dual promoter control will be created.

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溶酶体硅糖苷酶 NEU1、其细胞内特性、缺乏症和作为治疗剂的用途。
神经氨酸酶 1 (NEU1) 是一种溶酶体硅糖苷酶,可从硅氨酰聚糖中裂解末端 α 链接的硅酸残基。NEU1 在粗面内质网(RER)腔内以 N-糖基化蛋白的形式进行生物合成,与其保护蛋白/胰蛋白酶 A(CTSA)结合,然后形成溶酶体多酶复合体(LMC),该复合体还含有 β-半乳糖苷酶 1(GLB1)。与包括 NEU2 至 NEU4 在内的其他哺乳动物硅糖苷酶不同,NEU1 运输到溶酶体需要 NEU1 与 CTSA 结合、携带末端 6- 磷酸甘露糖(M6P)型 N-糖的 CTSA 与 M6P 受体(M6PR)结合以及在酸性 pH 下激活溶酶体内 NEU1。相反,在哺乳动物细胞中过量表达单个 NEU1 基因会导致细胞内 CTSA 降低到相对较低的水平时,细胞内 NEU1 蛋白在 RER 中因自我聚集而结晶。半乳糖醛酸症(SiD)和半乳糖醛酸症(GS)是分别由 NEU1 和 CTSA 基因突变引起的常染色体隐性溶酶体贮积病。这些不治之症与 NEU1 缺乏、神经内脏器官中的半乳糖苷过度积累以及全身性表现有关。我们建立了一种新型的 GS 模型小鼠,该小鼠携带同卵 Ctsa IVS6 + 1 g/a 突变,导致第 6 号外显子部分缺失,并同时缺乏 Ctsa 和 Neu1。GS小鼠出现了与青少年/成人GS患者相似的症状,如肌阵挛性发作、行为抑制、脸部畸形、水肿、Neu1缺乏导致的直肠凋亡以及与神经内脏炎症相关的硅氨酰聚糖堆积。我们开发了一种改良的 NEU1(modNEU1),它不会形成蛋白质晶体,而是通过共表达的 CTSA 转运到溶酶体。我们将利用携带 modNEU1 和 CTSA 基因并受双启动子控制的单一腺相关病毒 (AAV) 对 GS 和 SiD 进行体内基因治疗。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Glycoconjugate Journal
Glycoconjugate Journal 生物-生化与分子生物学
CiteScore
6.00
自引率
3.30%
发文量
63
审稿时长
1 months
期刊介绍: Glycoconjugate Journal publishes articles and reviews on all areas concerned with: function, composition, structure, biosynthesis, degradation, interactions, recognition and chemo-enzymatic synthesis of glycoconjugates (glycoproteins, glycolipids, oligosaccharides, polysaccharides and proteoglycans), biochemistry, molecular biology, biotechnology, immunology and cell biology of glycoconjugates, aspects related to disease processes (immunological, inflammatory, arthritic infections, metabolic disorders, malignancy, neurological disorders), structural and functional glycomics, glycoimmunology, glycovaccines, organic synthesis of glycoconjugates and the development of methodologies if biologically relevant, glycosylation changes in disease if focused on either the discovery of a novel disease marker or the improved understanding of some basic pathological mechanism, articles on the effects of toxicological agents (alcohol, tobacco, narcotics, environmental agents) on glycosylation, and the use of glycotherapeutics. Glycoconjugate Journal is the official journal of the International Glycoconjugate Organization, which is responsible for organizing the biennial International Symposia on Glycoconjugates.
期刊最新文献
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