蛋白水解应激相关蛋白的异常表达及纤溶酶在朊病毒疾病中的保护作用

IF 3.5 2区农林科学 Q2 INFECTIOUS DISEASES

Transboundary and Emerging Diseases Pub Date : 2025-02-26 DOI:10.1155/tbed/9527934

Yong-Chan Kim, Sae-Young Won, Byung-Hoon Jeong

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引用次数: 0

摘要

朊病毒疾病是由蛋白酶k抗性朊病毒蛋白（PrPSc）引起的致死性、不可逆的感染性神经退行性疾病。针对PrPSc，一些参与细胞降解机制的内源性蛋白酶可以被激活以去除PrPSc。然而，由于PrPSc表现出蛋白酶K抗性，我们推测不可降解的PrPSc诱导了细胞降解机制过度激活的正反馈，并与蛋白水解应激和朊病毒疾病进展的加剧相关。应用免疫组织化学（IHC）和免疫印迹技术（western blotting）研究ME7瘙痒病感染小鼠和散发性克雅氏病（CJD）患者感染后7个月脑内蛋白水解应激相关蛋白的表达模式。此外，我们利用SWISS-MODEL和HawkDock软件分析了朊病毒蛋白（PrP）与纳豆激酶和蚓激酶的三维结构和结合复合物。为了从根本上通过降解PrPSc来减少蛋白水解应激，我们对纤维蛋白溶解酶（包括纳豆激酶和蚓激酶）的PrPSc降解能力进行了体外评估。此外，我们评估了纳豆激酶和蚓激酶对ME7瘙痒病感染小鼠的保护作用。我们在ME7瘙痒病感染小鼠和散发性CJD患者的大脑中观察到蛋白水解应激相关蛋白的异常积累，包括CD10、组织蛋白酶B、组织蛋白酶D和基质金属蛋白酶9 （MMP9）。此外，我们发现纳豆激酶和蚓激酶可以稳定地与PrP结合。此外，我们发现来自ME7瘙痒病感染小鼠和散发性CJD患者的PrPSc在体外被纳豆激酶和蚓激酶显著降解。最后，我们发现纳豆激酶和蚓激酶对ME7瘙痒病感染小鼠的朊病毒病有体内保护作用。据我们所知，这是鉴定蛋白水解应激相关的新型潜在生物标志物以及纳豆激酶和蚓激酶治疗朊病毒疾病潜力的第一份报告。

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Abnormal Expression of Proteolytic Stress-Related Proteins and Protective Effect of Fibrinolytic Enzymes in Prion Diseases

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Abnormal Expression of Proteolytic Stress-Related Proteins and Protective Effect of Fibrinolytic Enzymes in Prion Diseases

Prion diseases are fatal, irreversible, and infectious neurodegenerative diseases caused by proteinase K-resistant prion protein (PrP^Sc). Against PrP^Sc, several endogenous proteases involved in cellular degradation mechanisms can be activated to remove PrP^Sc. However, since PrP^Sc shows proteinase K resistance, we presumed that undegradable PrP^Sc induces positive feedback on the overactivation of the cellular degradation mechanisms and is correlated with proteolytic stress and exacerbation of the progression of prion diseases. We investigated the expression pattern of proteolytic stress-related proteins in the brains of ME7 scrapie-infected mice at 7 months postinfection and sporadic Creutzfeldt–Jakob disease (CJD) patients using western blotting and immunohistochemistry (IHC). In addition, we analyzed the 3D structure and binding complexes of prion protein (PrP) with nattokinase and lumbrokinase using in silico programs, including SWISS-MODEL and HawkDock. To fundamentally reduce proteolytic stress by the degradation of PrP^Sc, we performed an in vitro evaluation of the PrP^Sc degradation abilities of fibrinolytic enzymes, including nattokinase and lumbrokinase. Furthermore, we assessed the protective effects of nattokinase and lumbrokinase in ME7 scrapie-infected mice. We observed an abnormal accumulation of proteolytic stress-related proteins, including CD10, cathepsin B, cathepsin D, and matrix metalloproteinase 9 (MMP9), in the brains of ME7 scrapie-infected mice and sporadic CJD patients. In addition, we identified that nattokinase and lumbrokinase can stably bind to PrP. Furthermore, we identified significant in vitro degradation of PrP^Sc derived from ME7 scrapie-infected mice and sporadic CJD patients by nattokinase and lumbrokinase. Last, we found in vivo protective effects of nattokinase and lumbrokinase against prion disease in ME7 scrapie-infected mice. To the best of our knowledge, this is the first report on the identification of proteolytic stress-related novel potential biomarkers and the therapeutic potential of nattokinase and lumbrokinase for prion diseases.

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来源期刊

Transboundary and Emerging Diseases 农林科学-传染病学

CiteScore

8.90

自引率

9.30%

发文量

350

审稿时长

1 months

期刊介绍： Transboundary and Emerging Diseases brings together in one place the latest research on infectious diseases considered to hold the greatest economic threat to animals and humans worldwide. The journal provides a venue for global research on their diagnosis, prevention and management, and for papers on public health, pathogenesis, epidemiology, statistical modeling, diagnostics, biosecurity issues, genomics, vaccine development and rapid communication of new outbreaks. Papers should include timely research approaches using state-of-the-art technologies. The editors encourage papers adopting a science-based approach on socio-economic and environmental factors influencing the management of the bio-security threat posed by these diseases, including risk analysis and disease spread modeling. Preference will be given to communications focusing on novel science-based approaches to controlling transboundary and emerging diseases. The following topics are generally considered out-of-scope, but decisions are made on a case-by-case basis (for example, studies on cryptic wildlife populations, and those on potential species extinctions): Pathogen discovery: a common pathogen newly recognised in a specific country, or a new pathogen or genetic sequence for which there is little context about — or insights regarding — its emergence or spread. Prevalence estimation surveys and risk factor studies based on survey (rather than longitudinal) methodology, except when such studies are unique. Surveys of knowledge, attitudes and practices are within scope. Diagnostic test development if not accompanied by robust sensitivity and specificity estimation from field studies. Studies focused only on laboratory methods in which relevance to disease emergence and spread is not obvious or can not be inferred (“pure research” type studies). Narrative literature reviews which do not generate new knowledge. Systematic and scoping reviews, and meta-analyses are within scope.