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Imaging alpha-synuclein pathology in Parkinson's disease
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作者 Ruiqing Ni 《Neural Regeneration Research》 2026年第4期1566-1567,共2页
Parkinson's disease(PD)is the second most common neurodegenerative disorder.The clinical manifestations of PD include motor symptoms,such as bradykinesia,resting tremor,rigidity,and nonmotor symptoms,which include... Parkinson's disease(PD)is the second most common neurodegenerative disorder.The clinical manifestations of PD include motor symptoms,such as bradykinesia,resting tremor,rigidity,and nonmotor symptoms,which include disturbances in sleep,gastrointestinal function,and olfaction.PD misdiagnosis rates have been reported to reach approximately 30%,partly owing to the heterogeneity of parkinsonism with non-PD pathologies,and the differential diagnosis of PD from neurodegenerative diseases such as multiple systemic atrophy(MSA)and progressive supranuclear palsy poses another unmet need. 展开更多
关键词 neurodegenerative diseases neurodegenerative disorder alpha synuclein pathology parkinsons disease pd Parkinsons disease resting tremor neurodegenerative disorderthe BRADYKINESIA
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Determinants of alpha-synuclein pathogenesis in Parkinson's disease
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作者 Oriol Barcenas Marc Estivill-Alonso Salvador Ventura 《Neural Regeneration Research》 2026年第4期1568-1569,共2页
Alpha-synuclein and Parkinson's disease:Neuronal damage and inflammation caused by the aggregation of alpha-synuclein(α-syn)are central to a group of disorders known as synucleopathies,which includes Parkinson... Alpha-synuclein and Parkinson's disease:Neuronal damage and inflammation caused by the aggregation of alpha-synuclein(α-syn)are central to a group of disorders known as synucleopathies,which includes Parkinson's disease(PD),dementia with Lewy bodies,and multiple system atrophy,among others.PD,the most common synucleinopathy,is the second most prevalent neurodegenerative disease after Alzheimer's disease,and it is the fastest growing.Its primary hallmark is the degeneration of dopaminergic neurons in the substantia nigra pars compacta,disrupting the communication with the striatum. 展开更多
关键词 parkinsons disease pd dementia parkinsons disease neuronal neurodegenerative disease multiple system atrophyamong alzheimers diseaseand Parkinsons disease alpha synuclein degeneration dopaminergic neurons
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Alpha-synuclein自身抗体用作帕金森病抗体治疗的探索研究 被引量:3
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作者 车环宇 赵凌志 +2 位作者 倪雪 滕国生 车翀 《中国免疫学杂志》 CAS CSCD 北大核心 2019年第23期2911-2915,共5页
目的:通过从外周血中分离B细胞并进行培养,对外周血中存在的alpha-synuclein(α-syn)自身抗体进行分析,以探索用α-syn自身抗体开发治疗帕金森病(PD)抗体药物的可行性。方法:采集健康捐赠人的外周血并分离外周血B细胞进行培养,对B细胞... 目的:通过从外周血中分离B细胞并进行培养,对外周血中存在的alpha-synuclein(α-syn)自身抗体进行分析,以探索用α-syn自身抗体开发治疗帕金森病(PD)抗体药物的可行性。方法:采集健康捐赠人的外周血并分离外周血B细胞进行培养,对B细胞培养上清进行ELISA结合活性分析,并用硫黄素T(ThT)法检测B细胞培养上清中α-syn自身抗体的生物学活性。结果:细胞培养13 d后,镜检发现B细胞扩增孔数可以达到90%以上,表明B细胞在实验条件下生长良好并能维持抗体分泌能力。ELISA结果表明检测的10530个样品中有48个可以和α-syn单体结合(OD 450>0.5),其中36个可以同时结合α-syn单体和聚合体(OD 450>0.5),并且该36个样品和α-syn家族蛋白β-synuclein以及γ-synuclein无交叉反应,具有α-syn结合特异性。用硫黄素T(ThT)法对该组样品进行的抑制聚合活性检测,结果表明36个样品中有9个样品能够显著性地抑制α-syn单体聚合,并且其中两个样品25G07和55F02的抑制率可以达到50%。结论:可以通过分离培养外周血B细胞获得具有生物学活性的α-syn自身抗体,用作治疗帕金森病的抗体药物研发。 展开更多
关键词 alpha-synuclein(α-syn) B细胞 自身抗体 帕金森病(PD)
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表达alpha-synuclein A53T神经干细胞系的建立
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作者 沈雁飞 柳明杰 《沈阳药科大学学报》 CAS CSCD 北大核心 2013年第6期470-473,共4页
目的建立表达alpha-synuleinA53T突变体的神经干细胞。方法采用Xho I/Hpa I双酶切paSynA53T-DsRed,将含SynA53T-DsRed片段连接到pBudCE4.1-1X-aSynA53T-DsRed的Xho I/PmeI位点构建pBudCE4.1-2X-aSynA53T-DsRed质粒。利用Lipofectamine2... 目的建立表达alpha-synuleinA53T突变体的神经干细胞。方法采用Xho I/Hpa I双酶切paSynA53T-DsRed,将含SynA53T-DsRed片段连接到pBudCE4.1-1X-aSynA53T-DsRed的Xho I/PmeI位点构建pBudCE4.1-2X-aSynA53T-DsRed质粒。利用Lipofectamine2000介导转染2μg的pBudCE4.1-2X-aSynA53T-DsRed到鼠源性神经干细胞(mNSCs)后24 h和72 h观察转染结果。结果成功构建重组质粒pBudCE4.1-2X-aSynA53T-DsRed,转染24 h后其表达率达到(57±3.52)%,72 h的表达率达到了(27.14±3.21)%。结论通过质粒重组及转染技术,成功获得了表达aSynA53T的神经干细胞,为揭示α-synA53T导致帕金森氏症的病理过程提供了平台。 展开更多
关键词 核突触蛋白 质粒 转染 表达
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Implications of alpha-synuclein nitration at tyrosine 39 in methamphetamine-induced neurotoxicity in vitro and in vivo 被引量:2
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作者 Hong-Hua Qiao Lin-Nan Zhu +5 位作者 Yue Wang Jia-Liang Hui Wei-Bing Xie Chao Liu Ling Chen Ping-Ming Qiu 《Neural Regeneration Research》 SCIE CAS CSCD 2019年第2期319-327,共9页
Methamphetamine is an amphetamine-type psychostimulant that can damage dopaminergic neurons and cause characteristic pathological changes similar to neurodegenerative diseases such as Parkinson's disease. However,... Methamphetamine is an amphetamine-type psychostimulant that can damage dopaminergic neurons and cause characteristic pathological changes similar to neurodegenerative diseases such as Parkinson's disease. However, its specific mechanism of action is still unclear. In the present study, we established a Parkinson's disease pathology model by exposing SH-SY5 Y cells and C57 BL/6 J mice to methamphetamine. In vitro experiments were performed with 0, 0.5, 1.0, 1.5, 2.0 or 2.5 mM methamphetamine for 24 hours or 2.0 mM methamphetamine for 0-, 2-, 4-, 8-, 16-, and 24-hour culture of SH-SY5 Y cells. Additional experimental groups of SH-SY5 Y cells were administered a nitric oxide inhibitor, 0.1 mM N-nitro-L-arginine, 1 hour before exposure to 2.0 mM methamphetamine for 24 hours. In vivo experiments: C57 BL/6 J mice were intraperitoneally injected with N-nitro-L-arginine(8 mg/kg), eight times, at intervals of 12 hours. Methamphetamine 15 mg/kg was intraperitoneally injected eight times, at intervals of 12 hours, but 0.5-hour after each N-nitro-L-arginine injection in the combined group. Western blot assay was used to determine the expression of nitric oxide synthase, α-synuclein(α-Syn), 5 G4, nitrated α-synuclein at the residue Tyr39(nT39 α-Syn), cleaved caspase-3, and cleaved poly ADP-ribose polymerase(PARP) in cells and mouse brain tissue. Immunofluorescence staining was conducted to measure the positive reaction of NeuN, nT39 α-Syn and 5 G4. Enzyme linked immunosorbent assay was performed to determine the dopamine levels in the mouse brain. After methamphetamine exposure, α-Syn expression increased; the aggregation of α-Syn 5 G4 increased; nT39 α-Syn, nitric oxide synthase, cleaved caspase-3, and cleaved PARP expression increased in the cultures of SH-SY5 Y cells and in the brains of C57 BL/6 J mice; and dopamine levels were reduced in the mouse brain. These changes were markedly reduced when N-nitro-L-arginine was administered with methamphetamine in both SH-SY5 Y cells and C57 BL/6 J mice. These results suggest that nT39 α-Syn aggregation is involved in methamphetamine neurotoxicity. 展开更多
关键词 nerve REGENERATION alpha-synuclein nitrated α-synuclein Parkinson's disease METHAMPHETAMINE N-nitro-L-arginine alpha-synuclein aggregation apoptosis NEUROTOXICITY neural REGENERATION
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Subcellular localization of alpha-synuclein aggregates and their interaction with membranes 被引量:4
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作者 Fabiana Miraglia Alessio Ricci +1 位作者 Lucia Rota Emanuela Colla 《Neural Regeneration Research》 SCIE CAS CSCD 2018年第7期1136-1144,共9页
For more than a decade numerous evidence has been reported on the mechanisms of toxicity of α-synuclein(αS) oligomers and aggregates in α-synucleinopathies.These species were thought to form freely in the cytopla... For more than a decade numerous evidence has been reported on the mechanisms of toxicity of α-synuclein(αS) oligomers and aggregates in α-synucleinopathies.These species were thought to form freely in the cytoplasm but recent reports of αS multimer conformations when bound to synaptic vesicles in physiological conditions,have raised the question about where αS aggregation initiates.In this review we focus on recent literature regarding the impact on membrane binding and subcellular localization of αS toxic species to understand how regular cellular function of αS contributes to pathology.Notably αS has been reported to mainly associate with specific membranes in neurons such as those of synaptic vesicles,ER/Golgi and the mitochondria,while toxic species of αS have been shown to inhibit,among others,neurotransmission,protein trafficking and mitochondrial function.Strategies interfering with αS membrane binding have shown to improve αS-driven toxicity in worms and in mice.Thus,a selective membrane binding that would result in a specific subcellular localization could be the key to understand how aggregation and pathology evolves,pointing out to αS functions that are primarily affected before onset of irreversible damage. 展开更多
关键词 alpha-synuclein oligomers aggregates subcellular localization membranes binding Parkinson's disease neurodegeneration alpha-synucleinopathies
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Nanomolar concentration of alpha-synuclein enhances dopaminergic neuronal survival via Akt pathway 被引量:2
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作者 Ji-Young Kim Beom Seok Jeon +1 位作者 Han-Joon Kim Tae-Beom Ahn 《Neural Regeneration Research》 SCIE CAS CSCD 2013年第35期3269-3274,共6页
Although alpha-synuclein is generally thought to have a pathological role in Parkinson's disease, accumulative evidence exists that alpha-synuclein has a neuroprotective effect. The aim of this study was to evaluate ... Although alpha-synuclein is generally thought to have a pathological role in Parkinson's disease, accumulative evidence exists that alpha-synuclein has a neuroprotective effect. The aim of this study was to evaluate the effect of extracellular alpha-synuclein on dopaminergic cell survival. We assessed cell viability using the 3-(4,5-dimethyt-thiazol-2-yt)-2,5-diphenyltertazolium bromide (MTT) assay both in undifferentiated SH-SY5Y (SHSY) cells and neuronally-differentiated SH-SY5Y (ndSHSY) cells after 24 hour treatment with monomeric alpha-synuclein at various concentrations (0 [control], 50, 100 nmol/L, 1 IJmol/L). To determine whether cell viability assessed by MTT assay was affected by cell proliferation, 5-bromo-2'-deoxyuridine (BrdU) incorporation assay was per- formed. Level of both Akt and phosphorylated Akt was measured using western blot method in ndSHSY cells with or without 24 hour alpha-synuclein treatment. Cell viability was increased in ndSHSY cells at the nanomolar concentration of alpha-synuclein, but not in SHSY cells. Proportion of BrdU-positive ndSHSY cells was decreased in alpha-synuclein-treated group compared with control group. Level of phosphorylated Akt in alpha-synuclein-treated group was higher compared with the control group. Our study shows that extracellular alpha-synuclein at nanomolar concentra- tion benefits dopaminergic cell survival via Akt pathway. 展开更多
关键词 neural regeneration alpha-synuclein neuronal survival nanomolar extracellular phosphorylatedAkt SH-SY5Y cell neuronal differentiation proliferation DOPAMINERGIC 5-bromo-2'-deoxyuridine grants-supported paper NEUROREGENERATION
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Navigating the dynamic landscape of alpha-synuclein morphology: a review of the physiologically relevant tetrameric conformation 被引量:1
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作者 Heather R.Lucas Ricardo D.Fernández 《Neural Regeneration Research》 SCIE CAS CSCD 2020年第3期407-415,共9页
N-acetylatedα-synuclein(αSyn)has long been established as an intrinsically disordered protein associated with a dysfunctional role in Parkinson’s disease.In recent years,a physiologically relevant,higher order conf... N-acetylatedα-synuclein(αSyn)has long been established as an intrinsically disordered protein associated with a dysfunctional role in Parkinson’s disease.In recent years,a physiologically relevant,higher order conformation has been identified as a helical tetramer that is tailored by buried hydrophobic interactions and is distinctively aggregation resistant.The canonical mechanism by which the tetramer assembles remains elusive.As novel biochemical approaches,computational methods,pioneering purification platforms,and powerful imaging techniques continue to develop,puzzling information that once sparked debate as to the veracity of the tetramer has now shed light upon this new counterpart inαSyn neurobiology.Nuclear magnetic resonance and computational studies on multimericαSyn structure have revealed that the protein folding propensity is controlled by small energy barriers that enable large scale reconfiguration.Alternatively,familial mutations ablate tetramerization and reconfigure polymorphic fibrillization.In this review,we will discuss the dynamic landscape ofαSyn quaternary structure with a focus on the tetrameric conformation. 展开更多
关键词 alpha-synuclein amyloid FIBRILS intrinsically disordered PROTEIN MULTIMER N-ACETYLATION oligomer Parkinson’s disease PROTEIN folding PROTEIN structure TETRAMER
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内源性神经毒素Salsolinol和N-甲基-(R)-salsolinol诱导共培养SH-SY5Y细胞中Alpha-synuclein的聚集 被引量:1
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作者 刘秀洁 甘巧玉 王馥丽 《生命科学仪器》 2022年第5期24-31,共8页
路易氏小体是帕金森病(PD)患者典型的病理特征,其主要由alpha-synuclein(α-syn)蛋白组成。α-syn蛋白在PD患者脑内的聚集通常伴随着T细胞的浸润和神经元细胞的退化。已有的研究表明1-甲基-4-苯基-1,2,3,4-四氢异喹啉(Salsolinol,Sal)N... 路易氏小体是帕金森病(PD)患者典型的病理特征,其主要由alpha-synuclein(α-syn)蛋白组成。α-syn蛋白在PD患者脑内的聚集通常伴随着T细胞的浸润和神经元细胞的退化。已有的研究表明1-甲基-4-苯基-1,2,3,4-四氢异喹啉(Salsolinol,Sal)N-甲基转移酶与内源性神经毒素1(R),2(N)-二甲基-6,7-二羟基-1,2,3,4-四氢异喹啉(N-甲基-(R)-salsolinol,NMSal)在PD患者淋巴细胞中的升高有关。本文采用稳定转染EGFP的人母细胞瘤SH-SY5Y(SH-EGFP)细胞和人多形性胶质母细胞瘤U87细胞和外周T淋巴细胞Jurkat三种细胞共培养模型来研究内源性神经毒素Sal和NMSal对共同培养体系中SH-EGFP细胞中α-syn蛋白的聚集作用。结果表明,Sal和NMSal可以诱导三细胞共培养体系中SH-EGFP细胞中α-syn的聚集,但不会引起与U87或是Jurkat共培养中SH-EGFP细胞中α-syn的聚集。同时我们还发现Sal和NMSal处理的三细胞共培养体系中SH-EGFP细胞中自噬蛋白LC3表达水平的升高,而自噬诱导剂雷帕霉素可以减少α-syn的聚集。以上结果表明,Jurkat细胞可以影响Sal和NMSal诱导的共培养体系SH-EGFP细胞中α-syn的聚集,并且自噬可能通过清除错误折叠的α-syn蛋白来保护神经元细胞。 展开更多
关键词 alpha-synuclein 蛋白聚集 共培养 SALSOLINOL N-甲基-(R)-salsolinol
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Alpha-synuclein truncation and disease
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作者 Caroline M. Ritchie Philip J. Thomas 《Health》 2012年第11期1167-1177,共11页
Alpha-synuclein is the major component of Lewy bodies, insoluble protein aggregates, found in patients with Parkinson’s disease, diffuse Lewy body disease, and the Lewy body variant of Alzheimer’s disease. Alpha-syn... Alpha-synuclein is the major component of Lewy bodies, insoluble protein aggregates, found in patients with Parkinson’s disease, diffuse Lewy body disease, and the Lewy body variant of Alzheimer’s disease. Alpha-synuclein has been found within Lewy bodies to contain many different modifications, including nitration, phosphorylation, ubiquitination, and truncation. C-terminally truncated forms of alpha-synuclein aggregate faster than the full-length protein in vitro, and are thus believed to play a role in Lewy body formation and disease progression. Pathological studies of post mortem brain tissue and the generation of transgenic mouse models further support a role of C-terminally truncated forms of alpha-synuclein in disease. Several enzymes, some of which function extracellularly, have been implicated in the production of these C-terminally truncated forms of alpha-synuclein. However, the enzymes responsible for alphasynuclein truncation in vivo have not yet been firmly established. 展开更多
关键词 alpha-synuclein Neurodegeneration Parkinson’s DISEASE LEWY Body PROTEASOME TRUNCATION Degradation Aggregation Protease
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Effects of lead exposure on alpha-synuclein and p53 transcription
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作者 Pei-Jun Zuo A. Bakr M. Rabie 《Journal of Biomedical Science and Engineering》 2009年第2期86-89,共4页
Objective: Epidemiological studies have found that lead exposure increases the risk for Park-inson’s disease and patients with Parkinson’s disease have lower odds of developing non-smoking-related cancer (1). It wou... Objective: Epidemiological studies have found that lead exposure increases the risk for Park-inson’s disease and patients with Parkinson’s disease have lower odds of developing non-smoking-related cancer (1). It would be inter-esting therefore to find the molecular links be-tween Parkinson’s disease and cancer. To do this, we studied mRNA expression of alpha-synuclein gene, a promising genetic marker for Parkinson’s disease, and expression of the tu-mor suppressor gene p53 after oxidative stress induced by lead. Methods: We used ATDC5 cell line as a model of tumor and treated by lead nitrate for 0, 2, 4, 16, 24 and 48 hours. The mRNAs of alpha-synuclein and p53 were quan-tified by reverse transcriptase polymerase chain reaction and expressed as mean (&amp;#177;SD) for 3 samples at each time point. Results: Ex-pression of both of alpha-synuclein and p53 mRNA increased with increasing exposure of lead treatment. The levels of alpha-synuclein and p53 mRNA were correlated with each other (r=0.9830;P&amp;lt;0.001). Conclusion: We propose that lead’s neurotoxicity in PD is caused by al-pha-synuclein expression and aggregation, which releases the inhibitory influence of al-pha-synuclein on p53 expression, thereby al-lowing p53 to act as the cell’s guardian of the genome and reduce tumorigenic potential. Treatments that reduce alpha-synuclein aggre-gation may need to account for a concomitant reduction in p53’s protective effect. 展开更多
关键词 alpha-synuclein P53 REAL-TIME PCR ATDC5 AGING CANCER
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The Application of Analytical Techniques to Alpha-Synuclein in Parkinson’s Disease
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作者 Olatayo Adedayo Olahanmi 《American Journal of Analytical Chemistry》 CAS 2024年第9期269-285,共17页
Parkinson’s disease (PD) is a progressive neurodegenerative disorder characterized by motor symptoms such as tremors, rigidity, and bradykinesia, as well as non-motor symptoms including cognitive impairment and mood ... Parkinson’s disease (PD) is a progressive neurodegenerative disorder characterized by motor symptoms such as tremors, rigidity, and bradykinesia, as well as non-motor symptoms including cognitive impairment and mood disorders. A hallmark of PD is the accumulation of alpha-synuclein, a presynaptic neuronal protein that aggregates to form Lewy bodies, leading to neuronal dysfunction and cell death. The study of alpha-synuclein and its pathological forms is crucial for understanding the etiology of PD and developing effective diagnostic and therapeutic strategies. Analytical techniques play a pivotal role in elucidating the structure, function, and aggregation mechanisms of alpha-synuclein. Biochemical methods such as Western blotting and enzyme-linked immunosorbent assay (ELISA) are employed to detect and quantify alpha-synuclein in biological samples, offering insights into its expression levels and post-translational modifications. Imaging techniques like immunohistochemistry and positron emission tomography (PET) allow for the visualization of alpha-synuclein aggregates in tissue samples and in vivo, respectively, facilitating the study of its spatial distribution and progression in PD Spectroscopic methods, including nuclear magnetic resonance (NMR) spectroscopy and mass spectrometry, provide detailed structural information on alpha-synuclein and its isoforms, aiding in the identification of conformational changes associated with aggregation. Emerging techniques such as cryo-electron microscopy (Cryo-EM) and single-molecule fluorescence enable high-resolution structural analysis and real-time monitoring of alpha-synuclein aggregation dynamics, respectively. The application of these analytical techniques has significantly advanced our understanding of the pathophysiological role of alpha-synuclein in PD. They have contributed to the identification of potential biomarkers for early diagnosis and the evaluation of therapeutic interventions targeting alpha-synuclein aggregation. Despite technical limitations and challenges in clinical translation, ongoing advancements in analytical methodologies hold promise for improving the diagnosis, monitoring, and treatment of Parkinson’s disease through a deeper understanding of alpha-synuclein pathology. 展开更多
关键词 Parkinson’s Disease alpha-synuclein TECHNIQUES
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Unfolded annealing molecular dynamics conformers for wild-type and disease-associated variants of alpha-synuclein show no propensity for beta-sheetformation
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作者 D. Balesh Z. Ramjan W.B. Floriano 《Journal of Biophysical Chemistry》 2011年第2期124-134,共11页
Aggregation of alpha-synuclein leads to the formation of Lewy bodies in the brains of patients affected by Parkinson's disease (PD). Native human alpha-synuclein is unfolded in solution but assumes a partial alpha... Aggregation of alpha-synuclein leads to the formation of Lewy bodies in the brains of patients affected by Parkinson's disease (PD). Native human alpha-synuclein is unfolded in solution but assumes a partial alpha-helical conformation upon transient binding to lipid membranes. Annealing Molecular Dynamics (AMD) was used to generate a diverse set of unfolded conformers of free monomeric wild-type alpha-synuclein and PD-associated mutants A30P and A53T. The AMD conformers were compared in terms of secondary structure, hydrogen bond network, solvent-accessible surface per residue, and molecular volume. The objective of these simulations was to identify structural properties near mutation sites and the non-amyloid component (NAC) region that differ between wild- type and disease-associated variants and may be associated to aggregation of alpha- synuclein. Based on experimental evidence, a hypothesis exists that aggregation involves the formation of intermolecular beta sheets. According to our results, disease-associated mutants of alpha-synuclein are no more propense to contain extended beta regions than wild-type alpha-synuclein. Moreover, extended beta structures (necessary for beta sheet formation) were not found at or around positions 30 and 53, or the NAC region in any unfolded conformer of wild-type, A30P or A53T alpha-synuclein, under the conditions of the simulations. These results do not support the hypothesis that the mutant's higher propensity to aggregation results solely from changes in amino acid sequence leading to changes in secondary structure folding propensity. 展开更多
关键词 alpha-synuclein Parkinson's DISEASE LEWY Body FORMATION Beta Sheet FORMATION Unfolding Molecular Simulations
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帕金森病中铁与Alpha-突触核蛋白的相互作用 被引量:8
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作者 王俊 宋宁 +2 位作者 徐华敏 姜宏 谢俊霞 《生理科学进展》 CAS CSCD 北大核心 2015年第3期180-184,共5页
帕金森病(Parkinson's disease,PD)的特异标志物Alpha-突触核蛋白的异常聚集往往伴有铁的沉积,说明铁与Alpha-突触核蛋白聚集之间存在一定联系。铁可以通过增加Alpha-突触核蛋白的产生及抑制其降解从而促进Alpha-突触核蛋白聚集。Al... 帕金森病(Parkinson's disease,PD)的特异标志物Alpha-突触核蛋白的异常聚集往往伴有铁的沉积,说明铁与Alpha-突触核蛋白聚集之间存在一定联系。铁可以通过增加Alpha-突触核蛋白的产生及抑制其降解从而促进Alpha-突触核蛋白聚集。Alpha-突触核蛋白作为一种高铁还原酶也可以影响细胞铁的代谢。本文就铁与Alpha-突触核蛋白参与PD的发病以及两者之间相互作用的机制进行综述。 展开更多
关键词 帕金森病 alpha-突触核蛋白
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以α-synuclein为靶点的抗帕金森病药物研究进展 被引量:15
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作者 沈琮 张兰 李林 《中国药理学通报》 CAS CSCD 北大核心 2014年第2期149-153,共5页
帕金森病(Parkinsons disease,PD)是常见的神经退行性疾病,目前对PD的药物治疗仅限于改善症状,尚缺乏能够延缓疾病进程并具有神经保护作用的药物。α-突触核蛋白(α-synuclein,α-syn)是一种位于神经元突触前末端、由140个氨基酸组成的... 帕金森病(Parkinsons disease,PD)是常见的神经退行性疾病,目前对PD的药物治疗仅限于改善症状,尚缺乏能够延缓疾病进程并具有神经保护作用的药物。α-突触核蛋白(α-synuclein,α-syn)是一种位于神经元突触前末端、由140个氨基酸组成的蛋白质,它的突变、聚集和过度积累与包括PD在内的一系列神经退行性疾病密切相关。开发针对α-syn及其相关靶点的药物,可能是控制PD等突触核蛋白病进程的有效途径。该文主要从抑制α-syn表达和聚集、促进其解聚和降解、调节其修饰状态等方面,对以α-syn为靶点的药物研究进展进行综述。 展开更多
关键词 Α-突触核蛋白 帕金森病 药物发现 神经退行性疾病 突触核蛋白病 药物靶点
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优化人alpha-syn基因疫苗免疫MPTP慢性PD小鼠的神经保护作用 被引量:2
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作者 王法祥 彭国光 +2 位作者 王加才 王少君 何卿玮 《第四军医大学学报》 CAS 北大核心 2009年第20期2125-2128,共4页
目的:探讨优化高分泌型人α-突触核蛋白(human alpha—synuclein,ha—syn)基因疫苗免疫MPTP慢性帕金森病小鼠的治疗效果和神经免疫保护作用.方法:建立慢性PD小鼠模型,采用神经毒素MPTP25mg/(kg·d),2次/wk,累计共10次... 目的:探讨优化高分泌型人α-突触核蛋白(human alpha—synuclein,ha—syn)基因疫苗免疫MPTP慢性帕金森病小鼠的治疗效果和神经免疫保护作用.方法:建立慢性PD小鼠模型,采用神经毒素MPTP25mg/(kg·d),2次/wk,累计共10次.建模后随机分为3组:优化基因疫苗组、疫苗组、PBS对照组;每次治疗前,每只动物分别在双侧后肢胫骨前肌部位注射5g/L布比卡因50μL,注射72h后,3组动物分别于同部位同深度注射优化基因疫苗、基因疫苗或PBS各50μL,1次/3wk,共3次.末次免疫后2wk观察行为学改变后,处死取脑.运用免疫荧光、免疫组化等方法观察酪氨酸羟化酶阳性细胞数,以及α-syn表达变化.结果:优化基因疫苗组、疫苗组小鼠爬杆能力与PBS对照组比较都得到明显改善,有统计学差异(P〈0.05);但优化基因疫苗组与疫苗组行为学评分间差异无统计学意义.优化基因疫苗组酪氨酸羟化酶阳性细胞数与其它两组相比增多约20%-68%(P〈0.05),α-syn表达减少约15%~45%(P〈0.05).结论:优化基因疫苗具有较强改善帕金森小鼠行为学的作用,能增强疫苗的免疫原性,促进受损黑质细胞修复,对帕金森病小鼠有更好的免疫治疗作用. 展开更多
关键词 帕金森病 MPTP 基因疫苗 免疫保护 alpha-突触核蛋白
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携带人alpha-突触核蛋白真核重组质粒构建及其SK-N-SH细胞表达 被引量:2
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作者 和青 杜婷婷 +2 位作者 宋宁 谢俊霞 姜宏 《青岛大学医学院学报》 CAS 2010年第5期377-379,383,共4页
目的构建携带人alpha-突触核蛋白真核重组质粒,检测其在人神经母细胞瘤SK-N-SH细胞中的表达及对细胞存活率的影响。方法 PCR扩增alpha-突触核蛋白基因,产物纯化后与pcDNA3.1(+)载体进行连接反应,构建pcDNA3.1(+)/alpha-突触核蛋白真核... 目的构建携带人alpha-突触核蛋白真核重组质粒,检测其在人神经母细胞瘤SK-N-SH细胞中的表达及对细胞存活率的影响。方法 PCR扩增alpha-突触核蛋白基因,产物纯化后与pcDNA3.1(+)载体进行连接反应,构建pcDNA3.1(+)/alpha-突触核蛋白真核重组质粒。Lipofectamine法转染人神经母细胞瘤SK-N-SH细胞,RT-PCR方法检测SK-N-SH细胞中alpha-突触核蛋白mRNA的表达,四甲基偶氮唑盐(MTT)法检测其对细胞存活率的影响。结果酶切鉴定及基因测序证明人alpha-突触核蛋白基因已被完整、正确地插入到pcDNA3.1(+)载体中。RT-PCR结果显示该表达载体转染SK-N-SH细胞后,细胞内alpha-突触核蛋白mRNA的表达水平明显增高,MTT方法检测结果显示该表达载体转染并未引起细胞存活率的改变。结论 alpha-突触核蛋白真核重组质粒构建成功,并可在SK-N-SH细胞内表达,且对细胞的存活率不产生任何影响,从而为进一步研究alpha-突触核蛋白在帕金森病发病机制中的作用奠定了基础。 展开更多
关键词 Α突触核蛋白 质粒 帕金森病
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α-Synuclein在功能性便秘患者结肠的表达及磷酸化修饰
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作者 宣琪 刘殿刚 +2 位作者 王爱磊 陈晶 崔叶青 《中国卫生检验杂志》 CAS 2017年第12期1679-1681,1685,共4页
目的研究α-Synuclein(α-syn)及磷酸化α-syn(P-syn)在功能性便秘患者结肠黏膜的表达。方法应用免疫荧光双重标记和显微图像分析技术,比较21例功能性便秘和22例对照组结肠黏膜α-syn和P-syn的表达情况。结果 2组肠黏膜神经元及胶质细... 目的研究α-Synuclein(α-syn)及磷酸化α-syn(P-syn)在功能性便秘患者结肠黏膜的表达。方法应用免疫荧光双重标记和显微图像分析技术,比较21例功能性便秘和22例对照组结肠黏膜α-syn和P-syn的表达情况。结果 2组肠黏膜神经元及胶质细胞均有α-syn和P-syn表达,存在共定位。功能性便秘组结肠黏膜层及黏膜下层α-syn积分光密度(IOD)分别为1 513.50±93.21和1 398.65±74.32,显著高于对照组(1 027.10±57.81和995.03±68.32),差异有统计学意义(P<0.05)。功能性便秘组结肠黏膜层及黏膜下层P-syn的IOD(790.25±39.41和432.09±18.99)显著高于对照组(535.87±35.72和310.90±27.26),差异有统计学意义(P<0.05)。结论结肠黏膜神经元及胶质细胞α-syn的聚集及磷酸化可能与功能性便秘发病机制相关。 展开更多
关键词 Α-突触核蛋白 磷酸化 功能性便秘 结肠
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pEGFP-N1-α-synuclein真核表达载体的构建
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作者 杨波 苑玉和 +2 位作者 金金 陈虹 陈乃宏 《武警医学院学报》 CAS 2009年第7期573-576,共4页
【目的】构建pEGFP-N1-α-synuclein真核表达载体,为研究帕金森病奠定基础。【方法】设计特异引物,PCR扩增α-synuclein cDNA并引入FLAG标签,克隆入pEGFP-N1质粒,对重组质粒进行酶切及测序,鉴定正确后转化Ecoli.DH5(大肠杆菌),大量扩增... 【目的】构建pEGFP-N1-α-synuclein真核表达载体,为研究帕金森病奠定基础。【方法】设计特异引物,PCR扩增α-synuclein cDNA并引入FLAG标签,克隆入pEGFP-N1质粒,对重组质粒进行酶切及测序,鉴定正确后转化Ecoli.DH5(大肠杆菌),大量扩增重组质粒。试剂盒纯化重组质粒。用Lipofectamine TM2000将重组质粒转染2937细胞,Western blotting检测融合蛋白在细胞内的表达。【结果】pEGFP-N1-α-synuclein重组质粒构建成功,Western blotting检测融合蛋白分子量为47kd,符合预期值。【结论】成功构建了人野生型α-synuclein与绿色荧光蛋白基因融合并加入FLAG标签的真核表达载体pEGFP-N1-α-synuclein。 展开更多
关键词 帕金森病 Α-synuclein PEGFP-N1 真核表达 融合蛋白
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松果菊苷对6-OHDA帕金森病模型大鼠海马α-Synuclein、β-actin蛋白表达影响随机平行对照研究 被引量:2
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作者 周紫婷 付贝贝 +3 位作者 覃威 陈诗雅 张龙惠 蔡晶 《实用中医内科杂志》 2018年第9期57-61,共5页
[目的]观察松果菊苷对6-OHDA帕金森病模型大鼠海马α-Synuclein、β-actin蛋白表达影响。[方法]使用随机平行对照方法,将72只SPF级SD雄性大鼠适应性饲养14d,按随机数字表法分为6组,空白对照组、假手术组、模型组、松果菊苷(低、中、高剂... [目的]观察松果菊苷对6-OHDA帕金森病模型大鼠海马α-Synuclein、β-actin蛋白表达影响。[方法]使用随机平行对照方法,将72只SPF级SD雄性大鼠适应性饲养14d,按随机数字表法分为6组,空白对照组、假手术组、模型组、松果菊苷(低、中、高剂量)组,12只/组。各组大鼠腹腔注射10%水合氯醛(30mg/kg)麻醉,固定于颅脑定位仪,消毒,沿颅顶正中线切开皮肤,钝性分离颅骨外膜,暴露大鼠颅骨前囟门;以前囟为坐标原点(大鼠脑定位立体图谱),确定前脑内侧束(MFB)坐标,MFB:前囟后4.8mm,矢状缝右侧1.2mm,硬脑下7.8mm;颅骨钻钻孔,立体定向靶点微量注射6-OHDA(2ug/uL,溶于0.1%抗坏血酸生理盐水),注射速度1uL/min,留针15min;骨蜡封闭大鼠脑部颅骨孔,消毒缝合皮肤,复制帕金森病模型,松果菊苷(低、中、高剂量)组(8 ug)、模型组(2ug);空白对照组、假手术组(与模型组等量生理盐水)。灌胃干预:复制成功模型,松果菊苷组(低20mg/kg、中40mg/kg,高80mg/kg),余各组均等体积生理盐水,1次/d,连续10d。PAGE胶蛋白电泳;免疫印迹(Western Blot,WB)法检测α-Synuclein、β-actin蛋白。[结果]模型复制48只大鼠,麻醉过度死亡3只,模型复制不成功2只,最终纳入结果分析43只,模型组10只,松果菊苷组低、中、高剂量组各11只。α-Synuclein蛋白水平假手术组、松果菊苷各组(低中高)均低于空白对照组(P<0.01);β-actin各组间无明显差异(P>0.05);α-Synuclein/β-actin假手术组、松果菊苷低剂量组、松果菊苷中剂量组、松果菊苷高剂量组均低于空白对照组(P<0.01)。[结论]松果菊苷干预帕金森病模型大鼠,可降低海马α-Synuclein表达。 展开更多
关键词 帕金森病 雄性SPF级SD大鼠 6-OHDA 动物模型 松果菊苷 高中低剂量 海马 脑定位立体图谱 靶点注射 蛋白电泳 免疫印迹(Western Blot WB) α-synuclein蛋白 β-actin蛋白 实验研究 随机平行对照研究
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