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CPAD Curated Protein Aggregation Database: A Repository of Manually Curated Experimental Data on Protein and Peptide Aggregation

机译:CPAD固化蛋白聚集数据库:关于蛋白质和肽聚集的手动固化实验数据的存储库

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摘要

Accurate distinction between peptide sequences that can form amyloid-fibrils or amorphous β-aggregates, identification of potential aggregation prone regions in proteins, and prediction of change in aggregation rate of a protein upon mutation(s) are critical to research on protein misfolding diseases, such as Alzheimer’s and Parkinson’s, as well as biotechnological production of protein based therapeutics. We have developed a Curated Protein Aggregation Database (CPAD), which has collected results from experimental studies performed by scientific community aimed at understanding protein/peptide aggregation. CPAD contains more than 2300 experimentally observed aggregation rates upon mutations in known amyloidogenic proteins. Each entry includes numerical values for the following parameters: change in rate of aggregation as measured by fluorescence intensity or turbidity, name and source of the protein, Uniprot and Protein Data Bank codes, single point as well as multiple mutations, and literature citation. The data in CPAD has been supplemented with five different types of additional information: (i) Amyloid fibril forming hexa-peptides, (ii) Amorphous β-aggregating hexa-peptides, (iii) Amyloid fibril forming peptides of different lengths, (iv) Amyloid fibril forming hexa-peptides whose crystal structures are available in the Protein Data Bank (PDB) and (v) Experimentally validated aggregation prone regions found in amyloidogenic proteins. Furthermore, CPAD is linked to other related databases and resources, such as Uniprot, Protein Data Bank, PUBMED, GAP, TANGO, WALTZ etc. We have set up a web interface with different search and display options so that users have the ability to get the data in multiple ways. CPAD is freely available at . The potential applications of CPAD have also been discussed.
机译:准确区分可形成淀粉样蛋白原纤维或无定形β-聚集体的肽序列,鉴定蛋白质中潜在的聚集倾向区域以及预测突变后蛋白质聚集率的变化对于研究蛋白质错误折叠疾病至关重要,例如阿尔茨海默氏症和帕金森氏症,以及蛋白质疗法的生物技术生产。我们已经开发了蛋白质蛋白质聚集数据库(CPAD),该数据库收集了科学界旨在了解蛋白质/肽聚集的实验研究结果。 CPAD包含超过2300种在实验中观察到的已知淀粉样蛋白发生突变后的聚集速率。每个条目均包含以下参数的数值:通过荧光强度或浊度测得的聚集率变化,蛋白质名称和来源,Uniprot和Protein Data Bank代码,单点和多重突变以及文献引用。 CPAD中的数据已补充了五种不同类型的附加信息:(i)形成淀粉样原纤维的六肽,(ii)非晶形聚集β的六肽,(iii)不同长度的形成淀粉样原纤维的肽,(iv)形成淀粉样蛋白原纤维的六肽,其晶体结构可在蛋白质数据库(PDB)和(v)产生淀粉样蛋白的蛋白质中经过实验验证的易于聚集的区域中。此外,CPAD链接到其他相关数据库和资源,例如Uniprot,Protein Data Bank,PUBMED,GAP,TANGO,WALTZ等。我们已经建立了具有不同搜索和显示选项的Web界面,以便用户能够获取数据有多种方式。 CPAD可从以下网站免费获得。还讨论了CPAD的潜在应用。

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