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Company: Thermo Scientific
Catalog#: 88881001
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A Workflow for Ultra-rapid Analysis of Histone Post-translational Modifications with Direct-injection Mass Spectrometry
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Date:
2020-09-20
[Abstract]  Chromatin modifications, like histone post translational modifications (PTMs), are critical for tuning gene expression and many other aspects of cell phenotype. Liquid chromatography coupled to mass spectrometry (LC-MS) has become the most suitable method to analyze histones and histone PTMs in a large-scale manner. Selected histone PTMs have known functions, and their aberrant regulation is linked to a wide variety of diseases, including cancer. However, histone analysis is scarcely used in diagnostics, partially due to the limited throughput and not ideal reproducibility of LC-MS based analysis. We describe a workflow that allows for high-throughput sample preparation is less than a day using 96-well plates. Following preparation, samples are sprayed into MS without LC, using an ... [摘要]  [抽象]像组蛋白翻译后修饰(PTM)一样,染色质修饰对于调节基因表达和细胞表型的许多其他方面至关重要。液相色谱-质谱联用(LC-MS)已成为最适合大规模分析组蛋白和组蛋白PTM的方法。选定的组蛋白PTM具有已知功能,其异常调节与包括癌症在内的多种疾病有关。但是,组蛋白分析很少用于诊断中,部分是由于通量有限且基于LC-MS的分析的重现性不理想。我们描述了一种使用96孔板进行少于一天的高通量样品制备的工作流程。制备后,使用自动直接进样(DI-MS)方法将样品喷雾到无LC的MS中。每次分析都可以通过45个PTM(甲基化,乙酰化和磷酸化(共151个组蛋白标记)和16个未修饰的组蛋白肽进行组蛋白变体的相对定量。由于没有残留或基于LC的批处理效应,该工作流程允许MS运行少于1分钟,并具有更高的重现性和耐用性。最后,我们描述了一种工程化的肽序列,用于精确监控样品制备的效率,可以在DI-MS运行期间检测到该效率。

[背景] 组蛋白是具有球形头部和N末端尾巴的碱性蛋白质,富含精氨酸和赖氨酸残基。一对典型的组蛋白H2A,H2B,H3和H4(称为核心组蛋白)形成一个八聚体,其周围147 ...

Karyopherin-β2 Inhibits and Reverses Aggregation and Liquid-liquid Phase Separation of the ALS/FTD-Associated Protein FUS
Author:
Date:
2020-08-20
[Abstract]  The study of RNA-binding proteins (RBP) offers insight into the mechanisms of pathologic protein aggregation in neurodegenerative diseases. We developed a protocol for purifying an RBP FUS and a nuclear import receptor (NIR) Kapβ2 and testing the ability of Kapβ2 to mitigate FUS aggregation and liquid-liquid phase separation. [摘要]  [摘要] RNA结合蛋白的研究(RBP)报价洞察病理蛋白聚集的神经变性疾病的机制。我们开发了用于纯化RBP FUS和核输入受体(NIR)Kapβ2 的协议,并测试Kapβ2 减轻FUS聚集和液-液相分离的能力。

[背景] 肌萎缩性脊髓侧索硬化症(ALS)和额颞叶痴呆(FTD)是神经变性疾病,其特征在于所述错误定位几个RNA结合蛋白的和聚集(RBP)(麦肯齐等人,2010;达克鲁斯和克利夫兰,2011; King 等,2012)。其中一种蛋白是FUS(融合在肉瘤中),一种核蛋白在ALS / FTD患者的神经元细胞质中定位不正确,然后经历液-液相转变,然后发生异常的相转变,形成不溶性聚集体(Altmeyer 等, 2015; Burke 等人,2015; Lin 等人,2015; Molliex 等人,2015; Murakami 等人,2015; Patel 等人,2015)(图1)。Karyopherin-β2(甲β2),一个核输入受体(NIR),已经建立了作为伴侣和disaggregase 蛋白与PY-核定位序列(NLS),诸如FUS(过等人,2018; Hofweber 等人。,2018;吉泽,等人。,2018)。以下方案被开发,以测试的能力甲β2抑制和反向FUS聚合和相分离的离体(过等人,2018)。

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