生物来源
rabbit
质量水平
抗体形式
serum
抗体产品类型
primary antibodies
克隆
polyclonal
种属反应性
Saccharomyces cerevisiae, human, vertebrates
制造商/商品名称
Upstate®
技术
ChIP: suitable
dot blot: suitable
western blot: suitable
NCBI登记号
UniProt登记号
运输
wet ice
靶向翻译后修饰
acetylation (Lys23)
基因信息
human ... H3C1(8350)
一般描述
组蛋白H3的N末端尾部从球状核小体核心突起,其可能发生几种不同类型的表观遗传修饰,从而影响细胞过程。这些修饰包括甲基或乙酰基与赖氨酸和精氨酸的共价连接,以及丝氨酸或苏氨酸的磷酸化。
免疫原
应用
代表性批次数据。
使用2 µL正常兔血清或2 µL抗乙酰组蛋白H3(Lys23)和Magna ChIP A试剂盒(目录号17-610),对从HeLa细胞制备的超声染色质(每IP 1 X 10e6细胞当量)进行染色质免疫沉淀。 使用对人GAPDH启动子区域具有特异性的对照引物作为阳性基因座,并使用MyoD引物作为阴性基因座,通过qPCR验证了乙酰基组蛋白H3(Lys23)相关DNA片段的成功免疫沉淀。数据表示为每个IP样品相对于每个扩增子和ChIP样品的输入染色质的输入百分比。
请参阅EZ-Magna ChIP A(目录号17-408)或EZ-ChIP(目录号17-371)协议以获取实验详细信息。
蛋白质印迹分析:
代表性批次数据。
用抗乙酰基组蛋白H3(Lys23)(1:100,000稀释)探测丁酸钠处理的HeLa细胞(泳道1,目录号17-305)和重组组蛋白H3(泳道2,目录号14-494)的酸提取物。
箭头表示乙酰基组蛋白H3(~17 kDa)
斑点印迹:
代表性批次数据。
将40 ng和4 ng量的不同修饰的组蛋白肽(见表1)转移至PVDF膜上,并用抗乙酰基组蛋白H3(Lys23)抗体(1:2000稀释度)进行探测。使用与HRP偶联的山羊抗兔IgG和化学发光检测系统可视化蛋白质。显示了60秒曝光的图像。
组蛋白
表观遗传学&核功能
生化/生理作用
外形
制备说明
分析说明
经丁酸钠处理过的HeLa细胞的酸提取物
法律信息
免责声明
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储存分类代码
10 - Combustible liquids
WGK
WGK 1
相关内容
Cancer is a complex disease manifestation. At its core, it remains a disease of abnormal cellular proliferation and inappropriate gene expression. In the early days, carcinogenesis was viewed simply as resulting from a collection of genetic mutations that altered the gene expression of key oncogenic genes or tumor suppressor genes leading to uncontrolled growth and disease (Virani, S et al 2012). Today, however, research is showing that carcinogenesis results from the successive accumulation of heritable genetic and epigenetic changes. Moreover, the success in how we predict, treat and overcome cancer will likely involve not only understanding the consequences of direct genetic changes that can cause cancer, but also how the epigenetic and environmental changes cause cancer (Johnson C et al 2015; Waldmann T et al 2013). Epigenetics is the study of heritable gene expression as it relates to changes in DNA structure that are not tied to changes in DNA sequence but, instead, are tied to how the nucleic acid material is read or processed via the myriad of protein-protein, protein-nucleic acid, and nucleic acid-nucleic acid interactions that ultimately manifest themselves into a specific expression phenotype (Ngai SC et al 2012, Johnson C et al 2015). This review will discuss some of the principal aspects of epigenetic research and how they relate to our current understanding of carcinogenesis. Because epigenetics affects phenotype and changes in epigenetics are thought to be key to environmental adaptability and thus may in fact be reversed or manipulated, understanding the integration of experimental and epidemiologic science surrounding cancer and its many manifestations should lead to more effective cancer prognostics as well as treatments (Virani S et al 2012).
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