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由来生物
human
リコンビナント
expressed in E. coli
アッセイ
≥90% (SDS-PAGE)
形状
aqueous solution
分子量
113.8 kDa
包装
pkg of 100 μg
テクニック
cell based assay: suitable
溶解性
water: soluble
輸送温度
dry ice
保管温度
−70°C
遺伝子情報
human ... HIST1H2BG(8339) , HIST2H2AC(8338) , HIST3H3(8290) , HIST4H4(121504)
詳細
Human recombinant histone octamer consisting of 2 molecules each of histones H2A (GenBank Accession No. NM_033445) amino acids 2-130(end) with a N-terminal His-tag, H2B (GenBank Accession No. NM_003528) amino acids 2-126(end) with a N-terminal His-tag, H3 (GenBank Accession No. NM_003532) amino acids 2-137(end) with a N-terminal His-tag, and H4 (GenBank Accession No. NM_003548) amino acids 2-103(end) with a N-terminal His-tag, expressed in an E. coli expression system.
Research Area: Cell Signaling
The histone octamer is a versatile protein assembly that has evolved to serve two opposing functions within the cell. It is required to bind and bend DNA to achieve fivefold compaction and partial charge neutralization of DNA, while also needing to release specific segments of DNA in a coordinated manner to allow the access of DNA-processing enzymes at the appropriate time. A modular assembly of histone dimers (consisting of either H2A and H2B or H3 and H4) binds to approximately 30 bp of DNA and is connected in a flexible yet stable manner to form a fundamental superhelical ′ramp′ with evenly spaced DNA-binding platforms.
The histone octamer is a versatile protein assembly that has evolved to serve two opposing functions within the cell. It is required to bind and bend DNA to achieve fivefold compaction and partial charge neutralization of DNA, while also needing to release specific segments of DNA in a coordinated manner to allow the access of DNA-processing enzymes at the appropriate time. A modular assembly of histone dimers (consisting of either H2A and H2B or H3 and H4) binds to approximately 30 bp of DNA and is connected in a flexible yet stable manner to form a fundamental superhelical ′ramp′ with evenly spaced DNA-binding platforms.
アプリケーション
Histone Octamer full length human has been used to incubate with 12-mesyloxy-NVP along with recombinant human histone H4 to investigate the potential of histones as targets for covalent adduct formation by drug-derived electrophiles.
生物化学的/生理学的作用
The nuclear DNA in eukaryotes is found to be associated with histones to form a compact complex called nucleosome. Histones neutralize the electrostatic nature of DNA and function as scaffolding proteins. Each core nucleosome contains two copies each of the core histones H2A, H2B, H3, and H4 to form an octameric complex. This octameric complex contains a central (H3-H4)2 tetramer flanked on both sides with H2A-H2B dimers. The octamer complex function in various stages of chromosome function, chromatin assembly and nucleosome formation. The histone dimer-tetramer interactions are also important in RNA transcription.
保管分類コード
10 - Combustible liquids
WGK
WGK 1
引火点(°F)
Not applicable
引火点(℃)
Not applicable
適用法令
試験研究用途を考慮した関連法令を主に挙げております。化学物質以外については、一部の情報のみ提供しています。 製品を安全かつ合法的に使用することは、使用者の義務です。最新情報により修正される場合があります。WEBの反映には時間を要することがあるため、適宜SDSをご参照ください。
毒物及び劇物取締法
劇物
Jan Code
SRP0408-100UG:
試験成績書(COA)
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Annals of botany, 108(7), 1235-1246 (2011-09-08)
In eukaryotes, chromatin remodelling complexes are shown to be responsible for nucleosome mobility, leading to increased accessibility of DNA for DNA binding proteins. Although the existence of such complexes in plants has been surmised mainly at the genetic level from
The nucleosomal core histone octamer at 3.1 A resolution: a tripartite protein assembly and a left-handed superhelix.
Proceedings of the National Academy of Sciences of the USA, 88, 10148-10152 (1991)
Covalent histone modification by an electrophilic derivative of the anti-HIV drug nevirapine
Molecules (Basel), 26(5), 1349-1349 (2021)
Histone octamer function in vivo: mutations in the dimer-tetramer interfaces disrupt both gene activation and repression.
The Embo Journal, 16, 2493-2506 (1997)
Histone chaperones and nucleosome assembly
Current Opinion in Structural Biology, 13(1), 6-14 (2003)
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