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131580-10-4

中文名稱 BETA- AMYLOID (1-16)
英文名稱 H-ASP-ALA-GLU-PHE-ARG-HIS-ASP-SER-GLY-TYR-GLU-VAL-HIS-HIS-GLN-LYS-OH
CAS 131580-10-4
分子式 C84H119N27O28
分子量 1955.01
MOL 文件 131580-10-4.mol
更新日期 2024/12/22 20:23:41
131580-10-4 結(jié)構(gòu)式 131580-10-4 結(jié)構(gòu)式

基本信息

中文別名
Β-淀粉樣蛋白 AMYLOID Β-PROTEIN (1-16)
Β-AMYLOID (1-16), HUMAN
AMYLOID BETA-PROTEIN (1-16) TRIFLUOROACETATE SALT
英文別名
β-Amyloid 1-16
DAEFRHDSGYEVHHQK
BETA-AMYLOID (1-16)
AMyloid b-Protein (1-16)
AMYLOID BETA-PROTEIN (1-16)
[Gln11] -β- Amyloid (1 - 16)
Amyloidβ-Protein(1-16)/β-Amyloid(1-16),human
Amyloid beta-Protein (1-16) trifluoroacetate salt
H-ASP-ALA-GLU-PHE-ARG-HIS-ASP-SER-GLY-TYR-GLU-VAL-HIS-HIS-GLN-LYS-OH
H-ASP-ALA-GLU-PHE-ARG-HIS-ASP-SER-GLY-TYR-GLU-VAL-HIS-HIS-GLN-LYS-OH USP/EP/BP
所屬類別
生物化工:多肽

物理化學性質(zhì)

密度1.57±0.1 g/cm3(Predicted)
儲存條件-15°C
溶解度溶于二甲基亞砜
形態(tài)固體
顏色White to off-white
水溶解性Soluble in water or aqueous buffer
序列H-Asp-Ala-Glu-Phe-Arg-His-Asp-Ser-Gly-Tyr-Glu-Val-His-His-Gln-Lys-OH
BETA- AMYLOID (1-16)價格(試劑級)
報價日期產(chǎn)品編號產(chǎn)品名稱CAS號包裝價格
2024/11/08HY-P1466BETA- AMYLOID (1-16)
β-Amyloid (1-16)
131580-10-41mg1100元
2024/11/08HY-P1466BETA- AMYLOID (1-16)
β-Amyloid (1-16)
131580-10-45mg3900元

常見問題列表

生物活性
β-Amyloid (1-16) 是可參與金屬結(jié)合的β-淀粉樣蛋白片段。 β-淀粉樣蛋白是在阿爾茨海默病患者的腦中形成淀粉樣斑塊的肽。
靶點

Amyloid-β

體內(nèi)研究

β-amyloid (1-16) fragment is considered as valid models to examine the contribution of the key histidine residues (His , His in mouse and His , His , His in human fragments) to the Ab–Cu 2+ interaction. Oxidation targets for β-Amyloid (1-16) are the histidine residues coordinated to the metal ions. Copper is bound to Aβ in senile plaque of Alzheimer’s disease with β-Amyloid (1-16) taking part in the coordination of the Cu 2+ ions. Cu 2+ and Zn 2+ are linked with the neurotoxicity of -Amyloid and free radical damage. β-amyloid (1-16) is the minimal amino acidic sequence display a Cu coordination mode which involves three Histidines (His6, His13 and His14). β-amyloid (1-16) is supposed to be involved in metal binding. Human β-amyloid interacts with zinc ions through its metal-binding domain 1-16. The C-tails of the two polypeptide chains of the rat Aβ(1-16) dimer are oriented in opposite directions to each other, which hinders the assembly of rat Aβ dimers into oligomeric aggregates. Thus, the differences in the structure of zinc-binding sites of human and rat β-Amyloid (1-16), their ability to form regular cross-monomer bonds, and the orientation of their hydrophobic C-tails could be responsible for the resistance of rats to Alzheimer's disease.

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