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- 文献和实验
- 技术资料
- 保存条件:
常温
- 保质期:
根据瓶身LOT号查询
- 英文名:
Glycine
- 库存:
有现货
- 供应商:
浙江羽翔生物科技有限公司
- CAS号:
56-40-6
- 规格:
5KG
属性
产品名称
甘氨酸, Vetec™, reagent grade, 98%
InChI key
DHMQDGOQFOQNFH-UHFFFAOYSA-N
InChI
1S/C2H5NO2/c3-1-2(4)5/h1,3H2,(H,4,5)
SMILES string
NCC(O)=O
grade
reagent grade
product line
Vetec™
assay
98%
form
powder
technique(s)
cell culture | plant: suitable
color
white to off-white
pH
5.9-6.4 (20 °C, 50 g/L)
pKa (25 °C)
(1) 2.35, (2) 9.60
2.35
mp
240 °C (dec.) (lit.)
Biochem/physiol Actions
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文献和实验The HDAC6/APOBEC3G complex regulates HIV-1 infectiveness by inducing Vif autophagic degradation.
Human immunodeficiency virus type 1 (HIV-1) has evolved a complex strategy to overcome the immune barriers it encounters throughout an organism thanks to its viral infectivity factor (Vif), a key protein for HIV-1 infectivity and in vivo pathogenesis. Vif interacts with and promotes "apolipoprotein B mRNA-editing enzyme-catalytic, polypeptide-like 3G" (A3G) ubiquitination and subsequent degradation by the proteasome, thus eluding A3G restriction activity against HIV-1. We found that cellular histone deacetylase 6 (HDAC6) directly interacts with A3G through its C-terminal BUZ domain (residues 841-1,215) to undergo a cellular co-distribution along microtubules and cytoplasm. The HDAC6/A3G complex occurs in the absence or presence of Vif, competes for Vif-mediated A3G degradation, and accounts for A3G steady-state expression level. In fact, HDAC6 directly interacts with and promotes Vif autophagic clearance, thanks to its C-terminal BUZ domain, a process requiring the deacetylase activity of HDAC6. HDAC6 degrades Vif without affecting the core binding factor β (CBF-β), a Vif-associated partner reported to be key for Vif- mediated A3G degradation. Thus HDAC6 antagonizes the proviral activity of Vif/CBF-β-associated complex by targeting Vif and stabilizing A3G. Finally, in cells producing virions, we observed a clear-cut correlation between the ability of HDAC6 to degrade Vif and to restore A3G expression, suggesting that HDAC6 controls the amount of Vif incorporated into nascent virions and the ability of HIV-1 particles of being infectious. This effect seems independent on the presence of A3G inside virions and on viral tropism. Our study identifies for the first time a new cellular complex, HDAC6/A3G, involved in the autophagic degradation of Vif, and suggests that HDAC6 represents a new antiviral factor capable of controlling HIV-1 infectiveness by counteracting Vif and its functions.
一异二聚体。两个亚单位的氨基酸组成除甘氨酸外,其余均很相似,但氨基酸的序列则相差明显。人血浆中SP40/40的含量为35~105μg/ml(平均62μg/ml),但在人精浆中却可高达15mg/ml,认为这与保护精子的活性有关。 SP40/40是MAC组装的调节蛋白。它可与C5b~7、C5b~8或C5b~9结合,对MAC的组装起抑制作用,从而可防止MAC的溶细胞作用。此外SP40/40与S蛋白还具有协同作用,可使MAC变为可溶性的而失去溶细胞作用。现知C8与SP40/40的结合部位是C8β、C9
配制Tris-甘氨酸SDS聚丙烯酰胺凝胶电泳分离胶所用溶液 溶液成分 不同体积(ml)凝胶液中各成分所需体积(ml) 5 10 15 20 25
110-550 兔1.36-2.26kg 14.2-56.7/kg 40-100/kg 牛(成) 27.0-60.8kg 11.4-19.0L 金黄地鼠(成
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