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- 保存条件:
Powder: -20°C, 3 years; 4°C, 2 years.In solvent: -80°C, 6 months; -20°C, 1 month.
- 库存:
货期:1-2天
- 供应商:
MedChemExpress LLC
- CAS号:
13553-79-2
- 规格:
10 mM * 1 mL/5 g/10 g/25 g/50 g/100 g
| 规格: | 10 mM * 1 mL | 产品价格: | ¥132.0 |
|---|---|---|---|
| 规格: | 5 g | 产品价格: | ¥120.0 |
| 规格: | 10 g | 产品价格: | ¥216.0 |
| 规格: | 25 g | 产品价格: | ¥457.0 |
| 规格: | 50 g | 产品价格: | ¥800.0 |
| 规格: | 100 g | 产品价格: | ¥1400.0 |
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Rifamycin S
CAS No. : 13553-79-2
MCE 国际站:Rifamycin S
产品活性:Rifamycin S 是一种醌和抗革兰氏阳性细菌 (包括 MRSA) 的抗生素。Rifamycin S 是涉及两个电子的可逆氧化还原系统的氧化形式。Rifamycin S 可以产生活性氧 (ROS) 并抑制微粒体脂质过氧化,并可用于肺结核和麻风病的研究。
研究领域:Anti-infection | Metabolic Enzyme/Protease | Immunology/Inflammation | NF-κB
作用靶点:Bacterial | Reactive Oxygen Species | Antibiotic
In Vitro: The inhibition of bacterial growth by Rifamycin SV is due to the production of active species of oxygen resulting from the oxidation-reduction cycle of Rifamycin SV in the cells. The aerobic oxidation of Rifamycin SV to Rifamycin S is induced by metal ions, such as Mn2+, Cu2+, and Co2+. The most effective metal ion is Mn2+.
In Vivo: Rat liver sub-mitochondrial particles also generated hydroxyl radical in the presence of NADH and Rifamycin S. NADH dehydrogenase (complex I) as the major component involved in the reduction of Rifamycin S. Compared to NADPH, NADH is almost as effective (Rifamycin S) in catalyzing the interactions of these antibiotics with rat liver microsomes. Rifamycin S is shown to be readily reduced to Rifamycin SV, the corresponding hydroquinone by Fe(II). Rifamycin S forms a detectable Fe(II)-(Rifamycin S)3 complex. The Fe:ATP induced lipid peroxidation is completely inhibited by Rifamycin S. Rifamycin S can interact with rat liver microsomes to undergo redox-cycling, with the subsequent production of hydroxyl radicals when iron complexes are present.
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文献和实验放线菌 Streptomyces mediterranei产生的抗菌素,有利福霉素 B. O. S. SV等类别。对革兰氏阳性菌、结核菌有强抗菌作用,对革兰氏阴性菌的抗菌作用很弱。对细菌的 RNA聚合酶在开始解读模板 DNA时显示有阻碍,但对真核细胞的 RNA聚合酶无抑制作用。一般认为能与大肠杆菌 RNA聚合酶的β亚单位相结合。
Clinical laboratory identification of Mycobacterium tuberculosis and the Mycobacterium avium-intracellulare complex (MAC) has been facilitated in recent years by new DNA and RNA amplification tests (1 -4 ). However, drug susceptibility
Methods to Identify and Characterize Inhibitors of Bacterial RNA Polymerase
RNA polymerase is essential to the viability of bacteria in all phases of growth and development and is a proven chemotherapeutic target as the cellular target of the rifamycin class of antibiotics. However, despite the characterization
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