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聚乙二醇二甲醚|Poly(ethylene glycol) dimethyl ether|24991-55-7|Adamas|98%+,MW 250|RG|100g
  • 探索价:
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  • 市场价:
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  • 探索编号:
    01050321
  • 原始编号:
    41332B
  • 分子式:
    H3CO(C2H4O)nCH3
  • MDL号:
  • CAS号:
    24991-55-7
  • 品牌:
    Adamas
  • 分子量:
  • 等级:
    RG
  • 参数/指标:
  • 规格:
    100ml
  • 货期:
    现货(当天发货)
  • 库存:
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基本信息
  • 聚乙二醇二甲醚
  • α-甲基-ω-甲氧基(氧-1,2-乙二基)的聚合物;聚乙二醇二甲醚
  • Poly(ethylene glycol) dimethyl ether
  • Poly(Ethylene Glycol) (N) Dimethyl Ether;Polyethylene Glycol 500 Dimethyl Ether;Poly(Ethylene Glycol) Dimethyl Ether;Polyethylene Glycol Dimethyl Ether 2000;Polyethylene Glycol Dimethyl Ether 250;Polyethylene Glycol Dimethyl Ether 500;Polyethylene Glycol 1000 Dimethyl Ether;Polyethylene Glycol 400 Dimethyl Ether
  • >230 °F
  • Colorless To Yellow To Brown Transparent Liquid
  • 密封阴凉干燥保存
产品参数
CAS号
24991-55-7
分子式
H3CO(C2H4O)nCH3
细胞效力(Cellular Effect)
Cell Type Value(nM) Reference
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
11A549 IC50 18.74 CHEMBL413
体外研究(In Vitro)

The target of rapamycin proteins regulate various cellular processes including autophagy, which may play a protective role in certain neurodegenerative and infectious diseases. Here we show that a primary small-molecule screen in yeast yields novel small-molecule modulators of mammalian autophagy. We first identified new small-molecule enhancers (SMER) and inhibitors (SMIR) of the cytostatic effects of rapamycin in Saccharomyces cerevisiae. Three SMERs induced autophagy independently of rapamycin in mammalian cells, enhancing the clearance of autophagy substrates such as mutant huntingtin and A53T alpha-synuclein, which are associated with Huntington's disease and familial Parkinson's disease, respectively. These SMERs, which seem to act either independently or downstream of the target of rapamycin, attenuated mutant huntingtin-fragment toxicity in Huntington's disease cell and Drosophila melanogaster models, which suggests therapeutic potential. We also screened structural analogs of these SMERs and identified additional candidate drugs that enhanced autophagy substrate clearance. Thus, we have demonstrated proof of principle for a new approach for discovery of small-molecule modulators of mammalian autophagy.

体内研究(In Vivo)

The target of rapamycin proteins regulate various cellular processes including autophagy, which may play a protective role in certain neurodegenerative and infectious diseases. Here we show that a primary small-molecule screen in yeast yields novel small-molecule modulators of mammalian autophagy. We first identified new small-molecule enhancers (SMER) and inhibitors (SMIR) of the cytostatic effects of rapamycin in Saccharomyces cerevisiae. Three SMERs induced autophagy independently of rapamycin in mammalian cells, enhancing the clearance of autophagy substrates such as mutant huntingtin and A53T alpha-synuclein, which are associated with Huntington's disease and familial Parkinson's disease, respectively.

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