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Pentamidine isethionate,140-64

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  • ¥331 - 1433
  • 爱必信(absin)
  • 上海
  • abs817318
  • 2025年07月13日
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  • 企业认证

    • 详细信息
    • 文献和实验
    • 技术资料
    • 保存条件

      Store at -20℃ for one year(Powder);Store at 2-4℃ for two weeks;Store at -20℃ for six months after dissolution.

    • 库存

      99

    • 供应商

      爱必信(上海)生物科技有限公司

    • CAS号

      140-64-7

    • 规格

      200mg/100mg/50mg/25mg

    规格:200mg产品价格:¥1433.0
    规格:100mg产品价格:¥877.0
    规格:50mg产品价格:¥506.0
    规格:25mg产品价格:¥331.0

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    抑制剂描述:

    产品名称:Pentamidine isethionate

    产品别名:见爱必信官网

    英文别名:Pentamidine isethionate

    靶点:Antibacterial

    CAS:140-64-7

    纯度:99%

    外观:见爱必信官网

    保存方法:Store at -20℃ for one year(Powder);Store at 2-4℃ for two weeks;Store at -20℃ for six months after dissolution.

    描述:

    Pentamidine isethionate is an antimicrobial agent for prevention and treatment of Pneumocystis pneumonia (PCP) caused by Pneumocystis jirovecii.

    溶解性:water : 59.3 mg/mL (100 mM)

    体外研究:

    Pentamidine is known experimentally to interfere with numerous cellular processes. Specifically, Pentamidine has been shown to bind to DNA in a nonintercalative manner and appears to preferentially bind to kinetoplast DNA in trypanosomes. Additionally, Pentamidine may inhibit RNA polymerase and ribosomal function, as well as nucleic acid, protein, phospholipid, and polyamine synthesis. Pentamidine also inhibits certain proteases, including trypsin, and impairs cellular oxygen consumption. Pentamidine has a potent in vitro antiprotozoal activity. Pentamidine displays cytotoxic activity against L. infantum promastigotes with IC50 of 2.5 μM. 2.5 μM Pentamidine induces early programmed cell death in 49.6% of L. infantum promastigotes. 2.5 μM Pentamidine induces a notorious decrease in promastigotes in both G1 and S phases relative to the control-untreated samples (G1:77.0 vs 15.0%; S:11.0 vs 2.4% for control- and pentamidine-treated promastigotes, resp). Pentamidine is able to bind with calf-thymus DNA (CT-DNA) and induces conformational changes in the DNA double helix. Pentamidine also binds with ubiquitin to modifiy the β-cluster of ubiquitin. Pentamidine is an inhibitor of phosphatase of regenerating liver (PRLs). 1 μg/mL of Pentamidine complete inhibits the activity of recombinant PTP1B in dephosphorylating a phos-photyrosine peptide. 10 μg/mL of Pentamidine completely inhibits the activities of recombinant PRL-1, PRL-2 and PRL-3 in dephosphorylating a phosphotyrosine peptide substrate. Incubation with Pentamidine (1 μg/mL) for 48 h reduces the activity of intracellular PRL phosphatases in transfected NIH3T3 cells by more than 85%. 10 μg/mL Pentamidine completely inhibits the growth of melanoma cell line (WM9), prostate carcinoma cell line (DU145 and C4–2), ovarian carcinoma cell line (Hey), colon carcinoma cell line (WM480), and lung carcinoma cell line (A549) which all express endogenous PRLs.

    体内研究:Pentamidine has a potent antiprotozoal activity in animal models. Pentamidine (0.3-9 mg/L) decreased the viability of P. carinii in experimental models in chick embryo lung epithelial cells and lung cells of rats with pneumonia. 5 mg/kg Pentamidine treatment for 2 weeks eradicates Pneumocystis carinii pneumonia in 75% of the animals. Pentamidine inhibits the growth of WM9 human melanoma tumors in nude mice. During the 16-week study period, the tumors in 250 μg pentamidine-treated mice stays at sizes similar to those at the treatment initiation point, whereas the tumors in the control mice grow so rapidly that humane sacrifice of the animals is required at the 4th week. Pentamidine induces significant necrosis that accounts for more than 50% of the tumor mass.

    产品信息订购:

      产品货号   产品名称   规格 价格 大包装及货期
      abs817318   Pentamidine isethionate   25mg   331.00   立即咨询
      abs817318   Pentamidine isethionate   50mg   506.00   立即咨询
      abs817318   Pentamidine isethionate   100mg   877.00   立即咨询
      abs817318   Pentamidine isethionate   200mg   1433.00   立即咨询

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      . Nature 439:993–997, 2006; Eirew et al. Nat Med 14:1384–1389, 2008; Raouf et al. Cell Stem Cell 3:109–118, 2008; Stingl et al. Differentiation 63:201–213, 1998; Jones et al. Cancer Res 64:3037–3045, 2004). Here, we describe a new methodology

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