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Growth inhibition of human melanoma tumor cells by the combination of sodium phenylacetate (NaPA) and substituted dextrans and one NaPA-dextran conjugate.

机译:苯乙酸钠(NaPA)与取代的右旋糖酐和一种NaPA-右旋糖酐缀合物的组合抑制人黑素瘤肿瘤细胞的生长。

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We have studied the cytostatic effects of sodium phenylacetate (NaPA) in association with several substituted dextrans on human tumor melanoma 1205LU cells. We show that NaPA alone inhibits the growth of these cells (IC50 = 3.9 mM) while a weak inhibitory effect appears at a concentration of 37 microM (10 microg/ml) for a dextran methyl carboxylate benzylamide (LS17-DMCB). The precursors of LS17-DMCB [T40 Dextran and carboxymethyl dextran (LS17-DMC)] did not affect the growth of 1205LU cells. To potentiate the inhibitory activity of NaPA at low concentrations (below 5.6 mM), we have tested NaPA and LS17-DMCB in physical mixture (association) or linked together covalently (this conjugate is termed 'LS17-NaPaC'). We have observed an increase of the 1205LU cell growth inhibition effect with NaPA in association (IC50 1.8 mM). For a concentration of 5 mM of NaPA (free in the case of association or linked in the case of conjugate), the association with dextran derivative exhibits a 4.6-fold higher efficacy than with NaPA alone (9 versus 41% surviving fraction), while the conjugate is 1.3-fold smaller (52% growth inhibition). By performing isobologram analysis of the IC50 data, we have shown a synergistic effect for a particular molar ratio of NaPA and LS17-DMCB (NaPA:LS17-DMCB = 0.35).
机译:我们已经研究了苯乙酸钠(NaPA)与几种取代的右旋糖酐对人肿瘤黑素瘤1205LU细胞的抑制作用。我们显示,单独的NaPA会抑制这些细胞的生长(IC50 = 3.9 mM),而对于葡聚糖甲基羧化苄基酰胺(LS17-DMCB),浓度为37 microM(10 microg / ml)时会出现弱抑制作用。 LS17-DMCB的前体[T40葡聚糖和羧甲基葡聚糖(LS17-DMC)]不会影响1205LU细胞的生长。为了增强低浓度(低于5.6 mM)NaPA的抑制活性,我们已经测试了NaPA和LS17-DMCB在物理混合物(缔合)中或共价连接在一起(此共轭物称为“ LS17-NaPaC”)。我们已经观察到与NaPA缔合(IC50 1.8 mM)可以提高1205LU细胞的生长抑制作用。对于浓度为5 mM的NaPA(在缔合情况下是游离的或在缀合物的情况下是连接的),与右旋糖酐衍生物的缔合比单独的NaPA表现出4.6倍的功效(9%对41%的存活分数),而结合物要小1.3倍(抑制52%的生长)。通过对IC50数据进行等效线分析,我们显示了特定摩尔比的NaPA和LS17-DMCB(NaPA:LS17-DMCB = 0.35)的协同效应。

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