17种β -[N-[N'-(2-氯乙基)-N'-亚硝基]氨基甲酰]氨基酸的新型类固醇偶联物及其对大鼠Noble Nb前列腺癌模型的抗肿瘤活性

Anti-cancer drug design Pub Date : 1998-10-01
W Tang, M R Schneider, G Eisenbrand
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引用次数: 0

摘要

合成了新型类固醇偶联物17 β -[N-[N'-(2-氯乙基)-N'-亚硝基]氨基甲酰]-甘酰-19-去甲睾酮(1)和17 β -[N-[N'-(2-氯乙基)-N'-亚硝基]氨基甲酰]- l- alyanyl-19-去甲睾酮(2),并对其与类固醇受体的亲和力和雄激素效应进行了表征。在50 mg/kg的剂量下,偶联物1和2对大鼠的nober Nb前列腺癌有较强的抑瘤作用,但也有明显的体重减轻。在两个进一步的实验中,偶联物2以25mg /kg的剂量治疗显示出高的抗肿瘤活性,无毒性迹象。偶联物2达到与近两倍摩尔剂量的环磷酰胺相同的肿瘤生长抑制作用。结果表明,在耐受良好的剂量下,2在Noble Nb模型中具有较高的抗肿瘤活性。低剂量等摩尔的N-(2-氯乙基)-N-亚硝基氨基甲酰(CNC)-丙氨酸和19-去甲睾酮混合物的毒性明显高于偶联物2,对体重的不良影响与高剂量偶联物大致相同。等摩尔剂量的cnc - l -丙氨酸具有高毒性,可导致所有动物早期死亡。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Novel steroid-linked conjugates of 17 beta-[N-[N'-(2-chloroethyl)-N'-nitroso]carbamoyl]amino acids and their antineoplastic activity against Noble Nb prostate carcinoma model in rats.

The novel steroid conjugates 17 beta-[N-[N'-(2-chloroethyl)-N'-nitroso] carbamoyl]-glycyl-19-nortestosterone (1) and 17 beta-[N-[N'-(2-chloroethyl)-N'-nitroso]carbamoyl]-L-alyanyl-19- nortestosterone (2) were synthesized and characterized with respect to affinity for steroid receptors and for androgenic efficacy. At an i.p. dosage of 50 mg/kg, conjugates 1 and 2 induced strong tumor inhibition of Nobel Nb prostate carcinoma in rats, but also a marked loss of body weight. In two further experiments, treatment with conjugate 2 at a dosage of 25 mg/kg demonstrated high antitumor activity without indication of toxicity. Conjugate 2 achieved the same tumor growth inhibition as a nearly twofold molar dose of cyclophosphamide. The results indicate reproducibly high antitumor activity of 2 in the Noble Nb model at a well tolerated dosage. A low dose equimolar mixture of unlinked N-(2-chloroethyl)-N-nitrosocarbamoyl (CNC)-alanine and 19-nortestosterone was significantly more toxic than conjugate 2, showing about the same adverse effect on the body weight as the conjugate at high dosage. CNC-L-alanine at equimolar dosage was highly toxic, causing early death of all animals.

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