Basu H S, Pellarin M, Feuerstein B G, Shirahata A, Samejima K, Deen D F, Marton L J
Department of Neurological Surgery, School of Medicine, University of California, San Francisco 94143.
Cancer Res. 1993 Sep 1;53(17):3948-55.
Computer graphics modeling and physicochemical studies of spermine-DNA interactions, as well as experiments in cell culture, indicate that a polyamine analogue with strong affinity for nucleic acids but poor ability to condense and aggregate DNA in vitro should act as an antiproliferative agent if it can enter cells. On the basis of our studies of polyamine-DNA interactions, we designed a pentamine, 1,19-bis(ethylamino)-5,10,15- triazanonadecane (BE-4-4-4-4), that had these characteristics. Measurement of melting temperature and ultraviolet light scattering studies show that the affinity of this analogue for calf-thymus DNA is about 4 times higher than that of spermine, whereas its ability to aggregate DNA is slightly poorer than that of spermine. Studies in U-87 MG, U-251 MG, SF-126, SF-188, SF-763, SF-767, and DAOY human brain tumor cells in tissue culture showed that treatment for more than 96 h with concentrations of 5 microM BE-4-4-4-4 or greater inhibited growth; decreased levels of putrescine, spermidine, and spermine; and decreased colony-forming ability in all cell lines. The cytotoxicity of the analogue varied among cell lines; DAOY and SF-767 were the most sensitive and the most resistant lines, respectively. In SF-763 cells, growth inhibition by BE-4-4-4-4 could be partially reversed by the addition of putrescine, spermidine, or spermine 1 day after BE-4-4-4-4 addition, but in U-251 MG cells, growth inhibition was reversed only by spermine and not by other polyamines. When any of the naturally occurring polyamines was added simultaneously with BE-4-4-4-4, growth inhibition was completely blocked. The data suggest that a threshold intracellular concentration of BE-4-4-4-4 is needed to manifest the growth-inhibitory and cytotoxic effects. In most cell lines, once that threshold level is reached, the growth-inhibitory and cytotoxic properties of the analogue are manifest irrespective of cellular polyamine levels. Further increases in the BE-4-4-4-4 concentration or incubation time reduce the intracellular polyamine levels but do not significantly increase growth inhibition. In U-87 MG and DAOY cells, however, prolonged incubation with higher concentrations of BE-4-4-4-4 causes additional growth inhibition along with depletion of intracellular polyamines.(ABSTRACT TRUNCATED AT 400 WORDS)
精胺与DNA相互作用的计算机图形建模和物理化学研究,以及细胞培养实验表明,如果一种对核酸具有强亲和力但在体外凝聚和聚集DNA能力较差的多胺类似物能够进入细胞,那么它应该具有抗增殖作用。基于我们对多胺与DNA相互作用的研究,我们设计了一种具有这些特性的五胺,即1,19 - 双(乙氨基)- 5,10,15 - 三氮杂十九烷(BE - 4 - 4 - 4 - 4)。熔点测量和紫外光散射研究表明,这种类似物对小牛胸腺DNA的亲和力比精胺高约4倍,而其聚集DNA的能力略逊于精胺。在组织培养中的U - 87 MG、U - 251 MG、SF - 126、SF - 188、SF - 763、SF - 767和DAOY人脑肿瘤细胞中的研究表明,用5 microM或更高浓度的BE - 4 - 4 - 4 - 4处理超过96小时会抑制生长;降低腐胺、亚精胺和精胺的水平;并降低所有细胞系的集落形成能力。该类似物的细胞毒性在不同细胞系中有所不同;DAOY和SF - 767分别是最敏感和最耐药的细胞系。在SF - 763细胞中,添加BE - 4 - 4 - 4 - 4一天后,添加腐胺、亚精胺或精胺可部分逆转BE - 4 - 4 - 4 - 4对生长的抑制作用,但在U - 251 MG细胞中,只有精胺能逆转生长抑制作用,其他多胺则不能。当任何一种天然存在的多胺与BE - 4 - 4 - 4 - 4同时添加时,生长抑制作用会被完全阻断。数据表明,需要一定的细胞内BE - 4 - 4 - 4 - 4阈值浓度才能表现出生长抑制和细胞毒性作用。在大多数细胞系中,一旦达到该阈值水平,该类似物的生长抑制和细胞毒性特性就会显现,而与细胞内多胺水平无关。BE - 4 - 4 - 4 - 4浓度或孵育时间的进一步增加会降低细胞内多胺水平,但不会显著增加生长抑制作用。然而,在U - 87 MG和DAOY细胞中,用更高浓度的BE - 4 - 4 - 4 - 4长时间孵育会导致额外的生长抑制以及细胞内多胺的消耗。(摘要截选至400字)
