Gregson S J, Howard P W, Hartley J A, Brooks N A, Adams L J, Jenkins T C, Kelland L R, Thurston D E
CRC Gene Targeted Drug Design Research Group, Cancer Research Laboratories, University of Nottingham, University Park, Nottingham NG7 2RD, UK.
J Med Chem. 2001 Mar 1;44(5):737-48. doi: 10.1021/jm001064n.
A novel sequence-selective pyrrolobenzodiazepine (PBD) dimer 5 (SJG-136) has been developed that comprises two C2-exo-methylene-substituted DC-81 (3) subunits tethered through their C8 positions via an inert propanedioxy linker. This symmetric molecule is a highly efficient minor groove interstrand DNA cross-linking agent (XL(50) = 0.045 microM) that is 440-fold more potent than melphalan. Thermal denaturation studies show that, after 18 h incubation with calf thymus DNA at a 5:1 DNA/ligand ratio, it increases the T(m) value by 33.6 degrees C, the highest value so far recorded in this assay. The analogous dimer 4 (DSB-120) that lacks substitution/unsaturation at the C2 position elevates melting by only 15.1 degrees C under the same conditions, illustrating the effect of introducing C2-exo-unsaturation which serves to flatten the C-rings and achieve a superior isohelical fit within the DNA minor groove. This behavior is supported by molecular modeling studies which indicate that (i) the PBD units are covalently bonded to guanines on opposite strands to form a cross-link, (ii) 5 has a greater binding energy compared to 4, and (iii) 4 and 5 have equivalent binding sites that span six base pairs. Dimer 5 is significantly more cytotoxic than 4 in a number of human ovarian cancer cell lines (e.g., IC(50) values of 0.0225 nM vs 7.2 nM, respectively, in A2780 cells). Furthermore, it retains full potency in the cisplatin-resistant cell line A2780cisR (0.024 nM), whereas 4 loses activity (0.21 microM) with a resistance factor of 29.2. This may be due to a lower level of inactivation of 5 by intracellular thiol-containing molecules. A dilactam analogue (21) of 5 that lacks the electrophilic N10-C11/N10'-C11' imine moieties has also been synthesized and evaluated. Although unable to interact covalently with DNA, 21 still stabilizes the helix (Delta T(m) = 0.78 degrees C) and has significant cytotoxicity in some cell lines (i.e., IC(50) = 0.57 microM in CH1 cells), presumably exerting its effect through noncovalent interaction with DNA.
一种新型的序列选择性吡咯并苯二氮卓(PBD)二聚体5(SJG - 136)已被研发出来,它由两个通过惰性丙二氧基连接子在其C8位连接的C2 - 外向亚甲基取代的DC - 81(3)亚基组成。这个对称分子是一种高效的小沟链间DNA交联剂(XL(50) = 0.045 μM),其效力比美法仑高440倍。热变性研究表明,在DNA/配体比例为5:1的条件下,与小牛胸腺DNA孵育18小时后,它使熔解温度(T(m))值升高33.6℃,这是该测定中迄今记录到的最高值。在相同条件下,C2位缺乏取代/不饱和的类似二聚体4(DSB - 120)仅使熔解温度升高15.1℃,这说明了引入C2 - 外向不饱和的作用,它能使C环变平并在DNA小沟内实现更好的等螺旋契合。分子模拟研究支持了这种行为,研究表明:(i)PBD单元与相反链上的鸟嘌呤共价结合形成交联;(ii)与4相比,5具有更大的结合能;(iii)4和5具有跨越六个碱基对的等效结合位点。在多种人卵巢癌细胞系中,二聚体5的细胞毒性明显高于4(例如,在A2780细胞中,IC(50)值分别为0.0225 nM和7.2 nM)。此外,它在顺铂耐药细胞系A2780cisR中仍保持全部效力(0.024 nM),而4失去活性(0.21 μM),耐药系数为29.2。这可能是由于5被细胞内含硫醇分子灭活的程度较低。还合成并评估了5的一种缺乏亲电N10 - C11/N10' - C11'亚胺基团的双内酰胺类似物(21)。尽管21不能与DNA共价相互作用,但它仍能稳定螺旋(ΔT(m) = 0.78℃),并且在一些细胞系中具有显著的细胞毒性(即,在CH1细胞中IC(50) = 0.57 μM),推测其通过与DNA的非共价相互作用发挥作用。
