Roy, Amit ; Das, Benu Brata ; Ganguly, Agneyo ; Dasgupta, Somdeb Bose ; Khalkho, Neeta V. M. ; Pal, Churala ; Dey, Sumit ; Giri, Venkatachalam Sesha ; Jaisankar, Parasuraman ; Dey, Sanjit ; Majumder, Hemanta K. (2008) An insight into the mechanism of inhibition of unusual bi-subunit topoisomerase I from Leishmania donovani by 3,3'-di-indolylmethane, a novel DNA topoisomerase I poison with a strong binding affinity to the enzyme Biochemical Journal, 409 . pp. 611-622. ISSN 0264-6021
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Official URL: http://www.biochemj.org/bj/409/0611/bj4090611.htm
Related URL: http://dx.doi.org/10.1042/BJ20071286
Abstract
DIM (3,3'-di-indolylmethane), an abundant dietary component of cruciferous vegetables, exhibits a wide spectrum of pharmacological properties. In the present study, we show that DIM is a potent inhibitor of Leishmania donovani topoisomerase I with an IC50 of 1.2 mM. Equilibrium dialysis shows that DIM binds strongly to the free enzyme with a binding constant of 9.73×10-9M. The binding affinity of DIM to the small subunit is 8.6-fold more than that of the large subunit of unusual LdTOP1LS (bi-subunit L. donovani topoisomerase I). DIM stabilizes topoisomerase I-DNA cleavage complexes in vitro and also in vivo. Like CPT (camptothecin), DIM inhibits the religation step when the drug was added to preformed topoisomerase I-DNA binary complex. Hence, DIM is similar to CPT with respect to its ability to form the topoisomerase I-mediated 'cleavable complexes' in vitro and in vivo. But unlike CPT, DIM interacts with both free enzyme and substrate DNA. Therefore DIM is a non-competitive class I inhibitor of topoisomerase I. DIM also inhibits the relaxation activity of the CPT-resistant mutant enzyme LdTOP1D39LS (N-terminal deletion of amino acids 1-39 of LdTOP1LS). The IC50 values of DIM in simultaneous and enzyme pre-incubation relaxation assays were 3.6 and 2.9 µ M respectively, which are higher than that of wild-type topoisomerase I (LdTOP1LS), indicating that the affinity of DIM to LdTOP1D39LS is less than that for LdTOP1LS. This is the first report on DIM as an L. donovani topoisomerase I poison. Our study illuminates a new mode of action of enzyme inhibition by DIM that might be exploited for rational drug design in human leishmaniasis.
Item Type: | Article |
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Source: | Copyright of this article belongs to Portland Press. |
Keywords: | Cleavable Complex; 3,3'-di-indolylmethane (DIM); Leishmania donovani; Reconstitution; Topoisomerase I; Topoisomerase Poison |
ID Code: | 87824 |
Deposited On: | 22 Mar 2012 07:55 |
Last Modified: | 22 Mar 2012 07:55 |
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