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Original Articles

Association of antitumor antibiotic Mithramycin with Mn2+ and the potential cellular targets of Mithramycin after association with Mn2+

, , , &
Pages 434-446 | Received 16 Aug 2013, Accepted 21 Jan 2014, Published online: 21 Feb 2014
 

Abstract

Mithramycin (MTR), an aureolic acid group of antitumor antibiotic is used for the treatment of several types of tumors. We have reported here the association of MTR with an essential micronutrient, manganese (Mn2+). Spectroscopic methods have been used to characterize and understand the kinetics and mechanism of complex formation between them. MTR forms a single type of complex with Mn2+ in the mole ratio of 2:1 [MTR: Mn2+] via a two step kinetic process. Circular dichroism (CD) spectroscopic study indicates that the complex [(MTR)2 Mn2+] has a right-handed twist conformation similar in structure with the complexes reported for Mg2+ and Zn2+. This conformation allows binding via minor groove of DNA with (G, C) base preference during the interaction with double-stranded B-DNA. Using absorbance, fluorescence, and CD spectroscopy we have shown that [(MTR)2 Mn2+] complex binds to double-stranded DNA with an apparent dissociation constant of 32 μM and binding site size of 0.2 (drug/nucleotide). It binds to chicken liver chromatin with apparent dissociation constant value 298 μM. Presence of histone proteins in chromatin inhibits the accessibility of the complex for chromosomal DNA. We have also shown that MTR binds to Mn2+ containing metalloenzyme manganese superoxide dismutase from Escherichia coli.

Acknowledgments

This work was funded from the intramural grant (MMDDA and BARD project) from the Department of Atomic Energy (DAE, Govt. of India). S.D thanks Council of Scientific and Industrial Research (CSIR), Govt. of India for the award of research fellowship.

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