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Metallo-tallysomycin (an anticancer drug metal complex) recognizes specific tumor cell, and noncovalently binds to DNA base pair to cleave sequence. Anticancer drug metal complexes, zinc- and cobalt-binding tallysomycins, were synthesized and purified in order to understand the functions of metal complexes. Complete exchangeable 1H-NMR signal assignment was accomplished by optimal pH- and temperature-dependent 1H-NMR studies. In addition, a recently developed NERD (2D NOESY-1-1 echo) experiment gave a detail structural feature which is useful for NMR-based solution state structure determination of complex. Results exhibit that nitrogen atoms of ¥â-aminoalanine, ¥â-hydroxyhistidine, imidazole, and pyrimidine ring are the metal binding sites with a Zn(¥±) ion, whereas Co(¥²) ion can bind to one and two equivalent of tallysomycin, respectively.
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