meso-Bromination of cyano- and aquacobalamins facilitates their processing into Co(II)-species by glutathione
Cyanocobalamin (CNCbl), a medicinal form of vitamin B 12 , is resistant to glutathione (GSH), and undergoes intracellular processing via reductive decyanation producing the Co(II)-form of Cbl (Cbl(II)) mediated by the CblC-protein. Alteration of the CblC-protein structure might inhibit CNCbl process...
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Veröffentlicht in: | Journal of biological inorganic chemistry 2023-09, Vol.28 (6), p.571-581 |
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Sprache: | eng |
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Zusammenfassung: | Cyanocobalamin (CNCbl), a medicinal form of vitamin B
12
, is resistant to glutathione (GSH), and undergoes intracellular processing via reductive decyanation producing the Co(II)-form of Cbl (Cbl(II)) mediated by the CblC-protein. Alteration of the CblC-protein structure might inhibit CNCbl processing. Here, we showed that introducing a bromine atom to the C10-position of the CNCbl corrin ring facilitates its reaction with GSH leading to the formation of Cbl(II) and cyanide dissociation. In a neutral medium, the reaction between C10-Br-CNCbl and GSH proceeds via the complexation of the reactants further leading to dimethylbenzimidazole (DMBI) substitution and electron transfer from GSH to the Co(III)-ion. The reaction is accelerated upon the GSH thiol group deprotonation. The key factors explaining the higher reactivity of C10-Br-CNCbl compared with unmodified CNCbl towards GSH are increasing the electrode potential of CNCbl two-electron reduction upon meso-bromination and the substantial labilization of DMBI, which was shown by comparing their reactions with cyanide and the p
K
a
values of DMBI protonation (p
K
a base-off
). Aquacobalamin (H
2
OCbl) brominated at the C10-position of the corrin reacts with GSH to give Cbl(II) via GSH complexation and subsequent reaction of this complex with a second GSH molecule, whereas unmodified H
2
OCbl generates glutathionyl-Cbl, which is resistant to further reduction by GSH.
Graphical abstract |
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ISSN: | 1432-1327 0949-8257 1432-1327 |
DOI: | 10.1007/s00775-023-02009-x |