1. Cadmium transport activity of four mercury transporters (MerC, MerE, MerF and MerT) and effects of the periplasmic mercury-binding protein MerP on Mer-dependent cadmium uptake
- Author
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Yasukazu Takanezawa, Ryosuke Nakamura, Yuka Ohshiro, Masako Kiyono, and Shimpei Uraguchi
- Subjects
inorganic chemicals ,0106 biological sciences ,Mercury binding ,chemistry.chemical_element ,medicine.disease_cause ,01 natural sciences ,Microbiology ,03 medical and health sciences ,Bacterial Proteins ,Cadmium transport ,Escherichia coli ,Genetics ,medicine ,Cation Transport Proteins ,Molecular Biology ,030304 developmental biology ,0303 health sciences ,Cadmium ,biology ,Membrane transport protein ,food and beverages ,Transporter ,Mercury ,Periplasmic space ,humanities ,Mercury (element) ,body regions ,chemistry ,Biochemistry ,Periplasmic Binding Proteins ,biology.protein ,010606 plant biology & botany - Abstract
Mercury superfamily proteins, i.e. inner membrane-spanning proteins (MerC, MerE, MerF and MerT) and a periplasmic mercury-binding protein (MerP), transport mercury into the cytoplasm. A previous study demonstrated that a Mer transporter homolog exhibits cadmium transport activity; based on this, the present study aimed to evaluate the cadmium transport activity of MerC, MerE, MerF and MerT and the effects of MerP co-expression in Escherichia coli. Bacteria expressing MerC, MerE, MerF or MerT without MerP were more sensitive to cadmium and significantly absorbed more cadmium than did the control strain. Expression of MerP in combination with MerC, MerE, MerF or MerT increased the bacterial sensitivity to cadmium and cadmium accumulation compared to a single expression of MerC, MerE, MerF or MerT. Cadmium uptake mediated by MerC, MerE, MerF or MerT was inhibited under cold or acidic conditions. These findings suggest that MerC, MerE, MerF and MerT are broad-spectrum heavy metal transporters that mediate both mercury and cadmium transport into cells and that MerP accelerates the cadmium transport ability of MerC, MerE, MerF and MerT.
- Published
- 2020
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