Cadmium-Substituted Concanavalin A and Its Trimeric Complexation

Concanavalin A (ConA) interacts with carbohydrates as a lectin, and recent reports proposed its application for detecting a diversity of viruses and pathogens. Structural studies have detailed the interaction between ConA and carbohydrates and the metal coordination environment with manganese and ca...

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Veröffentlicht in:Journal of microbiology and biotechnology 2018-12, Vol.28 (12), p.2106-2112
Hauptverfasser: Park, Yeo Reum, Kim, Da Som, Lee, Dong-Heon, Kang, Hyun Goo, Park, Jung Hee, Lee, Seung Jae
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Sprache:kor
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Zusammenfassung:Concanavalin A (ConA) interacts with carbohydrates as a lectin, and recent reports proposed its application for detecting a diversity of viruses and pathogens. Structural studies have detailed the interaction between ConA and carbohydrates and the metal coordination environment with manganese and calcium ions (Mn-Ca-ConA). In this study, ConA was crystallized with a cadmium-containing precipitant, and the refined structure indicates that Mn 2+ was replaced by Cd 2+ (Cd-Ca-ConA). The structural comparison with ConA demonstrates that the metal-coordinated residues of Cd-Ca-ConA, that is Glu8, Asp10, Asn14, Asp19, and His24, do not have conformational shifts, but residues for sugar binding, including Arg228, Tyr100, and Leu99, reorient their side chains, slightly. Previous studies demonstrated that excess cadmium ions can coordinate with other residues, including Glu87 and Glu183, which were not coordinated with Cd 2+ in this study. The trimeric ConA in this study coordinated Cd 2+ with other residues, including Asp80 and Asp82, for complex generation. The monomer does not have specific interaction near interface regions with the other monomer, but secondary cadmium coordinated with two aspartates (Asp80 and Asp82) from monomer 1 and one aspartate (Asp16) from monomer 2. This study demonstrated that complex generation was induced via coordination with secondary Cd 2+ and showed the application potential regarding the design of complex formation for specific interactions with target saccharides.
ISSN:1017-7825
1738-8872