Structural and kinetic characterization of Porphyromonas gingivalis glutaminyl cyclase

Author:

Lamers Sebastiaan1ORCID,Feng Qiaoli1,Cheng Yili2,Yu Sihong1,Sun Bo3,Lukman Maxwell1,Jiang Jie1,Ruiz-Carrillo David1ORCID

Affiliation:

1. Department of Biological Sciences , School of Science, Xi’an Jiaotong-Liverpool University , Suzhou , Jiangsu 215123 , China

2. Department of Health and Environmental Sciences , School of Science, Xi’an Jiaotong-Liverpool University , Suzhou , Jiangsu 215123 , China

3. Shanghai Advanced Research Institute, Chinese Academy of Sciences , Shanghai 201204 , China

Abstract

Abstract Porphyromonas gingivalis is a bacterial species known to be involved in the pathogenesis of chronic periodontitis, that more recently has been as well associated with Alzheimer’s disease. P. gingivalis expresses a glutaminyl cyclase (PgQC) whose human ortholog is known to participate in the beta amyloid peptide metabolism. We have elucidated the crystal structure of PgQC at 1.95 Å resolution in unbound and in inhibitor-complexed forms. The structural characterization of PgQC confirmed that PgQC displays a mammalian fold rather than a bacterial fold. Our biochemical characterization indicates that PgQC uses a mammalian-like catalytic mechanism enabled by the residues Asp149, Glu182, Asp183, Asp218, Asp267 and His299. In addition, we could observe that a non-conserved Trp193 may drive differences in the binding affinity of ligands which might be useful for drug development. With a screening of a small molecule library, we have identified a benzimidazole derivative rendering PgQC inhibition in the low micromolar range that might be amenable for further medicinal chemistry development.

Publisher

Walter de Gruyter GmbH

Subject

Clinical Biochemistry,Molecular Biology,Biochemistry

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