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Abstract
Prevotella intermedia is a major periodontopathogen contributing to human gingivitis and periodontitis. Such pathogens release proteases as virulence factors that cause deterrence of host defenses and tissue destruction. A new cysteine protease from the cysteine-histidine-dyad class, interpain A, was studied in its zymogenic and self-processed mature forms. The latter consists of a bivalved moiety made up by two subdomains. In the structure of a catalytic cysteine-to-alanine zymogen variant, the right subdomain interacts with an unusual prodomain, thus contributing to latency. Unlike the catalytic cysteine residue, already in its competent conformation in the zymogen, the catalytic histidine is swung out from its active conformation and trapped in a cage shaped by a backing helix, a zymogenic hairpin, and a latency flap in the zymogen. Dramatic rearrangement of up to 20A of these elements triggered by a tryptophan switch occurs during activation and accounts for a new activation mechanism for proteolytic enzymes. These findings can be extrapolated to related potentially pathogenic cysteine proteases such as Streprococcus pyogenes SpeB and Porphyromonas gingivalis periodontain.
Highlights
Prevotella intermedia is a major bacterial periodontal pathogen in humans together with Porphyromonas gingivalis, among others [5, 6]
Bacterial infection leads to the bacterial secretion or induction of host overproduction of proteolytic enzymes such as bacterial collagenases, matrix metalloproteases, and serine and cysteine proteases (CPs) [2, 7, 8]
Most studies on the bacterial proteolytic armamentarium in Periodontal disease (PD) have been performed with P. gingivalis [9]
Summary
Expression, Mutant Construction, and Purification of Pro-interpain A—Genomic DNA of P. intermedia was extracted from strain ATCC 25611. The structure of wt cd-InpA was solved with program AMoRe [32] using the coordinates corresponding to residues Ala121–Pro359 from ⌬N1pro-cd-InpA C154A and structurefactor amplitudes in the range 15–3.5 Å These calculations unambiguously confirmed P41212 as the correct space group and a unique solution was found at 48.5, 88.4, 223.7, 0.1172, 0.5977, and 0.1152 (␣, , ␥, x, y, and z; refined values after rigid-body refinement; see Ref. 32) and 41.7, 88.6, 115.6, 0.1940, 0.0880, and 0.7122 for each of the two molecules A and B in the asymmetric unit, respectively, with a combined score CCF/ crystallographic Rfactor, according to Ref. 32, of 54.4%/41.4%. The final coordinates of ⌬N1pro-cd-InpA C154A and wt cdInpA have been deposited with the Protein Data Bank at the Research Collaboratory for Structural Bioinformatics with access codes 3bb and 3bba
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