Streptococcus pneumoniae expresses two surface-exposed lipoproteins, PpmA and SlrA, which share homology with distinct families of peptidyl-prolyl isomerases (PPIases). In this study, we demonstrated for the first time that the lipoprotein cyclophilin, SlrA, can catalyze the cis-trans isomerization of proline containing tetrapeptides and that SlrA contributes to pneumococcal colonization. The substrate specificity of SlrA is typical for prokaryotic and eukaryotic cyclophilins, with Suc-Ala-AlaPro-Phe-p-nitroanilide (pNA) being the most rapidly catalyzed substrate. In a mouse pneumonia model the slrA knock-out D39⌬slrA did not cause significant differences in the survival times of mice compared with the isogenic wild-type strain. In contrast, a detailed analysis of bacterial outgrowth over time in the nasopharynx, airways, lungs, blood, and spleen showed a rapid elimination of slrA mutants from the upper airways but did not reveal significant differences in the lungs, blood, and spleen. These results suggested that SlrA is involved in colonization but does not contribute significantly to invasive pneumococcal disease. In cell culture infection experiments, the absence of SlrA impaired adherence to pneumococcal disease-specific epithelial and endothelial non-professional cell lines. Adherence of the slrA mutant could not be restored by exogenously added SlrA. Strikingly, deficiency in SlrA did not reduce binding activity to host target proteins, but resulted in enhanced uptake by professional phagocytes. In conclusion, SlrA is a functional, cyclophilin-type PPIase and contributes to pneumococcal virulence in the first stage of infection, namely, colonization of the upper airways, most likely by modulating the biological function of important virulence proteins.
Peptidyl-prolyl cis/trans isomerases (PPIases)6 are ubiquitous foldases, which accelerate the rate-limiting cis-trans or trans-cis conformational changes at Xaa-Pro bonds during protein folding in both eukaryotes and prokaryotes. There are three distinct families within the enzyme class of PPIases (EC 5.2.1.8): the cyclophilins, which bind the immunosuppressant cyclosporin A, the FK506-binding proteins, and the parvulins. The classical PPIase such as rotamase A of Escherichia coli is a member of the cyclophilin family (1, 2). The FK506-binding proteins all have high affinity for the immunosuppressant drug FK506 (3, 4). The ubiquitous bacterial trigger factor (5, 6) and the macrophage infectivity potentiator (Mip) protein of Legionella pneumophila (7) belong to the FK506-binding proteins. The parvulin family resembles enzymes such as parvulin, SurA, and PrsA. The E. coli parvulin 10 with its 92 amino acids is one of the smallest known PPIase enzymes and represents the prototype of this family (8). SurA contributes to the assembly of outer membrane proteins in Gram-negative bacteria (9). PrsA is considered to be involved in enzyme secretion and activation in Gram-positive bacteria (10 -12).Streptococcus pneumoniae (the pneumococcus) is a frequent colonizer of...
