6ESL

Crystal structure of the Legionella pneumoppila LapA

Summary for 6ESL

• Entry DOI: 10.2210/pdb6esl/pdb
• Descriptor: Bacterial leucyl aminopeptidase, ZINC ION (3 entities in total)
• Functional Keywords: aminopeptidase, legionella pneumophila, virulence factor, hydrolase
• Biological source: Legionella pneumophila
• Total number of polymer chains: 2
• Total formula weight: 88671.14

Authors

Richardson, K.,Garnett, J.A. (deposition date: 2017-10-22, release date: 2018-04-04, Last modification date: 2024-10-09)

Primary citation

White, R.C.,Gunderson, F.F.,Tyson, J.Y.,Richardson, K.H.,Portlock, T.J.,Garnett, J.A.,Cianciotto, N.P.
Type II Secretion-Dependent Aminopeptidase LapA and Acyltransferase PlaC Are Redundant for Nutrient Acquisition duringLegionella pneumophilaIntracellular Infection of Amoebas.
MBio, 9:-, 2018

PubMed Abstract: genes encoding LapA, LapB, and PlaC were identified as the most highly upregulated type II secretion (T2S) genes during infection of , although these genes had been considered dispensable on the basis of the behavior of mutants lacking either and or A mutant showed even higher levels of and transcripts, and a mutant showed heightening of mRNA levels, suggesting that the role of the LapA/B aminopeptidase is compensatory with respect to that of the PlaC acyltransferase. Hence, we made double mutants and found that mutants have an ~50-fold defect during infection of These data revealed, for the first time, the importance of LapA in any sort of infection; thus, we purified LapA and defined its crystal structure, activation by another T2S-dependent protease (ProA), and broad substrate specificity. When the amoebal infection medium was supplemented with amino acids, the defect of the mutant was reversed, implying that LapA generates amino acids for nutrition. Since the LapA and PlaC data did not fully explain the role of T2S in infection, we identified, via proteomic analysis, a novel secreted protein (NttD) that promotes infection of A mutant displayed an even greater (100-fold) defect, demonstrating that the LapA, PlaC, and NttD data explain, to a significant degree, the importance of T2S. LapA-, PlaC-, and NttD-like proteins had distinct distribution patterns within and outside the genus. LapA was notable for having as its closest homologue an protein. Transmission of to humans is facilitated by its ability to grow in species. We previously documented that type II secretion (T2S) promotes infection of Utilizing transcriptional analysis and proteomics, double and triple mutants, and crystal structures, we defined three secreted substrates/effectors that largely clarify the role of T2S during infection of Particularly interesting are the unique functional overlap between an acyltransferase (PlaC) and aminopeptidase (LapA), the broad substrate specificity and eukaryotic-protein-like character of LapA, and the novelty of NttD. Linking LapA to amino acid acquisition, we defined, for the first time, the importance of secreted aminopeptidases in intracellular infection. Bioinformatic investigation, not previously applied to T2S, revealed that effectors originate from diverse sources and distribute within the genus in unique ways. The results of this study represent a major advance in understanding ecology and pathogenesis, bacterial secretion, and the evolution of intracellular parasitism.

PubMed: 29666285
DOI: 10.1128/mBio.00528-18

Experimental method

X-RAY DIFFRACTION (1.87 Å)