Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis

Francisella tularensis is an extremely infectious pathogen and a category A bioterrorism agent. It causes the highly contagious zoonosis, Tularemia. Currently, FDA approved vaccines against tularemia are unavailable. F. tularensis outer membrane protein A (FopA) is a well-studied virulence determina...

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Autores principales: Nagaratnam, Nirupa, Martin-Garcia, Jose M., Yang, Jay-How, Goode, Matthew R., Ketawala, Gihan, Craciunescu, Felicia M., Zook, James D., Sonowal, Manashi, Williams, Dewight, Grant, Thomas D., Fromme, Raimund, Hansen, Debra T., Fromme, Petra
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9342783/
https://www.ncbi.nlm.nih.gov/pubmed/35913965
http://dx.doi.org/10.1371/journal.pone.0267370
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author Nagaratnam, Nirupa
Martin-Garcia, Jose M.
Yang, Jay-How
Goode, Matthew R.
Ketawala, Gihan
Craciunescu, Felicia M.
Zook, James D.
Sonowal, Manashi
Williams, Dewight
Grant, Thomas D.
Fromme, Raimund
Hansen, Debra T.
Fromme, Petra
author_facet Nagaratnam, Nirupa
Martin-Garcia, Jose M.
Yang, Jay-How
Goode, Matthew R.
Ketawala, Gihan
Craciunescu, Felicia M.
Zook, James D.
Sonowal, Manashi
Williams, Dewight
Grant, Thomas D.
Fromme, Raimund
Hansen, Debra T.
Fromme, Petra
author_sort Nagaratnam, Nirupa
collection PubMed
description Francisella tularensis is an extremely infectious pathogen and a category A bioterrorism agent. It causes the highly contagious zoonosis, Tularemia. Currently, FDA approved vaccines against tularemia are unavailable. F. tularensis outer membrane protein A (FopA) is a well-studied virulence determinant and protective antigen against tularemia. It is a major outer membrane protein (Omp) of F. tularensis. However, FopA-based therapeutic intervention is hindered due to lack of complete structural information for membrane localized mature FopA. In our study, we established recombinant expression, monodisperse purification, crystallization and X-ray diffraction (~6.5 Å) of membrane localized mature FopA. Further, we performed bioinformatics and biophysical experiments to unveil its structural organization in the outer membrane. FopA consists of 393 amino acids and has less than 40% sequence identity to known bacterial Omps. Using comprehensive sequence alignments and structure predictions together with existing partial structural information, we propose a two-domain organization for FopA. Circular dichroism spectroscopy and heat modifiability assay confirmed FopA has a β-barrel domain consistent with alphafold2’s prediction of an eight stranded β-barrel at the N-terminus. Small angle X-ray scattering (SAXS) and native-polyacrylamide gel electrophoresis revealed FopA purified in detergent micelles is predominantly dimeric. Molecular density derived from SAXS at 31 Å shows putative dimeric N-terminal β-barrels surrounded by detergent corona and connected to C-terminal domains via flexible linker. Disorder analysis predicts N- and C-terminal domains are interspersed by a long intrinsically disordered region and alphafold2 predicts this region to be largely unstructured. Taken together, we propose a dimeric, two-domain organization of FopA in the outer membrane: the N-terminal β-barrel is membrane embedded, provides dimerization interface and tethers to membrane extrinsic C-terminal domain via long flexible linker. Structure determination of membrane localized mature FopA is essential to understand its role in pathogenesis and develop anti-tularemia therapeutics. Our results pave the way towards it.
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spelling pubmed-93427832022-08-02 Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis Nagaratnam, Nirupa Martin-Garcia, Jose M. Yang, Jay-How Goode, Matthew R. Ketawala, Gihan Craciunescu, Felicia M. Zook, James D. Sonowal, Manashi Williams, Dewight Grant, Thomas D. Fromme, Raimund Hansen, Debra T. Fromme, Petra PLoS One Research Article Francisella tularensis is an extremely infectious pathogen and a category A bioterrorism agent. It causes the highly contagious zoonosis, Tularemia. Currently, FDA approved vaccines against tularemia are unavailable. F. tularensis outer membrane protein A (FopA) is a well-studied virulence determinant and protective antigen against tularemia. It is a major outer membrane protein (Omp) of F. tularensis. However, FopA-based therapeutic intervention is hindered due to lack of complete structural information for membrane localized mature FopA. In our study, we established recombinant expression, monodisperse purification, crystallization and X-ray diffraction (~6.5 Å) of membrane localized mature FopA. Further, we performed bioinformatics and biophysical experiments to unveil its structural organization in the outer membrane. FopA consists of 393 amino acids and has less than 40% sequence identity to known bacterial Omps. Using comprehensive sequence alignments and structure predictions together with existing partial structural information, we propose a two-domain organization for FopA. Circular dichroism spectroscopy and heat modifiability assay confirmed FopA has a β-barrel domain consistent with alphafold2’s prediction of an eight stranded β-barrel at the N-terminus. Small angle X-ray scattering (SAXS) and native-polyacrylamide gel electrophoresis revealed FopA purified in detergent micelles is predominantly dimeric. Molecular density derived from SAXS at 31 Å shows putative dimeric N-terminal β-barrels surrounded by detergent corona and connected to C-terminal domains via flexible linker. Disorder analysis predicts N- and C-terminal domains are interspersed by a long intrinsically disordered region and alphafold2 predicts this region to be largely unstructured. Taken together, we propose a dimeric, two-domain organization of FopA in the outer membrane: the N-terminal β-barrel is membrane embedded, provides dimerization interface and tethers to membrane extrinsic C-terminal domain via long flexible linker. Structure determination of membrane localized mature FopA is essential to understand its role in pathogenesis and develop anti-tularemia therapeutics. Our results pave the way towards it. Public Library of Science 2022-08-01 /pmc/articles/PMC9342783/ /pubmed/35913965 http://dx.doi.org/10.1371/journal.pone.0267370 Text en © 2022 Nagaratnam et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Nagaratnam, Nirupa
Martin-Garcia, Jose M.
Yang, Jay-How
Goode, Matthew R.
Ketawala, Gihan
Craciunescu, Felicia M.
Zook, James D.
Sonowal, Manashi
Williams, Dewight
Grant, Thomas D.
Fromme, Raimund
Hansen, Debra T.
Fromme, Petra
Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis
title Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis
title_full Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis
title_fullStr Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis
title_full_unstemmed Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis
title_short Structural and biophysical properties of FopA, a major outer membrane protein of Francisella tularensis
title_sort structural and biophysical properties of fopa, a major outer membrane protein of francisella tularensis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9342783/
https://www.ncbi.nlm.nih.gov/pubmed/35913965
http://dx.doi.org/10.1371/journal.pone.0267370
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