Outer Membrane Protein-Specific Monoclonal Antibodies Protect SCID Mice from Fatal Infection by the Obligate Intracellular Bacterial Pathogen <i>Ehrlichia chaffeensis</i>

Li, Julia Shu-yi; Yager, Eric J.; Reilly, Melissa; Freeman, C W J; Reddy, Ganta Roman; Reilly, Andrew; Chu, Frederick K.; Winslow, Gary M.

doi:10.4049/jimmunol.166.3.1855

Cited by 93 publications

(34 citation statements)

References 41 publications

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“…Previous studies in our laboratory and elsewhere have demonstrated that P28-19 is the most efficient and protective P28 paralog which provides protection against Ehrlichia [18], [19].…”

Section: Resultsmentioning

confidence: 68%

“…Studies from our laboratory and others have previously demonstrated the importance of antibodies in protection against Ehrlichia . Passive transfer of polyclonal immune sera or mAbs confers protection in SCID mice against E. muris and E. chaffeensis , respectively [18], [32]. Prior studies in mouse models have demonstrated that vaccination with P28 leads to immunity and clearance of Ehrlichia infection.…”

Section: Discussionmentioning

confidence: 99%

“…A previous study showed that mice immunized with the recombinant E. chaffeensis P28-19 (rP28) enhanced the spontaneous clearance of the infection in BALB/c mice [35]. A study by Li et al [18] indicated that a mAb directed against the E. chaffeensis P28-19 (OMP-1g) reduced the bacterial burden in SCID mice. Though they reported that the region spanning amino acids 68–90 of P28-19 of E. chaffeensis contains a B cell eptiope, subsequent studies by the group [19] utilized the 77–92 amino acid sequence to generate peptides.…”

Section: Discussionmentioning

confidence: 99%

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Structure-Based Vaccines Provide Protection in a Mouse Model of Ehrlichiosis

Thomas

Thirumalapura²,

Crocquet‐Valdes³

et al. 2011

PLoS ONE

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BackgroundRecent advances in bioinformatics have made it possible to predict the B cell and T cell epitopes of antigenic proteins. This has led to design of peptide based vaccines that are more specific, safe, and easy to produce. The obligately intracellular gram negative bacteria Ehrlichia cause ehrlichioses in humans and animals. As yet there are no vaccines to protect against Ehrlichia infection.Methodology/Principal FindingsWe applied the principle of structural vaccinology to design peptides to the epitopes of Ehrlichia muris outer membrane P28-19 (OMP-1/P28) and Ehrlichia Heat shock protein 60 (Hsp60/GroEL) antigenic proteins. Both P28-19 and Ehrlichia Hsp60 peptides reacted with polyclonal antibodies against E. canis and E. chaffeensis and could be used as a diagnostic tool for ehrlichiosis. In addition, we demonstrated that mice vaccinated with Ehrlichia P28-19 and Hsp60 peptides and later challenged with E. muris were protected against the pathogen.Conclusions/SignificanceOur results demonstrate the power of structural vaccines and could be a new strategy in the development of vaccines to provide protection against pathogenic microorganisms.

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“…Previous studies in our laboratory and elsewhere have demonstrated that P28-19 is the most efficient and protective P28 paralog which provides protection against Ehrlichia [18], [19].…”

Section: Resultsmentioning

confidence: 68%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 1 more Smart Citation

Structure-Based Vaccines Provide Protection in a Mouse Model of Ehrlichiosis

Thomas

Thirumalapura²,

Crocquet‐Valdes³

et al. 2011

PLoS ONE

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“…Interestingly, in an effort to find the protective mechanism mediated by a C. burnettii phase I vaccine (PI-V) strain, Zhang et al demonstrated that a switched IgG response to PI-V lipopolysaccharide (LPS) provided significant protection to the host to an extent comparable to PI-V vaccination against C. burnetii infection [68]. Similar observations have also been made in obligate intracellular Ehrlichia chaffeensis infections, where antibody recognizing the major outer membrane protein (OMP)-1g of E. chaffeensis protects SCID mice from ehrlichiosis, a vector-borne disease [69]. …”

Section: B Cells and Intracellular Infections: Lesson Learned Frommentioning

confidence: 96%

A re-evaluation of the role of B cells in protective immunity to Chlamydia infection

McSorley

2015

Immunology Letters

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Chlamydia trachomatis is the etiological agent of the most commonly reported bacterial sexual transmitted infection (STI) in North America and Europe. The control of Chlamydia infection is hindered by the asymptomatic nature of initial infection but the consequence of untreated infection seriously threatens the reproductive health of young women. Unfortunately, there is no licensed vaccine for Chlamydia vaccine, in part due to our incomplete understanding of the immune response to Chlamydia urogenital infection. It has been well established that T cell-mediated immunity plays a dominant role in protective immunity against Chlamydia and thus the importance of B cells is somewhat underappreciated. Here, we summarize recent progress on understanding the role of B cells during Chlamydia genital tract infections and discuss how B cells and humoral immunity make an effective contribution to host defense against important intracellular pathogens, including Chlamydia.

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“…Although E muris was originally described as a mouse pathogen, a closely related, if not identical pathogen, has been shown to infect humans (known as the E. muris -like agent, or EMLA; [4]). As an obligate intracellular pathogen, E. muris cannot replicate outside of host cells, although we have reported that the bacteria can be found extracellularly [5], a property that is presumably necessary to facilitate blood-borne transmission, and which at the same time may predispose the bacteria to clearance by antibodies [6]. E. muris infection, which is not fatal in immunocompetent mice and humans, nonetheless causes a number of clinical manifestations, including anemia, thrombocytopenia, splenomegaly, as well as hematological alterations, including myelopoiesis and perturbation of the hematopoietic stem cell niche [7].…”

Section: Discovery Of Cd11c+ B Cellsmentioning

confidence: 99%

CD11c+ T-bet+ memory B cells: Immune maintenance during chronic infection and inflammation?

Winslow

Papillion

Kenderes

et al. 2017

Cellular Immunology

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CD11c+ T-bet+ B cells have now been detected and characterized in different experimental and clinical settings, in both mice and humans. Whether such cells are monolithic, or define subsets of B cells with different functions is not yet known. Our studies have identified CD11c+ IgM+ CD19hi splenic IgM memory B cells that appear at approximately three weeks post-ehrlichial infection, and persist indefinitely, during low-level chronic ehrlichial infection. Although the CD11c+T-bet+ B cells we have described are distinct, they appear to share many features with similar cells detected under diverse conditions, including viral infections, aging, and autoimmunity. We propose that CD11c+ T-bet+ B cells as a group share characteristics of memory B cells that are maintained under conditions of inflammation and/or low-level chronic antigen stimulation. In some cases, these cells may be advantageous, by providing immunity to re-infection, but in others may be deleterious, by contributing to aged-associated autoimmune responses.

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Outer Membrane Protein-Specific Monoclonal Antibodies Protect SCID Mice from Fatal Infection by the Obligate Intracellular Bacterial Pathogen Ehrlichia chaffeensis

Cited by 93 publications

References 41 publications

Structure-Based Vaccines Provide Protection in a Mouse Model of Ehrlichiosis

Structure-Based Vaccines Provide Protection in a Mouse Model of Ehrlichiosis

A re-evaluation of the role of B cells in protective immunity to Chlamydia infection

CD11c+ T-bet+ memory B cells: Immune maintenance during chronic infection and inflammation?

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