Rotavirus Anti-VP6 Secretory Immunoglobulin A Contributes to Protection via Intracellular Neutralization but Not via Immune Exclusion

Corthésy, Blaise; Benureau, Yann; Perrier, Clémentine; Fourgeux, Cynthia; Parez, N.; Greenberg, Harry B.; Schwartz-Cornil, Isabelle

doi:10.1128/jvi.00927-06

Cited by 112 publications

(98 citation statements)

References 51 publications

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“…IgA, but not IgG, monoclonal antibodies administered by a hybridoma "backpack" tumor are sufficient to protect naive newborn mice from primary infection (56), while human RV-specific IgA as well as IgG antibodies are able to neutralize RV in cell culture (25). Additionally, RV-specific IgA but not IgG can confer resistance to infection by neutralizing virus intracellularly following transcytosis (40,57,58), and RV-specific serum IgA levels predict protection against severe clinical disease (59).…”

Section: Figurementioning

confidence: 99%

Plasmacytoid dendritic cells promote rotavirus-induced human and murine B cell responses

Deal

Lahl²,

Narváez³

et al. 2013

J. Clin. Invest.

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B cell-dependent immunity to rotavirus, an important intestinal pathogen, plays a significant role in viral clearance and protects against reinfection. Human in vitro and murine in vivo models of rotavirus infection were used to delineate the role of primary plasmacytoid DCs (pDCs) in initiating B cell responses. Human pDCs were necessary and sufficient for B cell activation induced by rotavirus. Type I IFN recognition by B cells was essential for rotavirus-mediated B cell activation in vitro and murine pDCs and IFN-α/β-mediated B cell activation after in vivo intestinal rotavirus infection. Furthermore, rotavirus-specific serum and mucosal antibody responses were defective in mice lacking functional pDCs at the time of infection. These data demonstrate that optimal B cell activation and virus-specific antibody secretion following mucosal infection were a direct result of pDC-derived type I IFN. Importantly, viral shedding significantly increased in pDC-deficient mice, suggesting that pDC-dependent antibody production influences viral clearance. Thus, mucosal pDCs critically influence the course of rotavirus infection through rotavirus recognition and subsequent IFN production and display powerful adjuvant properties to initiate and enhance humoral immunity.

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Section: Figurementioning

confidence: 99%

Plasmacytoid dendritic cells promote rotavirus-induced human and murine B cell responses

Deal

Lahl²,

Narváez³

et al. 2013

J. Clin. Invest.

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“…and triple-layered particles, conferring protection by intracellular neutralization following transcytosis in mice and also in vitro using polarized Caco-2 cells (46)(47)(48). The mechanism by which these antibodies interfere with RV replication is not yet understood, and it is postulated that they may interfere with early replication events by inducing conformational changes in the VP6 layer, or alternatively, the anti-VP6 antibodies may interfere with the secretory pathways during late replication, preventing virus assembly and release (47).…”

Section: Figurementioning

confidence: 99%

“…The mechanism by which these antibodies interfere with RV replication is not yet understood, and it is postulated that they may interfere with early replication events by inducing conformational changes in the VP6 layer, or alternatively, the anti-VP6 antibodies may interfere with the secretory pathways during late replication, preventing virus assembly and release (47). It is also known that not all anti-VP6 antibodies can neutralize RV replication intracellularly (49).…”

Section: Figurementioning

confidence: 99%

Rice-based oral antibody fragment prophylaxis and therapy against rotavirus infection

et al. 2013

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Rotavirus-induced diarrhea is a life-threatening disease in immunocompromised individuals and in children in developing countries. We have developed a system for prophylaxis and therapy against rotavirus disease using transgenic rice expressing the neutralizing variable domain of a rotavirus-specific llama heavy-chain antibody fragment (MucoRice-ARP1). MucoRice-ARP1 was produced at high levels in rice seeds using an overexpression system and RNAi technology to suppress the production of major rice endogenous storage proteins. Orally administered MucoRice-ARP1 markedly decreased the viral load in immunocompetent and immunodeficient mice. The antibody retained in vitro neutralizing activity after long-term storage (>1 yr) and boiling and conferred protection in mice even after heat treatment at 94°C for 30 minutes. High-yield, watersoluble, and purification-free MucoRice-ARP1 thus forms the basis for orally administered prophylaxis and therapy against rotavirus infections.

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“…Some anti-VP6 IgA mAbs, however, protect nonimmune mice from infection and clear chronic infection in SCID mice (2). The mechanism of the protection mediated by such Abs is still being investigated, but it is thought that they block the virus life cycle at the step of transcription, probably inside virus-infected cells (3). After the virus has entered the cell, the outer capsid is released, exposing the VP6-coated double-layer particle (DLP), which then is activated for transcription.…”

Section: R Otavirus (Rv)mentioning

confidence: 99%

“…After the virus has entered the cell, the outer capsid is released, exposing the VP6-coated double-layer particle (DLP), which then is activated for transcription. These anti-VP6 mAbs block viral transcription in vitro in a dose-dependent manner when introduced into a cell concurrently with DLPs or during transcytosis in the cell (3)(4)(5)(6). The specific role of such VP6 Abs in preventing or resolving human infection is still unclear.…”

Section: R Otavirus (Rv)mentioning

confidence: 99%

Functional Maturation of the Human Antibody Response to Rotavirus

Kallewaard

McKinney

et al. 2008

The Journal of Immunology

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Infant Abs induced by viruses exhibit poor functional activity compared with those of adults. The human B cell response to rotavirus is dominated by use of the VH1–46 gene segment in both adults and infants, but only adult sequences are highly mutated. We investigated in detail the kinetic, structural, and functional advantage conferred by individual naturally occurring somatic mutations in rotavirus-specific human Abs encoded by the immunodominant VH1–46 gene segment. Adult Abs achieved enhanced binding through naturally occurring somatic mutations in the H chain CDR2 region that conferred a markedly prolonged off-rate and a desirable increase in antiviral potency. Three-dimensional cryoelectron microscopy studies of Ag-Ab complexes revealed the mechanism of viral inhibition to be the binding of high-affinity Abs at the viral RNA release pore in the double-layer particle. These structure-function studies suggest a molecular basis for the poor quality of Abs made in infancy following virus infection or immunization.

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Rotavirus Anti-VP6 Secretory Immunoglobulin A Contributes to Protection via Intracellular Neutralization but Not via Immune Exclusion

Cited by 112 publications

References 51 publications

Plasmacytoid dendritic cells promote rotavirus-induced human and murine B cell responses

Plasmacytoid dendritic cells promote rotavirus-induced human and murine B cell responses

Rice-based oral antibody fragment prophylaxis and therapy against rotavirus infection

Functional Maturation of the Human Antibody Response to Rotavirus

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