Interaction of α
 V
 β
 3
 and α
 V
 β
 6
 Integrins with Human Parechovirus 1

Seitsonen, Jani; Susi, Petri; Heikkilä, Outi; Sinkovits, Robert S.; Laurinmäki, Pasi; Hyypiä, Timo; Butcher, Sarah J.

doi:10.1128/jvi.02176-09

Cited by 50 publications

(74 citation statements)

References 91 publications

(87 reference statements)

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“…Such a role for the RGD motif for HPeV1 has been shown through blocking experiments with RGD-containing peptides, antibodies (Abs), and mutations of the sequence, where deletion of the RGD motif is lethal (12)(13)(14)(15)(16). Studies of the HPeV1 virion in complex with both ␣ V ␤ 3 and ␣ V ␤ 6 integrins confirmed that they have overlapping binding sites on the predicted site of the RGD motif on the capsid surface (6). There are several potential neutralizing mechanisms for antibodies that bind specifically to viral capsid surfaces, e.g., antibodies may neutralize by obstructing a receptor-binding site, cause viral aggregation as a result of interlinking particles, or bind bivalently, preventing uncoating (17)(18)(19).…”

mentioning

confidence: 91%

“…HPeV infections mainly cause mild gastrointestinal symptoms, although HPeV are also associated with more severe central nervous system symptoms, such as meningitis and neonatal sepsis (2)(3)(4)(5). The HPeV genome is about 7,300 bases in length, enclosed in an icosahedrally symmetric capsid of 60 copies of each of the three capsid proteins VP0, VP3, and VP1 (1,6). HPeV lack the maturation cleavage of the capsid protein VP0 into VP4 and VP2, which is present in most picornaviruses (7).…”

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confidence: 99%

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Structural Basis of Human Parechovirus Neutralization by Human Monoclonal Antibodies

Shakeel

Westerhuis

Ora

et al. 2015

J Virol

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Since it was first recognized in 2004 that human parechoviruses (HPeV) are a significant cause of central nervous system and neonatal sepsis, their clinical importance, primarily in children, has started to emerge. Intravenous immunoglobulin treatment is the only treatment available in such life-threatening cases and has given moderate success. Direct inhibition of parechovirus infection using monoclonal antibodies is a potential treatment. We have developed two neutralizing monoclonal antibodies against HPeV1 and HPeV2, namely, AM18 and AM28, which also cross-neutralize other viruses. Here, we present the mapping of their epitopes using peptide scanning, surface plasmon resonance, fluorescence-based thermal shift assays, electron cryomicroscopy, and image reconstruction. We determined by peptide scanning and surface plasmon resonance that AM18 recognizes a linear epitope motif including the arginine-glycine-aspartic acid on the C terminus of capsid protein VP1. This epitope is normally used by the virus to attach to host cell surface integrins during entry and is found in 3 other viruses that AM18 neutralizes. Therefore, AM18 is likely to cause virus neutralization by aggregation and by blocking integrin binding to the capsid. Further, we show by electron cryomicroscopy, three-dimensional reconstruction, and pseudoatomic model fitting that ordered RNA interacts with HPeV1 VP1 and VP3. AM28 recognizes quaternary epitopes on the capsid composed of VP0 and VP3 loops from neighboring pentamers, thereby increasing the RNA accessibility temperature for the virus-AM28 complex compared to the virus alone. Thus, inhibition of RNA uncoating probably contributes to neutralization by AM28. IMPORTANCEHuman parechoviruses can cause mild infections to severe diseases in young children, such as neonatal sepsis, encephalitis, and cardiomyopathy. Intravenous immunoglobulin treatment is the only treatment available in such life-threatening cases. In order to develop more targeted treatment, we have searched for human monoclonal antibodies that would neutralize human parechoviruses 1 and 2, associated with mild infections such as gastroenteritis and severe infections of the central nervous system, and thus allow safe treatment. In the current study, we show how two such promising antibodies interact with the virus, modeling the atomic interactions between the virus and the antibody to propose how neutralization occurs. Both antibodies can cause aggregation; in addition, one antibody interferes with the virus recognizing its target cell, while the other, recognizing only the whole virus, inhibits the genome uncoating and replication in the cell. Human parechoviruses (HPeV) are single-stranded, positivesense RNA viruses in the Parechovirus genus within the Picornaviridae family (1). HPeV infections mainly cause mild gastrointestinal symptoms, although HPeV are also associated with more severe central nervous system symptoms, such as meningitis and neonatal sepsis (2-5). The HPeV genome is about 7,300 bases in length, enclose...

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confidence: 91%

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confidence: 99%

Structural Basis of Human Parechovirus Neutralization by Human Monoclonal Antibodies

Shakeel

Westerhuis

Ora

et al. 2015

J Virol

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“…However, the cleavage of VP0 into VP2 and VP4 does not appear in parechoviruses and the manner of how maturation and virus release is achieved for HPeVs remains largely unknown (Stanway et al, 1994). Nonetheless, the external appearance of HPeV particles has proved consistent with the external appearance of other picornaviruses, most closely resembling Foot and Mouth Disease Virus (FMDV) in the Aphthovirus genus as has recently been shown by cryoelectron microscopy and image reconstruction (Seitsonen et al, 2010).…”

Section: Wwwintechopencommentioning

confidence: 85%

“…The hydrophobic pocket is relatively well preserved among EVs and HRVs, resulting in a broad-spectrum anti-enteroviral and -rhinoviral activity of pleconaril. However, the capsid of HPeVs is different Seitsonen et al, 2010), indicating that the hydrophobic pocket differs from that of EVs. Indeed data from our laboratory show that HPeV1 and HPeV3 are resistant against pleconaril in vitro (Wildenbeest et al, 2010).…”

Section: Treatmentmentioning

confidence: 99%

Human Parechoviruses, New Players in the Pathogenesis of Viral Meningitis

Benschop

Wildenbeest²,

Wolthers³

2012

Meningitis

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“…The digitized micrographs were processed, and viral particles were picked as previously described (49). The initial models for the viruses at approximately 30-Å resolution were generated using a random model computation method with a subset of 150 far from focus particles (50).…”

Section: Methodsmentioning

confidence: 99%

Structure of the archaeal head-tailed virus HSTV-1 completes the HK97 fold story

Pietilä

Laurinmäki

Russell

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

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It has been proposed that viruses can be divided into a small number of structure-based viral lineages. One of these lineages is exemplified by bacterial virus Hong Kong 97 (HK97), which represents the head-tailed dsDNA bacteriophages. Seemingly similar viruses also infect archaea. Here we demonstrate using genomic analysis, electron cryomicroscopy, and image reconstruction that the major coat protein fold of newly isolated archaeal Haloarcula sinaiiensis tailed virus 1 has the canonical coat protein fold of HK97. Although it has been anticipated previously, this is physical evidence that bacterial and archaeal head-tailed viruses share a common architectural principle. The HK97-like fold has previously been recognized also in herpesviruses, and this study expands the HK97-like lineage to viruses from all three domains of life. This is only the second established lineage to include archaeal, bacterial, and eukaryotic viruses. Thus, our findings support the hypothesis that the last common universal ancestor of cellular organisms was infected by a number of different viruses.

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Interaction of α _V β ₃ and α _V β ₆ Integrins with Human Parechovirus 1

Cited by 50 publications

References 91 publications

Structural Basis of Human Parechovirus Neutralization by Human Monoclonal Antibodies

Structural Basis of Human Parechovirus Neutralization by Human Monoclonal Antibodies

Human Parechoviruses, New Players in the Pathogenesis of Viral Meningitis

Structure of the archaeal head-tailed virus HSTV-1 completes the HK97 fold story

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Interaction of α V β 3 and α V β 6 Integrins with Human Parechovirus 1

Cited by 50 publications

References 91 publications

Structural Basis of Human Parechovirus Neutralization by Human Monoclonal Antibodies

Structural Basis of Human Parechovirus Neutralization by Human Monoclonal Antibodies

Human Parechoviruses, New Players in the Pathogenesis of Viral Meningitis

Structure of the archaeal head-tailed virus HSTV-1 completes the HK97 fold story

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Interaction of α _V β ₃ and α _V β ₆ Integrins with Human Parechovirus 1