Integrin-Using Rotaviruses Bind α2β1 Integrin α2 I Domain via VP4 DGE Sequence and Recognize αXβ2 and αVβ3 by Using VP7 during Cell Entry

Graham, Kerr; Halász, Péter; Tan, Yan; Hewish, Marilyn J.; Takada, Yoshikazu; Mackow, Erich R.; Robinson, Martyn K.; Coulson, Barbara S.

doi:10.1128/jvi.77.18.9969-9978.2003

Cited by 141 publications

(204 citation statements)

References 54 publications

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“…The peptide sequence arginine-glycine-aspartic acid (RGD) is the laminin-binding domain to the ␣ 2␤1-integrin (28). The peptide sequence glycine-proline-arginine (GPR) is the fibrinogen-binding domain to the ␣ v␤3-integrin (13). The peptide sequence GHRP served as a negative control.…”

Section: Viral Assaysmentioning

confidence: 99%

“…Consistent with the in vivo findings, RRV was better able to replicate in cholangiocytes than hepatocytes. Because the ability of rotavirus to infect cells appears to be regulated by cell-surface expression of the integrins ␣ 2 ␤ 1 , ␣ 4 ␤ 1 , ␣ v ␤ 3 , and ␣ x ␤ 2 , which serve as viral receptors (8,13,14,16,21), the cholangiocyte was surveyed for integrin expression and found to uniquely express the ␣ 2 ␤ 1 -integrin when compared with hepatocytes. Based on this information, we hypothesized that expression of the ␣ 2 ␤ 1 -integrin serves as a determinant governing cholangiocyte susceptibility to RRV infection contributing to the mechanism by which rotavirus initiates the experimental model of biliary atresia.…”

mentioning

confidence: 99%

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Cholangiocyte expression of α₂β₁-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Jafri¹,

Donnelly²,

Allen³

et al. 2008

American Journal of Physiology-Gastrointestinal and Liver Physi

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lation of BALB/c mice with rhesus rotavirus (RRV) in the newborn period results in biliary epithelial cell (cholangiocyte) infection and the murine model of biliary atresia. Rotavirus infection of a cell requires attachment, which is governed in part by cell-surface expression of integrins such as ␣2␤1. We hypothesized that cholangiocytes were susceptible to RRV infection because they express ␣2␤1. RRV attachment and replication was measured in cell lines derived from cholangiocytes and hepatocytes. Flow cytometry was performed on these cell lines to determine whether ␣2␤1 was present. Cholangiocytes were blocked with natural ligands, a monoclonal antibody, or small interfering RNA against the ␣2-subunit and were infected with RRV. The extrahepatic biliary tract of newborn mice was screened for the expression of the ␣2␤1-integrin. Newborn mice were pretreated with a monoclonal antibody against the ␣2-subunit and were inoculated with RRV. RRV attached and replicated significantly better in cholangiocytes than in hepatocytes. Cholangiocytes, but not hepatocytes, expressed ␣2␤1 in vitro and in vivo. Blocking assays led to a significant reduction in attachment and yield of virus in RRV-infected cholangiocytes. Pretreatment of newborn pups with an anti-␣2 monoclonal antibody reduced the ability of RRV to cause biliary atresia in mice. Cell-surface expression of the ␣2␤1-integrin plays a role in the mechanism that confers cholangiocyte susceptibility to RRV infection. rhesus rotavirus; bile ducts; cholangiopathy BILIARY ATRESIA (BA) is a unique disease of infancy in which affected children develop fibroinflammatory obliteration of the biliary tract. It is the most common indication for pediatric liver transplantation (24). Because pathogenic viruses have been found in the livers of children afflicted with biliary atresia (10,12,18,26,29), a proposed etiology for biliary atresia is perinatal infection by a virus triggering inflammatory destruction of the biliary epithelium (3,23,32). A murine model of biliary atresia (30) supports a viral pathogenesis where newborn mice infected with rhesus rotavirus (RRV) develop inflammation within the portal tract (31) and extrahepatic bile duct obstruction (9, 27).Recently, it has been shown that in the murine model of biliary atresia, RRV targeted the biliary epithelial cell (cholangiocyte) for infection (1, 31). To determine the basis for cholangiocyte susceptibility to RRV, an in vitro model of RRV infection of the two dominant cell types found within the liver (cholangiocytes and hepatocytes) was established. Consistent with the in vivo findings, RRV was better able to replicate in cholangiocytes than hepatocytes. Because the ability of rotavirus to infect cells appears to be regulated by cell-surface expression of the integrins ␣ 2 ␤ 1 , ␣ 4 ␤ 1 , ␣ v ␤ 3 , and ␣ x ␤ 2 , which serve as viral receptors (8,13,14,16,21), the cholangiocyte was surveyed for integrin expression and found to uniquely express the ␣ 2 ␤ 1 -integrin when compared with hepatocytes. Based on this informat...

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Section: Viral Assaysmentioning

confidence: 99%

mentioning

confidence: 99%

Cholangiocyte expression of α₂β₁-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Jafri¹,

Donnelly²,

Allen³

et al. 2008

American Journal of Physiology-Gastrointestinal and Liver Physi

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“…Similarly, the uptake of adenovirus type 3 (Ad3) was recently shown to be dependent on the αV integrin and on Rac1-and Pak-1-dependent actin remodelling (Amstutz et al, 2008). Finally, α2β1, αXβ2, α4β1 and α4β7 integrins promote the entry of rotaviruses (Coulson et al, 1997;Graham et al, 2005;Graham et al, 2003;Graham et al, 2006;Guerrero et al, 2000;Hewish et al, 2000), although it remains to be seen whether this follows a phagocyticlike process.Overall, several viral and bacterial pathogens use integrin signalling to enter host cells in an actin-dependent process. Deciphering the molecular pathways that are used for local, transient, integrin-triggered actin and membrane remodelling should aid in the design of drugs that will help fight infection in vitro and in vivo.…”

mentioning

confidence: 99%

Integrin-dependent phagocytosis – spreading from microadhesion to new concepts

Dupuy

Caron

2008

Journal of Cell Science

215

184

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By linking actin dynamics to extracellular components, integrins are involved in a wide range of cellular processes that are associated with or require cytoskeletal remodelling and cellshape changes. One such function is integrin-dependent phagocytosis, a process that several integrins are capable of mediating and that allows the binding and clearance of particles. Integrin-dependent phagocytosis is involved in a wide range of physiological processes, from the clearance of microorganisms and apoptotic-cell removal to extracellular-matrix remodelling. Integrin signalling is also exploited by microbial pathogens for entry into host cells. Far from being a particular property of specific integrins and specialised cells, integrin-dependent uptake is emerging as a general, intrinsic ability of most integrins that is associated with their capacity to signal to the actin cytoskeleton. Integrin-mediated phagocytosis can therefore be used as a robust model in which to study integrin regulation and signalling. Journal of Cell Science 1774 distinct receptors can be devoted to particle recognition ('tethering' receptors) and stimulation of particle uptake ('tickling' receptors) (Zullig and Hengartner, 2004). Interestingly, zipper-like phagocytosis can also take place in non-professional phagocytes, either naturally or following transfection of phagocytic receptors (Caron and Hall, 1998;Underhill and Ozinsky, 2002).Similar to cell adhesion and migration, phagocytosis crucially depends on remodelling of the actin cytoskeleton and on membrane dynamics (DeMali and Burridge, 2003;Niedergang and Chavrier, 2004). Moreover, the signalling pathways that underlie these processes have several regulatory proteins in common, including Rho-family proteins Ridley et al., 2003). Interestingly, distinct Rho GTPases regulate actin polymerisation during phagocytosis and actually define several modes of phagocytosis that are phenotypically different. Indeed, during FcγR-dependent (also referred as type I) uptake, activation of Rac1 and Cdc42 is thought to drive the formation of local pseudopods and membrane ruffles that engulf the particles. By contrast, actin polymerisation during integrin-αMβ2-dependent (referred as type II) phagocytosis is regulated by RhoA activity, and particles that are bound to αMβ2 sink into cells without generating major protrusions (see below and Fig. 2) (Allen and Aderem, 1996; Caron and Hall, 1998).On the basis of the criteria defined above for phagocytosis (particle size, zipper-like receptor tickling, and actin-dependent and Rho-GTPase-dependent uptake), we review here the role of integrins in phagocytosis, both in professional phagocytes and also in cells that are not classically considered phagocytic. We highlight the similarities between the signalling basis of integrin function during adhesion and phagocytic uptake. Not only is phagocytosis the predominant function of certain integrins, it should be seen as an intrinsic ability of most integrins. By extension, integrin-mediated phagocytosis can be proposed a...

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“…The RV3-BB vaccine is derived from a neonatal rotavirus strain which binds to specific receptors in the newborn gut and is integrin independent and, may inherently offer protection from maternal antibodies. 34 In this study, high levels of IgA in colostrum or breast milk did not appear to inhibit the serum IgA response or stool excretion following 3 doses of RV3-BB rotavirus vaccine in either a neonatal schedule with the first dose at age 0-5 d or an infant schedule with the first dose at 8 weeks of age. These findings are consistent with studies from North India 25 and South Africa 26 which found little difference in anti-rotavirus IgA seroconversion irrespective of whether breastfeeding was withheld for either 30 minutes or one hour before and after RV1 vaccine administration.…”

Section: Discussionmentioning

confidence: 92%

“…However, a potential advantage of a vaccine based on a human neonatal rotavirus strain delivered at birth is the proposed intrinsic structural characteristics that enable it to avoid neutralisation by maternal and breast milk antibodies. 34 Data from the placebo group provided a negative control for the rate of natural rotavirus infection in this study population. Interestingly one of the participants in the placebo group was excreting RV3-BB rotavirus vaccine in the stool at both 20 weeks and 28 weeks, which suggested presence of this strain in the community.…”

Section: Discussionmentioning

confidence: 99%

Rotavirus specific maternal antibodies and immune response to RV3-BB neonatal rotavirus vaccine in New Zealand

Chen

Kirkwood

Bines

et al. 2017

Human Vaccines & Immunotherapeutics

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Background: Maternal antibodies, acquired passively via placenta and/or breast milk, may contribute to the reduced efficacy of oral rotavirus vaccines observed in children in developing countries. This study aimed to investigate the effect of rotavirus specific maternal antibodies on the serum IgA response or stool excretion of vaccine virus after any dose of an oral rotavirus vaccine, RV3-BB, in parallel to a Phase IIa clinical trial conducted at Dunedin Hospital, New Zealand. At the time of the study rotavirus vaccines had not been introduced in New Zealand and the burden of rotavirus disease was evident.Methods: Rotavirus specific IgG and serum neutralizing antibody (SNA) levels in cord blood and IgA levels in colostrum and breast milk samples collected »4 weeks, »20 weeks and »28 weeks after birth were measured. Infants were randomized to receive the first dose of vaccine at 0-5 d (neonatal schedule) or 8 weeks (infant schedule). Breast feeding was with-held for 30 minutes before and after vaccine administration. The relationship between rotavirus specific IgG and SNA levels in cord blood and IgA in colostrum and breast milk at the time of first active dose of RV3-BB vaccine and level of IgA response and stool excretion after 3 doses of vaccine was assessed using linear and logistic regression.Results: Forty infants received 3 doses of RV3-BB rotavirus vaccine and were included in the analysis of the neonatal and infant groups. Rotavirus specific IgA in colostrum (neonatal schedule group) and breast milk at 4 weeks (infant schedule group) was identified in 14/21 (67%) and 14/17 (82%) of infants respectively. There was little evidence of an association between IgA in colostrum or breast milk IgA at 4 weeks, or between cord IgG or SNA level, and IgA response or stool excretion after 3 doses of RV3-BB, or after one dose (neonatal schedule) (all p>0.05).Conclusions: The level of IgA in colostrum or breast milk and level of placental IgG and SNA did not impact on the serum IgA response or stool excretion following 3 doses of RV3-BB Rotavirus Vaccine administered using either a neonatal or infant schedule in New Zealand infants.

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Integrin-Using Rotaviruses Bind α2β1 Integrin α2 I Domain via VP4 DGE Sequence and Recognize αXβ2 and αVβ3 by Using VP7 during Cell Entry

Cited by 141 publications

References 54 publications

Cholangiocyte expression of α₂β₁-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Cholangiocyte expression of α₂β₁-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Integrin-dependent phagocytosis – spreading from microadhesion to new concepts

Rotavirus specific maternal antibodies and immune response to RV3-BB neonatal rotavirus vaccine in New Zealand

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Integrin-Using Rotaviruses Bind α2β1 Integrin α2 I Domain via VP4 DGE Sequence and Recognize αXβ2 and αVβ3 by Using VP7 during Cell Entry

Cited by 141 publications

References 54 publications

Cholangiocyte expression of α2β1-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Cholangiocyte expression of α2β1-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Integrin-dependent phagocytosis – spreading from microadhesion to new concepts

Rotavirus specific maternal antibodies and immune response to RV3-BB neonatal rotavirus vaccine in New Zealand

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Product

Resources

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Cholangiocyte expression of α₂β₁-integrin confers susceptibility to rotavirus-induced experimental biliary atresia

Cholangiocyte expression of α₂β₁-integrin confers susceptibility to rotavirus-induced experimental biliary atresia