A Novel Homozygous Mutation Affecting Integrin α6 in a Case of Junctional Epidermolysis Bullosa with Pyloric Atresia Detected In Utero by Ultrasound Examination

Gache, Yannick; Romero-Graillet, Christine; Spadafora, Anne; Lépinard, Catherine; Descamps, Philippe; Bardon, C. Blanchet; Ortonne, Jean Paul; Meneguzzi, Guerríno

doi:10.1046/j.1523-1747.1998.00373.x

Cited by 20 publications

(21 citation statements)

References 12 publications

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“…Because LN5 is the major ligand of the ␣6␤4 integrin receptor at the hemidesmosomes, we hypothesized that ␣6 integrin, a proposed HPV receptor (15), might be important for the infection of attached cells by virions preadsorbed to LN5. To test this hypothesis, we first utilized BOUA-SV cells, a keratinocyte-derived cell line which is homozygous null for ␣6 integrin (16). In independent experiments, all cell lines expressing ␣6 integrin were highly infectible by HPV-11 adsorbed to the LN5-rich ECM of HaCaT cells, whereas the BOUA-SV cells were only weakly infected by virions adsorbed to this LN5-rich substrate (Fig.…”

Section: Resultsmentioning

confidence: 99%

Keratinocyte-Secreted Laminin 5 Can Function as a Transient Receptor for Human Papillomaviruses by Binding Virions and Transferring Them to Adjacent Cells

Culp

Budgeon

Marinkovich

et al. 2006

J Virol

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147

118

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Human papillomaviruses (HPVs) replicate only in the terminally differentiating epithelium of the skin and mucosa. While infection of basal keratinocytes is considered a requirement for permissive infection, it remains unclear whether virions can specifically target basal cells for adsorption and uptake following epithelial wounding. We present evidence that HPV binds specifically to laminin 5 (LN5), a component of the extracellular matrix (ECM) secreted by migrating and basal keratinocytes. HPV type 11 capsids colocalized with LN5 in the ECM secreted by vaginal keratinocytes. Binding of both virions and virus-like particles to purified LN5 and to the LN5-rich ECM secreted by cultured keratinocytes was effectively blocked by pretreatment with anti-LN5 antibodies. HPV capsid binding to human cervical mucosa sections included the basement membrane which contains LN5. Cultured keratinocytes expressing ␣6 integrin, a transmembrane protein known to bind LN5, were readily infected by virions preadsorbed to LN5-containing substrates, whereas mutant keratinocytes lacking ␣6 integrin were relatively resistant to infection via this route. These findings suggest a model of natural HPV infection in which proliferating keratinocytes expressing ␣6 integrin at the site of epithelial wounding might be targeted by virions adsorbed transiently to LN5 secreted by migrating keratinocytes.Human papillomavirus (HPV) particles have been shown to adsorb to the plasma membranes of cultured cells via membrane-associated heparan sulfate proteoglycans (HSPGs) (18,20,33) or ␣6 integrin (CD49f) (15,26). Multiple HSPGs including CD44, syndecans and glypicans are expressed on the membranes of keratinocytes throughout the epidermis and mucosa (22,29). ␣6 integrin expression is generally restricted to basal keratinocytes where this transmembrane protein pairs with ␤4 integrin and contributes to the nucleation of hemidesmosomes connecting the keratin cytoskeleton to the basement membrane (BM) (reviewed in reference 28). Results from experiments utilizing several in vitro infection models suggest that the importance of a particular receptor in HPV adsorption/infection may differ between cell lines and viral genotypes (12,30,33).In addition to binding directly to membrane-associated glycoproteins, we recently found that HPV capsids are also capable of binding a component of the extracellular matrix (ECM) secreted by keratinocytes, but not by nonkeratinocyte cell lines (12). Here we show evidence that this secreted HPV adsorption receptor is laminin 5 (LN5), an epithelial laminin secreted by migrating keratinocytes as they invade wounded epithelium (reviewed in reference 27). In the context of the ECM secreted by cultured keratinocytes, HPV virions can use LN5 as an extracellular "transreceptor" by transiently binding LN5 and subsequently transferring to entry receptors on adjacent cells. In another viral system, human immunodeficiency virus (HIV) is hypothesized to transiently bind DC-SIGN (CD209) on immature dendritic cells within the epithelium an...

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Section: Resultsmentioning

confidence: 99%

Keratinocyte-Secreted Laminin 5 Can Function as a Transient Receptor for Human Papillomaviruses by Binding Virions and Transferring Them to Adjacent Cells

Culp

Budgeon

Marinkovich

et al. 2006

J Virol

Self Cite

147

118

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“…To further address this issue, we performed attachment assays using VLP of high-risk HPV16 and human epidermal keratinocytes as appropriate target cells. We took advantage of keratinocytes (BOUA-SV) isolated from a patient with a blistering skin disease that lacked ␣6 integrin expression due to a homozygous deletion (16). For comparison, human keratinocytes (KH-SV) isolated from healthy donor skin were used.…”

Section: Resultsmentioning

confidence: 99%

“…Keratinocytes deficient for ␣6 integrin expression (BOUA-SV) were derived from a patient with junctional epidermolysis bullosa carrying a homozygous mutation in the integrin ␣6 gene (16), and KH-SV keratinocytes were derived from a healthy donor. Both cell lines were immortalized by simian virus 40.…”

Section: Methodsmentioning

confidence: 99%

Different Heparan Sulfate Proteoglycans Serve asCellular Receptors for HumanPapillomaviruses

Shafti-Keramat

Handisurya

Kriehuber

et al. 2003

J Virol

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239

198

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Papillomaviruses replicate in stratified epithelia of skin and mucosa. Infection with certain human papillomavirus (HPV) types is the main cause of anogenital neoplasia, in particular cervical cancer. Early events of papillomavirus infectivity are poorly understood. While heparan sulfate proteoglycans (HSPGs) mediate initial binding to the cell surface, the class of proteins carrying heparan sulfates has not been defined. Here we examined two processes of papillomavirus infection, attachment of virus-like particles (VLP) to cells and infection with authentic HPV type 11 (HPV11) virions. Of the HSPGs, syndecan-1 is the major epithelial form and is strongly upregulated in wound edge keratinocytes. We employed K562 cells, which lack HSPGs except minor amounts of endogenous betaglycan, and stable clones that express cDNAs of syndecan-1, syndecan-4, or glypican-1. Binding of VLP correlated with levels of heparan sulfate on the cell surface. Parental K562 bound HPV16 VLP weakly, whereas all three K562 transfectants demonstrated enhanced binding, with the highest binding capacity observed for syndecan-1-transfected cells, which also expressed the most HSPG. For HPV11 infectivity assays, a high virion inoculum was required to infect K562 cells, whereas ectopic expression of syndecan-1 increased permissiveness eightfold and expression of syndecan-4 or glypican-1 fourfold. Infection of keratinocytes was eliminated by treatment with heparitinase, but not phospholipase C, further implicating the syndecan family of integral membrane proteins as receptor proteins. Human keratinocytes with a homozygous deletion of ␣6 integrin are permissive for HPV11 infection. These results indicate that several HSPGs can serve as HPV receptors and support a putative role for syndecan-1, rather than ␣6 integrin, as a primary receptor protein in natural HPV infection of keratinocytes.Papillomaviruses comprise a large group of species-and tissue-specific DNA tumor viruses found in higher vertebrates from chaffinches to humans and include more than 90 known human papillomavirus (HPV) genotypes. Papillomaviruses cause mainly benign epithelial papillomas or warts on skin and mucosa (condylomata acuminata). Several high-risk HPV types, most often HPV type 16 (HPV16), are the primary etiologic agents for anogenital malignancy, in particular cervical cancer, which is the second most common cause of cancerrelated deaths in women worldwide (41, 57). The papillomavirus virion consists of a nonenveloped capsid comprised of the L1 major and L2 minor structural proteins surrounding a minichromosome of ϳ8 kb of double-stranded closed circular and histone-associated DNA. Even in the absence of other viral proteins, the L1 protein self-assembles into empty capsids or virus-like particles (VLP) (24). Subunit vaccines based on VLP have been developed, and prophylactic immunizations have demonstrated safety and efficacy in preventing papillomavirus infection and associated neoplasia (18,23,25,28,44).Papillomaviruses do not complete their life cycle leading to pr...

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“…Two of the ␣6 integrin cases were lethal in the early postnatal period, and in one case an affected fetus with abnormalities in the skin and intestine was detected prenatally by ultrasound examination, and the pregnancy was terminated. Subsequent immunochemical analysis of the latter case revealed altered expression of ␣6␤4 integrin (22). Therefore, neither the ␣6 nor the ␤4 integrin databases provide definitive explanations for the clinical variability, i.e.…”

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confidence: 91%

“…Specifically, markedly reduced or absent staining for ␣6 and/or ␤4 integrin has been demonstrated in the skin of these patients, suggesting that the corresponding genes, ITGA6 and ITGB4, may harbor the mutations underlying this subset of EB (14 -16). Subsequently, a number of mutations in these two genes have been demonstrated, the majority of the mutations being found in the ␤4 integrin gene (10 -13, 17-20), whereas only three cases with mutations in the ␣6 integrin gene have been reported thus far (9,21,22). Two of the ␣6 integrin cases were lethal in the early postnatal period, and in one case an affected fetus with abnormalities in the skin and intestine was detected prenatally by ultrasound examination, and the pregnancy was terminated.…”

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confidence: 99%

Epidermolysis Bullosa with Congenital Pyloric Atresia: Novel Mutations in the β4 Integrin Gene (ITGB4) and Genotype/Phenotype Correlations

et al. 2001

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Epidermolysis bullosa with pyloric atresia (EB-PA: OMIM 226730), also known as Carmi syndrome, is a rare autosomal recessive genodermatosis that manifests with neonatal mucocutaneous fragility associated with congenital pyloric atresia. The disease is frequently lethal within the first year, but nonlethal cases have been reported. Mutations in the genes encoding subunit polypeptides of the ␣6␤4 integrin (ITGA6 and ITGB4) have been demonstrated in EB-PA patients. To extend the repertoire of mutations and to identify genotype-phenotype correlations, we examined seven new EB-PA families, four with lethal and three with nonlethal disease variants. DNA from patients was screened for mutations using heteroduplex analysis followed by nucleotide sequencing of PCR products spanning all ␤4 integrincoding sequences. Mutation analysis disclosed 12 distinct mutations, 11 of them novel. Four mutations predicted a premature termination codon as a result of nonsense mutations or small out-of-frame insertions or deletions, whereas seven were missense mutations. This brings the total number of distinct ITGB4 mutations to 33. The mutation database indicates that premature termination codons are associated predominantly with the lethal EB-PA variants, whereas missense mutations are more prevalent in nonlethal forms. However, the consequences of the missense mutations are position dependent, and substitutions of highly conserved amino acids may have lethal consequences. In general, indirect immunofluorescence studies of affected skin revealed negative staining for ␤4 integrin in lethal cases and positive, but attenuated, staining in nonlethal cases and correlated with clinical phenotype. The data on specific mutations in EB-PA patients allows prenatal testing and preimplantation genetic diagnosis in families at risk. Abbreviations EB-PA, epidermolysis bullosa with pyloric atresia BMZ, basement membrane zone CSGE, conformation-sensitive gel electrophoresis PTC, premature termination codon TEM, transmission electron microscopy ITGB4, ␤4 integrin gene Epidermolysis bullosa (EB) is a group of genodermatoses manifesting with blistering and erosions of the skin and mucous membranes as a result of mechanical trauma (1, 2). The clinical severity of EB is highly variable. In the mildest cases, blistering occurs primarily on the hands and feet with relatively little morbidity, whereas, in the most severe cases, the disease can be lethal perinatally or during the early postnatal period. Traditionally, EB has been divided into three broad categories based on clinical findings and ultrastructural demonstrations of

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A Novel Homozygous Mutation Affecting Integrin α6 in a Case of Junctional Epidermolysis Bullosa with Pyloric Atresia Detected In Utero by Ultrasound Examination

Cited by 20 publications

References 12 publications

Keratinocyte-Secreted Laminin 5 Can Function as a Transient Receptor for Human Papillomaviruses by Binding Virions and Transferring Them to Adjacent Cells

Keratinocyte-Secreted Laminin 5 Can Function as a Transient Receptor for Human Papillomaviruses by Binding Virions and Transferring Them to Adjacent Cells

Different Heparan Sulfate Proteoglycans Serve asCellular Receptors for HumanPapillomaviruses

Epidermolysis Bullosa with Congenital Pyloric Atresia: Novel Mutations in the β4 Integrin Gene (ITGB4) and Genotype/Phenotype Correlations

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