Role of sialic acid-containing molecules in paramyxovirus entry into the host cell: A minireview

Villar, Enrique; Barroso, Isabel Muñoz

doi:10.1007/s10719-006-5433-0

Cited by 122 publications

(97 citation statements)

References 132 publications

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“…Peak 2 from the 4 different cells consisted of SPG, GD1a and LST-a. Because both GD1a and SPG are receptors for HVJ, 32 Peaks 2 were further purified by reversed phase HPLC. Peaks 2 from PC3, DU145, LNcap and PNT2 were separated into 2, 3, 1 and 2 major components, respectively (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…The receptors of HVJ are GD1a and SPG. 32 Both gangliosides bearing N-acetylneuraminic acid attached on terminal galactose residues by a2-3 linkages that are recognized by HN protein of HVJ. 32 These molecules are thought to be widely distributed among various cell lines.…”

Section: Discussionmentioning

confidence: 99%

“…32 Both gangliosides bearing N-acetylneuraminic acid attached on terminal galactose residues by a2-3 linkages that are recognized by HN protein of HVJ. 32 These molecules are thought to be widely distributed among various cell lines. 32 However, when the cell surface gangliosides within prostate epithelium was precisely examined, GD1a gangliosides were found to be the most prevalent gangliosides among prostate cancer cell lines, including PC3 and DU145, whereas GD1a gangliosides were barely detectable in both hormone-sensitive prostate cancer LNCap cells and normal prostate epithelium using thin-layer chromatography.…”

Section: Discussionmentioning

confidence: 99%

“…32 These molecules are thought to be widely distributed among various cell lines. 32 However, when the cell surface gangliosides within prostate epithelium was precisely examined, GD1a gangliosides were found to be the most prevalent gangliosides among prostate cancer cell lines, including PC3 and DU145, whereas GD1a gangliosides were barely detectable in both hormone-sensitive prostate cancer LNCap cells and normal prostate epithelium using thin-layer chromatography. 43,44 Furthermore, when we determined the quantity of gangliosides in prostate cancer cell lines using HPLC, we found that SPG, another receptor for HVJ, also increased in hormonerefractory prostate cancer cells as well as GD1a.…”

Section: Discussionmentioning

confidence: 99%

“…This is also a receptor for HVJ. 32 The terminal sialic acid of SPG is transferred by ST3Gal VI. 45 Human ST3Gal VI gene is expressed by alternative promoter utilization and one of the 2 promoters is specifically activated in PC3 cells.…”

Section: Discussionmentioning

confidence: 99%

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Efficient eradication of hormone‐resistant human prostate cancers by inactivated Sendai virus particle

Kawaguchi

Miyamoto

Inoue

et al. 2009

Intl Journal of Cancer

138

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Hormone-refractory prostate cancer is one of the intractable human cancers in the world. Here, we examined the direct tumorkilling activity of inactivated Sendai virus particle [hemagglutinating virus of Japan envelope (HVJ-E)] through induction of Type I interferon (IFN) in the hormone-resistant human prostate cancer cell lines PC3 and DU145. Preferential binding of HVJ-E to PC3 and DU145 over hormone-sensitive prostate cancer cell and normal prostate epithelium was observed, resulting in a number of fused cells. After HVJ-E treatment, a number of IFNrelated genes were up-regulated, resulting in Type I IFN production in PC3 cells. Then, retinoic acid-inducible gene-I (RIG-I) helicase which activates Type I IFN expression after Sendai virus infection was up-regulated in cancer cells after HVJ-E treatment. Produced IFN-a and -b enhanced caspase 8 expression via Janus kinases/Signal Transducers and Activators of Transcription pathway, activated caspase 3 and induced apoptosis in cancer cells. When HVJ-E was directly injected into a mass of PC3 tumor cells in SCID (severe combined immunodeficiency) mice, a marked reduction in the bulk of each tumor mass was observed and 85% of the mice became tumor-free. Although co-injection of an antiasialo GM1 antibody with HVJ-E into each tumor mass slightly attenuated the tumor suppressive activity of HVJ-E, significant suppression of tumor growth was observed even in the presence of anti-asialo GM1 antibody. This suggests that natural killer cell activation made small contribution to tumor regression following HVJ-E treatment in hormone-resistant prostate cancer model in vivo. Thus, HVJ-E effectively targets hormone-resistant prostate cancer by inducing apoptosis in tumor cells, as well as activating anti-tumor immunity. '

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Section: Resultsmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

Section: Discussionmentioning

confidence: 99%

See 3 more Smart Citations

Efficient eradication of hormone‐resistant human prostate cancers by inactivated Sendai virus particle

Kawaguchi

Miyamoto

Inoue

et al. 2009

Intl Journal of Cancer

138

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Newcastle Disease Virus

Miller¹,

Afonso²

2011

Encyclopedia of Life Sciences

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Newcastle disease virus (NDV), a member of the Avulavirus genus in the Paramyxoviridae family, has a ribonucleic acid (RNA) genome that is negative sense, nonsegmented and single‐stranded. The genome codes for six structural proteins: nucleocapsid, phosphoprotein (P), matrix, fusion, hemagglutinin–neuraminidase and the RNA‐directed RNA polymerase, in addition to the nonstructural V protein that is produced by a frame shift in the P coding region. Virulent forms of NDV (vNDV) contain multiple basic amino acids in the fusion cleavage site along with a phenylalanine (F) at position 117, are found worldwide and are endemic in some countries. Infections of poultry species with vNDV lead to trade restrictions. Although all NDV strains are of one serotype, their genomes evolve over time, becoming more diverse. Strains of NDV have been used as viral vectors to formulate vaccines for other infectious diseases and experimentally to treat human cancers. The virus causes conjunctivitis in humans. Key Concepts: Virulent NDV (vNDV) is the aetiological agent of one of the most prevalent and virulent avian diseases in the world, and causes millions of birds to die, and significantly affects the poultry industries of many countries in Africa, Asia and South America. Lentogenic NDV (loNDV) is widely distributed in wild birds where it does not cause significant disease or clinical signs. Isolates of NDV are genetically diverse with at least two classes of viruses, each divided into 10 genotypes. Depending on the virulence of the NDV isolate and the immune status of the host, Newcastle disease produces a large range of clinical signs. The fusion protein cleavage site is a key determinant of virulence and a key element utilised for modern diagnostics and classification. Because all NDV isolates are of a single serotype vaccines prepared with any NDV isolate should protect against disease from any other NDV infection. Neutralising antibodies to the Fusion (F) and hemagglutinin–neuraminidase (HN) proteins of NDV are known to be important in preventing morbidity and morality from Newcastle disease. Even vaccinated birds with high antibody titre to NDV will become infected when exposed to virulent NDV and these vaccinated birds will shed virulent NDV in oral secretion and fecal matter. The genome of NDV has been used as a vaccine vector to carry foreign genes of other organisms for use in both animals and humans.

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Metabolisches Glykoengineering mit N‐Acyl‐Seiten‐ ketten‐modifizierten Mannosaminen

2016

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Beim metabolischen Glykoengineering (MGE) werden Zellen und Tiere mit nichtnatürlichen Derivaten von Monosacchariden behandelt. Diese werden nach ihrer Aufnahme ins Zytosol metabolisiert und anschließend auf neusynthetisierten Glykokonjugaten exprimiert. MGE wurde zuerst für sialylierte Glykane realisiert, mit N‐Acyl‐modifizierten Mannosaminen als Vorstufen für nichtnatürliche Sialinsäuren. Voraussetzung ist die Promiskuität der Enzyme des Roseman‐Warren‐Biosyntheseweges. Diese tolerieren spezifische Modifikationen der N‐Acyl‐Seitenkette von Mannosaminderivaten, z. B. Elongation mit Methylen‐Gruppen (aliphatische Modifikationen) oder Einfügen reaktiver Gruppen (bioorthogonale Modifikationen). Nichtnatürliche Sialinsäuren werden in Glykokonjugate von Zellen und Organen integriert. MGE hat faszinierende biologische Konsequenzen für die behandelten Zellen (aliphatisches MGE) und ermöglicht die Visualisierung der Topographie und Dynamik der sialylierten Glykane in vitro, ex vivo und in vivo (bioorthogonales MGE).

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Role of sialic acid-containing molecules in paramyxovirus entry into the host cell: A minireview

Cited by 122 publications

References 132 publications

Efficient eradication of hormone‐resistant human prostate cancers by inactivated Sendai virus particle

Efficient eradication of hormone‐resistant human prostate cancers by inactivated Sendai virus particle

Newcastle Disease Virus

Metabolisches Glykoengineering mit N‐Acyl‐Seiten‐ ketten‐modifizierten Mannosaminen

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