Human Adenoviruses of Subgenera B, C, and E with Various Tropisms Differ in Both Binding to and Replication in the Epithelial A549 and 293 Cells

Mei, Ya-Fang; Lindman, Kristina; Wadell, Göran

doi:10.1006/viro.2002.1359

Cited by 35 publications

(34 citation statements)

References 55 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…The main disadvantages with Ad5-based vectors appear to be low transduction of target cells and high preexisting immunity (2,13,20,24,34,48,68,74). In several cases, species B:2 adenoviruses have been shown to attach to host cells and deliver genes much more efficiently than other adenoviruses, including Ad5 (43,44,50,57,62). Thus, we believe that the identification of CD46 as a cellular receptor for these adenoviruses widens the understanding of adenovirus tropism and may also contribute to development of more effective adenovirus-based gene therapy vectors.…”

Section: Discussionmentioning

confidence: 99%

Adenovirus Type 11 Uses CD46 as a Cellular Receptor

Segerman

Atkinson

Marttila

et al. 2003

J Virol

309

252

View full text Add to dashboard Cite

Section: Discussionmentioning

confidence: 99%

Adenovirus Type 11 Uses CD46 as a Cellular Receptor

Segerman

Atkinson

Marttila

et al. 2003

J Virol

309

252

View full text Add to dashboard Cite

“…However, we have clearly demonstrated that the F7 vector has a dramatic effect on Ad5 vector detargeting, which substantiates its use as a platform for retargeting (in place of a mutated CAR binding fiber). Subgroup B viruses have been shown to have distinct cell targets, as previously described (20,(23)(24)(25)33), and it will be important to identify the receptor used by the subgroup B viruses as well as the functional ligand domain present in the F7 homotrimer. The extension of the non-CAR binding vectors to the F7F41S tandem platform represents a novel class of modified Ad5-based vectors that provides distinct advantages over traditional single-fiber swap chimeras.…”

Section: Discussionmentioning

confidence: 99%

“…A CAR binding serotype can be converted to a subgroup B receptor-targeted vector simply by genetically switching the fiber terminal exons (12). Subgroup B viruses can bind to many of the same cell types as CAR binding viruses, but there are also cell types that demonstrate differential affinity for the subgroup B fiber versus the CAR binding serotypes (20,(23)(24)(25)33). Another distinct class of fiber-containing adenoviruses is the enteric subgroup F viruses (serotypes 40 and 41).…”

mentioning

confidence: 99%

Subgroup B and F Fiber Chimeras Eliminate Normal Adenovirus Type 5 Vector Transduction In Vitro and In Vivo

Schoggins

Gall

Falck-Pedersen

2003

J Virol

View full text Add to dashboard Cite

Altering adenovirus vector (Ad vector) targeting is an important goal for a variety of gene therapy applications and involves eliminating or reducing the normal tropism of a vector and retargeting through a distinct receptor-ligand pathway. The first step of Ad vector infection is high-affinity binding to a target cellular receptor. For the majority of adenoviruses and Ad vectors, the fiber capsid protein serves this purpose, binding to the coxsackievirus and adenovirus receptor (CAR) present on a variety of cell types. In this study we have explored a novel approach to altering Ad type 5 (Ad5) vector targeting based on serotypic differences in fiber function. The subgroup B viruses bind to an unidentified receptor that is distinct from CAR. The subgroup F viruses are the only adenoviruses that express two distinct terminal exons encoding fiber open reading frames. We have constructed chimeric fiber adenoviruses that utilize the tandem fiber arrangement of the subgroup F genome configuration. By taking advantage of serotypic differences in fiber expression, fiber shaft length, and fiber binding efficiency, we have developed a tandem fiber vector that has low binding efficiency for the known fiber binding sites, does not rely on an Ad5-based fiber, and can be grown to high titer using conventional cell lines. Importantly, when characterizing these vectors in vivo, we find the subgroup B system and our optimal tandem fiber system demonstrate reduced liver transduction by over 2 logs compared to an Ad5 fiber vector. These attributes make the tandem fiber vector a useful alternative to conventional strategies for fiber manipulation of adenovirus vectors.

show abstract

“…(i) Several groups found that Ad3 and Ad7 do not use CD46 for infection (7, 21), (ii) Ad3 and Ad7 (group B1) and Ad35 (group B2) do not compete for binding on HeLa cells (31,35), and (iii) Ad11p fiber knob can completely block binding of wild-type Ad35 to A549 cells, while recombinant Ad35 fiber knob cannot completely block Ad11p binding (22,41). While these data suggest that Ad3 and Ad7 and probably Ad11 can use a receptor that is different from CD46, the nature of this receptor(s) remains elusive.…”

mentioning

confidence: 99%

A New Group B Adenovirus Receptor Is Expressed at High Levels on Human Stem and Tumor Cells

Tuve

Wang

Ware³

et al. 2006

J Virol

122

153

View full text Add to dashboard Cite

CD46 is used by human group B adenoviruses (Ads) as a high-affinity attachment receptor. Here we show evidence that several group B Ads utilize an additional receptor for infection of human cells, which is different from CD46. We tentatively named this receptor receptor X. Competition studies with unlabeled and labeled Ads, recombinant Ad fiber knobs, and soluble CD46 and CD46 antibodies revealed three different subgroups of group B Ads, in terms of their receptor usage. Group I (Ad16, -21, -35, and -50) nearly exclusively uses CD46. Group II (Ad3, -7p, and -14) utilizes receptor X and not CD46. Group III (Ad11p) uses both CD46 and the alternative receptor X. Interaction of group II and III Ads with receptor X occurs via the fiber knob. Receptor X is an abundantly expressed glycoprotein that interacts with group II and III Ads at relatively low affinity in a Ca 2؉ -dependent manner. This receptor is expressed at high levels on human mesenchymal and undifferentiated embryonic stem cells, as well as on human cancer cell lines. These findings have practical implications for stem cell and gene therapy.Human adenoviruses (Ads) have been classified into six subgroups (A to F) currently containing 51 serotypes. Group B Ads form two genetic clusters, B1 (Ad3, Ad7, Ad16, Ad21, and Ad50) and B2 (Ad11, Ad14, Ad34, and Ad35) (44). Most B1 Ads are mainly associated with acute respiratory disease and, unlike the species C Ads (e.g., Ad5), do not establish persistence (43). The B2 serotypes 11p, 34, and 35 have mainly been associated with infections of the kidneys and urinary tract. Recently, gene transfer vectors based on group B Ads have shown promise for cell and gene therapy. Vectors containing fibers from group B Ads efficiently transduce human cell types that are relatively refractory to infection with classical serotype Ad5 vectors, including malignant tumor cells (30, 39), hematopoietic stem cells (26,35,46), mesenchymal stem (MES) cells (9, 18), dendritic cells (DC) (5, 27, 28), lymphocytes (33), chorion villus cells, and endothelial cells (13).CD46 has been identified as a cellular receptor for group B Ads (7, 32, 37) whereby the two distal extracellular domains of CD46 are involved in Ad binding (6, 7). In humans, CD46 is a ubiquitously expressed membrane protein with complement regulatory functions.A series of data suggest the existence of an additional group B Ad receptor(s). (i) Several groups found that Ad3 and Ad7 do not use CD46 for infection (7, 21), (ii) Ad3 and Ad7 (group B1) and Ad35 (group B2) do not compete for binding on HeLa cells (31,35), and (iii) Ad11p fiber knob can completely block binding of wild-type Ad35 to A549 cells, while recombinant Ad35 fiber knob cannot completely block Ad11p binding (22,41). While these data suggest that Ad3 and Ad7 and probably Ad11 can use a receptor that is different from CD46, the nature of this receptor(s) remains elusive. In this study, we investigated receptor usage by group B Ads on human cells and laid the groundwork for identification of the receptor. Also, the...

show abstract

Human Adenoviruses of Subgenera B, C, and E with Various Tropisms Differ in Both Binding to and Replication in the Epithelial A549 and 293 Cells

Cited by 35 publications

References 55 publications

Adenovirus Type 11 Uses CD46 as a Cellular Receptor

Adenovirus Type 11 Uses CD46 as a Cellular Receptor

Subgroup B and F Fiber Chimeras Eliminate Normal Adenovirus Type 5 Vector Transduction In Vitro and In Vivo

A New Group B Adenovirus Receptor Is Expressed at High Levels on Human Stem and Tumor Cells

Contact Info

Product

Resources

About