Positively Charged Residues at the Five-Fold Symmetry Axis of Cell Culture-Adapted Foot-and-Mouth Disease Virus Permit Novel Receptor Interactions

Berryman, Stephen; Clark, Stuart; Kakker, N. K.; Silk, Rachel; Seago, Julian; Wadsworth, Jemma; Chamberlain, Kyle; Knowles, Nick J.; Jackson, Terry

doi:10.1128/jvi.01138-13

Cited by 29 publications

(43 citation statements)

References 55 publications

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“…In the coinfection competition assays, those cell-culture-adapted viruses swiftly outcompeted their parental competitors after only a limited number of passages (P 1-5 ), consistent with the presumed greater biological fitness the positively charged residues impart to the virus in cell culture (Table 4). Since CHO-K1 cells do not express any 'RGD'-binding integrin known to be used by FMDV, entry into these cells is postulated to be mediated by either HS or some non-integrin, non-HS receptors (Berryman et al, 2013;Jackson et al, 1996). While none of the viruses before gaining positively charged residues (P 0 or low passage populations) could replicate in CHO-K1 cells, the cell-culture-adapted variants manifested cytopathic effect, uniform small plaques (,1 mm diameter) and increase in virus titre between 1 and 24 h postinfection of CHO-K1 cells (Table 3).…”

Section: Selection and In Vitro Characterization Of Virusesmentioning

confidence: 99%

“…Therefore, it is of interest to map critical amino acid substitutions on the capsid accounting for the plasticity in receptor interaction. More importantly, they could also be potential leads for the rational design of cell-culture-adaptable vaccine seed strains through a reverse genetic approach (Berryman et al, 2013;Maree et al, 2011). In this study, we explored the sequence hotspots of probable adaptive significance in cell culture by comparing the capsid coding (P1) sequences and threedimensional structures generated thereof for multiple strains of FMDV serotype A representing WT viruses derived directly from infected cattle tongue epithelium and after passaging in three cell lines originating from different animal species.…”

Section: Introductionmentioning

confidence: 99%

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Cell culture adaptation mutations in foot-and-mouth disease virus serotype A capsid proteins: implications for receptor interactions

Mohapatra

Pandey

Devendra

et al. 2015

Journal of General Virology

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In this study we describe the adaptive changes fixed on the capsid of several foot-and-mouth disease virus serotype A strains during propagation in cell monolayers. Viruses passaged extensively in three cell lines (BHK-21, LFBK and IB-RS-2) consistently gained positively charged amino acids in the putative heparin-sulfate-binding pocket (VP2 bE-bF loop, VP1 C-terminus and VP3 b-B knob) surrounding the fivefold symmetry axis (VP1 bF-bG loop) and at other discrete sites on the capsid (VP3 bG-bH loop, VP1 C-terminus, VP2 bC strand and VP1 bG-bH loop). A lysine insertion in the VP1 bF-bG loop of two of the BHK-21-adapted viruses supports the biological advantage of positively charged residues acquired in cell culture. The charge transitions occurred irrespective of cell line, suggesting their possible role in ionic interaction with ubiquitous negatively charged cell-surface molecules such as glycosaminoglycans (GAG). This was supported by the ability of the cell-culture-adapted variants to replicate in the integrin-deficient, GAG-positive CHO-K1 cells and their superior fitness in competition assays compared with the lower passage viruses with WT genotypes. Substitutions fixed in the VP1 bG-bH loop ("3, "2 and +2 'RGD' positions) or in the structural element known to be juxtaposed against that loop (VP1 bB-bC loop) suggest their possible role in modulating the efficiency and specificity of interaction of the 'RGD' motif with a v -integrin receptors. The nature and location of the substitutions described in this study could be applied in the rapid cell culture adaptation of viral strains for vaccine production.

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Section: Selection and In Vitro Characterization Of Virusesmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Cell culture adaptation mutations in foot-and-mouth disease virus serotype A capsid proteins: implications for receptor interactions

Mohapatra

Pandey

Devendra

et al. 2015

Journal of General Virology

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“…The affinity to avb6 integrins was high, measured at K D ¼ 0.22 nmol/L, whereas binding to other integrins, including avb3, avb5, and avb1, was more than 80-fold lower (21,25). The selective binding to avb6 integrins was shown to be dependent on the DLXXL motif in the carboxy a-helical loop next to the RGD domain at the apex of the loop domain in the peptide (23,26,44,45).…”

Section: Discussionmentioning

confidence: 90%

“…We generated the replication-selective integrin-targeted Ad5-3D-A20T mutant expressing the small avb6-peptide ligand A20FMDV2. The A20FMDV2 peptide was derived from the GH-loop in VP1 in the capsid of the FMDV and is essential for infection in clovenhoofed animals (44). The affinity to avb6 integrins was high, measured at K D ¼ 0.22 nmol/L, whereas binding to other integrins, including avb3, avb5, and avb1, was more than 80-fold lower (21,25).…”

Section: Discussionmentioning

confidence: 99%

The Novel Oncolytic Adenoviral Mutant Ad5-3Δ-A20T Retargeted to αvβ6 Integrins Efficiently Eliminates Pancreatic Cancer Cells

Man

Davies

Coughlan

et al. 2018

Molecular Cancer Therapeutics

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Metastatic pancreatic ductal adenocarcinomas (PDAC) are incurable due to the rapid development of resistance to all current therapeutics. Oncolytic adenoviral mutants have emerged as a promising new strategy that negates such resistance. In contrast to normal tissue, the majority of PDACs express the avb6 integrin receptor. To exploit this feature, we modified our previously reported oncolytic adenovirus, AdDD, to selectively target avb6 integrins to facilitate systemic delivery. Structural modifications to AdDD include the expression of the small but potent avb6-binding peptide, A20FMDV2, and ablation of binding to the native coxsackie and adenovirus receptor (CAR) within the fiber knob region. The resultant mutant, Ad5-3D-A20T, infected and killed avb6 integrin-expressing cells more effectively than the parental wild-type (Ad5wt) virus and AdDD. Viral uptake through avb6 integrins rather than native viral receptors (CAR, avb3 and avb5 integrins) promoted viral propagation and spread. Superior efficacy of Ad5-3D-A20T compared with Ad5wt was demonstrated in 3D organotypic cocultures, and similar potency between the two viruses was observed in Suit-2 in vivo models. Importantly, Ad5-3D-A20T infected pancreatic stellate cells at low levels, which may further facilitate viral spread and cancer cell elimination either as a single agent or in combination with the chemotherapy drug, gemcitabine. We demonstrate that Ad5-3D-A20T is highly selective for avb6 integrin-expressing pancreatic cancer cells, and with further development, this new and exciting strategy can potentially be extended to improve the systemic delivery of adenoviruses to pancreatic cancer patients. Mol Cancer Ther; 17(2); 575-87. Ó2018 AACR.

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“…112,129,[133][134][135][136][137][138] Furthermore, alternative cell entry pathways exist and can be applied in future to improve cell adaptation. 134,135,139 Continued reverse genetic approaches to rapidly adapt African FMDV to BHK-21 cell culture will greatly enhance the ability to produce region-specific vaccines tailored to current circulating strains.…”

Section: Design Of Improved Inactivated Vaccinesmentioning

confidence: 99%

Challenges and prospects for the control of foot-and-mouth disease: an African perspective

Maree¹,

Kasanga²,

Scott³

et al. 2014

VMRR

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Abstract:The epidemiology of foot-and-mouth disease (FMD) in Africa is unique in the sense that six of the seven serotypes of FMD viruses (Southern African Territories [SAT] 1, SAT2, SAT3, A, O, and C), with the exception of Asia-1, have occurred in the last decade. Due to underreporting of FMD, the current strains circulating throughout sub-Saharan Africa are in many cases unknown. For SAT1, SAT2, and serotype A viruses, the genetic diversity is reflected in antigenic variation, and indications are that vaccine strains may be needed for each topotype. This has serious implications for control using vaccines and for choice of strains to include in regional antigen banks. The epidemiology is further complicated by the fact that SAT1, SAT2, and SAT3 viruses are maintained and spread by wildlife, persistently infecting African buffalo in particular. Although the precise mechanism of transmission of FMD from buffalo to cattle is not well understood, it is facilitated by direct contact between these two species.Once cattle are infected they may maintain SAT infections without the further involvement of buffalo. No single strategy for control of FMD in Africa is applicable. Decision on the most effective regional control strategy should focus on an ecosystem approach, identification of primary endemic areas, animal husbandry practices, climate, and animal movement. Within each ecosystem, human behavior could be integrated in disease control planning. Different regions in sub-Saharan Africa are at different developmental stages and are thus facing unique challenges and priorities in terms of veterinary disease control. Many science-based options targeting improved vaccinology, diagnostics, and other control measures have been described. This review therefore aims to emphasize, on one hand, the progress that has been achieved in the development of new technologies, including research towards improved tailored vaccines, appropriate vaccine strain selection, vaccine potency, and diagnostics, and how it relates to the conditions in Africa. On the other hand, we focus on the unique epidemiological, ecological, livestock farming and marketing, socioeconomic, and governance issues that constrain effective FMD control. Any such new technologies should have the availability of safe livestock products for trade as the ultimate goal.

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Positively Charged Residues at the Five-Fold Symmetry Axis of Cell Culture-Adapted Foot-and-Mouth Disease Virus Permit Novel Receptor Interactions

Cited by 29 publications

References 55 publications

Cell culture adaptation mutations in foot-and-mouth disease virus serotype A capsid proteins: implications for receptor interactions

Cell culture adaptation mutations in foot-and-mouth disease virus serotype A capsid proteins: implications for receptor interactions

The Novel Oncolytic Adenoviral Mutant Ad5-3Δ-A20T Retargeted to αvβ6 Integrins Efficiently Eliminates Pancreatic Cancer Cells

Challenges and prospects for the control of foot-and-mouth disease: an African perspective

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