Formation of Covalently Modified Folding Intermediates of Simian Virus 40 Vp1 in Large T Antigen-Expressing Cells

Watanabe, Marika; Phamduong, Ellen; Huang, Chu-Han; Itoh, Noriko; Bernal, J J; Nakanishi, Akira; Rundell, Kathleen; Gjoerup, Ole; Kasamatsu, Harumi

doi:10.1128/jvi.00955-12

Cited by 2 publications

(2 citation statements)

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“…Therefore, inhibitors of Hsp70 would be expected to curtail cell growth as well as polyomavirus replication by creating a less favorable milieu for the virus to thrive, and perhaps even causing selective apoptosis of infected cells (Wright et al, 2008). Moreover, Hsp70 and the cochaperone Hsp40 have been implicated in the correct folding of the SV40 VP-1 capsid protein into functional pentamers (Li et al, 2009; Watanabe et al, 2013). Accordingly, an Hsp70 inhibitor, MAL2-11B, has been shown to cause one log reduction of BKV viral load in HK2 cells at concentrations of 15 μM, and a fivefold reduction in SV40 DNA replication at a concentration of 100 μM (Wright et al, 2009).…”

Section: Discussionmentioning

confidence: 99%

Inhibition of large T antigen ATPase activity as a potential strategy to develop anti-polyomavirus JC drugs

et al. 2014

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Introduction This study evaluates polyomavirus JC (JCV) large T antigen (LTA) as a potential target for drug development. LTA is a hexameric protein with a helicase activity that is powered by ATP binding and hydrolysis. The helicase and ATPase function is critical for viral replication. Methods Recombinant JCV LTA was produced in an Escherichia coli based expression plasmid. ATPase activity was measured using the malachite green assay. A high throughput screen was completed using a brain-biased library of 75,000 drug-like compounds selected for physicochemical properties consistent with blood brain barrier permeability. Results Five compounds showed non-competitive inhibition of ATPase activity with an EC50 ≤ 15 μM. Modest antiviral activity was demonstrated in an immunofluorescence assay for JCV VP-1 expression in COS7 cells (EC50 15, 18, 20, 27, and 52 μM respectively). The compounds also inhibited viral replication in a real time PCR assay at comparable concentrations. LD50 in the MTS96 and Cell TiterGlo assays was >100 μM for all compounds in COS7 as well as HEK293 cells. However, two compounds inhibited cell proliferation in culture with IC50 values of 43 and 34 μM respectively. Despite substantial amino acid similarity between polyomavirus JC, BK and SV40 proteins, these compounds differ from those previously reported to inhibit SV40 LTA ATPase in chemical structure as well as a non-competitive mechanism of inhibition. Conclusion LTA ATPase is a valid target for discovery. Additional screening and chemical optimization is needed to develop clinically useful compounds with less toxicity, which should be measured by metabolic as well as cell proliferation assays.

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Section: Discussionmentioning

confidence: 99%

Inhibition of large T antigen ATPase activity as a potential strategy to develop anti-polyomavirus JC drugs

et al. 2014

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“…COS-7 cells (ATCC ® CRL-1651™) are transformed with an origin-defective mutant of Simian Virus 40 (SV40) [As a polyomavirus, SV40 has an intricate structure. The capsid is comprised of the major capsid protein VP1 and the minor capsid proteins VP2 and VP3 (Watanabe et al, 2013 )]. The α3 nAChRs, α4 nAChRs and β2 nAChRs have been shown to be expressed on the surface of COS-7 cells (Neff et al, 1995 ).…”

Section: In Vitro Cellular Models Used In Parallel With Pc12...mentioning

confidence: 99%

The cellular model for Alzheimer's disease research: PC12 cells

Xie

Deng

Zhai

et al. 2023

Front. Mol. Neurosci.

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Alzheimer's disease (AD) is a common age-related neurodegenerative disease characterized by progressive cognitive decline and irreversible memory impairment. Currently, several studies have failed to fully elucidate AD's cellular and molecular mechanisms. For this purpose, research on related cellular models may propose potential predictive models for the drug development of AD. Therefore, many cells characterized by neuronal properties are widely used to mimic the pathological process of AD, such as PC12, SH-SY5Y, and N2a, especially the PC12 pheochromocytoma cell line. Thus, this review covers the most systematic essay that used PC12 cells to study AD. We depict the cellular source, culture condition, differentiation methods, transfection methods, drugs inducing AD, general approaches (evaluation methods and metrics), and in vitro cellular models used in parallel with PC12 cells.

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Formation of Covalently Modified Folding Intermediates of Simian Virus 40 Vp1 in Large T Antigen-Expressing Cells

Cited by 2 publications

References 51 publications

Inhibition of large T antigen ATPase activity as a potential strategy to develop anti-polyomavirus JC drugs

Inhibition of large T antigen ATPase activity as a potential strategy to develop anti-polyomavirus JC drugs

The cellular model for Alzheimer's disease research: PC12 cells

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