Abstract

Marek's disease (MD) is a neoplastic disease of poultry caused by Marek's disease virus (MDV), a highly contagious alphaherpesvirus. Meq, the major MDV oncoprotein, induces neoplastic transformation of T-cells through several mechanisms, including inhibition of apoptosis. In contrast, the chicken anemia virus (CAV)-encoded protein apoptin (VP3) is a powerful inducer of apoptosis of tumor cells, a property that is exploited for anticancer therapeutics. Although the molecular mechanisms of selective induction of tumor cell apoptosis by apoptin are not fully understood, its tumor cell–restricted nuclear translocation is thought to be important. Co-infection with MDV and CAV is common in many countries, CAV antigens are readily detectable in MD lymphomas, and the MDV-transformed T-lymphoblastoid cell lines such as MSB-1 is widely used for propagating CAV for vaccine production. As MDV-transformed cell lines express high levels of Meq, we examined here whether CAV-encoded apoptin interacts with Meq in these cells. Using immunofluorescence microscopy, we found that apoptin and Meq co-localize to the nucleus, and biochemical analysis indicated that the two proteins do physically interact. Using a combination of Meq mutagenesis and co-immunoprecipitation, we demonstrate that apoptin interacts with Meq within a region between amino acids 130 and 140. Results from the IncuCyte assay suggested that Meq inhibits apoptin-induced apoptosis activity. In summary, our findings indicate that Meq interacts with and inhibits apoptin. Insights into this novel interaction between Meq and apoptin will relevance for pathogenesis of coinfections of the two viruses and in CAV vaccine production using MDV-transformed cell lines.

Highlights

  • As a rapid-onset neoplastic disease of chickens, Marek’s disease (MD), caused by the highly contagious Marek’s disease virus (MDV), is generally considered an excellent model for studying virus-induced T-cell lymphomas

  • Co-infection with MDV and chicken anemia virus (CAV) is common in many countries, CAV antigens are readily detectable in MD lymphomas, and the MDV-transformed T-lymphoblastoid cell lines such as MSB-1 is widely used for propagating CAV for vaccine production

  • We reported that Meq interacts with CtBP via the proline-leucine-aspartic acid-leucine-serine (PLDLS) motif, an interaction critical for induction of lymphomas [9]

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Summary

INTRODUCTION

As a rapid-onset neoplastic disease of chickens, Marek’s disease (MD), caused by the highly contagious Marek’s disease virus (MDV), is generally considered an excellent model for studying virus-induced T-cell lymphomas. The ability of apoptin to induce apoptosis selectively in transformed cells, but not in normal cells, is thought to be related to its accumulation in the nucleus, since apoptin has a cytoplasmic location in untransformed cells. This is dependent on nuclear localization (NLS) and nuclear export (NES) signals present respectively at the N and C terminal of apoptin [17, 18]. Experimental studies showed infection of MD lymphomas by CAV [32] Since both MSB-1 and MD lymphomas express high levels of Meq, we examined whether there is any physical and functional interaction between apoptin and Meq

RESULTS
DISCUSSION
MATERIALS AND METHODS

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