4.4 Article

Susceptibility to viral infection is enhanced by stable expression of 3A or 3AB proteins from foot-and-mouth disease virus

期刊

VIROLOGY
卷 380, 期 1, 页码 34-45

出版社

ACADEMIC PRESS INC ELSEVIER SCIENCE
DOI: 10.1016/j.virol.2008.06.040

关键词

FMDV non-structural proteins; stable and transient expression; effect on cells; virus growth modulation

类别

资金

  1. CICYT [BIO2005-07592C02-01]
  2. MEC [CSD2006-07, BFU-2005-00948]
  3. Fundacion Severo Ochoa

向作者/读者索取更多资源

The foot-and-mouth disease virus (FMDV) 3A protein is involved in virulence and host range. A distinguishing feature of FMDV 313 among picornaviruses is that three non-identical copies are encoded in the Viral RNA and required for optimal replication in cell culture. Here, we have studied the involvement of the 3AB region on vital infection using constitutive and transient expression systems. BHK-21 stably transformed clones expressed low levels of FMDV 3A or 3A(B) proteins in the cell cytoplasm. Transformed cells stably expressing these proteins did not exhibit inner cellular rearrangements detectable by electron Microscope analysis. Upon FMDV infection, clones expressing either 3A alone OF 3A(B) proteins showed a significant increase in the percentage of infected cells, the number of plaque forming units and the virus yield. The 3A-enhancing effect was specific for FMDV as no increase in viral multiplication was observed in transformed clones infected with another picornavirus, encephalomyocarditis virus, or the negative-strand RNA virus vesicular stomatitis virus. A potential role of 3A protein in viral RNA translation was discarded by the lack of effect on FMDV IRES-dependent translation. Increased viral susceptibility was not caused by a released factor; neither the supernatant of transformed clones nor the addition of purified 3A protein to the infection medium was responsible for this effect. Unlike stable expression, high levels of 3A or 3A(B) protein transient expression led to unspecific inhibition of viral infection. Therefore, the effect observed on viral yield, which inversely Correlated with the intracellular levels of 3A protein, suggests a transacting role operating on the FMDV multiplication cycle. (C) 2008 Elsevier Inc. All rights reserved.

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