DocumentCode :
1596221
Title :
The 3a Protein of SARS-coronavirus Induces Apoptosis in Vero E6 Cells
Author :
Waye, Mary M Y ; Law, Patrick T W ; Wong, Chi-Hang ; Au, Thomas C C ; Chuck, Chi-Pang ; Kong, Siu- Kai ; Chan, Paul K S ; To, Ka-Fai ; Lo, Anthony W I ; Chan, Judy Y W ; Suen, Yick-Keung ; Chan, H. Y Edwin ; Fung, Kwok-Pui ; Sung, Joseph J Y ; Lo, Y. M De
Author_Institution :
Dept. of Biochem., Hong Kong Univ., Shatin
fYear :
2006
Firstpage :
7482
Lastpage :
7485
Abstract :
An outbreak of severe acute respiratory syndrome (SARS) occurred in China and the first case emerged in mid November 2002. The etiologic agent of this disease was found to be a previously unknown coronavirus, SARS-CoV. The detailed pathology of SARS-CoV infection and the host response to the viral infection are still not known. The 3a gene encodes a non-structural viral protein which is predicted to be a transmembrane protein. In this study, we showed that the 3a protein was localized to the endoplasmic reticulum (ER) in 3a-transfected monkey kidney Vero E6 cells. In vitro experiments of chromatin condensation and DNA fragmentation suggest that the 3a protein may trigger apoptosis. Our data show that over-expression of a single SARS-CoV protein can induce apoptosis in vitro. Thus GFP-3a fusion protein could also be used as a biosensor for monitoring the cytopathic features of SARS infection, e.g. lymphopenia, in animal model systems, similar to nucleocapsid and 7a proteins
Keywords :
DNA; biosensors; cellular biophysics; diseases; microorganisms; pneumodynamics; proteins; 3a gene encoding; 3a protein; 3a-transfected monkey kidney; DNA fragmentation; SARS; SARS-CoV; Vero E6 cells; apoptosis; biosensor; chromatin condensation; coronavirus; endoplasmic reticulum; severe acute respiratory syndrome; transmembrane protein; viral protein; Bioinformatics; Biomembranes; Diseases; Erbium; Genomics; Humans; In vitro; Pathology; Proteins; Sequences;
fLanguage :
English
Publisher :
ieee
Conference_Titel :
Engineering in Medicine and Biology Society, 2005. IEEE-EMBS 2005. 27th Annual International Conference of the
Conference_Location :
Shanghai
Print_ISBN :
0-7803-8741-4
Type :
conf
DOI :
10.1109/IEMBS.2005.1616242
Filename :
1616242
Link To Document :
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