The E1B 19,000-molecular-weight protein of group C adenoviruses prevents tumor necrosis factor cytolysis of human cells but not of mouse cells
LR Gooding, L Aquino, PJ Duerksen-Hughes… - Journal of …, 1991 - Am Soc Microbiol
LR Gooding, L Aquino, PJ Duerksen-Hughes, D Day, TM Horton, SP Yei, WS Wold
Journal of virology, 1991•Am Soc MicrobiolTumor necrosis factor (TNF) is a multifunctional immunoregulatory protein that is secreted by
activated macrophages and is believed to have antiviral activities. We reported earlier that
when mouse C3HA fibroblasts are infected with human adenoviruses, the 289R and 243R
proteins encoded by region E1A render the cells susceptible to lysis by TNF, and a 14,700-
molecular-weight protein (14.7 K protein) encoded by region E3 protects the cells against
lysis by TNF. We now report that the 19,000-molecular-weight (19K)(176R) protein encoded …
activated macrophages and is believed to have antiviral activities. We reported earlier that
when mouse C3HA fibroblasts are infected with human adenoviruses, the 289R and 243R
proteins encoded by region E1A render the cells susceptible to lysis by TNF, and a 14,700-
molecular-weight protein (14.7 K protein) encoded by region E3 protects the cells against
lysis by TNF. We now report that the 19,000-molecular-weight (19K)(176R) protein encoded …
Tumor necrosis factor (TNF) is a multifunctional immunoregulatory protein that is secreted by activated macrophages and is believed to have antiviral activities. We reported earlier that when mouse C3HA fibroblasts are infected with human adenoviruses, the 289R and 243R proteins encoded by region E1A render the cells susceptible to lysis by TNF, and a 14,700-molecular-weight protein (14.7K protein) encoded by region E3 protects the cells against lysis by TNF. We now report that the 19,000-molecular-weight (19K) (176R) protein encoded by the E1B transcription unit can protect human HEL-299 fibroblasts and human ME-180 cervical carcinoma cells against lysis by TNF. This was determined by infecting cells with adenovirus double mutants that lack region E3 and do or do not express the E1B-19K protein and by measuring cytolysis by using a short-term (18-h) 51Cr-release assay. Under these assay conditions, the 51Cr release was specific to TNF and was not a consequence of the cyt phenotype associated with E1B-19K protein-negative mutants. Also, by using virus double mutants that lack E3 in combination with other early regions, we found that E1A, the E1B-55K protein-encoding gene, E3, and E4 are not required to protect HEL-299 cells against TNF cytolysis. Three additional human cancer cell lines (HeLa, HCT8, and RC29) and a simian virus 40-transformed WI38 cell line (VA-13) also required E1B for protection against TNF cytolysis, indicating that the E1B-19K protein is required to protect many if not all human cell types against lysis by TNF when infected by adenovirus. The E1B-19K protein was not able to protect six different adenovirus-infected mouse cell lines against TNF lysis, even though the protein was shown to be efficiently expressed in one of the cell lines. HEL-299 or ME-180 cells infected by a mutant that lacks the E1B-19K protein but retains region E3 were not lysed by TNF, indicating that one or more of the E3 proteins can protect these cells against TNF lysis in the absence of the E1B-19K protein. Thus, the E3-14.7K but not the E1B-19K protein can protect adenovirus-infected mouse cells against TNF cytolysis, whereas the E1B-19K protein as well as one or more of the E3 proteins can protect adenovirus-infected human cells against TNF cytolysis.
American Society for Microbiology