Distinct domains of M-T2, the myxoma virus tumor necrosis factor (TNF) receptor homolog, mediate extracellular TNF binding and intracellular apoptosis inhibition
- Publication Type:
- Journal Article
- Citation:
- Journal of Virology, 1997, 71 (3), pp. 2171 - 2181
- Issue Date:
- 1997-03-01
Closed Access
Filename | Description | Size | |||
---|---|---|---|---|---|
2008005711OK.pdf | 617.54 kB |
Copyright Clearance Process
- Recently Added
- In Progress
- Closed Access
This item is closed access and not available.
The myxoma virus tumor necrosis factor (TNF) receptor homolog, M-T2, is expressed both as a secreted glycoprotein that inhibits the cytolytic activity of rabbit TNF-α and as an endoglycosidase H-sensitive intracellular species that prevents myxoma virus-infected CD4+ T lymphocytes from undergoing apoptosis. To compare the domains of M-T2 mediating extracellular TNF inhibition and intracellular apoptosis inhibition, recombinant myxoma viruses expressing nested C-terminal truncations of M-T2 protein were constructed. One mutant, ΔL113, containing intact copies of only two cysteine-rich domains, was not secreted and was incapable of binding rabbit TNF-α yet retained full ability to inhibit virus-induced apoptosis of RL-5 cells. Thus, the minimal domain of intracellular M-T2 protein required to inhibit apoptosis is distinct from that required by the extracellular M-T2 for functional TNF-α binding and inhibition. This is the first report of a virus-encoded immunomodolar protein with two distinct antiimmune properties.
Please use this identifier to cite or link to this item: