Cytomegalovirus pp65 limits dissemination but is dispensable for persistence
Daniel Malouli, … , Louis J. Picker, Klaus Früh
Daniel Malouli, … , Louis J. Picker, Klaus Früh
Published April 1, 2014
Citation Information: J Clin Invest. 2014;124(5):1928-1944. https://doi.org/10.1172/JCI67420.
View: Text | PDF
Research Article Virology

Cytomegalovirus pp65 limits dissemination but is dispensable for persistence

Abstract

The most abundantly produced virion protein in human cytomegalovirus (HCMV) is the immunodominant phosphoprotein 65 (pp65), which is frequently included in CMV vaccines. Although it is nonessential for in vitro CMV growth, pp65 displays immunomodulatory functions that support a potential role in primary and/or persistent infection. To determine the contribution of pp65 to CMV infection and immunity, we generated a rhesus CMV lacking both pp65 orthologs (RhCMVΔpp65ab). While deletion of pp65ab slightly reduced growth in vitro and increased defective particle formation, the protein composition of secreted virions was largely unchanged. Interestingly, pp65 was not required for primary and persistent infection in animals. Immune responses induced by RhCMVΔpp65ab did not prevent reinfection with rhesus CMV; however, reinfection with RhCMVΔUS2-11, which lacks viral-encoded MHC-I antigen presentation inhibitors, was prevented. Unexpectedly, induction of pp65b-specific T cells alone did not protect against RhCMVΔUS2-11 challenge, suggesting that T cells targeting multiple CMV antigens are required for protection. However, pp65-specific immunity was crucial for controlling viral dissemination during primary infection, as indicated by the marked increase of RhCMVΔpp65ab genome copies in CMV-naive, but not CMV-immune, animals. Our data provide rationale for inclusion of pp65 into CMV vaccines but also demonstrate that pp65-induced T cell responses alone do not recapitulate the protective effect of natural infection.

Authors

Daniel Malouli, Scott G. Hansen, Ernesto S. Nakayasu, Emily E. Marshall, Colette M. Hughes, Abigail B. Ventura, Roxanne M. Gilbride, Matthew S. Lewis, Guangwu Xu, Craig Kreklywich, Nathan Whizin, Miranda Fischer, Alfred W. Legasse, Kasinath Viswanathan, Don Siess, David G. Camp II, Michael K. Axthelm, Christoph Kahl, Victor R. DeFilippis, Richard D. Smith, Daniel N. Streblow, Louis J. Picker, Klaus Früh

×

Figure 4

RhCMVΔpp65ab is persistently secreted from infected animals.

Options: View larger image (or click on image) Download as PowerPoint
RhCMVΔpp65ab is persistently secreted from infected animals. (A) The tim...
(A) The time line depicts the time points of inoculation with different RhCMV constructs and the days when cocultures were started from urine. Time points marked with asterisks indicate additional days in which cocultures were positive for Δpp65ab, but the data are not shown. PID, postinoculation day. (B) Immunoblot for the indicated antigens in lysates from representative viral cocultures with urine collected on the indicated dpi. The presence of RhCMV-IE1, RhCMV-pp65b, SIVgag, and SIVretanef in cell lysates was detected by immunoblot using antibodies specific for the respective antigens (IE, pp65) or for epitope tags fused to SIVgag or SIVretanef. Note that, initially, secreted RhCMV expressed IE, but not pp65, whereas superinfection with WTgag and Δpp65retanef is indicated by the appearance of pp65-containing virus expressing the respective antigens. As positive control (Con), coculture lysates from a RM inoculated with WTgag and WTretanef is included.