2014
DOI: 10.3390/v6020808
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Noncanonical Expression of a Murine Cytomegalovirus Early Protein CD8 T-Cell Epitope as an Immediate Early Epitope Based on Transcription from an Upstream Gene

Abstract: Viral CD8 T-cell epitopes, represented by viral peptides bound to major histocompatibility complex class-I (MHC-I) glycoproteins, are often identified by “reverse immunology”, a strategy not requiring biochemical and structural knowledge of the actual viral protein from which they are derived by antigen processing. Instead, bioinformatic algorithms predicting the probability of C-terminal cleavage in the proteasome, as well as binding affinity to the presenting MHC-I molecules, are applied to amino acid sequen… Show more

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Cited by 7 publications
(12 citation statements)
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References 53 publications
(68 reference statements)
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“…In essence, for an observation period of 1 year, epitope-specific responses were highly variable between the three HCTs and far from continuity within any of the three HCTs. For the response to IDEs m123/IE1 and m164, both of which are expressed in the IE phase of the viral gene expression program ( 53 , 89 ), the time of the peak acute response was variable and contraction was not pronounced. One may discuss contraction at 10 and 6 weeks in HCT #1 and HCT #3, respectively, but not in HCT #2.…”
Section: Resultsmentioning
confidence: 99%
See 1 more Smart Citation
“…In essence, for an observation period of 1 year, epitope-specific responses were highly variable between the three HCTs and far from continuity within any of the three HCTs. For the response to IDEs m123/IE1 and m164, both of which are expressed in the IE phase of the viral gene expression program ( 53 , 89 ), the time of the peak acute response was variable and contraction was not pronounced. One may discuss contraction at 10 and 6 weeks in HCT #1 and HCT #3, respectively, but not in HCT #2.…”
Section: Resultsmentioning
confidence: 99%
“…To account for different kinetic classes of viral protein expression, stimulator cells in the assay were metabolically arrested in the “IE” phase, or in the “E” phase, or were allowed to proceed to the “late” (L) phase. As a remark, IE phase expression of the antigenic peptide assigned to the E Phase protein m164 has recently been shown to result from a transcript starting within an upstream IE gene ( 89 ). With the exception of a minor residual recognition of the Ala-variant L459A of the m145 E-phase peptide, which is paralleled by a still high constitutive proteasome combined processing score (Figure 4 A, upper panel), the recognition of IDEs was abolished by the C-terminal replacements with Ala.…”
Section: Resultsmentioning
confidence: 99%
“…A virus-specific cytolytic T lymphocyte (CTL) line specific for the D d -presented immunodominant viral epitope m164 Fink et al, 2014) was generated by four rounds of restimulation of CD8 + memory T cells, which were derived from the spleen of latently mCMV-infected female (sry − ) BALB/c mice, with the respective synthetic m164 peptide at a concentration of 10 −9 M Lemmermann et al, 2010). For cytoimmunotherapy of the infection, 1 × 10 6 CTL were infused intravenously together with the HC.…”
Section: Adoptive Cell Transfermentioning
confidence: 99%
“…Virus replication was quantitated on day 14, because group A recipients would die of multiple organ CMV disease and BM aplasia soon afterwards (Mutter et al, 1988). CTL specific for the m164 epitope of mCMV were chosen because the epitope is very special in that it is encoded by transcripts of the viral Early (E) phase gene ORFm164 as well as by a transcript from an upstream Immediate-Early (IE) phase gene (Fink et al, 2014;Renzaho et al, 2019). Accordingly, m164 epitope-specific CTL have the chance to recognize the corresponding D d -presented antigenic peptide on infected cells in the IE phase as well in the E phase of the viral replicative cycle, and this likely enhances the antiviral activity.…”
Section: Transfer Of Virus-specific Cd8 + T Cells Controls the Infectmentioning
confidence: 99%
“…We tried to address these points in our group over the past years and provided evidence strongly supporting the hypothesis that MI is driven by viral epitopes presented by latently infected host-tissue cells of non-hematopoietic origin (Seckert et al 2011;Torti et al 2011). We are currently investigating if mCMV gene m164, a second driver of MI in the H2 d haplotype (Holtappels et al 2002;Fink et al 2014), is also expressed in latency as a TEL.…”
Section: T Cell Bmemory Inflation^as a Results Of Latency-associated Gmentioning
confidence: 99%