Localization of Epstein-Barr virus cytotoxic T cell epitopes using recombinant vaccinia: implications for vaccine development.

Khanna, Rajiv; Burrows, Scott R.; Kurilla, Michael G.; Jacob, Catherine; Misko, Ihor S.; Sculley, T. B.; Kieff, E; Moss, Denis J.

doi:10.1084/jem.176.1.169

Cited by 359 publications

(237 citation statements)

References 27 publications

Supporting

Mentioning

233

Contrasting

Order By: Relevance

“…Human fetal thymic cells (containing 1  10 7 thymocytes, thymocytes: thymic epithelial cells and other stromal cells  1 : 1; immature and mature NKT cells were positively depleted) (17,18) were transplanted into thymi of anaesthetised SCID mice. The chimaeras were then intrathymically challenged with EBV (10 7 pfu) (14,21). The challenge was repeated once after 6 days.…”

Section: Human-thymus-scid Chimaeras and Humanised Xenogeneic Tumour-mentioning

confidence: 99%

EBV-Induced Human CD8+ NKT Cells Synergise CD4+ NKT Cells Suppressing EBV-Associated Tumours Upon Induction of Th1-Bias

Xiao

Zhou

et al. 2009

Cell Mol Immunol

View full text Add to dashboard Cite

Section: Human-thymus-scid Chimaeras and Humanised Xenogeneic Tumour-mentioning

confidence: 99%

EBV-Induced Human CD8+ NKT Cells Synergise CD4+ NKT Cells Suppressing EBV-Associated Tumours Upon Induction of Th1-Bias

Xiao

Zhou

et al. 2009

Cell Mol Immunol

View full text Add to dashboard Cite

“…Although blocking experiments were not undertaken in all patients investigated, the data obtained showed the same characteristics for the EBV-specific CTL response as reported for healthy individuals. [13][14][15] It can be substantially blocked by antibodies directed against CD3 or CD8, while anti-CD4 or anti-MHC class II show no effect, and the main effector cells are CD8-positive CTLs. MHC class I restriction is further underlined by experiments using EBNA-derived nonapeptides presented by autologous PHA blasts, which demonstrated that the EBV-directed CTLs recognize only the peptide known to be associated with HLA-B8 (therefore matching the patients HLA-haplotype), whereas another, HLA-A11-restricted EBV-peptide did not lead to a significant lysis.…”

Section: Discussionmentioning

confidence: 99%

“…11,12 This surveillance is based mainly on CD8-positive HLA-restricted memory T cells found in the peripheral blood of seropositive individuals which can be reactivated in vitro by challenge with autologous EBVinfected B cells. [13][14][15][16][17] In immunosuppressed individuals, reactivation of this latent EBV infection can lead to the outgrowth of EBV-transformed B lymphocytes with unregulated polyclonal or monoclonal lymphoproliferation, of which the latter has a rapidly progressive and uniformly fatal course. 18,19 For this reason, the EBV-directed CTL response has been carefully investigated after allogeneic BMT, where up to 30% of the recipients of allografts from mismatched or matched unrelated donors may develop EBV lymphoma.…”

mentioning

confidence: 99%

Assessment and characterization of the cytolytic T lymphocyte response against Epstein–Barr virus in patients with non-Hodgkin’s lymphoma after autologous peripheral blood stem cell transplantation

Nolte

Buhmann

Straka

et al. 1998

Bone Marrow Transplant

View full text Add to dashboard Cite

Summary:The cytolytic T lymphocyte (CTL) response has often been used to assess the reconstitution of T cell function after allogeneic or autologous bone marrow transplantation (BMT). Less is known, however, about the reconstitution of the CTL response after peripheral blood stem cell transplantation (PBSCT). Therefore, we investigated the CTL response against Epstein-Barr virus (EBV) of patients undergoing autologous PBSCT. CTLs of six patients with relapsed non-Hodgkin's lymphoma and multiple myeloma were established before and at different times after PBSCT by in vitro stimulation of peripheral blood lymphocytes with autologous EBVtransformed lymphoblastoid cell lines (LCLs). The efficiency of T cell priming by LCLs was assessed at the time of initiation of CTL lines; the proliferative response was strongly reduced during the first 4 months and increased 5 months or more following PBSCT. Cytolytic activity was measured after three or four restimulations of CTLs. All patients investigated had a detectable EBV-specific CTL response which was poor during the first weeks after transplantation, accompanied by a strong non-MHC-restricted cytotoxic activity and a high proportion of CD56-positive T cells. Five or more months after PBSCT, a specific CTL response against EBV was seen which was similar to the situation prior to PBSCT, while the unspecific cytotoxic response decreased. Blocking experiments with monoclonal anti-CD3, anti-CD8 or anti-MHC I antibodies resulted in substantial inhibition of autologous LCL lysis, whereas anti-CD4 or anti-MHC II antibodies had no effect. Finally, autologous PHA blasts of a patient with the HLA haplotype A1/9+, B5/8+, Cw4/7+, were loaded with various EBNA-derived nonapeptides known to be presented by HLA B8 or A11, and exposed to autologous, EBV-directed In the last few years, autologous peripheral blood stem cell transplantation (PBSCT) has been established as a standard treatment for relapsed aggressive non-Hodgkin's lymphoma and has proven advantageous when compared with autologous or allogeneic bone marrow transplantation (BMT). 1-5 However, in contrast to autologous or allogeneic BMT, little information is available concerning the reconstitution of the immune system following autologous peripheral blood stem cell transplantation (PBSCT). As after BMT, the CD4/CD8 ratio seems to be inversed after PBSCT, but lymphocyte subpopulations and functions recover more rapidly, including the proliferative response to mitogens and the cytotoxic activity of lymphocytes after stimulation with high-dose IL-2 (lymphocyte-activated killer cells, LAK). [6][7][8][9][10] Previous investigations mainly examined non-specific lymphocyte functions in patients undergoing autologous PBSCT and the reconstitution of the antigen-specific cytolytic T lymphocyte (CTL) response has not been evaluated so far. Therefore, we examined the CTL response of these patients to Epstein-Barr virus (EBV), a widespread lymphotropic herpes virus. Most people are infected with EBV by adulthood, and the life-long persist...

show abstract

“…45 The observation that the GAr does not inhibit priming of CTL is important and consistent with reports describing the presence of EBNA-1-specific CTL in EBV-seropositive individuals. [31][32][33][34][35][36] As antigen presentation by professional APC, most likely DC, is crucial to the initiation of virusspecific CTL responses, the presence of EBNA-1-specific CTL in EBV-positive donors suggests that antigen processing for MHC class I by specialized APC is not hampered by the GAr. In case EBV-specific CTL are induced through the direct route following EBV infection of DC, these observations would indicate that antigen presentation in DC differs intrinsically from presentation by 'nonprofessional' APC.…”

Section: Discussionmentioning

confidence: 99%

“…Although EBNA-1-specific CTL have been described in infectious mononucleosis patients and healthy carriers, they cannot recognize EBV-infected cells. [31][32][33][34][35][36] The failure to recognize endogenously expressed EBNA-1 has been attributed to the glycine-alanine repeat (GAr) domain in the EBNA-1 sequence that protects EBNA-1 from proteasomal degradation and subsequent presentation in the context of MHC class I. 37,38 This successful immune-evasion strategy points to the unique opportunity to hide cells expressing transgenes from CTLmediated target-cell destruction by incorporation of the GAr sequence into the transgene.…”

Section: Introductionmentioning

confidence: 99%

Creation of immune ‘stealth’ genes for gene therapy through fusion with the Gly-Ala repeat of EBNA-1

et al. 2003

View full text Add to dashboard Cite

A major obstacle in gene-therapy protocols is T-cellmediated destruction of transgene-expressing cells. Therefore new approaches are needed to prevent rapid clearance of transduced cells. We exploited the Gly-Ala repeat (GAr) domain of the Epstein-Barr virus nuclear antigen-1, since the GAr prevents cytotoxic T-lymphocyte-epitope generation. Here we show that three different enzymes (viz. the E. coli LacZ gene encoded b-galactosidase, firefly luciferase, and HSV1 thymidine kinase) fused with the GAr retained their function. Moreover, linking GAr with b-galactosidase successfully prevented recognition of GAr-LacZ-expressing cells by b-galactosidase-specific CTL. Nonetheless, vaccination with a GAr-LacZ adenovirus or with an allogeneic cell line expressing GAr-LacZ resulted in the induction of b-galspecific CTL. This demonstrates that the GAr domain does not inhibit crosspresentation of antigens, but only affects breakdown of endogenously synthesized proteins. These data demonstrate how the GAr domain can be exploited to create immuno'stealth' genes by hiding transgene products from CTL-mediated immune attack.

show abstract

Localization of Epstein-Barr virus cytotoxic T cell epitopes using recombinant vaccinia: implications for vaccine development.

Cited by 359 publications

References 27 publications

EBV-Induced Human CD8+ NKT Cells Synergise CD4+ NKT Cells Suppressing EBV-Associated Tumours Upon Induction of Th1-Bias

EBV-Induced Human CD8+ NKT Cells Synergise CD4+ NKT Cells Suppressing EBV-Associated Tumours Upon Induction of Th1-Bias

Assessment and characterization of the cytolytic T lymphocyte response against Epstein–Barr virus in patients with non-Hodgkin’s lymphoma after autologous peripheral blood stem cell transplantation

Creation of immune ‘stealth’ genes for gene therapy through fusion with the Gly-Ala repeat of EBNA-1

Contact Info

Product

Resources

About