AI Article Synopsis
- Human cytomegalovirus (CMV) poses significant challenges for patients undergoing bone marrow and stem cell transplants, with a critical role played by CD8 T-lymphocytes in fighting the virus.
- The study utilized flow analysis and chromium release assays to examine CMV-specific CD8 T-lymphocytes in blood samples from transplant donors and recipients, noting differences in cytotoxicity and T-cell receptor repertoire.
- The researchers suggest that CMV reactivation in transplant recipients may enhance the functionality of CMV-specific CD8 T-lymphocytes, potentially influencing vaccine development for enhancing cellular immunity against CMV.
Article Abstract
Background: Human cytomegalovirus (CMV) is a ubiquitous herpesvirus that is an important complication of bone marrow and allogeneic stem-cell transplant (HSCT). CD8 T-lymphocytes have an important role in immunity against CMV, but correlation between antigen-specific subpopulations of these cells and protection are still unclear.
Methods: Flow analysis with fluorescently-conjugated human leukocyte antigen (HLA) class I tetramers (Tet) was used to investigate levels of CMV-specific CD8 T-lymphocytes in peripheral blood monocyte cells (PBMC) samples from HSCT donors and recipients and their ability to produce interferon (IFN)-gamma on stimulation with either CMV antigenic peptide or nonspecific mitogenic stimulation. Chromium release assays were used to evaluate ex vivo CMV-specific cytotoxicity associated with the PBMC samples.
Results: Use of Tet in conjunction with fluorescently conjugated anti-T-cell receptor (TCR) beta-chain variable (Vbeta) monoclonal antibodies indicated that the Vbeta repertoires associated with Tet cells seen in two HSCT recipients were similar to the Vbeta repertoires of the Tet cells in their HSCT donors. Significant ex vivo cytotoxicity against peptide-loaded targets was measured from several recipient samples after transplant. However, PBMC from the HSCT donors, even when containing populations of CMV-specific Tet cells capable of secreting IFN-gamma in response to peptide stimulation, possessed no ex vivo CMV-specific cytotoxicity.
Conclusions: We hypothesize that in the setting of the reconstituting immune system of HSCT recipients, CMV reactivation may stimulate a functional change in CMV-specific CD8 T-lymphocytes, rendering them able to directly lyse target cells presenting CMV antigens without in vitro stimulation. These findings have important implications for development of vaccines designed to induce protective cellular immunity to CMV in transplant recipients.
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| http://dx.doi.org/10.1097/00007890-200209150-00023 | DOI Listing |
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