Reconstitution of CD8 T Cells is Essential for the Prevention of Multiple-organ Cytomegalovirus Histopathology After Bone Marrow Transplantation

Overview

Journal J Gen Virol

Specialty Microbiology

Date 1998 Sep 25

PMID 9747717

Citations 69

Authors

J Podlech

R Holtappels

N Wirtz

H P Steffens

M J Reddehase

Affiliations

Soon will be listed here.

Abstract

Cytomegalovirus (CMV) infection in the period of temporary immunodeficiency after haematoablative treatment and bone marrow transplantation (BMT) is associated with a risk of graft failure and multiple-organ CMV disease. The efficacy of immune system reconstitution is decisive for the prevention of CMV pathogenesis after BMT. Previous data in murine model systems have documented a redundancy in the immune effector mechanisms controlling CMV. CD8 T cells proved to be relevant but not irreplaceable as antiviral effectors. Specifically, in a state of long-term in vivo depletion of the CD8 T-cell subset, CD4 T cells were educed to become deputy effectors controlling CMV by a mechanism involving antiviral cytokines. It is of medical importance to know whether one can trust in this 'flexible defence' in all clinical settings. It is demonstrated here that reconstitution of CD8 T cells is crucial for the prevention of fatal multiple-organ CMV disease under the specific conditions of BMT.

Citing Articles

Cytomegalovirus inhibitors of programmed cell death restrict antigen cross-presentation in the priming of antiviral CD8 T cells.

Ebert S, Bohm V, Buttner J, Brune W, Brinkmann M, Holtappels R PLoS Pathog. 2024; 20(8):e1012173.

PMID: 39146364 PMC: 11349235. DOI: 10.1371/journal.ppat.1012173.

Direct antigen presentation is the canonical pathway of cytomegalovirus CD8 T-cell priming regulated by balanced immune evasion ensuring a strong antiviral response.

Buttner J, Becker S, Fink A, Brinkmann M, Holtappels R, Reddehase M Front Immunol. 2023; 14:1272166.

PMID: 38149242 PMC: 10749961. DOI: 10.3389/fimmu.2023.1272166.

Immunotherapy of cytomegalovirus infection by low-dose adoptive transfer of antiviral CD8 T cells relies on substantial post-transfer expansion of central memory cells but not effector-memory cells.

Holtappels R, Becker S, Hamdan S, Freitag K, Podlech J, Lemmermann N PLoS Pathog. 2023; 19(11):e1011643.

PMID: 37972198 PMC: 10688903. DOI: 10.1371/journal.ppat.1011643.

B cells going viral in the CNS: Dynamics, complexities, and functions of B cells responding to viral encephalitis.

Cardani-Boulton A, Boylan B, Stetsenko V, Bergmann C Immunol Rev. 2022; 311(1):75-89.

PMID: 35984298 PMC: 9804320. DOI: 10.1111/imr.13124.

Memory CD8 T Cells Protect against Cytomegalovirus Disease by Formation of Nodular Inflammatory Foci Preventing Intra-Tissue Virus Spread.

Holtappels R, Podlech J, Freitag K, Lemmermann N, Reddehase M Viruses. 2022; 14(6).

PMID: 35746617 PMC: 9229300. DOI: 10.3390/v14061145.