Donor Serostatus Has an Impact on Cytomegalovirus-Specific Immunity, Cytomegaloviral Disease Incidence, and Survival in Seropositive Hematopoietic Cell Transplant Recipients

Ugarte-Torres, Alejandra; Hoegh-Petersen, Mette; Liu, Yiping; Zhou, Feng; Williamson, Tyler; Quinlan, Dan; Sy, Sarah; Roa, Lina; Khan, Faisal; Fonseca, Kevin; Russell, James A.; Storek, Jan

doi:10.1016/j.bbmt.2010.07.020

Cited by 45 publications

(42 citation statements)

References 50 publications

(66 reference statements)

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“…The present results are consistent with reports from other transplant settings, in particular when ATG is administered as GvHD prophylaxis and when the donor is CMV seronegative; [11][12][13] similarly, the profound state of immune suppression here prevents or impairs the prompt recovery of anti-CMV immunity, this latter recently associated with a better protection from overall infections in the context of haplo-HSCT with PT-Cy. 14 Abbreviations: BM = bone marrow; HCT-CI = hematopoietic cell transplantation-specific comorbidity index; MAC = myeloablative conditioning; MDS = myelodisplastic syndrome; MPS = myeloproliferative syndrome; NMA = nonmyeloablative; RIC = reduced-intensity conditioning.…”

supporting

confidence: 81%

The patient’s CMV serological status affects clinical outcome after T-cell replete haplo-HSCT and post-transplant cyclophosphamide

Crocchiolo

Castagna

Fürst

et al. 2016

Bone Marrow Transplant

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supporting

confidence: 81%

The patient’s CMV serological status affects clinical outcome after T-cell replete haplo-HSCT and post-transplant cyclophosphamide

Crocchiolo

Castagna

Fürst

et al. 2016

Bone Marrow Transplant

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“…4 Furthermore, 60% of the cohort underwent myeloablative conditioning. Interestingly, our assertion that strategies that result in full donor chimerism might offer little antiviral protection in the context of R1/D2 transplants is supported by the clinical outcome data of these studies, 4,5 as well as by a smaller study that demonstrated persistence of recipient-derived CMV-specific T cells in T-deplete but not T-replete HSCT. 12 The latter study used an in vitro T-cell depletion strategy with Campath-1M plus complement, which results in depletion of mainly donor T cells while leaving recipient T cells intact.…”

Section: Discussionsupporting

confidence: 56%

“…This may explain the apparent discrepancy between our results and those in a large group of patients undergoing HSCT incorporating antithymocyte globulin. 5 Although reconstitution of CMV-specific T-cell immunity was slower in those with CMV seronegative donors, with a coincident increase in CMVrelated complications, almost 50% of the cohort developed clinically significant GvHD, and chimerism was fully donor in all evaluable R1/D2 patients by 3 months post-HSCT.…”

Section: Discussionmentioning

confidence: 99%

“…1,2 In high-risk cases in which the recipient is seropositive, this is likely to be the most prolonged when the donor is seronegative (D2), as immunity is then reliant on the development of a primary immune response. [3][4][5] After myeloablative conditioning, the establishment of protective immunity may be delayed still further by the incorporation of T-cell depletion strategies aimed at reducing the risk for graft-vs-host disease (GvHD).…”

Section: Introductionmentioning

confidence: 99%

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CMV promotes recipient T-cell immunity following reduced-intensity T-cell–depleted HSCT, significantly modulating chimerism status

Sellar

Vargas

Henry

et al. 2015

Blood

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Key Points• CMV serostatus significantly influences chimerism levels after T-cell-depleted allogeneic transplantation.• CMV-specific T cells are exclusively of recipient origin after R1/D2 T-cell-depleted transplants and appear to provide protective immunity.Cytomegalovirus (CMV) remains a significant cause of morbidity after allogeneic hematopoietic stem cell transplantation (HSCT). Clinical risk varies according to a number of factors, including recipient/donor CMV serostatus. Current dogma suggests risk is greatest in seropositive recipient (R1)/seronegative donor (D2) transplants and is exacerbated by T-cell depletion. We hypothesized that in the setting of reduced-intensity T-celldepleted conditioning, recipient-derived CMV-specific T cells escaping deletion may contribute significantly to CMV-specific immunity and might therefore also influence chimerism status. We evaluated 105 recipients of alemtuzumab-based reduced-intensity HSCT and collated details on CMV infection episodes and T-cell chimerism. We used CMV-specific HLA multimers to enumerate CMV-specific T-cell numbers and select cells to assess chimerism status in a subset of R1/D2 and R1/seropositive donor patients. We show that in R1/D2 patients, CMV-specific T cells are exclusively of recipient origin, can protect against recurrent CMV infections, and significantly influence the chimerism status toward recipients. The major findings were replicated in a separate validation cohort. T-cell depletion in the R1/D2 setting may actually, therefore, foster more rapid reconstitution of protective antiviral immunity by reducing graft-vs-host directed alloreactivity and the associated elimination of the recipient T-cell compartment. Finally, conversion to donor chimerism after donor lymphocytes is associated with clinically occult transition to donor-derived immunity. (Blood. 2015;125(4):731-739)

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“…None of the D-/R+ LTx patients included in this analysis developed CMV disease and only 5.9% developed CMV infection. The marked difference in the observed rates of CMV infection or disease between D-/R+ and D+/R+ patient may be related to R+ LTx patients having only partial immunity to the CMV strain carried by the D+ organ (17). Whereas recipients of D-organs have preexisting T cell-specific immunity to protect against reactivation of their native CMV strain, many recipients of D+ organs may require several months to develop T cell-specific immunity that confers protection against CMV superinfection by the donor strain.…”

Section: Discussionmentioning

confidence: 99%

Late-Onset Cytomegalovirus (CMV) in Lung Transplant Recipients: Can CMV Serostatus Guide the Duration of Prophylaxis?

Schoeppler

Lyu

Grazia

et al. 2013

American Journal of Transplantation

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Evidence supports the use of 12 months of cytomegalovirus prophylaxis in all at-risk lung transplants; whether cytomegalovirus serostatus can be used to further optimize this duration remains to be determined. The purpose of this retrospective study was to determine if cytomegalovirus serostatus of both donor and recipient were associated with lateonset cytomegalovirus. The primary outcome was the proportion of lung transplants that developed cytomegalovirus infection or disease during the 180-day period following 6 months of prophylaxis in each at-risk serotype. Two hundred forty-four consecutive lung transplants were evaluated, 131 were included.

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Donor Serostatus Has an Impact on Cytomegalovirus-Specific Immunity, Cytomegaloviral Disease Incidence, and Survival in Seropositive Hematopoietic Cell Transplant Recipients

Cited by 45 publications

References 50 publications

The patient’s CMV serological status affects clinical outcome after T-cell replete haplo-HSCT and post-transplant cyclophosphamide

The patient’s CMV serological status affects clinical outcome after T-cell replete haplo-HSCT and post-transplant cyclophosphamide

CMV promotes recipient T-cell immunity following reduced-intensity T-cell–depleted HSCT, significantly modulating chimerism status

Late-Onset Cytomegalovirus (CMV) in Lung Transplant Recipients: Can CMV Serostatus Guide the Duration of Prophylaxis?

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