Cellular Immunity to Predict the Risk of Cytomegalovirus Infection in Kidney Transplantation: A Prospective, Interventional, Multicenter Clinical Trial

Jarque, Marta; Crespo, Elena; Melilli, Edoardo; Gutiérrez, A. Domínguez; Moreso, Francesc; Guirado, Lluís; Revuelta, Ignacio; Montero, Núria; Torrás, Joan; Riera, Lluı́s; Meneghini, Maria; Taco, Omar; Manonelles, Anna; Paúl, Javier; Serón, Daniel; Facundo, Carme; Vernet, Salvador Gil; Grinyó, Josep M.; Bestard, Oriol

doi:10.1093/cid/ciz1209

Cited by 49 publications

(75 citation statements)

References 29 publications

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“…A recent multicenter double-blind randomized clinical trial included adult kidney transplant recipients who were anti-CMV antibody donor positive / recipient positive prior to transplantation ( 44 ). This clinical trial used T-SPOT®.CMV and assigned SOT recipients into the interventional groups.…”

Section: Resultsmentioning

confidence: 99%

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Use of T Cell Mediated Immune Functional Assays for Adjustment of Immunosuppressive or Anti-infective Agents in Solid Organ Transplant Recipients: A Systematic Review

et al. 2020

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Background: Defining the optimal dosage of the immunosuppressive or duration of anti-infective agents is a challenge in solid organ transplant (SOT) recipients. We aimed to systematically review the literature regarding the use of T cell mediated immune functional assays (IFAs) for adjustment of the immunosuppressive or anti-infective agents in SOT recipients. Methods: We systematically searched PubMed, Scopus, EMBASE, Web of Science (WOS), Cochrane Central Register of Controlled Trials (CENTRAL), and ClinicalTrials.gov to find human interventional studies or study protocols that used either in-house or commercially available IFAs for adjustment of the immunosuppressive or anti-infective agents in SOT recipients. Results: We included six clinical trials and six study protocols. Four out of the six clinical trials used interferon-γ release assays for cytomegalovirus (IGRA-CMV), and five out of the six registered study protocols planned to use IGRA-CMV for adjustment of anti-CMV antiviral (Valganciclovir) prophylaxis or preemptive therapy in SOT recipients. Primary or secondary anti-CMV prophylaxes were discontinued in SOT recipients who had positive IGRA-CMV results without an increase in the rate of CMV infection or reactivation. Among other IFAs, one clinical trial used interferon-γ release assays for tuberculosis (IGRA-TB), and one study used ImmuKnow for adjustment of the duration and dosage of isoniazid and tacrolimus, respectively. Conclusion: Our systematic review supports a promising role for the IGRA-CMVs for adjustment of the duration of anti-CMV antiviral prophylaxis in SOT recipients. There are limited data to support the use of IFAs other than IGRA-CMVs for adjustment of Rezahosseini et al. Immune Functional Assays in SOT-Recipients immunosuppressive or anti-infective agents. Further multicenter randomized clinical trials using IFAs other than IGRA-CMVs may help in personalized immunosuppressive or prophylactic anti-infective therapy in SOT recipients.

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Section: Resultsmentioning

confidence: 99%

“…The cut-off to discriminate low- and high-risk SOT recipients were 20 spots per 300,000 PBMCs. Both low- and high-risk SOT recipients underwent randomization to receive either anti-CMV prophylaxis (for 3 months) or preemptive antiviral therapy ( 44 ). In addition, T-SPOT®.CMV was done 15 days post-transplantation in both groups.…”

Section: Resultsmentioning

confidence: 99%

Use of T Cell Mediated Immune Functional Assays for Adjustment of Immunosuppressive or Anti-infective Agents in Solid Organ Transplant Recipients: A Systematic Review

et al. 2020

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“…61 CMV peptides from the three following open reading frames (UL48, UL83, and UL123) are recognized by more than half of individuals. 48 Interestingly, IE-1 (UL123)-specific CD8 + T cells are associated with less CMV reactivation in SOTR, 62,63 probably because UL123 is the first CMV protein to be expressed in infected cells. In vitro, CMV-specific CD8 + T cells are able to exert antiviral effector functions trough interferon-γ (IFN-γ) production.…”

Section: Cmv-specific Cd8 + T Cellsmentioning

confidence: 99%

“…In patients undergoing CMV disease that are resistant to antiviral treatments, second-line therapies are associated with important adverse effects, and no other therapeutic option is currently available 5. Importantly, it has been shown that a quicker immune reconstitution of both αβ and γδ T cell compartments after HCT or a better quality of the αβ and γδ T cell responses in SOTR is correlated with a lower incidence of CMV infection and disease 34,63,[176][177][178]. These observations highlight the importance of an efficient cellular immune response for preventing CMV infection.Adoptive transfer of CMV-reactive T cells therefore represents an attractive approach in both HCTR and SOTR, in order to boost the cellular immune response and achieve long-term protection against CMV infection.…”

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confidence: 99%

“…(Immunotec),63,218 by Jarque and colleagues, and for pp-65 or IE1 at 40 IFN-γ spots/3.10 5 PBMC 219 (Immunotec).At the beginning of transplantation to predict the risk of CMV infection or diseaseIn D + R − patients, T-SPOT > 10 IFN-γ spots/3.10 5 PBMC was found in 30% of patients and was associated with a lower incidence of CMV infection, demonstrating that seronegative recipients could have a protective CMV-specific αβ T CMI 220. In R + patients, at day 0 and more predictively at day 15 post-transplantation, T-SPOT > 20 IFN-γ spots/3.10 5 PBMC for IE1 was highly associated with the absence of any CMV infection in patients who did not receive T-cell-depleting agents as induction therapy 63. Indeed, we have previously shown that R + patients with positive IE1 T-SPOT at day 0 of transplantation,…”

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Understanding human γδ T cell biology toward a better management of cytomegalovirus infection

Kaminski

Marsères

Cosentino

et al. 2020

Immunological Reviews

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is a 200-to 300-nm virus, which belongs to the beta herpes virus family. CMV seroprevalence ranges from 40% in Canada to 90% in Brazil and China. 1 Whereas it is almost asymptomatic in immunocompetent individuals, it is responsible for significant morbidity and mortality in immunocompromised patients and pregnant women. In solid organ transplant recipients (SOTR), hematopoietic cell transplant recipients (HCTR), or human immunodeficiency virus (HIV) patients, CMV causes a multiorgan disease with a large clinical spectrum, which has been well defined recently in the CMV Drug Development Forum. 2 During pregnancy, CMV

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Clinical and immunological characteristics for BK polyomavirus‐associated nephropathy after kidney transplantation

Siripoon,

Apiwattanakul,

Mongkolrattanakul

et al. 2023

Immunity Inflam & Disease

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IntroductionBK polyomavirus (BKPyV)‐associated nephropathy (BKPyVAN) can cause a significant risk of allograft impairment after kidney transplantation (KT). Intact BKPyV‐specific immunity is associated with viral containment. This study investigated BKPyV‐specific immunological factors among KT recipients.MethodsThis prospective study in a single transplant center from January 2019 to August 2019 assessed associations between clinical and immunological characteristics, with a focus on BKPyV‐cell‐specific immunity and BKPyVAN, among KT recipients aged ≥15 years. The numbers of interferon‐gamma (IFN‐γ)‐producing CD4+ T, CD8+ T, natural killer (NK), and natural killer T (NKT) cells were measured after stimulation with large T antigen and viral capsid protein 1 (VP1).ResultsIn total, 100 KT recipients were included (mean age ± SD, 42 ± 11 years); 35% of the recipients were female patients, and 70% had received induction immunosuppressive therapy. The 1‐year cumulative incidence of high‐level BKPyV DNAuria (possible BKPyVAN) and (presumptive BKPyVAN) was 18%. Among 40 patients with immunological factor data, pre‐KT %NK cells (hazard ratio [HR], 1.258; 95% confidence interval [CI], 1.077–1.469; p = .004) and %VP1‐specific NK cells (HR, 1.209; 95% CI, 1.055–1.386; p = .006) were factors independently associated with possible and presumptive BKPyVAN. KT recipients with possible and presumptive BKPyVAN were more likely to exhibit significant mean coefficients of %NK, %VP1‐specific NK, and %NKT cells at 1 month after KT than before KT (all p < .05).ConclusionIndividuals with nonspecific and VP1‐specific NK cells before KT and increasing numbers of these cells after KT may be at risk for high‐level BKPyV DNAuria and presumptive BKPyVAN. Further studies are needed to determine the utility of BKPyV‐specific innate immune surveillance in predicting the occurrence of BKPyVAN.

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Cellular Immunity to Predict the Risk of Cytomegalovirus Infection in Kidney Transplantation: A Prospective, Interventional, Multicenter Clinical Trial

Cited by 49 publications

References 29 publications

Use of T Cell Mediated Immune Functional Assays for Adjustment of Immunosuppressive or Anti-infective Agents in Solid Organ Transplant Recipients: A Systematic Review

Use of T Cell Mediated Immune Functional Assays for Adjustment of Immunosuppressive or Anti-infective Agents in Solid Organ Transplant Recipients: A Systematic Review

Understanding human γδ T cell biology toward a better management of cytomegalovirus infection

Clinical and immunological characteristics for BK polyomavirus‐associated nephropathy after kidney transplantation

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