Class II Human Leukocyte Antigen Epitope Mismatch Predicts De Novo Donor‐Specific Antibody Formation After Liver Transplantation

Kubal, Chandrashekhar A.; Mangus, Richard S.; Ekser, Burçin; Mihaylov, Plamen; Ceballos, Brian; Higgins, Nasra; Chalasani, Naga; Ghabril, Marwan; Nephew, Lauren; Lobashevsky, Andrew L.

doi:10.1002/lt.25286

Cited by 29 publications

(41 citation statements)

References 28 publications

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“…It is unknown whether unique effector functions of IgG4 subclass DSA in the presence of higher HLA expression directly contributed to the subclinical histopathology phenotypes observed in these studies or whether a predominant IgG4 subclass serves solely as a biomarker of a prolonged smoldering humoral response. It is important to recall that higher HLA eplet mismatch loads were observed with DSA presence and strength, as previously reported,[31][32][33] and also with IgG4 subclass DSA. This is consistent with a scenario in which higher alloimmune burden drives DSA development and evolution over time to a more mature IgG4 humoral response.Our findings are consistent with other studies that have shown IgG4 DSA in recipients with chronically rejected kidney and liver allografts.…”

supporting

confidence: 76%

“…Patients with detectable class II DSA, compared to those without, had a higher median (interquartile range) total class II eplet mismatch (33 vs 26 ) and HLA-DQ alone mismatch (12 [8][9][10][11][12][13][14][15][16] vs 8 [4][5][6][7][8][9][10][11][12][13][14][15]). Similarly, total class II eplet mismatch was higher for those with MFI sum >20 000 vs ≤20 000 (40 [28-51] vs 28 [19][20][21][22][23][24][25][26][27][28][29][30][31][32][33][34][35]). Among subjects with class II DSA, total class II eplet mismatch was higher for those with maximum MFI > 20 000 vs ≤20 000 (39 vs 30 [21][22][23][24][25][26][27][28][29][30]…”

Section: Incidence and Strength Of Hla Class II Dsamentioning

confidence: 99%

“…Among subjects with class II DSA, total class II eplet mismatch was higher for those with maximum MFI > 20 000 vs ≤20 000 (39 [25-53] vs 30 [21][22][23][24][25][26][27][28][29][30][31][32][33][34][35][36][37][38][39][40]). Similarly, total class II eplet mismatch was higher for those with MFI sum >20 000 vs ≤20 000 (40 [28-51] vs 28 [19][20][21][22][23][24][25][26][27][28][29][30][31][32][33][34][35]). To further explore DSA attributes, which may aid in cluster prediction, we interrogated IgG subclass composition.…”

Section: Incidence and Strength Of Hla Class II Dsamentioning

confidence: 99%

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IgG4 donor-specific HLA antibody profile is associated with subclinical rejection in stable pediatric liver recipients

Jackson

Kanaparthi

Burrell

et al. 2020

American Journal of Transplantation

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The impact of donor-specific HLA antibody (DSA) following liver transplantation remains controversial. We hypothesized DSA IgG subclass characteristics, compared to total DSA IgG, might correlate with specific histopathological phenotype(s) of subclinical graft injury. We therefore studied 129 stable, arguably "clinically ideal," pediatric liver recipients at the time of a screening biopsy to enter an immunosuppression withdrawal trial. Sixty-five (50%) subjects tested positive for class II DSA.IgG subclass profile was characterized by mean fluorescence intensity (MFI) and normalized subclass composition (>5%). A prominent IgG4 DSA profile was strongly correlated with greater HLA mismatch, a histopathological phenotype characterized by the presence of interface activity (with variable degrees of fibrosis), and a transcriptional profile of attenuated T cell-mediated rejection. Specifically, compared to those without class II DSA, those with IgG4 class II DSA MFI sum >2000 exhibited an odds ratio (OR) of 20.79 (95% confidence interval [CI] 4.38-98.69) and IgG4 subclass composition >5% exhibited an OR of 8.99 (95% CI 2.70-29.9). Our data suggest that IgG4 DSA may serve as a useful biomarker to identify, among clinically and biochemically stable liver transplant recipients, a subset with histological and transcriptional features indicative of an active, suboptimally controlled alloimmune response. K E Y W O R D S alloantibody, clinical research/practice, histocompatibility, immunosuppressive regimensminimization/withdrawal, liver transplantation/hepatology, pediatrics, rejection: subclinical S U PP O RTI N G I N FO R M ATI O N Additional supporting information may be found online in the Supporting Information section. How to cite this article: Jackson AM, Kanaparthi S, Burrell BE, et al. IgG4 donor-specific HLA antibody profile is associated with subclinical rejection in stable pediatric liver recipients. Am

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supporting

confidence: 76%

Section: Incidence and Strength Of Hla Class II Dsamentioning

confidence: 99%

Section: Incidence and Strength Of Hla Class II Dsamentioning

confidence: 99%

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IgG4 donor-specific HLA antibody profile is associated with subclinical rejection in stable pediatric liver recipients

Jackson

Kanaparthi

Burrell

et al. 2020

American Journal of Transplantation

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“…The development of post‐transplant de novo DSA can occur in the absence of pretransplant HLA sensitization and has been shown to impact long‐term allograft survival. DSA that arises post‐transplant is primarily directed toward donor HLA class II mismatches and occurs in the setting of inadequate immunosuppression and/or increased HLA class II mismatching . The incidence of de novo DSA depends upon allograft type ranging from 12% in primary kidney transplants with a median time to development of 4 years and up to 30% in lung recipients within the first year post‐transplant .…”

Section: Antibodies In Organ Transplantationmentioning

confidence: 99%

B cells in transplant tolerance and rejection: friends or foes?

et al. 2019

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Our understanding of the role of B cells in organ transplantation remains incomplete and continues to grow. The majority of research has focused on the detrimental role of antibodies that drive the development of pathogenesis of the transplanted organ. However, it has been shown that not all donor-specific antibodies are harmful and in some circumstances can even promote tolerance through the mechanism of accommodation. Furthermore, B cells can have effects on transplanted organs through their interaction with T cells, namely antigen presentation, cytokine production, and costimulation. More recently, the role and importance of Bregs was introduced to the field of transplantation. Due to this functional and ontogenetic heterogeneity, targeting B cells in transplantation may bring undesired immunologic side effects including increased rejection. Therefore, the selective control of B cells that contribute to the humoral response against donor antigens will continue to be an important and challenging area of research and potentially lead to improved long-term transplant outcomes.

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“…Considerable research has been devoted to investigating the impact of the number of eplet mismatches between donor and recipient on HLA antibody formation and graft survival. Patients who were transplanted with a higher number of mismatched eplets have a higher risk for donor-specific HLA antibody formation after transplantation (Daniels et al 2018;Duquesnoy et al 2008a;Kubal et al 2018;McCaughan et al 2018;Walton et al 2018;Wiebe et al 2013). Moreover, additional studies suggest that matching based on the number of eplets may lead to an improved graft outcome in kidney (Wiebe et al 2013), heart (Sullivan et al 2015), lung (Walton et al 2016), liver (Ekong et al 2019), and cornea transplantation (Bohringer et al 2010).…”

Section: Introductionmentioning

confidence: 99%

PIRCHE-II: an algorithm to predict indirectly recognizable HLA epitopes in solid organ transplantation

Geneugelijk

Spierings

2019

Immunogenetics

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Human leukocyte antigen (HLA) mismatches between donors and recipients may lead to alloreactivity after solid organ transplantation. Over the last few decades, our knowledge of the complexity of the HLA system has dramatically increased, as numerous new HLA alleles have been identified. As a result, the likelihood of alloreactive responses towards HLA mismatches after solid organ transplantation cannot easily be assessed. Algorithms are promising solutions to estimate the risk for alloreactivity after solid organ transplantation. In this review, we show that the recently developed PIRCHE-II (Predicted Indirectly ReCognizable HLA Epitopes) algorithm can be used to minimize alloreactivity towards HLA mismatches. Together with the use of other algorithms and simulation approaches, the PIRCHE-II algorithm aims for a better estimated alloreactive risk for individual patients and eventually an improved graft survival after solid organ transplantation.

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Class II Human Leukocyte Antigen Epitope Mismatch Predicts De Novo Donor‐Specific Antibody Formation After Liver Transplantation

Cited by 29 publications

References 28 publications

IgG4 donor-specific HLA antibody profile is associated with subclinical rejection in stable pediatric liver recipients

IgG4 donor-specific HLA antibody profile is associated with subclinical rejection in stable pediatric liver recipients

B cells in transplant tolerance and rejection: friends or foes?

PIRCHE-II: an algorithm to predict indirectly recognizable HLA epitopes in solid organ transplantation

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