Understanding the Causes of Kidney Transplant Failure: The Dominant Role of Antibody-Mediated Rejection and Nonadherence

Sellarès, Joana; Freitas, D. G. de; Mengel, Michael; Reeve, J.; Einecke, G.; Sis, B.; Hidalgo, Luis; Famulski, Konrad S.; Matas, Arthur J.; Halloran, Philip F.

doi:10.1111/j.1600-6143.2011.03840.x

Cited by 1,320 publications

(1,214 citation statements)

References 37 publications

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“…Thus, it is important to define these survival issues in terms of actual phenotypes of failure, by studies attributing causality to observed kidney failures. In our attribution analysis (52), we found some kidneys that fail in the context of intercurrent medical illnesses, possibly explaining the impact of recipient age (and age-related comorbidities) on death censored late kidney loss as well as recipient death (52).…”

Section: Discussionmentioning

confidence: 99%

Comparing Molecular Assessment of Implantation Biopsies With Histologic and Demographic Risk Assessment

Kreepala

Famulski

Chang

et al. 2013

American Journal of Transplantation

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We hypothesized that measurement of previously defined acute kidney injury-induced transcripts at the time of implantation would add a new dimension to existing methods based on donor factors, histology and recipient factors. We analyzed microarray results from implantation biopsies taken after reperfusion from 70 kidneys from 53 deceased donors. We used two definitions of early dysfunction: serum creatinine > 265 umol/L at day 7 posttransplant; and dialysis in the first week. The strongest correlate with early dysfunction was the mean expression of 30 injury transcripts. Older donor and recipient age were associated with early dysfunction, but histologic lesions were not. Prediction was best when the injury transcript expression was combined with donor or recipient age, particularly in standard criteria donors. In contrast, although extended criteria donor kidneys had a high risk of early dysfunction, no variables tested, including injury transcripts, predicted risk significantly, probably because these kidneys were allocated preferentially to old, high risk recipients. The injury transcripts did not predict late function, which was mainly associated with donor age. Thus, measurement of injury-induced transcripts at the time of implantation improves the prediction of early kidney dysfunction, but risk prediction may fail when old kidneys are transplanted into old recipients.

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Section: Discussionmentioning

confidence: 99%

Comparing Molecular Assessment of Implantation Biopsies With Histologic and Demographic Risk Assessment

Kreepala

Famulski

Chang

et al. 2013

American Journal of Transplantation

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“…After censoring for death, however, similar findings remain, and it is likely that chronic alloimmune damage is a major cause of graft loss in this cohort as reported elsewhere. [28][29][30][31][32] Finally, HLA typing methods have evolved, such that the HLA antigens identified in one donor may be more fully resolved than the other donor or in the recipient. 33 Where this resolution discrepancy existed, we classified the antigens as equivalent.…”

Section: Discussionmentioning

confidence: 99%

Re-Examining Risk of Repeated HLA Mismatch in Kidney Transplantation

Tinckam

Rose

Hariharan

et al. 2016

JASN

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Kidney retransplantation is a risk factor for decreased allograft survival. Repeated mismatched HLA antigens between first and second transplant may be a stimulus for immune memory responses and increased risk of alloimmune damage to the second allograft. Historical data identified a role of repeated HLA mismatches in allograft loss. However, evolution of HLA testing methods and a modern transplant era necessitate re-examination of this role to more accurately risk-stratify recipients. We conducted a contemporary registry analysis of data from 13,789 patients who received a second kidney transplant from 1995 to 2011, of which 3868 had one or more repeated mismatches. Multivariable Cox proportional hazards modeling revealed no effect of repeated mismatches on all-cause or death-censored graft loss. Analysis of predefined subgroups, however, showed that any class 2 repeated mismatch increased the hazard of death-censored graft loss, particularly in patients with detectable panel-reactive antibody before second transplant (hazard ratio [HR], 1.15; 95% confidence interval [95% CI], 1.02 to 1.29). Furthermore, in those who had nephrectomy of the first allograft, class 2 repeated mismatches specifically associated with all-cause (HR, 1.30; 95% CI, 1.07 to 1.58) and death-censored graft loss (HR, 1.41; 95% CI, 1.12 to 1.78). These updated data redefine the effect of repeated mismatches in retransplantation and challenge the paradigm that repeated mismatches in isolation confer increased immunologic risk. We also defined clear recipient categories for which repeated mismatches may be of greater concern in a contemporary cohort. Additional studies are needed to determine appropriate interventions for these recipients. 27: 283327: -284127: , 201627: . doi: 10.1681 Kidney retransplantation is generally viewed to increase risk for immunologic damage and graft loss. The increased risk is attributed to the formation of T and B memory cells to mismatched HLA antigens in the original donors. Re-exposure to a repeated HLA antigen mismatched (RMM) in a subsequent donor potentially invokes alloimmune memory responses, resulting in earlier allograft damage and loss. J Am Soc NephrolThe nature and magnitude of this potential risk have changed with reanalysis over time. Whereas a number of studies have described worse allograft survival when repeated antigens are mismatched at the HLA-DR locus, 1-3 with RMM at class 1 (HLA-A or -B) not influencing outcomes, others have shown a beneficial effect of RMM on graft survival 4,5 or a neutral effect. 6,7 A more recent analysis showed an effect of class 1 RMM on graft survival, with no differences seen with class 2 RMM. 8

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“…However, ''IF/TA'' should only be diagnosed if the underlying etiology of fibrosis and tubular atrophy is not clear (5). With protocol biopsies and detailed clinical information a cause of graft dysfunction can be recognized in most cases, with the majority being due to chronic rejection (9,10,12,16). Therefore, within this review we will use not use the term IF/TA but rather discuss renal fibrosis in general given that there is little to no evidence that the allograft fibrosis as part of IF/TA or any other allograft pathology differs significantly from the fibrosis observed in other progressive diseases of native kidneys.…”

Section: Introductionmentioning

confidence: 99%

“…IF/TA is detectable in about 40% of kidney allografts at 3-6 months (6,7) and increases to about 65% at 2 years (8). IF/TA is a non-specific lesion induced by various immune and non-immune injuries to the graft (9,10) and an independent risk factor for late graft loss, particularly in grafts from expanded criteria donors, irrespective of whether a specific disease was diagnosed in the allograft or not (11)(12)(13)(14)(15). However, ''IF/TA'' should only be diagnosed if the underlying etiology of fibrosis and tubular atrophy is not clear (5).…”

Section: Introductionmentioning

confidence: 99%

Renal Allograft Fibrosis: Biology and Therapeutic Targets

Floege

2015

American Journal of Transplantation

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Understanding the Causes of Kidney Transplant Failure: The Dominant Role of Antibody-Mediated Rejection and Nonadherence

Cited by 1,320 publications

References 37 publications

Comparing Molecular Assessment of Implantation Biopsies With Histologic and Demographic Risk Assessment

Comparing Molecular Assessment of Implantation Biopsies With Histologic and Demographic Risk Assessment

Re-Examining Risk of Repeated HLA Mismatch in Kidney Transplantation

Renal Allograft Fibrosis: Biology and Therapeutic Targets

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