The Histological Spectrum and Clinical Significance of T Cell–mediated Rejection of Kidney Allografts

Filippone, Edward J.; Farber, John L.

doi:10.1097/tp.0000000000004438

Cited by 4 publications

(1 citation statement)

References 103 publications

(240 reference statements)

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“…A common histological finding in renal transplant biopsies is mild allograft inflammation that does not meet the threshold for classification as acute rejection (AR), often termed “borderline rejection” (BL). 1 Most patients with BL can go on to achieve excellent long-term outcomes; however, a smaller subset are at risk of developing more extensive inflammation and early graft loss without intervention. There is currently no consensus on best management for these patients, presenting a clinical dilemma given the risks of unnecessary escalation of immunosuppression.…”

Section: Transitional B-cell Cytokines Risk Stratify Early Borderline...mentioning

confidence: 99%

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2023

Transplantation

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Section: Transitional B-cell Cytokines Risk Stratify Early Borderline...mentioning

confidence: 99%

Research Highlights

Short

Issa

2023

Transplantation

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Banff 2022 Kidney Commentary: Reflections and Future Directions

Rabant,

Adam,

Aubert

et al. 2024

Transplantation

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In September 2022, in Banff, Alberta, Canada, the XVIth Banff meeting, corresponding to the 30th anniversary of the Banff classification, was held, leading to 2 recent publications. Discussions at the Banff meeting focused on proposing improvements to the Banff process as a whole. In line with this, a unique opportunity was offered to a selected group of 16 representatives from the pathology and transplant nephrology community, experts in the field of kidney transplantation, to review these 2 Banff manuscripts. The aim was to provide an insightful commentary, to gauge any prospective influence the proposed changes may have, and to identify any potential areas for future enhancement within the Banff classification. The group expressed its satisfaction with the incorporation of 2 new entities, namely “microvascular inflammation/injury donor-specific antibodies–negative and C4d negative” and “probable antibody-mediated rejection,” into category 2. These changes expand the classification, facilitating the capture of more biopsies and providing an opportunity to explore the clinical implications of these lesions further. However, we found that the Banff classification remains complex, potentially hindering its widespread utilization, even if a degree of complexity may be unavoidable given the intricate pathophysiology of kidney allograft pathology. Addressing the histomorphologic diagnosis of chronic active T cell–mediated rejection (CA TCMR), potentially reconsidering a diagnostic-agnostic approach, as for category 2, to inflammation in interstitial fibrosis and tubular atrophy and chronic active T cell–mediated rejection was also an important objective. Furthermore, we felt a need for more evidence before molecular diagnostics could be routinely integrated and emphasized the need for clinical and histologic context determination and the substantiation of its clinical impact through rigorous clinical trials. Finally, our discussions stressed the ongoing necessity for multidisciplinary decision-making regarding patient care.

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Detection of Subclinical Rejection in Pediatric Kidney Transplantation: Current and Future Practices

Ettenger,

Seifert,

Blydt‐Hansen

et al. 2024

Pediatric Transplantation

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IntroductionThe successes in the field of pediatric kidney transplantation over the past 60 years have been extraordinary. Year over year, there have been significant improvements in short‐term graft survival. However, improvements in longer‐term outcomes have been much less apparent. One important contributor has been the phenomenon of low‐level rejection in the absence of clinical manifestations—so‐called subclinical rejection (SCR).MethodsTraditionally, rejection has been diagnosed by changes in clinical parameters, including but not limited to serum creatinine and proteinuria. This review examines the shortcomings of this approach, the effects of SCR on kidney allograft outcome, the benefits and drawbacks of surveillance biopsies to identify SCR, and new urine and blood biomarkers that define the presence or absence of SCR.ResultsSerum creatinine is an unreliable index of SCR. Surveillance biopsies are the method most utilized to detect SCR. However, these have significant drawbacks. New biomarkers show promise. These biomarkers include blood gene expression profiles and donor derived‐cell free DNA; urine gene expression profiles; urinary cytokines, chemokines, and metabolomics; and other promising blood and urine tests.ConclusionSpecific emphasis is placed on studies carried out in pediatric kidney transplant recipients.Trial Registration: ClinicalTrials.gov: NCT03719339

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The Histological Spectrum and Clinical Significance of T Cell–mediated Rejection of Kidney Allografts

Cited by 4 publications

References 103 publications

Research Highlights

Research Highlights

Banff 2022 Kidney Commentary: Reflections and Future Directions

Detection of Subclinical Rejection in Pediatric Kidney Transplantation: Current and Future Practices

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