Kidney Graft Dysfunction Clinical Trial
Official title:
Impact of Acute and Chronic Individual Histological Lesions and Composite Scores in Implantation Biopsies on Short-term and Long-term Kidney Allograft Outcomes
The morphology of transplanted kidney is considered to be important for graft outcomes in early and late posttransplant period. Individual histological lesions at the time of kidney transplantation, such as sclerosis of glomeruli, vascular narrowing and interstitial fibrosis, and composite histological lesions, which integrate histopathological findings in different compartments, showed association with suboptimal graft outcomes. However there are no consistent association between individual or composite lesions and transplant outcomes. Some possible explanations for such inconsistent results are non-uniformity in grading histological lesions or in defining graft outcomes. Furthermore, studies vary in terms of patient selection, and some results are not corrected for covariates. It is also unclear, whether acute biopsy features associated with the donor kidney can provide prognostic information, in addition to the chronic lesions? This single-center study aimed to evaluate which acute and chronic histological lesions and composite histological scores in donor kidney intraoperative biopsies alone or in combination with clinical variables are best associated with short- and long-term kidney graft outcomes, such as impairment of early kidney allograft function, immunological acute kidney allograft rejection, pyelonephritis, allograft function at 1, 3, 6, 12 months, 2, 3, 4 and 5 years, and graft survival at 1 and 5 years.
130 consecutive patients with end-stage renal disease (ESRD), receiving a kidney only
transplant from April 2005 to December 2010 in a single center, and having both
intraoperative biopsies with ≥ 7 glomeruli and ≥ 1 arteries and complete follow-up data up
to 5 years were included in the study.
Intraoperative biopsy consisted of preimplant biopsy (at the backtable, 1 core) and
30-minutes postreperfusion biopsy (1 core), which were taken in order to study the impact of
ischemia/reperfusion injury on transplant outcomes and to serve a reference for subsequent
biopsies.
Donor population included live donors (32.6%), ideal deceased donors (50%),
expanded-criteria donors (7.9%) and 9.0% of non-heart-beating donors. Donors were subjected
to donor evaluation protocol in accordance with local guidelines, including a standard
clinical, instrumental and laboratory examination.
All recipients and donors were Caucasians.
Histological scoring Needle (14-18-gauge) biopsies were obtained and tissue was fixed in 10%
buffered formalin and embedded in paraffin. A 3-4 µm sections of preimplant and
postreperfusion kidney allograft implantation biopsies (KALIMBO) were stained for light
microscopy with hematoxylin-eosin (3 slides), periodic acid-Schiff (3 slides), and Masson's
trichrome (1 slide). A minimum of 21 tissue sections were examined for each biopsy.
Banff-1997 criteria for posttransplant biopsies, Banff-2016 criteria for preimplant
biopsies, as well as criteria suggested by Remuzzi et al. (1999) and Cosyns et al. (1998)
were applied for scoring.
Based on the estimation of individual acute and chronic lesions, the acute, chronic and
total posttransplant and preimplant Banff scores, Remuzzi score, and acute, chronic and
total lesion indexes by Cosyns were calculated. In addition, previously published composite
histological scores, such as chronic allograft damage index (CADI), donor damage score
(DDS), chronic damage score (CDS), and interstitial fibrosis and fibrous thickening score
(CIV) were computed.
Clinical risk factors and outcomes examined The analysis was performed 60 months later after
the last transplant in the study population. Donor, graft and recipient characteristics and
transplant outcomes were extracted from archival patient records and outpatient cards
blinded to all pathologic data. Data were retrieved on donor source, sex and age, and cause
of death, donation after cardiac death or expanded criteria donation for deceased donors.
Recipient's pretransplant variables included: age, gender, cause of ESRD, body mass index
(BMI), dialysis modality and duration, previous transplants, and presence of chronic
arterial hypertension, defined as a regular intake of antihypertensive drugs. The
information related to transplantation (cold ischemia time and second warm ischemia time)
was also obtained. Posttransplant data retrieved were limited to initial graft function
(immediate, delayed or slow), and the number and time of occurrence of acute rejection
episodes or pyelonephritis, and time of graft failure defined as return to dialysis therapy.
All recipients received triple maintenance immunosuppressive therapy consisting of
calcineurin-inhibitor (cyclosporine or tacrolimus), mycophenolate mofetil, and steroid. Each
patient, enrolled in this study, was followed for five years until death/return to dialysis
or until December 2015.
The end points of the study were impairment of early kidney allograft function,
immunological acute kidney allograft rejection, pyelonephritis, allograft function at 1, 3,
6, 12 months, 2, 3, 4 and 5 years, and graft survival at 1 and 5 years.
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Status | Clinical Trial | Phase | |
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Withdrawn |
NCT01492894 -
Kidney Allograft Dysfunction Without Reversible Causes
|
Phase 4 |