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Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival

BACKGROUND: There is no consistent association between individual histological lesions and composite scores in donor kidney biopsy and transplant outcomes. OBJECTIVE: To evaluate which acute or chronic individual histological lesions and composite scores in donor kidney were associated with graft su...

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Autores principales: Trailin, A. V., Nykonenko, T. N., Ostapenko, T. I., Vildanov, S. R., Nykonenko, O. S.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Avicenna Organ Transplantation Institute 2019
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6416998/
https://www.ncbi.nlm.nih.gov/pubmed/30891166
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author Trailin, A. V.
Nykonenko, T. N.
Ostapenko, T. I.
Vildanov, S. R.
Nykonenko, O. S.
author_facet Trailin, A. V.
Nykonenko, T. N.
Ostapenko, T. I.
Vildanov, S. R.
Nykonenko, O. S.
author_sort Trailin, A. V.
collection PubMed
description BACKGROUND: There is no consistent association between individual histological lesions and composite scores in donor kidney biopsy and transplant outcomes. OBJECTIVE: To evaluate which acute or chronic individual histological lesions and composite scores in donor kidney were associated with graft survival in the recipient. METHODS: We investigated the association of individual histological lesions and 8 composite scoring systems in implantation biopsies of cadaveric (n=101) and living (n=29) kidneys with 5-year death-censored graft survival. RESULTS: We found a high frequency of chronic lesions in donor kidneys, mostly associated with arteriosclerosis, and less dependent from donor age. Acute, chronic, and total Banff scores for post-transplant biopsies, chronic and total Banff scores for pre-implant biopsies, donor damage score and chronic damage score predicted death-censored graft loss. However, only chronic and total Banff-scores had significant effects in multivariate model. Chronic pre-implant and total post-transplant Banff scores demonstrated the highest area under the curve (AUC) of 0.722 and 0.717, respectively. Among individual lesions, glomerulosclerosis ≥20%, interstitial inflammation >0, arteriosclerosis =3, arteriolar hyalinosis >0, and interstitial fibrosis >0, assessed with Banff-grading criteria, were associated with lower allograft survival. We created the Donor Kidney Damage Index (DKDI), by summing regression coefficients for these lesions, which yielded the AUC of 0.747. When combined with retransplantation, cold ischemia time and acute rejection, DKDI, chronic pre-implant and total post-transplant Banff scores further improved their predictive accuracy, yielding AUCs of 0.842, 0.807, and 0.802, respectively. CONCLUSION: DKDI, chronic pre-implant and total post-transplant Banff scores alone and combined with clinical variables may facilitate decision making in post-transplant period.
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spelling pubmed-64169982019-03-19 Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival Trailin, A. V. Nykonenko, T. N. Ostapenko, T. I. Vildanov, S. R. Nykonenko, O. S. Int J Organ Transplant Med Original Article BACKGROUND: There is no consistent association between individual histological lesions and composite scores in donor kidney biopsy and transplant outcomes. OBJECTIVE: To evaluate which acute or chronic individual histological lesions and composite scores in donor kidney were associated with graft survival in the recipient. METHODS: We investigated the association of individual histological lesions and 8 composite scoring systems in implantation biopsies of cadaveric (n=101) and living (n=29) kidneys with 5-year death-censored graft survival. RESULTS: We found a high frequency of chronic lesions in donor kidneys, mostly associated with arteriosclerosis, and less dependent from donor age. Acute, chronic, and total Banff scores for post-transplant biopsies, chronic and total Banff scores for pre-implant biopsies, donor damage score and chronic damage score predicted death-censored graft loss. However, only chronic and total Banff-scores had significant effects in multivariate model. Chronic pre-implant and total post-transplant Banff scores demonstrated the highest area under the curve (AUC) of 0.722 and 0.717, respectively. Among individual lesions, glomerulosclerosis ≥20%, interstitial inflammation >0, arteriosclerosis =3, arteriolar hyalinosis >0, and interstitial fibrosis >0, assessed with Banff-grading criteria, were associated with lower allograft survival. We created the Donor Kidney Damage Index (DKDI), by summing regression coefficients for these lesions, which yielded the AUC of 0.747. When combined with retransplantation, cold ischemia time and acute rejection, DKDI, chronic pre-implant and total post-transplant Banff scores further improved their predictive accuracy, yielding AUCs of 0.842, 0.807, and 0.802, respectively. CONCLUSION: DKDI, chronic pre-implant and total post-transplant Banff scores alone and combined with clinical variables may facilitate decision making in post-transplant period. Avicenna Organ Transplantation Institute 2019 2019-02-01 /pmc/articles/PMC6416998/ /pubmed/30891166 Text en
spellingShingle Original Article
Trailin, A. V.
Nykonenko, T. N.
Ostapenko, T. I.
Vildanov, S. R.
Nykonenko, O. S.
Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival
title Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival
title_full Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival
title_fullStr Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival
title_full_unstemmed Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival
title_short Significance of the Pathologic Findings in Implantation Biopsies for Kidney Allografts Survival
title_sort significance of the pathologic findings in implantation biopsies for kidney allografts survival
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6416998/
https://www.ncbi.nlm.nih.gov/pubmed/30891166
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