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Potential Impact of Microarray Diagnosis of T Cell–Mediated Rejection in Kidney Transplants: The INTERCOM Study
Authors:P. F. Halloran  A. B. Pereira  J. Chang  A. Matas  M. Picton  D. De Freitas  J. Bromberg  D. Serón  J. Sellarés  G. Einecke  J. Reeve
Affiliation:1. Alberta Transplant Applied Genomics Centre, University of Alberta, , Edmonton, AB, Canada;2. Department of Medicine, Division of Nephrology and Transplant Immunology, University of Alberta, , Edmonton, AB, Canada;3. Department of Nephrology, Santa Casa de Misericordia de Belo Horizonte, , Belo Horizonte, Brazil;4. School of Medicine, Federal University of Minas Gerais, , Belo Horizonte, Brazil;5. University of Minnesota, , Minneapolis, MN;6. Department of Renal Medicine, Manchester Royal Infirmary, , Manchester, England;7. University of Maryland School of Medicine, , Baltimore, MD;8. Servei de Nefrologia, Hospital Vall d'Hebron, , Barcelona, Spain;9. Medical School of Hannover, , Hannover, Germany;10. Department of Laboratory Medicine and Pathology, University of Alberta, , Edmonton, AB, Canada
Abstract:
We previously developed a microarray‐based test for T cell‐mediated rejection (TCMR) in a reference set of 403 biopsies. To determine the potential impact of this test in clinical practice, we undertook INTERCOM, a prospective international study of 300 indication biopsies from 264 patients ( ClinicalTrials.gov NCT01299168). Biopsies from six centers—Baltimore, Barcelona, Edmonton, Hannover, Manchester and Minneapolis—were analyzed by microarrays, assigning TCMR scores by an algorithm developed in the reference set and comparing TCMR scores to local histology assessment. The TCMR score correlated with histologic TCMR lesions—tubulitis and interstitial infiltration. The accuracy for primary histologic diagnoses (0.87) was similar to the reference set (0.89). The TCMR scores reclassified 77/300 biopsies (26%): 16 histologic TCMR were molecularly non‐TCMR; 15 histologic non‐TCMR were molecularly TCMR, including 6 with polyoma virus nephropathy; and all 46 “borderline” biopsies were reclassified as TCMR (8) or non‐TCMR (38). Like the reference set, discrepancies were primarily in situations where histology has known limitations, for example, in biopsies with scarring and inflammation/tubulitis potentially from other diseases. Neither the TCMR score nor histologic TCMR was associated with graft loss. Thus the molecular TCMR score has potential to add new insight, particularly in situations where histology is ambiguous or potentially misleading.
Keywords:Classifier  kidney transplant  microarrays  molecular diagnostics  T cell–  mediated rejection
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