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Clinical Trial Details — Status: Recruiting

Administrative data

NCT number NCT04239703
Other study ID # ATAGC05
Secondary ID
Status Recruiting
Phase
First received
Last updated
Start date December 1, 2019
Est. completion date December 2025

Study information

Verified date June 2024
Source University of Alberta
Contact Konrad S Famulski, PhD
Phone 1 780 492 1725
Email konrad@ualberta.ca
Is FDA regulated No
Health authority
Study type Observational

Clinical Trial Summary

Demonstrate the relationship between DD-cfDNA levels and HLA antibodies in blood, and the Molecular Microscope® (MMDx) Diagnostic System results in indication biopsies.


Description:

There is a need for better screening of kidney transplant patients for rejection. Patients with kidney transplants are routinely tested (creatinine, urine protein, histology and donor specific antibody (DSA) as standard of care to detect rejection, but these tests are not adequate. Rejection is often missed by these tests (false negatives) and other processes such as acute kidney injury can produce false-positive results. Moreover, histology has a high interobserver disagreement diagnosing rejection, and cannot accurately assess acute injury. A definitive molecular assessment of rejection and injury in kidney biopsies has emerged - the Molecular Microscope® Diagnostic System (MMDx) - developed by the Alberta Transplant Applied Genomics Centre, University of Alberta. Now a new screening test is being introduced: the monitoring of donor-derived cell-free DNA (DD-cfDNA) released in the blood by the kidney during rejection. The Natera Inc DD-cfDNA Prospera® test is based on the massively multiplex PCR that targets 13,392 single nucleotide polymorphisms and targeted sequences are quantified by Next Generation Sequencing. The Prospera® test done on kidney transplant recipients detected "active rejection" and differentiated it from borderline rejection and no rejection. It is likely, however, that DD-cfDNA test may miss some T cell-mediated rejection (TCMR) cases and the distinction between early and fully developed antibody-mediated rejection (ABMR) was not tested. No study has actually examined the DD-cfDNA results in kidney transplants with acute or chronic kidney disease (AKI and CKD). DD-cfDNA measurements have only been correlated with histology, a flawed standard. DD-cf-DNA test must now be calibrated against MMDx that is based on global gene expression, the new standard for biopsy interpretation. The present study will calibrate centrally measured (Natera Inc) DD-cfDNA levels obtained at the time of an indication biopsy against the MMDx measurements of TCMR, and ABMR (early-stage, fully-developed, and late-stage), AK, and atrophy-fibrosis. We will compare blood DD-cfDNA measurements in 600 samples at the time of 300 indication biopsies to the MMDx results, as well as central assessment of HLA antibody (One Lambda) in 300 blood samples, interpreted centrally as DSA based on the tissue typing results. This study is an extension of the INTERCOMEX ClinicalTrials.gov Identifier: NCT01299168. We have collected 1014 kidney biopsies and corresponding blood samples. Due to considerable interest from participating centers, we extend this study to the total of 1300 biopsies and 3900 blood samples.


Recruitment information / eligibility

Status Recruiting
Enrollment 300
Est. completion date December 2025
Est. primary completion date December 2024
Accepts healthy volunteers No
Gender All
Age group N/A and older
Eligibility Inclusion Criteria: - All kidney transplant recipients undergoing a kidney biopsy for clinical indications, as determined by their physician or surgeon, will be eligible to enroll in the study. Exclusion Criteria: - Patients will be excluded from the study if they decline participation or are unable to give informed consent or multiple organ recipients.

Study Design


Related Conditions & MeSH terms


Intervention

Diagnostic Test:
MMDx
Portion of kidney transplant indication biopsy
Prospera
Transplant patient blood sample
HLA antibody
Transplant patient blood sample

Locations

Country Name City State
Australia Department of Nephrology, The Royal Melbourne Hospital 1 South East Melbourne
Canada University of Alberta, Department of Medicine Edmonton Alberta
Canada ST. Paul's Hospital, 6A Providence Building, 1081 Burrard Street Vancouver British Columbia
Croatia University Hospital Merkur Renal Division Zagreb
Czechia Institute for Clinical and Experimental Medicine (IKEM) Prague
Germany Charite-Medical University of Berlin Department of Nephrology Berlin
Lithuania Centre of Nephrology, Vilnius University Hospital Santaros Klinikos Vilnius
Poland Department of Nephrology and Transplantation Medical University in Bialystok Bialystok
Poland University Hospital nr1 Bydgoszcz, Klinika Transplantologii Bydgoszcz
Poland Medical University of Gdansk Klinika Nefrologii Transplantologii i Chorób Wewnetrznych Gdansk
Poland Medical University of Silesia Katowice
Poland Department of Transplantation and General Surgery, Wojewodzki Hospital Poznan
Poland Department of Nephrology, Transplantation and Internal Medicine, University Hospital n.2 Szczecin
Poland Pomeranian Medical University, Samodzielny Publiczny Woj. Szpital Zespolony, Oddzial Nefrologii i Transplantacji Nerek Szczecin
Poland Medical University of Warsaw, Department of Transplantation Medicine, Nephrology and Internal Diseases Warsaw
Poland The Children's Memorial Health Institute, Department of Nephrology, Kidney Transplantation and Hypertension Warsaw
Poland Transplant Medicine & Nephrology Clinic, Medical University of Warsaw Warsaw
Poland Wroclaw Medical University, Department of Nephrology and Transplantation Medicine Wroclaw
Slovenia Department of Nephrology, University Medical Centre Ljubljana
Switzerland University Hospital Zurich Zürich
United States The Johns Hopkins University, School of Medicine Baltimore Maryland
United States University of Maryland School of Medicine Baltimore Maryland
United States Cleveland Clinic Cleveland Ohio
United States University Hospitals Cleveland Medical Ctr. Cleveland Ohio
United States Detroit Medical Center, Harper University Hospital of Wayne State University Detroit Michigan
United States Henry Ford Hospital Detroit Michigan
United States Intermountain Transplant Services Murray Utah
United States Virginia Commonwealth University Medical Center Richmond Virginia
United States Barnes-Jewish Hospital, Washington University at St. Louis Saint Louis Missouri
United States Division of Nephrology & UW Organ Transplant Center University of Washington Seattle Washington
United States Tampa General Hospital Tampa Florida

Sponsors (3)

Lead Sponsor Collaborator
University of Alberta Natera, Inc., One Lambda

Countries where clinical trial is conducted

United States,  Australia,  Canada,  Croatia,  Czechia,  Germany,  Lithuania,  Poland,  Slovenia,  Switzerland, 

References & Publications (6)

Gauthier PT, Madill-Thomsen KS, Demko Z, Prewett A, Gauthier P, Halloran PF; Trifecta-Kidney Investigators. Distinct Molecular Processes Mediate Donor-derived Cell-free DNA Release From Kidney Transplants in Different Disease States. Transplantation. 2024 — View Citation

Halloran PF, Madill-Thomsen KS, Reeve J. The Molecular Phenotype of Kidney Transplants: Insights From the MMDx Project. Transplantation. 2024 Jan 1;108(1):45-71. doi: 10.1097/TP.0000000000004624. Epub 2023 Dec 13. — View Citation

Halloran PF, Reeve J, Madill-Thomsen KS, Demko Z, Prewett A, Billings P; Trifecta Investigators. The Trifecta Study: Comparing Plasma Levels of Donor-derived Cell-Free DNA with the Molecular Phenotype of Kidney Transplant Biopsies. J Am Soc Nephrol. 2022 — View Citation

Halloran PF, Reeve J, Madill-Thomsen KS, Demko Z, Prewett A, Gauthier P, Billings P, Lawrence C, Lowe D, Hidalgo LG; the Trifecta Investigators. Antibody-mediated Rejection Without Detectable Donor-specific Antibody Releases Donor-derived Cell-free DNA: R — View Citation

Halloran PF, Reeve J, Madill-Thomsen KS, Kaur N, Ahmed E, Cantos C, Al Haj Baddar N, Demko Z, Liang N, Swenerton RK, Zimmermann BG, Van Hummelen P, Prewett A, Rabinowitz M, Tabriziani H, Gauthier P, Billings P; Trifecta Investigators*. Combining Donor-der — View Citation

Madill-Thomsen KS, Halloran PF. Precision diagnostics in transplanted organs using microarray-assessed gene expression: concepts and technical methods of the Molecular Microscope(R) Diagnostic System (MMDx). Clin Sci (Lond). 2024 Jun 5;138(11):663-685. doi: 10.1042/CS20220530. — View Citation

Outcome

Type Measure Description Time frame Safety issue
Primary Calibration of Prospera test for T cell-mediated rejection Calibration of DD-cfDNA test cut-off values against the probability of T cell-mediated rejection in the biopsy as reported by MMDx. 18 months
Primary Calibration of Prospera test for antibody-mediated rejection Calibration of DD-cfDNA test cut-off values against the probability of antibody-mediated rejection in the biopsy as reported by MMDx. 18 months
Primary Calibration of Prospera test for kidney injury Calibration of DD-cfDNA test cut-off values against the probability of acute and chronic kidney injury in the biopsy as reported by MMDx. 18 months
Primary Report calibrated Prospera test results for rejection Report new DD-cfDNA test cut-off values for rejection 6 months
Primary Report calibrated Prospera test results for kidney injury Report new DD-cfDNA test cut-off values for acute and chronic kidney injury 6 month
Secondary Determine if Prospera blood test can replace kidney biopsy test Determine if Prospera test, as calibrated by this DD-cfDNA-HLA-MMDx study, will avoid need for indication biopsy when kidney transplant function deteriorates. This will be based on the consensus between participating clinicians. 6 months
Secondary Assessment of donor-specific antibody status Report and compare the DSA status based on centralized and local HLA antibody measurement. 6 months
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