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© Northwestern University, NUTORC Discordant Serology and Nucleic Acid Testing Results for HIV, HBV and HCV in 2010 Nicole Theodoropoulos 1,3, Marek Nowicki 4, Claudia Chinchilla-Reyes 4, Carol Pancoska 5, Andres Jaramillo 6, Tom Mone 7, Rick Hasz 8, Martin D. Jendrisak 6, Daniela P Ladner 2,3, Michael G Ison 1-3 1 Divisions of Infectious Diseases and 2 Organ Transplantation, 3 Northwestern University Transplant Outcomes Research Collaborative, Northwestern University, 4 Mendez National Institute of Transplantation, 5 Labs Inc, 6 Gift of Hope Organ & Tissue Donor Network, 7 OneLegacy, 8 Gift of Life Donor Program American Transplant Congress – Boston, Massachusetts June 3, 2012
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© Northwestern University, NUTORC Disclosures I have no financial relationships to disclose within the past 12 months relevant to my presentation. I do not intend to reference unlabeled/unapproved uses of drugs or products in my presentation.
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© Northwestern University, NUTORC Background: Significant Organ Shortage Organ Transplants (2010)28,663 Current Waitlist Candidates114,425 Deaths on Waitlist (2010)~10,000 *Waiting list deaths includes removals for death, too sick to transplant, and those non-transplanted removals identified to have died within seven days of removal from linkage to SSDMF data. Based on OPTN data as of April 16, 2010. http://optn.transplant.hrsa.gov/
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© Northwestern University, NUTORC Background: Donor Screening Policy OPTN Policy 2.2: Donor Evaluation o Requires OPO to: Obtain a medical & social history of the donor Review the donor’s chart Perform a physical examination of the donor Perform FDA licensed, approved, or cleared screening tests Serology for: HIV, HCV, HBsAg, HBcAb, CMV, EBV, and syphilis Additional testing may be done at the discretion of the OPO or accepting transplant center OPTN Policy 4.1: Screening Donors for HIV o Prohibits the use of donors with + HIV test result o Defines a donor at “increased risk of HIV, HBV or HCV transmission” OPO must inform transplant center if the donor is increased risk Transplant Center must obtain special consent from the recipient to use organs from an increased risk donor http://optn.transplant.hrsa.gov/policiesAndBylaws/policies.asp Rogers et al. MMWR. 1994; 43(RR-8):1-17.
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© Northwestern University, NUTORC Background: Nucleic Acid Testing (NAT) NAT can detect recent infection NAT increasingly used for donor screening 3,4 Window Periods by assay type 1,2 1 Kucirka L et al. Am J Transplant 2011;11(6):1188-200. 2 Kucirka L et al. Am J Transplant 2011;11(6):1176-87. 3 Orlowski et al. Am J Transplant. 2009; 9: 555. 4 Thedoropoulos N et al. Abstract LB17. ATC 2012. VirusSerologyNAT HIV22 days9 days HBV44 days22 days HCV66 days7 days YearHIV NATHBV NATHCV NAT 200878% of OPOs34% of OPOs78% of OPOs 201193% of OPOs75% of OPOs95% of OPOs
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© Northwestern University, NUTORC Background: Nucleic Acid Testing (NAT) 1 Humar et al. Am J Transplant. 2010; 10: 889-899. Recent Consensus Conference reviewed issues related to use of NAT for donor screening 1 o Estimated the impact of false positive testing o Recommended NAT screening of increased risk donors and those with inadequate risk information only
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© Northwestern University, NUTORC Study Objectives To quantify the number of additional infections detected when NAT is added to routine serologic screening To attempt to quantify non-reproducibly positive NAT rates
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© Northwestern University, NUTORC Methods: Sites & Serologic Screening Screening data on all potential deceased organ donors was obtained from 3 US OPO-affiliated laboratories in 2010, representing: o 15 Organ Procurement Organizations o ~35% of the US Donor Pool All potential deceased organ donors were screened for HIV, HBV, and HCV according to current OPTN Policy o Genetic Systems HIV-1/HIV-2 plus O EIA ( Bio-Rad Laboratories ) o Genetic Systems HBsAg EIA 3.0 ( Bio-Rad Laboratories ) o ORTHO HBc ELISA Test System ( Ortho-Clinical Diagnostics, Inc. ) o ORTHO HCV Version 3.0 ELISA Test System ( Ortho-Clinical Diagnostics, Inc. ) o All assays performed according to the package insert
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© Northwestern University, NUTORC Methods: NAT Screening Lab ALab BLab C Year Initiated NAT2008 2004 Average NAT Volume 2 donors/week33 donors/week23 donors/week Assay SystemPCR TMA Donors ScreenedAll OPTN-defined increased risk donors All potential deceased organ donors* All potential deceased organ donors ConfirmationNone confirmedAt request of client As part of TMA assay Polymerase Chain Reaction (PCR) Assays o COBAS Ampliscreen HIV-1 Test Version 1.5, Roche Molecular Systems o COBAS Ampliscreen HCV Test Version 2.0, Roche Molecular Systems o COBAS HBV Ampliscreen, Roche Molecular systems* Transcription-Mediated Amplification (TMA) Assay o Procleix HIV-1/HCV Assay, Gen-Probe, Inc. *HBV NAT performed for all PDOD from 4/5 client OPOs
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© Northwestern University, NUTORC Results: Serologic Screening 22 donors positive for both HBsAg and HBcAb. Lab Total ScreenedHIV EIA +HBs Ag +HBc Ab +HCV Ab + A387101911 B1,760715193150 C1,83022213488 Total3,977 10 (0.3%) 37 (0.9%) 346 (8.7%) 249 (6.3%)
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© Northwestern University, NUTORC Results: NAT Screening LabHIV NATHBV NATHCV NAT A540 B1,7605011,760 C1,8100 Total Screened3,6245013,624 Total NAT Screening Volumes by Lab
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© Northwestern University, NUTORC Results: HIV NAT Screening HIVSerology +Serology - NAT +8 (0.2%)10 (0.3%) NAT -1 (0.03%)3,605 (99.5%)
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© Northwestern University, NUTORC Results: HIV NAT Non-Reproducible Results 10 HIV seronegative donors with + NAT o One PCR-based lab o 2/10 NAT were repeated and were found to be non- reproducibly positive (NRP) o The lab performed an extensive quality investigation Examination of the equipment and lab by the assay manufacturer Re-training of lab technicians Technician monitoring Machine sterilization No definite root cause was determined Lab changed to a TMA NAT platform Lab C used TMA for NAT o Built-in confirmatory step o All initial NAT + results were confirmed by discriminatory assay
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© Northwestern University, NUTORC Results: HBV NAT Screening HBVSerology +Serology - NAT +8 (0.9%)*0 NAT -60 (12%) ° 433 (86.4%) *4 isolated +HBcAb; 4 +HBsAg and +HBcAb ° 56/60 were isolated +HBcAb
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© Northwestern University, NUTORC Results: HCV NAT Screening HCVSerology +Serology - NAT +173 (4.8%)5 (0.1%) NAT -64 (1.8%) 3,382 (93.3%)
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© Northwestern University, NUTORC Conclusions NAT was positive in 15 (0.4%) seronegative donors All HIV antibody negative/NAT positive results resulted from one PCR-based lab o 20% were shown to be non-reproducibly positive o Built-in confirmatory step in the TMA NAT may account for fewer NRP results seen with this assay 1 Rapid and robust quality assurance is key 1.8% PODs screened were HCV Ab+/NAT – 12% PODs screened were HBV Ab+/NAT – o HBV Ab + and HCV Ab+ donors have variable utilization 2,3 o The use of NAT screening could improve utilization of HBV Ab + and HCV Ab + donor organs 1 Chinchilla-Reyes C et al. Abstract 387. ATC 2012. 2 Kucirka LM et al. Am J Transplant 2010 May;10(5):1238-46. 3 Taylor RM et al. Transplant Proc 2010;42:4479-87.
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© Northwestern University, NUTORC Future Directions We intend to ask OPOs to share their primary donor screening data We plan to link this data with OPTN donor data to determine o The true incidence of seronegative, NAT positive donors o The effect of NAT screening on organ utilization o The false positive rates of NAT in the deceased organ donor population o The effect of the type of NAT assay (PCR vs TMA) on false positive results All donor screening results should be collected in a national database
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© Northwestern University, NUTORC Questions? Nicole Theodoropoulos, MD 312-695-5054 n-theodoropoulos@md.northwestern.edu nicoletheo15@gmail.com
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