| Literature DB >> 32342596 |
Laurie D Snyder1, John Belperio2, Marie Budev3, Courtney Frankel1, Jerry Kirchner4, Tereza Martinu5, Megan L Neely1, John M Reynolds1, Pali Shah6, Lianne G Singer5, Jamie L Todd1, Wayne Tsuang3, Samuel Weigt2, Scott M Palmer1.
Abstract
Long-term survival after lung transplant lags behind that of other commonly transplanted organs, reflecting the current incomplete understanding of the mechanisms involved in the development of posttransplant lung injury, rejection, infection, and chronic allograft dysfunction. To address this unmet need, 2 ongoing National Institute of Allergy and Infectious Disease funded studies through the Clinical Trials in Organ Transplant Consortium (CTOT) CTOT-20 and CTOT-22 were dedicated to understanding the clinical factors and biological mechanisms that drive chronic lung allograft dysfunction and those that maintain cytomegalovirus polyfunctional protective immunity. The CTOT-20 and CTOT-22 studies enrolled 800 lung transplant recipients at 5 North American centers over 3 years. Given the number and complexity of subjects included, CTOT-20 and CTOT-22 utilized innovative data transfers and capitalized on patient-entered data collection to minimize site manual data entry. The data were coupled with an extensive biosample collection strategy that included DNA, RNA, plasma, serum, bronchoalveolar lavage fluid, and bronchoalveolar lavage cell pellet. This Special Article describes the CTOT-20 and CTOT-22 protocols, data and biosample strategy, initial results, and lessons learned through study execution.Entities:
Keywords: clinical research/practice; infection and infectious agents - viral: cytomegalovirus (CMV); lung (allograft) function/dysfunction; lung transplantation/pulmonology; quality of life (QOL); rejection: acute; translational research/science
Mesh:
Year: 2020 PMID: 32342596 PMCID: PMC7323580 DOI: 10.1111/ajt.15957
Source DB: PubMed Journal: Am J Transplant ISSN: 1600-6135 Impact factor: 8.086