Non-invasive early detection of acute transplant rejection via nanosensors of granzyme B activity

被引:0
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作者
Quoc D. Mac
Dave V. Mathews
Justin A. Kahla
Claire M. Stoffers
Olivia M. Delmas
Brandon Alexander Holt
Andrew B. Adams
Gabriel A. Kwong
机构
[1] Georgia Tech College of Engineering and Emory School of Medicine,Wallace H. Coulter Department of Biomedical Engineering
[2] Emory University,Emory Transplant Center
[3] Emory University School of Medicine,Department of Surgery
[4] Parker H. Petit Institute of Bioengineering and Bioscience,The Georgia Immunoengineering Consortium
[5] Institute for Electronics and Nanotechnology,undefined
[6] Georgia Tech,undefined
[7] Integrated Cancer Research Center,undefined
[8] Georgia Tech,undefined
[9] Emory University and Georgia Tech,undefined
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The early detection of the onset of transplant rejection is critical for the long-term survival of patients. The diagnostic gold standard for detecting transplant rejection involves a core biopsy, which is invasive, has limited predictive power and carries a morbidity risk. Here, we show that nanoparticles conjugated with a peptide substrate specific for the serine protease granzyme B, which is produced by recipient T cells during the onset of acute cellular rejection, can serve as a non-invasive biomarker of early rejection. When administered systemically in mouse models of skin graft rejection, these nanosensors preferentially accumulate in allograft tissue, where they are cleaved by granzyme B, releasing a fluorescent reporter that filters into the recipient’s urine. Urinalysis then discriminates the onset of rejection with high sensitivity and specificity before features of rejection are apparent in grafted tissues. Moreover, in mice treated with subtherapeutic levels of immunosuppressive drugs, the reporter signals in urine can be detected before graft failure. This method may enable routine monitoring of allograft status without the need for biopsies.
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页码:281 / 291
页数:10
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