Original article
English
Ronald P Pelletier1, Gregg Hadley 1, Patrick Adams 1, Mitchell L Henry 1, Zhangsheng Yu 2, Ronald M Ferguson 1
1-Comprehensive Transplant Center, The Ohio State University Medical Centers, Columbus, Ohio 2-Division of Biostatistics, The Ohio State University College of Public Health
IJMBS 2009;1(1):7-15
Abstract
Background: Chronic renal allograft loss is considered as immunologically mediated when donor-specific alloantibodies are detected. However, remotely detected alloantibodies with lack of detection more proximate to graft loss occurrence may obscure the humoral association with graft damage.
Methods: We retrospectively reviewed 609 patients multiply tested post-transplant for detectable alloantibodies and correlated their results with clinical outcomes.
Results: Most patients had no detectable post-transplant alloantibodies (Group 1, n = 393), some converted from non-detectable to detectable alloantibodies (Group 2, n = 97), some always had detectable post-transplant alloantibodies (Group 3, n = 69), and some demonstrated alloantibodies that subsequently became undetectable (Group 4, n = 50). The incidence of death-censored graft survival for Group 4 patients was similar to Group 2 and 3 patients, and greater than Group 1 patients. Further, interstitial fibrosis/tubular atrophy (IF/TA) free survival was significantly worse (p=0.018) for Group 4 versus Group 1 recipients. Also, Group 4 versus Group 1 IF/TA-free survival was worse when recipients were regrouped based solely on anti-HLA class II (p=0.006), but not anti-HLA class I (p=ns) antibodies.
Conclusions: Detectable anti-HLA antibodies, even remotely, post-transplant identifies recipients at greater risk for IF/TA associated graft loss when compared to patients without detectable alloantibodies.
Keywords: Anti-HLA antibodies, chronic allograft nephropathy, IF/TA, graft failure.
Link/DOI: http://journals.sfu.ca/ijmbs/index.php/ijmbs/article/view/13/40