Background/Aims: The tumour necrosis factor (TNF)-2 promoter allele, which
elicits elevated expression of TNF-a, is in linkage disequilibrium with the
extended haplotype HLA-A1-B8-DR3-DQ2. TNF-2 and HLA-DR3 have been implicat
ed in renal and cardiac graft rejection and loss. Cytomegalovirus (CMV) inf
ection has been associated with chronic allograft rejection. We examined th
e relationship between HLA-DR3, promoter allele TNF-2 and cytomegalovirus i
n relation to chronic rejection following liver transplantation.
Methods: (i) Retrospective analysis of HLA-DR3 was performed in 307 liver t
ransplant recipients and 283 donors. (ii) Prospective analysis of TNF-ar pr
omoter allele status, HLA-DR3 status and cytomegalovirus infection was asse
ssed in 123 recipients.
Results: (i) Retrospective analysis, Recipient HLA-DR3 (relative risk 1.9;
95% C.I. 1.01-3.58) was a risk factor for chronic rejection, (ii) Prospecti
ve analysis. Recipient HLA-DR3 was a risk factor for chronic rejection (rel
ative risk 3.41; 95% C.I. 1.66-7.03) which was elevated further by superimp
osed CMV infection (relative risk 5.01; 95% C.I. 2-12.55). Recipient TNF-2
was associated,vith chronic rejection (relative risk 2.29; 95% C,I, 0.9-5.8
3) through linkage to HLA-DR3.
Conclusions: Recipient HLA-DR3, TNF-2 status and CMV infection were inter-r
elated risk factors for chronic rejection of liver grafts. (C) 2001 Europea
n Association for the Study of the Liver. Published by Elsevier Science B,V
, All rights reserved.