| Literature DB >> 29722117 |
Christopher J Rivard1, Tatsu Tanabe2, Miguel A Lanaspa1, Hironosuke Watanabe2, Shunichiro Nomura2, Ana Andres-Hernando1, Krystle Garth1, Mitsuhiro Sekijima3, Takuji Ishimoto1, Yuichi Ariyoshi2, Gabriela E Garcia1, Jigesh Shah3, Boyd Lennan2, Masayuki Tasaki3, Thomas Pomposelli2, Akira Shimizu3, David H Sachs2,3, Richard J Johnson1, Kazuhiko Yamada2.
Abstract
We have previously reported that co-transplantation of the kidney with vascularized donor thymus from α-1,3-galactosyltransferase gene knockout pigs with an anti-CD154 with rituximab-based regimen led to improved xenograft survival in baboons with donor-specific unresponsiveness. However, nephrotic syndrome emerged as a complication in which the glomeruli showed mild mesangial expansion with similarities to minimal change disease (MCD) in humans. Since MCD is associated with CD80 expression in glomeruli and elevated urinary excretion, we evaluated a potential role for CD80 in xenograft nephropathy. Study 1 confirmed high urinary CD80 excretion in nephrotic animals with renal xenografts showing CD80 expression in glomeruli. In Study 2, baboons receiving xenografts received CTLA4-Ig once a week from the second postoperative week or no CTLA4-Ig. The non-CTLA4-Ig group developed severe proteinuria with modest mesangial expansion with high urinary excretion of CD80 and documented CD80 expression in glomerular podocytes. All of the recipients in non-CTLA4-Ig groups had to be euthanized before POD 60. In contrast, CTLA4-Ig group showed a marked reduction in proteinuria and survived significantly longer, up to 193 days. These results demonstrate that anti-CD80 targeted therapy represents a promising strategy for reduction of proteinuria following renal xeno-transplantation with improved survival.Entities:
Keywords: CD80; kidney transplantation; large animal model; proteinuria; xenograft
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Year: 2018 PMID: 29722117 PMCID: PMC6407427 DOI: 10.1111/tri.13273
Source DB: PubMed Journal: Transpl Int ISSN: 0934-0874 Impact factor: 3.782