Anti-complement 5 antibody ameliorates antibody-mediated rejection after liver transplantation in rats

被引:1
|
作者
Tajima, Tetsuya [1 ]
Hata, Koichiro [1 ]
Kusakabe, Jiro [1 ]
Miyauchi, Hidetaka [1 ]
Badshah, Joshua Sam [2 ]
Kageyama, Shoichi [1 ]
Zhao, Xiangdong [1 ]
Kim, Sung-Kwon [3 ]
Tsuruyama, Tatsuaki [4 ]
Kirchner, Varvara A. [2 ]
Watanabe, Takeshi [5 ]
Uemoto, Shinji [1 ,6 ]
Hatano, Etsuro [1 ]
机构
[1] Kyoto Univ, Grad Sch Med, Dept Surg, Div Hepatobiliary Pancreat Surg & Transplantat, Kyoto, Japan
[2] Stanford Univ, Dept Surg, Div Abdominal Transplantat, Sch Med, Stanford, CA USA
[3] Alexion Pharmaceut Inc, New Haven, CT USA
[4] Kyoto Univ, Grad Sch Med, Dept Drug Discovery Med, Pathol Div, Kyoto, Japan
[5] Kyoto Univ, Inst Frontier Life & Med Sci, Div Immunol, Kyoto, Japan
[6] Shiga Univ Med Sci, Otsu, Japan
来源
FRONTIERS IN IMMUNOLOGY | 2023年 / 14卷
关键词
antibody-mediated rejection (AMR); liver transplantation; complement; 5; eculizumab; donor-specific antibody (DSA); INHIBITOR ECULIZUMAB; ALLOGRAFT-REJECTION; HLA ANTIBODIES; IMPACT; DESENSITIZATION; PRESERVATION; GENERATION; APOPTOSIS; SURVIVAL; INNATE;
D O I
10.3389/fimmu.2023.1186653
中图分类号
R392 [医学免疫学]; Q939.91 [免疫学];
学科分类号
100102 ;
摘要
Antibody-mediated rejection (AMR) remains a refractory rejection after donor-specific antibody (DSA)-positive or blood-type incompatible liver transplantation (LT), even in the era of pre-transplant rituximab desensitization. This is due to the lack of not only effective post-transplant treatments but also robust animal models to develop/validate new interventions. Orthotopic LT from male Dark Agouti (DA) to male Lewis (LEW) rats was used to develop a rat LT-AMR model. LEW were pre-sensitized by a preceding skin transplantation from DA 4-6 weeks before LT (Group-PS), while sham procedure was performed in non-sensitized controls (Group-NS). Tacrolimus was daily administered until post-transplant day (PTD)-7 or sacrifice to suppress cellular rejections. Using this model, we validated the efficacy of anti-C5 antibody (Anti-C5) for LT-AMR. Group-PS+Anti-C5 received Anti-C5 intravenously on PTD-0 and -3. Group-PS showed increased anti-donor (DA) antibody-titers (P <0.001) and more C4d deposition in transplanted livers than in Group-NS (P <0.001). Alanine aminotransferase (ALT), alkaline phosphatase (ALP), total bile acid (TBA), and total bilirubin (T-Bil) were all significantly higher in Group-PS than in Group-NS (all P <0.01). Thrombocytopenia (P <0.01), coagulopathies (PT-INR, P =0.04), and histopathological deterioration (C4d+h-score, P <0.001) were also confirmed in Group-PS. Anti-C5 administration significantly lowered anti-DA IgG (P <0.05), resulting in decreased ALP, TBA, and T-Bil on PTD-7 than in Group-PS (all P <0.01). Histopathological improvement was also confirmed on PTD-1, -3, and -7 (all P <0.001). Of the 9,543 genes analyzed by RNA sequencing, 575 genes were upregulated in LT-AMR (Group-PS vs. Group-NS). Of these, 6 were directly associated with the complement cascades. In particular, Ptx3, Tfpi2, and C1qtnf6 were specific to the classical pathway. Volcano plot analysis identified 22 genes that were downregulated by Anti-C5 treatment (Group-PS+Anti-C5 vs. Group-PS). Of these, Anti-C5 significantly down-regulated Nfkb2, Ripk2, Birc3, and Map3k1, the key genes that were amplified in LT-AMR. Notably, just two doses of Anti-C5 only on PTD-0 and -3 significantly improved biliary injury and liver fibrosis up to PTD-100, leading to better long-term animal survival (P =0.02). We newly developed a rat model of LT-AMR that meets all the Banff diagnostic criteria and demonstrated the efficacy of Anti-C5 antibody for LT-AMR.
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页数:17
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