Pollock-BarZiv Stacey M, den Hollander Neal, Ngan Bo-Yee, Kantor Paul, McCrindle Brian, West Lori J, Dipchand Anne I
Department of Pediatrics, Division of Cardiology, The Hospital for Sick Children/University of Toronto, Toronto, Ontario, Canada.
Circulation. 2007 Sep 11;116(11 Suppl):I172-8. doi: 10.1161/CIRCULATIONAHA.107.709022.
There is an elevated risk for poor outcomes after heart transplant (HTx) in patients sensitized to human leukocyte antigens including graft dysfunction, acute cellular and antibody-mediated (AMR) rejection, and cardiac allograft vasculopathy. We report our experience with human leukocyte antigens-sensitized pediatric HTx recipients.
We identified pediatric HTx patients with elevated pre-HTx Panel Reactive Antibody (Class I/II; > 10%), or a positive T- or B-cell crossmatch. Thirteen patients met criteria (5 female, 39%). The median age at HTx was 7 months (3.5 months to 15.5 years). Nine were infants who had prior palliation for congenital heart disease. Four were older patients (median 7.3 years; 4.8 to 15.5 years): 2 had congenital heart disease (Fontan), 2 were re-HTx. B-cell therapies were used in all patients, guided by assessment of CD19+ and CD20+ cells. Immunosuppression included thymoglobulin induction, and tacrolimus, mycophenolate mofetil, and steroids. Daily plasmapheresis +/- intravenous immunoglobulin G was used if there was a positive crossmatch on day 1, with a gradual, biopsy-guided weaning schedule. Rituximab was used when AMR was detected on biopsy: more recently (n=3), used empirically perioperatively. AMR was confirmed in 9 patients within median 0.9 months post-HTx. Seven had early acute cellular rejection (> or = ISHLT Grade 2 R) with no hemodynamic compromise or graft dysfunction. There were 4 deaths post-HTx (range, 11 days to 9 months). The median follow-up of 9 survivors was 1.7 years (0.3 to 3.7 years). Of 7 patients > 6 months post-HTx, no AMR or cardiac allograft vasculopathy was observed at a mean of 1.9+1.1 years post-HTx and no cardiac allograft vasculopathy.
Despite aggressive management, acute cellular rejection and AMR occurred frequently early post-HTx. An algorithm of B cell-directed strategies can be effective in managing these patients with reasonable intermediate-term outcomes.
在对人类白细胞抗原致敏的患者中,心脏移植(HTx)后出现不良结局的风险升高,包括移植功能障碍、急性细胞性和抗体介导的(AMR)排斥反应以及心脏同种异体移植血管病变。我们报告了我们对人类白细胞抗原致敏的小儿心脏移植受者的经验。
我们确定了心脏移植前群体反应性抗体(I/II类;>10%)升高或T细胞或B细胞交叉配型阳性的小儿心脏移植患者。13例患者符合标准(5例女性,占39%)。心脏移植时的中位年龄为7个月(3.5个月至15.5岁)。9例为婴儿,曾因先天性心脏病接受过姑息治疗。4例为年龄较大的患者(中位年龄7.3岁;4.8至15.5岁):2例患有先天性心脏病(Fontan手术),2例为再次心脏移植。所有患者均采用B细胞疗法,以CD19+和CD20+细胞评估为指导。免疫抑制包括使用抗胸腺细胞球蛋白诱导治疗,以及使用他克莫司、霉酚酸酯和类固醇。如果第1天交叉配型呈阳性,则每日进行血浆置换并酌情加用静脉注射免疫球蛋白G,并采用逐步的、活检指导的撤药方案。当活检检测到AMR时使用利妥昔单抗:最近(n = 3),在围手术期经验性使用。9例患者在心脏移植后中位0.9个月内确诊为AMR。7例患者发生早期急性细胞排斥反应(≥ISHLT 2R级),无血流动力学损害或移植功能障碍。心脏移植后有4例死亡(范围为11天至9个月)。9例存活者的中位随访时间为1.7年(0.3至3.7年)。在心脏移植后>6个月的7例患者中,在心脏移植后平均1.9±1.1年时未观察到AMR或心脏同种异体移植血管病变。
尽管采取了积极的管理措施,但急性细胞排斥反应和AMR在心脏移植后早期仍频繁发生。一种针对B细胞的策略算法在管理这些患者方面可能有效,并能取得合理的中期结局。
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