Autoantibodies against cytochrome P450s in sera of children treated with immunosuppressive drugs

S. Lytton, U. Berg, A. Németh, M. Ingelman-Sundberg
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引用次数: 22

Abstract

Treatment with the immunosuppressive drugs cyclosporin and tacrolimus, the mainstays of anti‐graft rejection and autoimmune disease therapy, is limited by their hepato‐ and nephrotoxicity. The metabolic conversion of these compounds to more easily excretable products is catalysed mainly by hepatic cytochrome P4503A4 (CYP3A4) but also involves extrahepatic CYP3A5 and other P450 forms. We set out to study whether or not exposure to cyclosporin and FK506 in children undergoing organ transplantation leads to formation of autoantibodies against P450s. Immunoblotting analysis revealed anti‐CYP reactivity in 16% of children on CyA for anti‐graft rejection or treatment of nephrosis (n = 67), 31% of kidney transplant patients switched from CyA to FK506 (n = 16), and 21% of kidney and or liver transplant patients on FK506 (n = 14). In contrast, the frequency of reactive immunoblots was only 8·5% among the normal paediatric controls (n = 25) and 7% among adult kidney transplant patients on CyA or FK506 (n = 30). The CYP2C9+ sera were able to immunoprecipitate in vitro translated CYP2C9 and the immunoblot reactivity showed striking correlation to peaks in the age at onset of drug exposure. Sera were isoform selective as evidenced from Western blotting using human liver microsomes and heterologously expressed human P450s. These findings suggest that anti‐cytochrome P450 autoantibodies, identified on the basis of their specific binding in immunoblots, are significantly increased among children on immunosuppressive drugs and in some cases are associated with drug toxicity and organ rejection.
免疫抑制药物治疗儿童血清抗细胞色素p450自身抗体的研究
免疫抑制药物环孢素和他克莫司是抗移植排斥反应和自身免疫性疾病治疗的主要药物,由于其肝和肾毒性而受到限制。这些化合物代谢转化为更容易排泄的产物主要由肝细胞色素P4503A4 (CYP3A4)催化,但也涉及肝外CYP3A5和其他形式的P450。我们着手研究接受器官移植的儿童暴露于环孢素和FK506是否会导致针对p450的自身抗体的形成。免疫印迹分析显示,16%接受CyA治疗的儿童(n = 67)具有抗CYP反应性,31%的肾移植患者从CyA转向FK506 (n = 16), 21%的肾和/或肝移植患者接受FK506 (n = 14)。相比之下,在正常儿童对照组(n = 25)中,反应性免疫印迹的频率仅为8.5%,在使用CyA或FK506的成人肾移植患者(n = 30)中,反应性免疫印迹的频率仅为7%。CYP2C9+血清能够免疫沉淀体外翻译的CYP2C9,免疫印迹反应性与药物暴露开始年龄的峰值有显著的相关性。通过使用人肝微粒体和异源表达的人p450进行Western blotting,证明了血清具有异构体选择性。这些发现表明,抗细胞色素P450自身抗体(基于其在免疫印迹中的特异性结合)在使用免疫抑制药物的儿童中显著增加,在某些情况下与药物毒性和器官排斥有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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