Early conversion to belatacept post-transplantation: state of the art and expert opinion

Johan Noble, Dany Anglicheau, Gilles Blancho, Dominique Bertrand, Lionel Couzi, Antoine Durrbach, Philippe Grimbert, Nassim Kamar, Yannick Le Meur, Bruno Moulin, Lionel Rostaing
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Abstract

The standard immunosuppressive treatment after organ transplantation typically includes a calcineurin inhibitor (tacrolimus or cyclosporine A), an antimetabolite (mycophenolic acid) or an mTOR inhibitor, and corticosteroids. However, these treatments are associated with multiple side effects, including nephrotoxicity. Belatacept, a fusion protein blocking the CD80/86 costimulation pathway, emerges as an effective and well-tolerated alternative. Initial phase III studies showed that de novo belatacept improves renal function and reduces the incidence of donor-specific antibodies, despite a higher rate of acute cellular rejections. Early conversion studies (within the first 6 months post-transplantation) demonstrate significant improvement in renal function, particularly when conversion is performed early. However, the risk of acute rejection and opportunistic infections must be monitored. This article summarizes the available studies on early conversion to belatacept in kidney transplanted patients.

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器官移植后的标准免疫抑制治疗通常包括钙神经蛋白抑制剂(他克莫司或环孢素 A)、抗代谢药(霉酚酸)或 mTOR 抑制剂以及皮质类固醇。然而,这些治疗方法都有多种副作用,包括肾毒性。贝拉替塞普(Belatacept)是一种阻断CD80/86成本刺激途径的融合蛋白,是一种有效且耐受性良好的替代疗法。最初的 III 期研究显示,尽管急性细胞排斥反应的发生率较高,但从头开始使用贝拉替塞能改善肾功能,降低供体特异性抗体的发生率。早期转换研究(移植后 6 个月内)显示,肾功能显著改善,尤其是在早期转换时。但是,必须监测急性排斥反应和机会性感染的风险。本文总结了有关肾移植患者早期转用贝拉替赛的现有研究。
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