Rocuronium-specific antibodies drive perioperative anaphylaxis but can also function as reversal agents in preclinical models

罗库溴铵 苏伽马德克斯 过敏反应 医学 抗体 药理学 免疫学 神经肌肉阻滞 麻醉 过敏 插管
作者
Alice Dejoux,Qianqian Zhu,Christelle Ganneau,Odile Richard,Ophélie Godon,Julien Lemaître,Francis Relouzat,François Huetz,Aurélien Sokal,Alexis Vandenberghe,Cyprien Pecalvel,Lise Hunault,Thomas Derenne,Caitlin M. Gillis,Bruno Iannascoli,Y Wang,Thierry Rose,Christel Mertens,P. Nicaise‐Roland,Patrick England
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:16 (764)
标识
DOI:10.1126/scitranslmed.ado4463
摘要

Neuromuscular blocking agents (NMBAs) relax skeletal muscles to facilitate surgeries and ease intubation but can lead to adverse reactions, including complications because of postoperative residual neuromuscular blockade (rNMB) and, in rare cases, anaphylaxis. Both adverse reactions vary between types of NMBAs, with rocuronium, a widely used nondepolarizing NMBA, inducing one of the longest rNMB durations and highest anaphylaxis incidences. rNMB induced by rocuronium can be reversed by the synthetic γ-cyclodextrin sugammadex. However, in rare cases, sugammadex can provoke anaphylaxis. Thus, additional therapeutic options are needed. Rocuronium-induced anaphylaxis is proposed to rely on preexisting rocuronium-binding antibodies. To understand the pathogenesis of rocuronium-induced anaphylaxis and to identify potential therapeutics, we investigated the memory B cell antibody repertoire of patients with suspected hypersensitivity to rocuronium. We identified polyclonal antibody repertoires with a high diversity among V(D)J genes without evidence of clonal groups. When recombinantly expressed, these antibodies demonstrated specificity and low affinity for rocuronium without cross-reactivity for other NMBAs. Moreover, when these antibodies were expressed as human immunoglobulin E (IgE), they triggered human mast cell activation and passive systemic anaphylaxis in transgenic mice, although their affinities were insufficient to serve as reversal agents. Rocuronium-specific, high-affinity antibodies were thus isolated from rocuronium-immunized mice. The highest-affinity antibody was able to reverse rocuronium-induced neuromuscular blockade in nonhuman primates with kinetics comparable to that of sugammadex. Together, these data support the hypothesis that antibodies cause anaphylactic reactions to rocuronium and pave the way for improved diagnostics and neuromuscular blockade reversal agents.
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