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首页> 外文期刊>Dermatology and Therapy >Association Between Secondary Botulinum Toxin?A Treatment Failure in Cosmetic Indication and Anti-Complexing Protein Antibody Production
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Association Between Secondary Botulinum Toxin?A Treatment Failure in Cosmetic Indication and Anti-Complexing Protein Antibody Production

机译:二次肉毒杆菌毒素之间的关系?化妆品指示和抗络蛋白抗体生产中的治疗失败

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IntroductionBotulinum toxin?A (BoT/A) treatment failure (BTF) affects patients subjected to repeated BoT/A exposure for cosmetic indications. BoT/A’s general formulation contains core BoT/A and complexing proteins. BTF may be caused by antibody-induced treatment failure. Antibodies against core BoT/A can occur; however, anti-complexing protein antibodies have never been demonstrated, and tools for anti-complexing protein antibody detection have not been developed. The aim of this study was to evaluate immune involvement in BoT/A-nonresponsive patients.MethodsPatients suspected of nonresponsiveness to BoT/A for cosmetic indications were recruited. All volunteers were categorized as BoT/A-responsive or BoT/A-tolerant according to frontalis testing with onabotulinumtoxinA (onaA). Twenty-two BoT/A-tolerant volunteers were recruited separately for frontalis testing with incobotulinumtoxinA (incoA). Anti-BoT/A and anti-complexing protein antibodies were quantified by special ELISA using sera from blood sampled before and after frontalis testing.ResultsSignificantly higher levels of IgG against complexing protein were detected in onaA-tolerant sera but not in onaA-responders, leading to proposals that anti-complexing protein antibodies could cause onaA unresponsiveness. Some onaA-tolerant patients according to frontalis test with incoA were responsive to incoA. Newly developed absorption ELISA confirmed that incoA-responsive sera predominantly contained IgG against complexing proteins, whereas incoA-tolerant sera contained significant levels of IgG against core BoT/A. The presence of anti-complexing protein antibodies higher than 90.75% in sera of onaA-tolerant patients could respond to incoA. The ELISA technique might be employed as a tool to predict incoA responsiveness. Our frontalis testing after incoA treatment showed that anti-incoA IgG levels were not increased by incoA.ConclusionsBoT/A-exposed patients may develop antibodies against core botulinum toxin and complexing proteins. Our study is the first to demonstrate that anti-complexing protein antibodies cause BTF. High levels of antibodies against complexing proteins can cause onaA unresponsiveness, although some patients were still incoA-responsive. Our developed ELISA to detect anti-complexing protein antibodies can determine whether onaA-tolerant patients respond to incoA without incoA frontalis testing.
机译:介绍植物毒素?A(BOT / A)治疗失败(BTF)影响患者对化妆品指示的重复BOT /暴露的患者。 BOT / A的一般配方含有核心机器人/ A和络合蛋白。 BTF可能是由抗体诱导的治疗失败引起的。可能发生针对核心机器人/ A的抗体;然而,从未证明抗络蛋白抗体,并且尚未开发用于抗络蛋白抗体检测的工具。本研究的目的是评估BOT / A-An-Nonrevigensive患者的免疫参与。招募了涉嫌非响应性的非响应性的植物态度/ A用于化妆注目的患者。所有志愿者按照与OnaboTulinumtoxina(ONAA)的骨前测试进行分类为BOT / A响应或机器人/耐用性。用Incobotulinumtoxina(incoa)分别招募二十二个机器人/耐受志愿者。通过特殊的ELISA定量抗BOT / A和抗络蛋白抗体,使用Frontalis检测前后的血液中的血清量化。在耐受血清中检测到对络合蛋白的血糖中较高水平的IgG水平,但不在onaa-respacters中,引领提出抗络合蛋白抗体可能导致ONAA反应性。根据incoa的额度前型试验的一些耐植物患者对incoa敏感。新开发的吸收ELISA证实,INCOA响应性血清主要含有IgG,反对络合蛋白,而耐氯酸型血清含有显着水平的IgG对核心机器人/ A.在耐荷荷奈血清中,抗络合蛋白抗体高于90.75%,可以对incoa进行响应。 ELISA技术可以作为预测INCOA响应性的工具。我们的刻录物治疗后的胸骨菌测试表明,incoa.clclusionsbot / a-pootos患者可能不会增加抗蛋解Igg水平可能会对核心毒素毒素和络合蛋白的抗体产生抗体。我们的研究是第一个证明抗络蛋白抗体导致BTF的研究。对络合蛋白的高水平抗体可导致ONAA无响应,尽管一些患者仍然是incOA响应。我们开发的ELISA检测抗络蛋白抗体可以确定ONAA耐受患者是否应对incOA而没有incoa前型测试。

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