U.S. Army Medical Research Institute of Chemical Defense, Gunpowder, MD, 21010, USA.
BASF, Research Triangle, Durham, NC, 27709, USA.
Mol Med. 2022 Jun 3;28(1):61. doi: 10.1186/s10020-022-00487-4.
Botulinum neurotoxins (BoNTs) are highly potent, select agent toxins that inhibit neurotransmitter release at motor nerve terminals, causing muscle paralysis and death by asphyxiation. Other than post-exposure prophylaxis with antitoxin, the only treatment option for symptomatic botulism is intubation and supportive care until recovery, which can require weeks or longer. In previous studies, we reported the FDA-approved drug 3,4-diaminopyridine (3,4-DAP) reverses early botulism symptoms and prolongs survival in lethally intoxicated mice. However, the symptomatic benefits of 3,4-DAP are limited by its rapid clearance. Here we investigated whether 3,4-DAP could sustain symptomatic benefits throughout the full course of respiratory paralysis in lethally intoxicated rats. First, we confirmed serial injections of 3,4-DAP stabilized toxic signs and prolonged survival in rats challenged with 2.5 LD BoNT/A. Rebound of toxic signs and death occurred within hours after the final 3,4-DAP treatment, consistent with the short half-life of 3,4-DAP in rats. Based on these data, we next investigated whether the therapeutic benefits of 3,4-DAP could be sustained throughout the course of botulism by continuous infusion. To ensure administration of 3,4-DAP at clinically relevant doses, three infusion dose rates (0.5, 1.0 and 1.5 mg/kg∙h) were identified that produced steady-state serum levels of 3,4-DAP consistent with clinical dosing. We then compared dose-dependent effects of 3,4-DAP on toxic signs and survival in rats intoxicated with 2.5 LD BoNT/A. In contrast to saline vehicle, which resulted in 100% mortality, infusion of 3,4-DAP at ≥ 1.0 mg/kg∙h from 1 to 14 d after intoxication produced 94.4% survival and full resolution of toxic signs, without rebound of toxic signs after infusion was stopped. In contrast, withdrawal of 3,4-DAP infusion at 5 d resulted in re-emergence of toxic sign and death within 12 h, confirming antidotal outcomes require sustained 3,4-DAP treatment for longer than 5 d after intoxication. We exploited this novel survival model of lethal botulism to explore neurophysiological parameters of diaphragm paralysis and recovery. While neurotransmission was nearly eliminated at 5 d, neurotransmission was significantly improved at 21 d in 3,4-DAP-infused survivors, although still depressed compared to naïve rats. 3,4-DAP is the first small molecule to reverse systemic paralysis and promote survival in animal models of botulism, thereby meeting a critical treatment need that is not addressed by post-exposure prophylaxis with conventional antitoxin. These data contribute to a growing body of evidence supporting the use of 3,4-DAP to treat clinical botulism.
肉毒神经毒素(BoNTs)是高度有效的选择性毒素,可抑制运动神经末梢的神经递质释放,导致肌肉麻痹和窒息死亡。除了接触后使用抗毒素进行预防外,症状性肉毒中毒的唯一治疗选择是插管和支持性护理,直到康复,这可能需要数周或更长时间。在之前的研究中,我们报告了美国食品和药物管理局批准的药物 3,4-二氨基吡啶(3,4-DAP)可逆转早期肉毒中毒症状并延长致死性中毒小鼠的存活时间。然而,3,4-DAP 的症状益处受到其快速清除的限制。在这里,我们研究了 3,4-DAP 是否可以在致死性中毒大鼠的整个呼吸麻痹过程中维持症状益处。首先,我们证实了在接受 2.5 LD BoNT/A 挑战的大鼠中,连续注射 3,4-DAP 可稳定毒性体征并延长存活时间。最后一次 3,4-DAP 治疗后数小时内,毒性体征和死亡出现反弹,与 3,4-DAP 在大鼠中的半衰期短一致。基于这些数据,我们接下来研究了 3,4-DAP 的治疗益处是否可以通过连续输注在肉毒中毒过程中持续存在。为了确保以临床相关剂量给予 3,4-DAP,确定了三种输注剂量率(0.5、1.0 和 1.5 mg/kg·h),可产生与临床剂量一致的 3,4-DAP 稳态血清水平。然后,我们比较了 3,4-DAP 在接受 2.5 LD BoNT/A 中毒的大鼠中对毒性体征和存活的剂量依赖性影响。与生理盐水载体相比,后者导致 100%死亡率,从中毒后 1 天至 14 天以 3,4-DAP 输注 1.0 mg/kg·h 及以上剂量可产生 94.4%的存活率和完全缓解毒性体征,而在停止输注后无毒性体征反弹。相比之下,在 5 天时停止 3,4-DAP 输注会导致毒性体征重新出现,并在 12 小时内死亡,证实解毒剂的结果需要在中毒后持续给予 3,4-DAP 治疗超过 5 天。我们利用这种新型致命性肉毒中毒的存活模型来探索膈神经麻痹和恢复的神经生理参数。虽然在 5 天时神经传递几乎被消除,但在 3,4-DAP 输注的幸存者中,在 21 天时神经传递显著改善,尽管与未接触的大鼠相比仍有抑制。3,4-DAP 是第一种逆转全身瘫痪并促进肉毒中毒动物模型存活的小分子,从而满足了接触后预防常规抗毒素无法解决的关键治疗需求。这些数据为越来越多的支持使用 3,4-DAP 治疗临床肉毒中毒的证据做出了贡献。
