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LepVax a defined subunit vaccine that provides effective pre-exposure and post-exposure prophylaxis of M. leprae infection

机译:LepVax一种确定的亚单位疫苗可提供有效的暴露前和暴露后预防麻风杆菌感染的方法

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摘要

Sustained elimination of leprosy as a global health concern likely requires a vaccine. The current standard, BCG, confers only partial protection and precipitates paucibacillary (PB) disease in some instances. When injected into mice with the T helper 1 (Th1)-biasing adjuvant formulation Glucopyranosyl Lipid Adjuvant in stable emulsion (GLA-SE), a cocktail of three prioritized antigens (ML2055, ML2380 and ML2028) reduced M. leprae infection levels. Recognition and protective efficacy of a single chimeric fusion protein incorporating these antigens, LEP-F1, was confirmed in similar experiments. The impact of post-exposure immunization was then assessed in nine-banded armadillos that demonstrate a functional recapitulation of leprosy. Armadillos were infected with M. leprae 1 month before the initiation of post-exposure prophylaxis. While BCG precipitated motor nerve conduction abnormalities more rapidly and severely than observed for control infected armadillos, motor nerve injury in armadillos treated three times, at monthly intervals with LepVax was appreciably delayed. Biopsy of cutaneous nerves indicated that epidermal nerve fiber density was not significantly altered in M. leprae-infected animals although Remak Schwann cells of the cutaneous nerves in the distal leg were denser in the infected armadillos. Importantly, LepVax immunization did not exacerbate cutaneous nerve involvement due to M. leprae infection, indicating its safe use. There was no intraneural inflammation but a reduction of intra axonal edema suggested that LepVax treatment might restore some early sensory axonal function. These data indicate that post-exposure prophylaxis with LepVax not only appears safe but, unlike BCG, alleviates and delays the neurologic disruptions caused by M. leprae infection.
机译:持续消除麻风病是全球对健康的关注,很可能需要疫苗。当前的BCG标准仅提供部分保护,在某些情况下会加剧丘脑(PB)疾病。当以稳定的乳剂(GLA-SE)将偏爱T辅助剂1(Th1)的佐剂Glucopyranosyl脂质佐剂注射到小鼠体内时,三种优先抗原(ML2055,ML2380和ML2028)的混合物降低了麻风杆菌的感染水平。在类似的实验中证实了掺入这些抗原的单个嵌合融合蛋白LEP-F1的识别和保护功效。然后,在暴露于麻风病的9条带状犰狳中评估暴露后免疫的影响。暴露后预防开始前1个月,犰狳感染了麻风杆菌。尽管BCG比对照感染的犰狳更迅速,更严重地引起运动神经传导异常,但每月用LepVax治疗3次的犰狳运动神经损伤明显延迟。皮肤神经活检表明,在麻风分枝杆菌感染的动物中,表皮神经纤维密度没有显着改变,尽管远端腿部皮肤神经的Remak Schwann细胞在被感染的犰狳中密度更高。重要的是,LepVax免疫并没有由于麻风支原体感染而加剧皮肤神经受累,表明其安全使用。没有神经内炎症,但轴突内水肿减轻表明LepVax治疗可恢复一些早期的感觉轴突功能。这些数据表明,用LepVax进行暴露后预防不仅看起来安全,而且与BCG不同,它可以缓解并延迟由麻风杆菌感染引起的神经系统破坏。

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