Vukicevic M, Fiorini E, Siegert S, Carpintero R, Rincon-Restrepo M, Lopez-Deber P, Piot N, Ayer M, Rentero I, Babolin C, Bravo-Veyrat S, Giriens V, Morici C, Beuzelin M, Gesbert A, Rivot S, Depretti S, Donati P, Streffer J, Pfeifer A, Kosco-Vilbois M H
AC Immune SA, Lausanne, Switzerland.
Biomedical Sciences, University of Antwerp, Antwerp, Belgium.
Brain Commun. 2022 Feb 4;4(1):fcac022. doi: 10.1093/braincomms/fcac022. eCollection 2022.
Pyroglutamate amyloid beta3-42 (pGlu-Abeta3-42), a highly amyloidogenic and neurotoxic form of Abeta, is N-terminally truncated to form a pyroglutamate and has recently been proposed as a key target for immunotherapy. Optimized ACI-24, a vaccine in development for the treatment and prevention of Alzheimer's disease, focuses the antibody response on the first 15 N-terminal amino acids of Abeta (Abeta1-15). Importantly, clinical data with an initial version of ACI-24 incorporating Abeta1-15, established the vaccine's safety and tolerability with evidence of immunogenicity. To explore optimized ACI-24's capacity to generate antibodies to pGlu-Abeta3-42, pre-clinical studies were carried out. Vaccinating mice and non-human primates demonstrated that optimized ACI-24 was well-tolerated and induced an antibody response against Abeta1-42 as expected, as well as high titres of IgG reactive with pyroGlu-Abeta. Epitope mapping of the polyclonal response confirmed these findings revealing broad coverage of epitopes particularly for Abeta peptides mimicking where cleavage occurs to form pGlu-Abeta3-42. These data are in striking contrast to results obtained with other clinically tested Abeta targeting vaccines which generated restricted and limited antibody diversity. Taken together, our findings demonstrate that optimized ACI-24 vaccination represents a breakthrough to provide a safe immune response with a broader Abeta sequence recognition compared to previously tested vaccines, creating binders to pathogenic forms of Abeta important in pathogenesis including pGlu-Abeta3-42.
焦谷氨酸淀粉样蛋白β3-42(pGlu-Aβ3-42)是Aβ的一种高度淀粉样变性和神经毒性形式,其N端被截短形成焦谷氨酸,最近被提议作为免疫治疗的关键靶点。优化后的ACI-24是一种正在开发的用于治疗和预防阿尔茨海默病的疫苗,它将抗体反应集中在Aβ的前15个N端氨基酸(Aβ1-15)上。重要的是,最初版本的包含Aβ1-15的ACI-24的临床数据证实了该疫苗的安全性和耐受性,并具有免疫原性证据。为了探索优化后的ACI-24产生针对pGlu-Aβ3-42抗体的能力,开展了临床前研究。给小鼠和非人类灵长类动物接种疫苗表明,优化后的ACI-24耐受性良好,并如预期那样诱导了针对Aβ1-42的抗体反应,以及高滴度的与焦谷氨酸化Aβ反应的IgG。多克隆反应的表位作图证实了这些发现,揭示了表位的广泛覆盖,特别是对于模拟形成pGlu-Aβ3-42的切割位点的Aβ肽段。这些数据与其他经临床测试的靶向Aβ疫苗所获得的结果形成了鲜明对比,后者产生的抗体多样性有限。综上所述,我们的研究结果表明,与先前测试的疫苗相比,优化后的ACI-24疫苗接种代表了一项突破,能够提供一种具有更广泛Aβ序列识别能力的安全免疫反应,产生针对包括pGlu-Aβ3-42在内的在发病机制中起重要作用的致病性Aβ形式的结合物。
