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与CRM197偶联的A组链球菌J8肽候选疫苗在小鼠和非人类灵长类动物中的免疫原性。

Immunogenicity in mice and non-human primates of the Group A Streptococcal J8 peptide vaccine candidate conjugated to CRM197.

作者信息

Caro-Aguilar Ivette, Ottinger Elizabeth, Hepler Robert W, Nahas Deborah D, Wu Chengwei, Good Michael F, Batzloff Michael, Joyce Joseph G, Heinrichs Jon H, Skinner Julie M

机构信息

Merck Research Labs; Merck & Co. Inc; West Point, PA, USA.

出版信息

Hum Vaccin Immunother. 2013 Mar;9(3):488-96. doi: 10.4161/hv.23224. Epub 2012 Dec 18.

Abstract

Vaccine development for Group A streptococcal (GAS) infection has been extensively focused on the N-terminal hypervariable or the C-terminal conserved regions of the M protein, a major virulence factor of GAS. We evaluated the immunogenicity and functional activity of the conserved C-terminal peptide vaccine candidate, J8, conjugated to CRM197, in two mouse strains: C3H (H2(k)) and Balb/c (H2(d)), and in rhesus macaques. Mice were immunized with J8-CRM197 formulated with Amorphous Aluminum Hydroxyphosphate Sulfate Adjuvant (AAHSA), and non-human primates were immunized with J8-CRM197 formulated with AAHSA, ISCOMATRIX (TM) adjuvant, or AAHSA/ISCOMATRIX adjuvant. J8-CRM197 was immunogenic in mice from both H2(k) and H2(d) backgrounds, and the antibodies generated bound to the surface of four different GAS serotypes and had functional bacterial opsonic activity. Mice immunized with J8-CRM197/AAHSA demonstrated varying degrees of protection from lethal challenge. We also demonstrated that J8-CRM197 is immunogenic in non-human primates. Our data confirm the utility of J8 as a potential GAS vaccine candidate and demonstrate that CRM197 is an acceptable protein carrier for this peptide.

摘要

A群链球菌(GAS)感染的疫苗研发主要聚焦于GAS主要毒力因子M蛋白的N端高变区或C端保守区。我们评估了与CRM197偶联的保守C端肽疫苗候选物J8在两种小鼠品系(C3H(H2(k))和Balb/c(H2(d)))以及恒河猴中的免疫原性和功能活性。用含无定形硫酸羟基磷酸铝佐剂(AAHSA)的J8-CRM197免疫小鼠,用含AAHSA、ISCOMATRIX(TM)佐剂或AAHSA/ISCOMATRIX佐剂的J8-CRM197免疫非人灵长类动物。J8-CRM197在H2(k)和H2(d)背景的小鼠中均具有免疫原性,产生的抗体可结合四种不同GAS血清型的表面并具有功能性细菌调理活性。用J8-CRM197/AAHSA免疫的小鼠对致死性攻击表现出不同程度的保护作用。我们还证明J8-CRM197在非人灵长类动物中具有免疫原性。我们的数据证实了J8作为潜在GAS疫苗候选物的效用,并证明CRM197是该肽可接受的蛋白载体。

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