腺病毒 5 型载体疟疾疫苗表达 CSP 和 AMA1。A 部分：血清阴性成年人的安全性和免疫原性。

Adenovirus 5-vectored P. falciparum vaccine expressing CSP and AMA1. Part A: safety and immunogenicity in seronegative adults.

机构信息

U.S. Military Malaria Vaccine Program, Naval Medical Research Center, Silver Spring, Maryland, United States of America.

出版信息

PLoS One. 2011;6(10):e24586. doi: 10.1371/journal.pone.0024586. Epub 2011 Oct 7.

BACKGROUND

Models of immunity to malaria indicate the importance of CD8+ T cell responses for targeting intrahepatic stages and antibodies for targeting sporozoite and blood stages. We designed a multistage adenovirus 5 (Ad5)-vectored Plasmodium falciparum malaria vaccine, aiming to induce both types of responses in humans, that was tested for safety and immunogenicity in a Phase 1 dose escalation trial in Ad5-seronegative volunteers.

METHODOLOGY/PRINCIPAL FINDINGS: The NMRC-M3V-Ad-PfCA vaccine combines two adenovectors encoding circumsporozoite protein (CSP) and apical membrane antigen-1 (AMA1). Group 1 (n = 6) healthy volunteers received one intramuscular injection of 2×10∧10 particle units (1×10∧10 each construct) and Group 2 (n = 6) a five-fold higher dose. Transient, mild to moderate adverse events were more pronounced with the higher dose. ELISpot responses to CSP and AMA1 peaked at 1 month, were higher in the low dose (geomean CSP = 422, AMA1 = 862 spot forming cells/million) than in the high dose (CSP = 154, p = 0.049, AMA1 = 423, p = 0.045) group and were still positive at 12 months in a number of volunteers. ELISpot depletion assays identified dependence on CD4+ or on both CD4+ and CD8+ T cells, with few responses dependent only on CD8+ T cells. Intracellular cytokine staining detected stronger CD8+ than CD4+ T cell IFN-γ responses (CSP p = 0.0001, AMA1 p = 0.003), but similar frequencies of multifunctional CD4+ and CD8+ T cells secreting two or more of IFN-γ, TNF-α or IL-2. Median fluorescence intensities were 7-10 fold higher in triple than single secreting cells. Antibody responses were low but trended higher in the high dose group and did not inhibit growth of cultured P. falciparum blood stage parasites.

SIGNIFICANCE

As found in other trials, adenovectored vaccines appeared safe and well-tolerated at doses up to 1×10∧11 particle units. This is the first demonstration in humans of a malaria vaccine eliciting strong CD8+ T cell IFN-γ responses.

TRIAL REGISTRATION

ClinicalTrials.govNCT00392015.

背景

疟疾免疫模型表明，CD8+T 细胞应答对于靶向肝细胞内阶段以及抗体对于靶向疟原虫孢子和血液阶段至关重要。我们设计了一种多阶段腺病毒 5（Ad5）载体的恶性疟原虫疟疾疫苗，旨在诱导人类产生这两种类型的反应，该疫苗在 Ad5 血清阴性志愿者中进行的 1 期剂量递增试验中进行了安全性和免疫原性测试。

方法/主要发现：NMRC-M3V-Ad-PfCA 疫苗结合了两种编码环子孢子蛋白（CSP）和顶膜抗原-1（AMA1）的腺病毒载体。第 1 组（n=6）健康志愿者接受了一次肌肉内注射 2×10∧10 个粒子单位（每个构建体 1×10∧10），第 2 组（n=6）接受了五倍高剂量。高剂量组更明显地出现短暂的轻度至中度不良反应。ELISpot 对 CSP 和 AMA1 的反应在 1 个月时达到峰值，低剂量组（几何均数 CSP=422，AMA1=862 个斑点形成细胞/百万）高于高剂量组（CSP=154，p=0.049，AMA1=423，p=0.045），并且在许多志愿者中，12 个月时仍呈阳性。ELISpot 耗竭测定表明 CD4+或 CD4+和 CD8+T 细胞均依赖，只有少数反应仅依赖 CD8+T 细胞。细胞内细胞因子染色检测到更强的 CD8+T 细胞 IFN-γ 反应（CSP p=0.0001，AMA1 p=0.003），但 CD4+和 CD8+T 细胞分泌两种或更多 IFN-γ、TNF-α或 IL-2 的多功能细胞频率相似。三重分泌细胞的中荧光强度比单分泌细胞高 7-10 倍。抗体反应较低，但高剂量组呈上升趋势，且不抑制培养的恶性疟原虫血液阶段寄生虫的生长。