Phase 1 study of two merozoite surface protein 1 (MSP1(42)) vaccines for Plasmodium falciparum malaria.

PLoS clinical trials Pub Date : 2007-01-01 Epub Date: 2007-04-06 DOI:10.1371/journal.pctr.0020012

Elissa Malkin, Carole A Long, Anthony W Stowers, Lanling Zou, Sanjay Singh, Nicholas J MacDonald, David L Narum, Aaron P Miles, Andrew C Orcutt, Olga Muratova, Samuel E Moretz, Hong Zhou, Ababacar Diouf, Michael Fay, Eveline Tierney, Philip Leese, Siddhartha Mahanty, Louis H Miller, Allan Saul, Laura B Martin

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引用次数: 47

Abstract

Objectives: To assess the safety and immunogenicity of two vaccines, MSP1(42)-FVO/Alhydrogel and MSP1(42)-3D7/Alhydrogel, targeting blood-stage Plasmodium falciparum parasites.

Design: A Phase 1 open-label, dose-escalating study.

Setting: Quintiles Phase 1 Services, Lenexa, Kansas between July 2004 and November 2005.

Participants: Sixty healthy malaria-naïve volunteers 18-48 y of age.

Interventions: The C-terminal 42-kDa region of merozoite surface protein 1 (MSP1(42)) corresponding to the two allelic forms present in FVO and 3D7 P. falciparum lines were expressed in Escherichia coli, refolded, purified, and formulated on Alhydrogel (aluminum hydroxide). For each vaccine, volunteers in each of three dose cohorts (5, 20, and 80 microg) were vaccinated at 0, 28, and 180 d. Volunteers were followed for 1 y.

Outcome measures: The safety of MSP1(42)-FVO/Alhydrogel and MSP1(42)-3D7/Alhydrogel was assessed. The antibody response to each vaccine was measured by reactivity to homologous and heterologous MSP1(42), MSP1(19), and MSP1(33) recombinant proteins and recognition of FVO and 3D7 parasites.

Results: Anti-MSP1(42) antibodies were detected by ELISA in 20/27 (74%) and 22/27 (81%) volunteers receiving three vaccinations of MSP1(42)-FVO/Alhydrogel or MSP1(42)-3D7/Alhydrogel, respectively. Regardless of the vaccine, the antibodies were cross-reactive to both MSP1(42)-FVO and MSP1(42)-3D7 proteins. The majority of the antibody response targeted the C-terminal 19-kDa domain of MSP1(42), although low-level antibodies to the N-terminal 33-kDa domain of MSP1(42) were also detected. Immunofluorescence microscopy of sera from the volunteers demonstrated reactivity with both FVO and 3D7 P. falciparum schizonts and free merozoites. Minimal in vitro growth inhibition of FVO or 3D7 parasites by purified IgG from the sera of the vaccinees was observed.

Conclusions: The MSP1(42)/Alhydrogel vaccines were safe and well tolerated but not sufficiently immunogenic to generate a biologic effect in vitro. Addition of immunostimulants to the Alhydrogel formulation to elicit higher vaccine-induced responses in humans may be required for an effective vaccine.

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恶性疟原虫疟疾两种卵裂子表面蛋白1(MSP1(42))疫苗的一期研究。

目的:评价MSP1(42)-FVO/Alhydrogel和MSP1(42)-3D7/Alhydrogel两种针对血期恶性疟原虫的疫苗的安全性和免疫原性。设计:1期开放标签、剂量递增研究。环境:2004年7月至2005年11月期间，位于堪萨斯州Lenexa的Quintiles Phase 1 Services。参与者:60名健康志愿者malaria-naïve，年龄18-48岁。干预措施:在大肠杆菌中表达与FVO和3D7恶性疟原虫中存在的两种等位基因形式相对应的裂殖子表面蛋白1(MSP1(42))的c端42- kda区域，重新折叠、纯化并在醛水凝胶(氢氧化铝)上配制。对于每种疫苗，三个剂量组(5、20和80微克)中的志愿者分别在0、28和180天接种疫苗。志愿者随访1年。结果测量:评估MSP1(42)-FVO/Alhydrogel和MSP1(42)-3D7/Alhydrogel的安全性。通过对同源和异源MSP1(42)、MSP1(19)和MSP1(33)重组蛋白的反应性以及对FVO和3D7寄生虫的识别来检测每种疫苗的抗体应答。结果:接种3次MSP1(42)-FVO/Alhydrogel和MSP1(42)-3D7/Alhydrogel的志愿者中，分别有20/27(74%)和22/27(81%)检测到抗MSP1(42)抗体。无论采用何种疫苗，抗体均与MSP1(42)-FVO和MSP1(42)-3D7蛋白发生交叉反应。大多数抗体应答针对MSP1的c端19 kda结构域(42)，尽管也检测到针对MSP1的n端33 kda结构域的低水平抗体(42)。志愿者血清的免疫荧光显微镜显示对FVO和3D7恶性疟原虫分裂体和游离分裂子都有反应。从接种者血清中纯化的IgG对FVO或3D7寄生虫的体外生长抑制作用很小。结论:MSP1(42)/醛水凝胶疫苗是安全且耐受性良好的，但其免疫原性不足以在体外产生生物学效应。为了制造出有效的疫苗，可能需要在醛水凝胶制剂中加入免疫刺激剂，以在人体内引起更高的疫苗诱导应答。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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