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单点突变对重组蓖麻毒素 A 链亚单位疫苗抗原稳定性和免疫原性的影响。

Effect of single-point mutations on the stability and immunogenicity of a recombinant ricin A chain subunit vaccine antigen.

机构信息

Macromolecule and Vaccine Stabilization Center; Department of Pharmaceutical Chemistry; University of Kansas; Lawrence, KS USA.

出版信息

Hum Vaccin Immunother. 2013 Apr;9(4):744-52. doi: 10.4161/hv.22998. Epub 2013 Apr 1.

Abstract

There is great interest in the design and development of highly thermostable and immunogenic protein subunit vaccines for biodefense. In this study, we used two orthogonal and complementary computational protein design approaches to generate a series of single-point mutants of RiVax, an attenuated recombinant ricin A chain (RTA) protein subunit vaccine antigen. As assessed by differential scanning calorimetry, the conformational stabilities of the designed mutants ranged from 4°C less stable to 4.5°C more stable than RiVax, depending on solution pH. Two more thermostable (V18P, C171L) and two less thermostable (T13V, S89T) mutants that displayed native-like secondary and tertiary structures (as determined by circular dichroism and fluorescence spectral analysis, respectively) were tested for their capacity to elicit RTA-specific antibodies and toxin-neutralizing activity. Following a prime-boost regimen, we found qualitative differences with respect to specific antibody titers and toxin neutralizing antibody levels induced by the different mutants. Upon a second boost with the more thermostable mutant C171L, a statistically significant increase in RTA-specific antibody titers was observed when compared with RiVax-immunized mice. Notably, the results indicate that single residue changes can be made to the RiVax antigen that increase its thermal stability without adversely impacting the efficacy of the vaccine.

摘要

人们对设计和开发具有高热稳定性和免疫原性的蛋白质亚单位疫苗以用于生物防御非常感兴趣。在这项研究中,我们使用了两种正交且互补的计算蛋白质设计方法,对减毒重组蓖麻毒素 A 链(RTA)蛋白亚单位疫苗抗原 RiVax 进行了一系列单点突变。通过差示扫描量热法评估,设计突变体的构象稳定性在取决于溶液 pH 值的情况下,比 RiVax 分别低 4°C 或高 4.5°C。两个更耐热的(V18P、C171L)和两个更不耐热的(T13V、S89T)突变体(通过圆二色性和荧光光谱分析分别确定具有天然样的二级和三级结构)被测试了它们诱导 RTA 特异性抗体和毒素中和活性的能力。在进行一次加强免疫后,我们发现不同突变体引起的特异性抗体滴度和毒素中和抗体水平存在定性差异。在用更耐热的突变体 C171L 进行第二次加强免疫后,与 RiVax 免疫的小鼠相比,观察到 RTA 特异性抗体滴度有统计学意义的增加。值得注意的是,结果表明可以对 RiVax 抗原进行单点突变,从而提高其热稳定性,而不会对疫苗的功效产生不利影响。

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