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Disruption of the Putative Vascular Leak Peptide Sequence in the Stabilized Ricin Vaccine Candidate RTA1-33/44-198.

机译：在稳定的蓖麻毒素疫苗候选物RTa1-33 / 44-198中破坏推定的血管渗漏肽序列。

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Vitetta and colleagues identified and characterized a putative vascular leak peptide (VLP) consensus sequence in recombinant ricin toxin A- chain (RTA) that contributed to dose-limiting human toxicity when RTA was administered intravenously in large quantities during chemotherapy. We disrupted this potentially toxic site within the more stable RTA1-33/44-198 vaccine immunogen and determined the impact of these mutations on protein stability, structure and protective immunogenicity using an experimental intranasal ricin challenge model in BALB/c mice to determine if the mutations were compatible. Single amino acid substitutions at the positions corresponding with RTA D75 (to A, or N) and V76 (to I, or M) had minor effects on the apparent protein melting temperature of RTA1-33/44-198 but all four variants retained greater apparent stability than the parent RTA. Moreover, each VLP( ) variant tested provided protection comparable with that of RTA1-33/44-198 against supralethal intranasal ricin challenge as judged by animal survival and several biomarkers. To understand better how VLP substitutions and mutations near the VLP site impact epitope structure, we introduced a previously described thermal stabilizing disulfide bond (R48C/T77C) along with the D75N or V76I substitutions in RTA1-33/44-198. The D75N mutation was compatible with the adjacent stabilizing R48C/T77C disulfide bond and the Tm was unaffected, whereas the V76I mutation was less compatible with the adjacent disulfide bond involving C77. A crystal structure of the RTA1-33/44-198 R48C/T77C/D75N variant showed that the structural integrity of the immunogen was largely conserved and that a stable immunogen could be produced from E. coli. We conclude that it is feasible to disrupt the VLP site in RTA1-33/44-198 with little or no impact on apparent protein stability or protective efficacy in mice and such variants can be stabilized further by introduction of a disulfide bond.

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作者
J. M. Davis J. R. Compton K. E. Steele L. Janosi P. M. Legler;
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年度 2013
页码 1-26
总页数 26
原文格式 PDF
正文语种 eng
中图分类工业技术;
关键词
Amino acid substitutions; Amino acids; Balbc mice; Cd(Circular dichroism); Dichroism; Dosage; Histopathology; Immunity; Immunogens; Lung; Mice; Mutagens; Peptides; Petides; Proteins; Recombinant vaccines; Reprints; Ricin; Statistical analysis; Survival(General); Vaccines; Vlp(Vascular leak peptides); X ray crystallography;

机译：氨基酸取代;氨基酸; Balbc小鼠; Cd（圆二色性）;二色性;剂量;组织病理学;免疫;免疫原;肺;小鼠;诱变剂;肽;肽;蛋白质;重组疫苗;重印;蓖麻毒素;统计分析;存活（一般）;疫苗; Vlp（血管渗漏肽）; X射线晶体学;

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1. Disruption of the Putative Vascular Leak Peptide Sequence in the Stabilized Ricin Vaccine Candidate RTA1-33/44-198 [J] . Charles B. Millard, Gary R. Matyas, Jaimee R. Compton, Toxins . 2013,第2期

机译：稳定的蓖麻毒素疫苗候选RTA1-33 / 44-198中假定的血管泄漏肽序列的破坏。
2. Evaluation of a ricin vaccine candidate (RVEc) for human toxicity using an in vitro vascular leak assay [J] . Porter Aimee, Phillips Gary, Smith Leonard, Toxicon: An International Journal Devoted to the Exchange of Knowledge on the Poisons Derived from Animals, Plants and Microorganisms . 2011,第1期

机译：使用体外血管渗漏试验评估蓖麻毒候选疫苗（RVEc）对人的毒性
3. An engineered Plasmodium falciparum C-terminal 19-kilodalton merozoite surface protein 1 vaccine candidate induces high levels of interferon-gamma production associated with cellular immune responses to specific peptide sequences in Gambian adults naturally exposed to malaria. [J] . Bisseye C, Yindom LM, Simpore J, Clinical and Experimental Immunology: An Official Journal of the British Society for Immunology . 2011,第3期

机译：在自然暴露于疟疾的冈比亚成年人中，工程化的恶性疟原虫C端19-千达尔顿裂殖子表面蛋白1疫苗候选物诱导了高水平的干扰素-γ产生，这与针对特定肽序列的细胞免疫反应有关。
4. Evolutionary analysis and prediction of peptide vaccine candidates for Nipah virus fusion protein [C] . Farzana Hossain, A.S.M. Rubayet-Ul-Alam 2016 International Conference on Medical Engineering, Health Informatics and Technology . 2016

机译：尼帕病毒融合蛋白候选肽疫苗的进化分析和预测
5. Consensus GII.4 virus like particles; a vaccine candidate biophysical characterization, stabilization, and adjuvants binding studies. [D] . Alabdulkarim, Abdullah Saad A. 2016

机译：共识GII.4病毒样颗粒；候选疫苗的生物物理特性，稳定性和佐剂结合研究。
6. Disruption of the Putative Vascular Leak Peptide Sequence in the Stabilized Ricin Vaccine Candidate RTA1-33/44-198 [O] . Laszlo Janosi, Jaimee R. Compton, Patricia M. Legler, 2013

机译：稳定的蓖麻毒素疫苗候选RTA1-33 / 44-198中假定的血管泄漏肽序列的破坏。
7. Disruption of the Putative Vascular Leak Peptide Sequence in the Stabilized Ricin Vaccine Candidate RTA1-33/44-198 [O] . Charles B. Millard, Gary R. Matyas, Jon M. Davis, 2013

机译：在稳定的蓖麻毒素候选疫苗RTa1-33 / 44-198中破坏推定的血管渗漏肽序列

Disruption of the Putative Vascular Leak Peptide Sequence in the Stabilized Ricin Vaccine Candidate RTA1-33/44-198.

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