Muro Antonio, Casanueva Patricia, López-Abán Julio, Ramajo Vicente, Martínez-Fernández Antonio R, Hillyer George V
Laboratorio de Parasitología, Facultad de Farmacia, Universidad de Salamanca, Avda, Campo Charro s/n 37007 Salamanca, España.
J Parasitol. 2007 Aug;93(4):817-23. doi: 10.1645/GE-1050R1.1.
Vaccination with fatty acid-binding proteins (FABPs) from Fasciola hepatica has been shown to confer significant levels of protection against challenge infection in mice, rabbits, and sheep. A recombinant 15-kDa FABP (rFh15) has been purified and also shown to be an immunoprotective molecule. From the rFh15 molecule sequence 2, 12- and 10-mer putative T-cell epitopes were identified, the first an Fh15Ta of amino acid sequence IKMVSSLKTKIT, and the second an Fh15Tb of amino acid sequence VKAVTTLLKA. The synthesized oligonucleotides were cloned individually into a pGEX-2TK expression vector. The overexpressed fusion protein was affinity purified using glutathione S-transferase (GST) by competitive elution with excess reduced glutathione. These GST fusion proteins were emulsified in Freund adjuvant for rabbit immunizations or further purified as peptides after digestion with thrombin. The purified 12- and 10-mer peptides were either emulsified in Freund adjuvant for immunizations in rabbits or used in an adjuvant-adaptation (ADAD) system, followed by challenge infection with F. hepatica metacercariae in mice and rabbits. In vaccinated-challenged rabbits, the highest levels of protection were found in those treated with GST-epitopes (Fh15Ta 48.2% and Fh15Tb 59.1% reduction, respectively), as compared to GST-immunized controls. Moreover, those immunized with Fh15Ta had higher (84%) numbers of immature flukes as compared with Fh15Tb (41%) or GST alone (64%). The rabbits immunized with the putative T-cell epitopes in adjuvant had a 13% reduction in flukes in those with Fh15Ta and also were highest with immature flukes (46%). In vaccinated mice challenged with a lethal number of metacercariae, both CD-1 and BALB/c mice treated with complete ADAD-GST-Ta had the highest (40%) survival rates of all groups by 47 days postinfection. Thus the Fh15Ta and Fh15Tb polypeptide epitopes warrant further study as a potential vaccine against F. hepatica. Antibody isotype studies in mice revealed a mixed Thl/Th2 response to vaccination.
用来自肝片吸虫的脂肪酸结合蛋白(FABP)进行疫苗接种已被证明能在小鼠、兔子和绵羊中对攻击感染提供显著水平的保护。一种重组15 kDa FABP(rFh15)已被纯化,并且也被证明是一种免疫保护分子。从rFh15分子序列中鉴定出2个、12肽和10肽的推定T细胞表位,第一个是氨基酸序列为IKMVSSLKTKIT的Fh15Ta,第二个是氨基酸序列为VKAVTTLLKA的Fh15Tb。合成的寡核苷酸被分别克隆到pGEX - 2TK表达载体中。通过用过量还原型谷胱甘肽进行竞争性洗脱,利用谷胱甘肽S - 转移酶(GST)对过表达的融合蛋白进行亲和纯化。这些GST融合蛋白在弗氏佐剂中乳化用于兔子免疫,或在用凝血酶消化后作为肽进一步纯化。纯化的12肽和10肽要么在弗氏佐剂中乳化用于兔子免疫,要么用于佐剂适应(ADAD)系统,随后用肝片吸虫尾蚴对小鼠和兔子进行攻击感染。在接种疫苗后受到攻击的兔子中,与GST免疫对照组相比,用GST表位处理的兔子(Fh15Ta和Fh15Tb分别减少48.2%和59.1%)的保护水平最高。此外,与Fh15Tb(41%)或单独的GST(64%)相比,用Fh15Ta免疫的兔子未成熟吸虫数量更高(84%)。在佐剂中用推定T细胞表位免疫的兔子中,Fh15Ta组的吸虫数量减少了13%,并且未成熟吸虫数量也是最高的(46%)。在用致死数量的尾蚴攻击的接种疫苗的小鼠中,到感染后47天时,用完全ADAD - GST - Ta处理的CD - 1和BALB/c小鼠在所有组中的存活率最高(40%)。因此,Fh15Ta和Fh15Tb多肽表位作为一种潜在的抗肝片吸虫疫苗值得进一步研究。对小鼠的抗体亚型研究揭示了对疫苗接种的混合Th1/Th2反应。
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