首页> 外文OA文献 >An enzymatically inactivated hemoglobinase from Necator americanus induces neutralizing antibodies against multiple hookworm species and protects dogs against heterologous hookworm infection
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An enzymatically inactivated hemoglobinase from Necator americanus induces neutralizing antibodies against multiple hookworm species and protects dogs against heterologous hookworm infection

机译:来自美洲Necator的酶灭活的血红蛋白酶诱导针对多种钩虫物种的中和抗体,并保护狗免受异源钩虫感染

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摘要

Hookworms digest hemoglobin from erythrocytes via a proteolytic cascade that begins with the aspartic protease, APR-1. Ac-APR-1 from the dog hookworm, Ancylostoma caninum, protects dogs against hookworm infection via antibodies that neutralize enzymatic activity and interrupt blood-feeding. Toward developing a human hookworm vaccine, we expressed both wild-type (Na-APR-1(wt)) and mutant (Na-APR-1(mut)-mutagenesis of the catalytic aspartic acids) forms of Na-APR-1 from the human hookworm, Necator americanus. Refolded Na-APR-1(wt) was catalytically active, and Na-APR-1(mut) was catalytically inactive but still bound substrates. Vaccination of canines with Na-APR-1(mut) and heterologous challenge with A. caninum resulted in significantly reduced parasite egg burdens (P=0.034) and weight loss (P=0.022). Vaccinated dogs also had less gut pathology, fewer adult worms, and reduced blood loss compared to controls but these did not reach statistical significance. Vaccination with Na-APR-1(mut) induced antibodies that bound the native enzyme in the parasite gut and neutralized enzymatic activity of Na-APR-1(wt) and APR-1 orthologues from three other hookworm species that infect humans. IgG1 against Na-APR-1(mut) was the most prominently detected antibody in sera from people resident in high-transmission areas for N. americanus, indicating that natural boosting may occur in exposed humans. Na-APR-1(mut) is now a lead antigen for the development of an antihematophagy vaccine for human hookworm disease.
机译:钩虫通过蛋白水解级联从红细胞消化血红蛋白,该蛋白水解级联始于天冬氨酸蛋白酶APR-1。来自犬钩虫Ancylostoma caninum的Ac-APR-1通过中和酶促活性并中断供血的抗体保护犬免受钩虫感染。为了开发人类钩虫疫苗,我们表达了Na-APR-1的野生型(Na-APR-1(wt))和突变型(Na-APR-1(mut)-诱变的天冬氨酸突变)形式,人类钩虫,美洲轮虫。重新折叠的Na-APR-1(wt)具有催化活性,而Na-APR-1(mut)具有催化惰性,但仍与底物结合。用Na-APR-1(mut)进行犬疫苗接种以及用犬链孢菌进行异源攻击可显着降低寄生虫卵负担(P = 0.034)和体重减轻(P = 0.022)。与对照组相比,接种疫苗的狗的肠道病理也更少,成虫也更少,失血量也减少了,但这些都没有统计学意义。用Na-APR-1(mut)疫苗接种的抗体结合了寄生虫肠道中的天然酶,并中和了来自其他三种感染人类钩虫的Na-APR-1(wt)和APR-1直向同源物的酶活性。针对Na-APR-1(mut)的IgG1是来自美国猪笼草高传播地区居民的血清中最显着检测到的抗体,这表明暴露在外的人类可能发生自然免疫。 Na-APR-1(mut)现在是用于开发人类钩虫病抗嗜血疫苗的先导抗原。

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