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用克氏锥虫核糖体P1和P2蛋白的C末端区域进行免疫接种,可诱导年轻和老年小鼠产生具有长期持续时间的交叉反应性抗体,并伴有心脏功能和结构改变。

Immunization with the C-terminal region of Trypanosoma cruzi ribosomal P1 and P2 proteins induces long-term duration cross-reactive antibodies with heart functional and structural alterations in young and aged mice.

作者信息

Motrán C C, Fretes R E, Cerbán F M, Rivarola H W, Vottero de Cima E

机构信息

Departamento de Bioquímica Clínica, Universidad Nacional de Córdoba, Córdoba, 5000, Argentina.

出版信息

Clin Immunol. 2000 Nov;97(2):89-94. doi: 10.1006/clim.2000.4919.

Abstract

The R13 peptide sequence (EEEDDDMGFGLFD) that corresponds to the C-terminal region of Trypanosoma cruzi ribosomal P1 and P2 proteins differs from the eukariotic P concensus sequence EESDDDMGFGLFD (H13) only in a nonconservative amino acid substitution. The immunization of BALB/c mice with R13 synthetic peptide coupled to a carrier protein (OVA) induces specific (anti-R13) and autoreactive (anti-H13 and anti-heart) antibodies as well as heart functional alterations. Since aged human and experimental animals are impaired in their responses to most foreign antigens but they produce greater amounts of autoantibodies, in this work we used aged mice as an experimental model able to exaggerate the autoimmune component of the R13-induced response in case it was present. We studied whether these antibodies generated in the absence of the parasite would induce pathological changes in heart tissues. The levels of antibodies against R13 (foreign antigen) and H13 (autoantigen) studied comparatively in 2- and 12-month-old mice 10 days after the third immunization with R13 coupled to OVA were, as we expected for a foreign antigen, higher in almost all sera from 2-month-old mice tested than in sera from 12-month-old mice. Besides, these specific and cross-reactive antibody response remain elevated as long as 150 days post third immunization. In addition, the isotype pattern that recognizes R13 and the self-sequence H13 showed no differences between sera from young and aged mice. Moreover, when ECG traces were obtained from immunized mice, the heart functional alterations observed at 10 days continued at 80 and 150 days after the third immunization, showing an association with the levels of antibodies. In addition, despite the fact that the heart tissue morphology showed no alterations 10 days post third immunization, several abnormalities in the tissue architecture were revealed at 80 and 150 days post third immunization. This report demonstrates the biological relevance of R13-induced cross-reactive antibodies in some of the electrophysiologic and histological changes found in T. cruzi-infected mammalians.

摘要

与克氏锥虫核糖体P1和P2蛋白C端区域相对应的R13肽序列(EEEDDDMGFGLFD)与真核生物P共有序列EESDDDMGFGLFD(H13)仅在一个非保守氨基酸取代上有所不同。用与载体蛋白(OVA)偶联的R13合成肽免疫BALB/c小鼠可诱导特异性(抗R13)和自身反应性(抗H13和抗心脏)抗体以及心脏功能改变。由于老年人类和实验动物对外来抗原的反应受损,但会产生更多自身抗体,在本研究中,我们使用老年小鼠作为实验模型,以在存在自身免疫成分的情况下夸大R13诱导反应中的自身免疫成分。我们研究了在无寄生虫情况下产生的这些抗体是否会诱导心脏组织发生病理变化。在用与OVA偶联的R13进行第三次免疫10天后,对2个月和12个月大的小鼠中针对R13(外来抗原)和H13(自身抗原)的抗体水平进行了比较研究,正如我们对外来抗原所预期的那样,在几乎所有测试的2个月大小鼠血清中,这些抗体水平高于12个月大小鼠血清中的水平。此外,这些特异性和交叉反应性抗体反应在第三次免疫后长达150天仍保持升高。此外,识别R13和自身序列H13的同种型模式在年轻和老年小鼠血清之间没有差异。此外,当从免疫小鼠获取心电图记录时,第三次免疫后10天观察到的心脏功能改变在第三次免疫后80天和150天仍持续存在,显示出与抗体水平相关。此外,尽管第三次免疫后10天心脏组织形态未显示改变,但在第三次免疫后80天和150天发现组织结构存在一些异常。本报告证明了R13诱导的交叉反应性抗体在克氏锥虫感染哺乳动物中发现的一些电生理和组织学变化中的生物学相关性。

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