首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Identification of an immunodominant and highly immunopathogenic determinant in the retinal interphotoreceptor retinoid-binding protein (IRBP)
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Identification of an immunodominant and highly immunopathogenic determinant in the retinal interphotoreceptor retinoid-binding protein (IRBP)

机译:视网膜光感受器类维生素A结合蛋白(IRBP)中免疫显性和高度致病性的决定因素的鉴定

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摘要

Interphotoreceptor retinoid-binding protein (IRBP), a glycoprotein specific for the retina and pineal gland, induces inflammatory changes in these two organs in immunized animals. We report here on the identification of an immunodominant determinant of bovine IRBP that is highly immunogenic and immunopathogenic in the Lewis rat. The peptide, which comprises the sequence 1169-1191 of bovine IRBP, was shown to be immunodominant by its capacity to stimulate lymphocytes sensitized against whole IRBP. A comparison was made between peptide 1169-1191 and another peptide, 1158-1180, which is nondominant but is immunogenic and immunopathogenic in the Lewis rat. Peptide 1169-1191 was found to be superior in its immunological capacities; the minimal dose of 1169-1191 needed to induce cellular immune response or disease in Lewis rats (0.02-0.1 nmol/rat) is congruent to 1,000 times smaller than that of 1158-1180. In addition, unlike the ocular disease induced by 1158-1180, the disease produced by 1169-1191 resembled that induced by whole IRBP in its kinetics and histopathological features. The immunological activity of 1169-1191 in the Lewis rat was localized to the 10 residues at the COOH terminus; no such activity was exhibited by the truncated peptide 1169-1188, which comprises the 20 residues at the NH2 terminus of the full peptide. The usefulness of this unique experimental system in analyzing the role of immunodominance in peptide immunogenicity and immunopathogenicity is underscored.
机译:受体间类视黄醇结合蛋白(IRBP)是视网膜和松果体特有的糖蛋白,可在免疫动物的这两个器官中引起炎症变化。我们在这里报告有关在Lewis大鼠中具有高度免疫原性和免疫致病性的牛IRBP的免疫决定因素的鉴定。包含牛IRBP序列1169-1191的肽具有刺激免疫对整个IRBP致敏的淋巴细胞的能力,因此具有免疫优势。在肽1169-1191和另一种肽1158-1180之间进行了比较,该肽在Lewis大鼠中是非主要但具有免疫原性和免疫致病性。发现肽1169-1191具有更好的免疫学能力。在Lewis大鼠中诱导细胞免疫应答或疾病所需的最低剂量1169-1191(0.02-0.1nmol /大鼠)相当于1158-1180的1,000倍。此外,与1158-1180引起的眼部疾病不同,1169-1191产生的疾病在动力学和组织病理学特征上与整个IRBP诱发的疾病相似。 Lewis大鼠的1169-1191免疫活性被定位在COOH末端的10个残基上。截短的肽1169-1188没有表现出这种活性,截短的肽1169-1188在完整肽的NH2末端包含20个残基。强调了这种独特的实验系统在分析免疫优势在肽免疫原性和免疫致病性中的作用。

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