糖蛋白gp 115和弹性蛋白在鸡眼和其他组织中的广泛共分布

Alfonso Colombatti , Alessandro Poletti , Giorgio M. Bressan , Antonino Carbone , Dino Volpin
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引用次数: 26

摘要

用亲和纯化的抗鸡gp 115单克隆抗体和亲和纯化的抗鸡tropoelastin单克隆抗体冷冻切片,通过亲和-生物素免疫过氧化物酶技术研究相应抗原的分布规律。用层粘连蛋白和纤维连接蛋白抗体进行比较。gp115和对流层弹性蛋白抗体在检查的几个组织中定位于相同的结构。角膜内皮膜和脉络膜中的Bruch膜呈阳性,角膜上皮膜呈阴性。这两种抗体在角膜基质中都表现出特殊的点状反应性,在结膜和角膜-巩膜交界处显示出非常细的纤维状图案。肝脏、心脏和大血管、横纹肌和皮肤对抗弹力蛋白和gp 115抗体表现出相似的模式。反应性的分布差异不大:肠平滑肌细胞的细胞周基质可被gp 115染色,而对弹力蛋白抗体未染色。然而,gp115和tropoelastin抗体的反应性在肺平滑肌细胞簇中分布相似。肾小管周围基质也不像脑实质内血管那样与对偶弹性蛋白抗体发生反应;而gp 115抗体在两个位点均存在反应性。我们将一些组织中缺乏明显的共分布解释为靶抗原与抗体反应的相对可用性的变化,而不是gp 115和tropoelastin分布的质量差异的结果。通过使用抗gp 115单克隆抗体,不发生交叉反应,可能识别不同的表位,表明一些抗体(但不是所有抗体)与脑实质内血管反应;而在其他组织中的分布模式是相同的。这表明,在弹性蛋白水平检测不到的血管中,gp 115分子的某些表位可能由于被其他成分或分子的不同构象所掩盖而无法识别。
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Widespread Codistribution of Glycoprotein gp 115 and Elastin in Chick Eye and Other Tissues

Frozen sections of chick tissues were exposed to affinity-purified monoclonal antibodies raised against chick gp 115 and to affinity-purified antibodies raised against chick tropoelastin to study the distribution pattern of the corresponding antigens by the avidin-biotin immunoperoxidase technique. Laminin and fibronectin antibodies were used for comparison. Gp 115 and tropoelastin antibodies localized to the same structure in several of the tissues examined. The endothelial membrane of the cornea and Bruch's membrane in the choroid were positive, while the corneal epithelial membrane was negative. Both antibodies displayed a peculiar punctate reactivity in the corneal stroma and a very fine fibrillar pattern in the conjunctiva and at the corneal-scleral junction. Liver, heart and large vessels, striated muscle and skin showed a similar pattern both for tropoelastin and gp 115 antibodies. Few differences were seen in the distribution of the reactivity: the pericellular matrix of intestinal smooth muscle cells was stained by gp 115 but not by tropoelastin antibodies. However, the reactivity of gp 115 and tropoelastin antibodies was similarly distributed in the lung smooth muscle cell clusters. The peritubular matrix in the kidney did also not react with tropoelastin antibodies as did the brain intraparenchymal vessels; whereas gp 115 antibody reactivity was present in both sites. We interpret these lack of apparent codistribution in some tissues as a variation in the relative availability of the target antigen for the reaction with the antibody and not as a consequence of a qualitative difference in the distribution of gp 115 and tropoelastin. By the use of anti gp 115 monoclonal antibodies that do not cross-react, and presumably recognize different epitopes, it was shown that some but not all antibodies, react with brain intraparenchymal blood vessels; whereas the pattern of distribution in other tissues was the same. This suggests that in vessels with an undetectable level of elastin, certain epitopes of gp 115 molecule might not be recognized as a result of being masked by other components or by a different conformation of the molecule.

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