抗体识别来自细胞粘附蛋白的肽序列:N-和e -钙粘蛋白。

Peptide research Pub Date : 1996-09-01
K L Lutz, L A Szabo, D L Thompson, T J Siahaan
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引用次数: 0

摘要

细胞间连接对药物的细胞旁递送提出了巨大的挑战。钙粘蛋白是钙依赖性细胞-细胞粘附分子,负责这些连接的形成和调节。抗E-cadherin单克隆抗体可与E-cadherin (uvomorulin)结合,通过抑制cadherin-cadherin相互作用抑制细胞-细胞粘附。本研究的目的是利用这种单克隆抗E-cadherin抗体来定位E-和N-cadherin的细胞外结构域。这是通过使用两种不同的酶联免疫吸附测定(ELISA),常规间接ELISA和固定化肽ELISA来完成的。这种抗e -钙粘蛋白抗体可以识别来自每个细胞外区域的两个肽。通过绘制钙粘蛋白的胞外结构域,可以识别在细胞-细胞粘附中具有离散作用的肽。这将有助于设计可以调节细胞间连接以改善药物传递的合成肽。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antibody recognition of peptide sequences from the cell-cell adhesion proteins: N- and E-cadherins.

Intercellular junctions present a formidable challenge for the paracellular delivery of drugs. Cadherins are calcium-dependent cell-cell adhesion molecules, which are responsible for the formation and regulation of these junctions. Anti-E-cadherin monoclonal antibody can bind to E-cadherin (uvomorulin) and inhibit cell-cell adhesion through the inhibition of cadherin-cadherin interactions. The objective of this study was to utilize this monoclonal anti-E-cadherin antibody to map the extracellular domains of E- and N-cadherin. This was accomplished by using two different enzyme-linked immunosorbent assays (ELISAs), a regular indirect ELISA and an immobilized-peptide ELISA. Two peptides from each extracellular domain were recognized by this anti-E-cadherin antibody. By mapping the extracellular domains of cadherins, peptides that have discrete roles in cell-cell adhesion can be identified. This will aid in the design of synthetic peptides that can modulate intercellular junctions to improve drug delivery.

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