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通过生物素的磷脂衍生物将抗生物素蛋白附着于红细胞可提供抗补体免疫红细胞。

Avidin attachment to red blood cells via a phospholipid derivative of biotin provides complement-resistant immunoerythrocytes.

作者信息

Muzykantov V R, Smirnov M D, Klibanov A L

机构信息

Institute of Experimental Cardiology, National Cardiology Research Center, Moscow, Russian Federation.

出版信息

J Immunol Methods. 1993 Feb 3;158(2):183-90. doi: 10.1016/0022-1759(93)90212-p.

Abstract

Preincubation of red blood cells (RBC) in an aqueous dispersion of biotin-phosphatidylethanolamine (biotin-PE) provides binding sites for avidin on the surface of these cells (up to 5 x 10(5) avidin molecules per cell). Previously we have shown that biotin covalently attached to the surface of RBC by a chemical reaction with biotin N-hydroxysuccinimide ester permits attachment of avidin to these cells, resulting in the activation of the alternative pathway of complement with subsequent cell lysis. However, avidin attached to RBC via biotin-PE did not cause complement activation. This is not due to the stabilizing action of biotin-PE. In contrast, various phospholipids, including biotin-PE, enhance the lysis of RBC induced by hemolytic antibodies via the classical complement pathway. The potential of avidin-coated RBC to act as activators of the complement alternative pathway depends on the method of biotin attachment to RBC. Complement-resistant avidin-coated RBC can specifically bind biotinylated antibodies. These immunoerythrocytes effectively and specifically bind to the antigen-coated surface and are not lysed by complement even in the presence of soluble antigen. These data extend the possible applications of immunoerythrocytes in drug targeting.

摘要

将红细胞(RBC)在生物素 - 磷脂酰乙醇胺(生物素 - PE)的水分散液中进行预孵育,可在这些细胞表面提供抗生物素蛋白的结合位点(每个细胞可达5×10⁵个抗生物素蛋白分子)。此前我们已经表明,通过与生物素N - 羟基琥珀酰亚胺酯的化学反应将生物素共价连接到RBC表面,可使抗生物素蛋白附着于这些细胞,从而激活补体替代途径并导致随后的细胞裂解。然而,通过生物素 - PE附着于RBC的抗生物素蛋白并不会引起补体激活。这并非由于生物素 - PE的稳定作用。相反,包括生物素 - PE在内的各种磷脂,可通过经典补体途径增强溶血抗体诱导的RBC裂解。抗生物素蛋白包被的RBC作为补体替代途径激活剂的潜力取决于生物素附着于RBC的方法。抗补体的抗生物素蛋白包被的RBC可特异性结合生物素化抗体。这些免疫红细胞能有效且特异性地结合抗原包被的表面,即使在存在可溶性抗原的情况下也不会被补体裂解。这些数据扩展了免疫红细胞在药物靶向中的可能应用。

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