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一种通过噬菌体展示技术鉴定的用于细胞凋亡分子成像的新型肽载体。

A new peptidic vector for molecular imaging of apoptosis, identified by phage display technology.

作者信息

Laumonier Catherine, Segers Jérôme, Laurent Sophie, Michel Alain, Coppée Frédérique, Belayew Alexandra, Elst Luce Vander, Muller Robert N

机构信息

Department of General, Organic and Biomedical Chemistry, NMR and Molecular Imaging Laboratory, University of Mons-Hainaut, Mons, Belgium.

出版信息

J Biomol Screen. 2006 Aug;11(5):537-45. doi: 10.1177/1087057106288220. Epub 2006 Jun 7.

Abstract

Phosphatidylserine (PS) exposure on the cell surface is an early marker of apoptosis. To select PS binding peptides as vectors of contrast agents to image apoptosis, a phage library has been exposed to perfused mouse livers. Phages not retained on control livers during the first perfusions were used for selections on apoptotic livers in a second series of perfusions. Four selected phages were further evaluated for binding to PS-coated enzyme-linked immunosorbent assay (ELISA) plates. They presented an apparent affinity constant (Ka app) for PS ranging from 6.08x10(10) M to 1.62x10(11)M. These phages did not bind to phosphatidylcholine, and competition with annexin V confirmed their specific interaction with PS. The phage with the highest affinity-bound PS in ELISA with a Ka app=(1.6+/-0.2)x10(11)M. It carried the TLVSSL peptide that was synthesized. Specific competition with annexin V and with the synthetic peptide was performed and confirms the specificity of the interaction.

摘要

细胞表面磷脂酰丝氨酸(PS)暴露是细胞凋亡的早期标志物。为了筛选出能作为造影剂载体用于凋亡成像的PS结合肽,将一个噬菌体文库作用于灌注的小鼠肝脏。在首次灌注期间未保留在对照肝脏上的噬菌体用于第二轮灌注中在凋亡肝脏上进行筛选。对四个筛选出的噬菌体进一步评估其与包被有PS的酶联免疫吸附测定(ELISA)板的结合情况。它们对PS的表观亲和常数(Ka app)范围为6.08×10¹⁰ M至1.62×10¹¹ M。这些噬菌体不与磷脂酰胆碱结合,与膜联蛋白V的竞争证实了它们与PS的特异性相互作用。在ELISA中具有最高亲和力的噬菌体结合PS,Ka app =(1.6±0.2)×10¹¹ M。它携带合成的TLVSSL肽。进行了与膜联蛋白V和合成肽的特异性竞争,证实了相互作用的特异性。

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