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首页> 外文期刊>Bioorganic and medicinal chemistry >Synthesis and screening of a cyclic peptide library: discovery of small-molecule ligands against human prolactin receptor.
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Synthesis and screening of a cyclic peptide library: discovery of small-molecule ligands against human prolactin receptor.

机译:环状肽文库的合成和筛选:发现针对人类催乳素受体的小分子配体。

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摘要

Prolactin receptor is involved in normal lactation and reproduction; however, excessive prolactin levels can cause various reproductive disorders such as prolactinomas. Small-molecule antagonists against the human prolactin receptor (hPRLr) thus have potential clinical applications and may serve as useful molecular probes in biomedical research. In this work, we synthesized a large, support-bound cyclic peptide library (theoretical diversity of 1.2x10(7)) on 90-microm TentaGel beads and screened it against the extracellular domain of hPRLr. To facilitate hit identification, each TentaGel bead was spatially segregated into outer and inner layers, with a cyclic peptide displayed on the bead surface while the bead interior contained the corresponding linear peptide. The identity of a positive bead was revealed by sequencing the linear encoding peptide within the bead by partial Edman degradation/mass spectrometry. Screening of the library resulted in 20 hits, two of which were selected for further analysis and shown to bind to hPRLr with dissociation constants of 2-3 microM.
机译:催乳素受体参与正常的泌乳和生殖。但是,催乳素水平过高会导致各种生殖疾病,如催乳素瘤。因此,针对人类催乳激素受体(hPRLr)的小分子拮抗剂具有潜在的临床应用,并可作为生物医学研究中的有用分子探针。在这项工作中,我们在90微米的TentaGel磁珠上合成了一个大型的,与支持物结合的环状肽文库(理论多样性为1.2x10(7)),并针对hPRLr的胞外域进行了筛选。为了便于命中识别,将每个TentaGel珠在空间上分为外层和内层,并在珠表面上显示环状肽,而珠内部包含相应的线性肽。通过部分Edman降解/质谱法对小珠内的线性编码肽进行测序,可以揭示阳性小珠的身份。文库的筛选导致20个命中,其中两个被选作进一步分析,并显示以2-3 microM的解离常数与hPRLr结合。

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