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首页> 外文期刊>Langmuir: The ACS Journal of Surfaces and Colloids >Probing Peptide Sequences on Their Ability to Generate Affinity Sites in Molecularly Imprinted Polymers
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Probing Peptide Sequences on Their Ability to Generate Affinity Sites in Molecularly Imprinted Polymers

机译:探测肽序列在分子印迹聚合物中产生亲和位点的能力

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摘要

An array of 4000 defined and addressable tripeptides on a polymer-coated glass slide is used to synthesize molecularly imprinted polymer (MIP) nanoparticles. This work is undertaken to systematically probe the impact of the peptide sequence on the ability to generate affinity MIPs. The polymer affinity is assessed by measuring the fluorescence of bound MIP nanoparticles at each peptide spot on the surface after washing the array to remove any low-affinity polymer. The generic composition commonly used in the preparation of MIPs against proteins seems to be equally suitable for imprinting hydrophobic and hydrophilic tripeptides. The amino acids frequently contributing to the formation of high-affinity MIPs include T, F, D, N, Y, W, and P. The amino acids that rarely contribute to the formation of high-affinity interactions with MIPs are G, V, A, L, I, and M. These observations are confirmed by computational modeling. The basic technique proposed here may be applicable in optimizing polymer compositions for the production of high-affinity MIPs or, more specifically, for the selection of appropriate amino acid sequences when peptide epitopes are used instead of whole protein imprinting.
机译:聚合物涂层玻璃载玻片上的4000个定义和可寻址的三肽阵列用于合成分子印迹聚合物(MIP)纳米颗粒。该工作是为了系统地探测肽序列对产生亲和力MIPS的能力的影响。通过在洗涤阵列后测量表面上的每个肽点处的结合MIP纳米颗粒的荧光来评估聚合物亲和力,以除去任何低亲和聚合物。常用于蛋白质MIPS的通用组合物似乎同样适用于印刷疏水性和亲水性三肽。经常促进高亲和力MIP的形成的氨基酸包括T,F,D,N,Y,W和P.很少有助于形成与MIPS的高亲和相互作用的氨基酸是G,V, A,L,I和M.通过计算建模确认这些观察结果。此处所提出的基本技术可适用于优化用于生产高亲和力MIP的聚合物组合物,或者更具体地,在使用肽表位而不是全蛋白质印记时选择适当的氨基酸序列。

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