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聚丙烯酸微凝胶对共有肽的结合与释放

Binding and release of consensus peptides by poly(acrylic acid) microgels.

作者信息

Bysell Helena, Schmidtchen Artur, Malmsten Martin

机构信息

Department of Pharmacy, Uppsala University, SE-751 23 Uppsala, Sweden.

出版信息

Biomacromolecules. 2009 Aug 10;10(8):2162-8. doi: 10.1021/bm9003354.

Abstract

The interaction between positively charged consensus peptides and poly(acrylic acid) microgels was investigated with micromanipulator-assisted light microscopy and confocal laser scanning microscopy. Peptide binding and release was monitored by microgel deswelling and swelling for monodisperse multiples of heparin-binding Cardin and Weintraub motifs, (AKKARA)(n) (1 <or= n <or= 4) and (ARKKAAKA)(n) (1 <or= n <or= 3), as well as the corresponding titratable (AHHAHA)(4) and (AHHHAAHA)(3) peptides (A, K, R and H, refering to alanine, lysine, arginine, and histidine, respectively). When fully charged, these peptides distribute homogenously throughout the microgels and display concentration-dependent deswelling, which increases with increasing peptide length. Both (AKKARA)(4) and (ARKKAAKA)(3) display potent and fast microgel deswelling but only marginal subsequent electrolyte-induced desorption. In contrast, reducing the peptide charge for (AHHAHA)(4) and (AHHHAAHA)(3) at neutral and high pH, or the peptide length, substantially reduces the peptide affinity for the microgels and facilitates rapid peptide release. Taken together, the results also show that quite short peptides of moderate charge density interact strongly and cause extensive gel deswelling of oppositely charged microgels, precluding peptide release. They also show, however, that desirable triggered release can be achieved with peptides of lower charge density.

摘要

利用微操纵器辅助光学显微镜和共聚焦激光扫描显微镜研究了带正电荷的共有肽与聚丙烯酸微凝胶之间的相互作用。通过微凝胶的溶胀和收缩来监测肽的结合和释放情况,这些肽包括肝素结合卡丹和温特劳布基序的单分散倍数,即(AKKARA)(n)(1≤n≤4)和(ARKKAAKA)(n)(1≤n≤3),以及相应的可滴定肽(AHHAHA)(4)和(AHHHAAHA)(3)(A、K、R和H分别代表丙氨酸、赖氨酸、精氨酸和组氨酸)。当完全带电时,这些肽均匀分布在整个微凝胶中,并呈现出浓度依赖性的溶胀,这种溶胀随着肽长度的增加而增大。(AKKARA)(4)和(ARKKAAKA)(3)都表现出强烈且快速的微凝胶溶胀,但随后只有少量的电解质诱导解吸。相比之下,在中性和高pH条件下降低(AHHAHA)(4)和(AHHHAAHA)(3)的肽电荷或缩短肽长度,会显著降低肽对微凝胶的亲和力,并促进肽的快速释放。综上所述,结果还表明,电荷密度适中的相当短的肽会强烈相互作用,并导致带相反电荷的微凝胶大量溶胀,从而阻止肽的释放。然而,结果也表明,电荷密度较低的肽可以实现理想的触发释放。

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