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Amino Acid-Dependent Attenuation of Toll-like Receptor Signaling by Peptide-Gold Nanoparticle Hybrids

机译:肽-金纳米粒子杂种的Toll样受体信号的氨基酸依赖性衰减。

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Manipulation of immune responsiveness using nanodevices provides a potential approach to treat human diseases. Toll-like receptor (TLR) signaling plays a central role in the pathophysiology of many acute and chronic human inflammatory diseases, and pharmacological regulation of TLR responses is anticipated to be beneficial in many of these inflammatory conditions. Here we describe the discovery of a unique class of peptide-gold nanoparticle hybrids that exhibit a broad inhibitory activity on TLR signaling, inhibiting signaling through TLRs 2, 3, 4, and 5. As exemplified using TLR4, the nanoparticles were found to inhibit both arms of TLR4 signaling cascade triggered by the prototypical ligand, lipopolysaccharide (LPS). Through structure-activity relationship studies, we identified the key chemical components of the hybrids that contribute to their immunomodulatory activity. Specifically, the hydrophobicity and aromatic ring structure of the amino acids on the peptides were essential for modulating TLR4 responses. This work enhances our fundamental understanding of the role of nanoparticle surface chemistry in regulating innate immune signaling, and identifies specific nanoparticle hybrids that may represent a unique class of anti-inflammatory therapeutics for human inflammatory diseases.
机译:使用纳米装置操纵免疫应答性提供了治疗人类疾病的潜在方法。 Toll样受体(TLR)信号在许多急性和慢性人类炎症性疾病的病理生理学中起着核心作用,TLR反应的药理学调节有望在许多此类炎症性疾病中受益。在这里,我们描述了发现一类独特的肽-金纳米颗粒杂种的发现,该杂种对TLR信号传导具有广泛的抑制活性,抑制了通过TLR 2、3、4和5的信号传导。 TLR4信号臂由原型配体脂多糖(LPS)触发。通过结构-活性关系研究,我们确定了有助于其免疫调节活性的杂种的关键化学成分。具体而言,肽上氨基酸的疏水性和芳香环结构对于调节TLR4反应至关重要。这项工作增强了我们对纳米颗粒表面化学在调节先天性免疫信号传导中作用的基础理解,并鉴定了特定的纳米颗粒杂种,这些杂种代表了人类炎性疾病的独特抗炎治疗剂。

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