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Long-circulating 15 nm micelles based on amphiphilic 3-helix peptide-peg conjugates

机译:基于两亲性3-螺旋肽-PEG共轭物的长循环15 nm胶束

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Figure Persented: Generating stable, multifunctional organic nanocarriers will have a significant impact on drug formulation. However, it remains a significant challenge to generate organic nanocarriers with a long circulation half-life, effective tumor penetration, and efficient clearance of metabolites. We have advanced this goal by designing a new family of amphiphiles based on coiled-coil 3-helix bundle forming peptide-poly(ethylene glycol) conjugates. The amphiphiles self-assemble into monodisperse micellar nanoparticles, 15 nm in diameter. Using the 3-helix micelles, a drug loading of ~8 wt % was obtained using doxorubicin and the micelles showed minimal cargo leakage after 12 h of incubation with serum proteins at 37 °C. In vivo pharmacokinetics studies using positron emission tomography showed a circulation half-life of 29.5 h and minimal accumulation in the liver and spleen. The demonstrated strategy, by incorporating unique protein tertiary structure in the headgroup of an amphiphile, opens new avenues to generate organic nanoparticles with tunable stability, ligand clustering, and controlled disassembly to meet current demands in nanomedicine.
机译:可能的图:生成稳定的多功能有机纳米载体将对药物配方产生重大影响。然而,产生具有长的循环半衰期,有效的肿瘤渗透和有效清除代谢物的有机纳米载体仍然是一项重大挑战。我们通过基于卷曲螺旋3-螺旋束形成肽-聚(乙二醇)共轭物设计一个新的两亲家族来实现此目标。两亲物自组装成直径为15 nm的单分散胶束纳米颗粒。使用3螺旋胶束,使用阿霉素可获得约8 wt%的载药量,并且在37°C与血清蛋白孵育12小时后,胶束显示出最小的货物泄漏。使用正电子发射断层显像的体内药代动力学研究表明,循环半衰期为29.5小时,并且在肝脏和脾脏中的积累最小。通过在两亲物的头基中引入独特的蛋白质三级结构,已证明的策略为开发具有可调稳定性,配体簇和受控分解的有机纳米颗粒开辟了新途径,从而满足了纳米药物的当前需求。

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