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Berunda Polypeptides: Multi-Headed Fusion Proteins Promote Subcutaneous Administration of Rapamycin to Breast Cancer In Vivo

机译:Berunda多肽:多头融合蛋白促进雷帕霉素对乳腺癌的体内皮下给药。

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Recombinant Elastin-Like Polypeptides (ELPs) serve as attractive scaffolds for nanoformulations because they can be charge-neutral, water soluble, high molecular weight, monodisperse, biodegradable, and decorated with functional proteins. We recently reported that fusion of the FK-506 binding protein 12 (FKBP) to an ELP nanoparticle (FSI) reduces rapamycin (Rapa) toxicity and enables intravenous (IV) therapy in both a xenograft breast cancer model and a murine autoimmune disease model. Rapa has poor solubility, which leads to variable oral bioavailability or drug precipitation following parenteral administration. While IV administration is routine during chemotherapy, cytostatic molecules like Rapa would require repeat administrations in clinical settings. To optimize FKBP/Rapa for subcutaneous (SC) administration, this manuscript expands upon first-generation FSI nanoparticles ( Rh ~ 25 nm) and compares them with two second-generation carriers (FA and FAF) that: i) do not self-assemble; ii) retain a hydrodynamic radius ( Rh ~ 7 nm) above the renal filtration cutoff; iii) increase tumor accumulation; and iv) have either one (FA) or two (FAF) drug-binding FKBP domains per ELP protein.
机译:重组弹性蛋白样多肽(ELP)可以用作纳米制剂的诱人支架,因为它们可以是电荷中性的,水溶性,高分子量,单分散性,可生物降解的,并可以用功能蛋白修饰。最近,我们报道了FK-506结合蛋白12(FKBP)与ELP纳米颗粒(FSI)的融合降低了雷帕霉素(Rapa)的毒性,并能够在异种移植乳腺癌模型和鼠自身免疫性疾病模型中进行静脉(IV)治疗。拉帕的溶解性差,导致肠胃外给药后口服生物利用度变化或药物沉淀。虽然在化疗期间常规静脉内给药,但像Rapa这样的细胞抑制分子将需要在临床环境中重复给药。为了优化用于皮下(SC)给药的FKBP / Rapa,该手稿扩展了第一代FSI纳米颗粒(R h 〜25 nm),并将它们与两种第二代载体(FA和FAF)进行了比较:i)不要自行组装; ii)保留肾滤过边界以上的流体力学半径(R h 〜7 nm); iii)增加肿瘤积累; iv)每个ELP蛋白具有一个(FA)或两个(FAF)药物结合性FKBP结构域。

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