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Lipid nanoparticles loaded with butamben and designed to improve anesthesia at inflamed tissues

机译:脂质纳米粒子用丁剑纳装载并旨在改善发炎组织的麻醉

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摘要

The most frequently used local anesthetics (LA) for local infiltration have an ionizable amine in the range of pH 7.6-8.9. Effective anesthesia of inflamed tissues is a great challenge, especially because the induced local acidosis decreases the fraction of the neutral (more potent) LA species in situ. To solve this limitation, the butyl-substituted benzocaine analogue butamben (BTB) - that has no ionizable amine group close to the physiological pH - could be useful if it was not for its low solubility. To overcome the solubility problem, an optimized formulation for BTB using nanostructured lipid carriers (NLC) was developed by a factorial design and characterized using DLS, XRD, DSC and cryo-EM. The release kinetics and cytotoxicity of the new formulation were measured in vitro, while the in vivo tests assessed its effectiveness on healthy and inflamed tissues, in rats. The optimized NLC_(BTB) formulation showed desirable physicochemical properties (size = 235.6 ± 3.9 nm, polydispersity = 0.182 ± 0.006 and zeta potential = -23.6 ± 0.5 mV), high (99.5%) encapsulation efficiency and stability during 360 days of storage at room temperature. NLC_(BTB) prolonged the release of butamben and decreased its in vitro cytotoxicity without inducing any in vivo toxic alteration. In the inflammatory hyperalgesia model, the NLC_(BTB) formulation showed potential for the management of inflammatory pain, displaying greater analgesic effectiveness (40%) and a prolonged effect.
机译:用于局部浸润的最常用的局部麻醉剂(LA)在pH 7.6-8.9的范围内具有可电离的胺。发炎组织的有效麻醉是一个巨大的挑战,特别是因为诱导的当地酸中毒降低了原位中性(更有效)LA物种的级分。为了解决这种限制,丁基取代的苯并催化丁香蛋白(BTB) - 如果不是其低溶解度,则没有可电离的胺基靠近生理pH的可电离胺基。为了克服溶解度问题,通过占型设计开发了使用纳米结构脂质载体(NLC)的BTB的优化配方,并使用DLS,XRD,DSC和Cryo-EM表征。在体外测量新配方的释放动力学和细胞毒性,而体内试验在大鼠中评估其对健康和发炎组织的有效性。优化的NLC_(BTB)制剂显示出理想的物理化学性质(尺寸= 235.6±3.9nm,Polydispersity = 0.182±0.006和Zeta电位= -23.6±0.5 mV),在360天的储存期间,高(99.5%)封装效率和稳定性室内温度。 NLC_(BTB)延长了Butamben的释放,并降低了其体外细胞毒性,而不会诱导任何体内有毒的改变。在炎症性痛觉过敏模型中,NLC_(BTB)制剂显示出炎症疼痛的管理,呈现更大的镇痛效果(40%)和延长效应。

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  • 来源
    《Biomaterials Science》 |2021年第9期|共12页
  • 作者单位

    Department of Biochemistry and Tissue Biology Institute of Biology University of Campinas - UNICAMP Campinas Sao Paulo Brazil;

    Department of Structural and Functional Biology Institute of Biology UNICAMP Brazil;

    Department of Biochemistry and Tissue Biology Institute of Biology University of Campinas - UNICAMP Campinas Sao Paulo Brazil;

    Department of Biochemistry and Tissue Biology Institute of Biology University of Campinas - UNICAMP Campinas Sao Paulo Brazil;

    Department of Biochemistry and Tissue Biology Institute of Biology University of Campinas - UNICAMP Campinas Sao Paulo Brazil;

    Faculty of Health Sciences Federal University of Grande Dourados Dourados MS Brazil;

    Department of Structural and Functional Biology Institute of Biology UNICAMP Brazil;

    Department of Structural and Functional Biology Institute of Biology UNICAMP Brazil;

    Department of Analytical Chemistry Institute of Chemistry UNICAMP Brazil;

    Department of Structural and Functional Biology Institute of Biology UNICAMP Brazil;

    Department of Biochemistry and Tissue Biology Institute of Biology University of Campinas - UNICAMP Campinas Sao Paulo Brazil;

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  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 计量学;
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