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首页> 外文期刊>Journal of Turbulence >Ocular Cubosome Drug Delivery System for Timolol Maleate: Preparation, Characterization, Cytotoxicity, Ex Vivo, and In Vivo Evaluation
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Ocular Cubosome Drug Delivery System for Timolol Maleate: Preparation, Characterization, Cytotoxicity, Ex Vivo, and In Vivo Evaluation

机译:用于蒂莫尔马来酸的眼科委托药物递送系统:制备,表征,细胞毒性,离体和体内评价

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摘要

Glaucoma is an ocular disease featuring increased intraocular pressure (IOP) and its primary treatment strategy is to lower IOP by medication. Current ocular drug delivery in treating glaucoma is confronting a variety of challenges, such as low corneal permeability and bioavailability due to the unique anatomical structure of the human eye. To tackle these challenges, a cubosome drug delivery system for glaucoma treatment was constructed for timolol maleate (TM) in this study. The TM cubosomes (liquid crystalline nanoparticles) were prepared using glycerol monooleate and poloxamer 407 via high-pressure homogenization. These constructed nanoparticles appeared spherical using transmission electron microscopy and had an average particle size of 142 nm, zeta potential of -6.27 mV, and over 85% encapsulation efficiency. Moreover, using polarized light microscopy and small-angle X-ray scattering (SAXS), it was shown that the TM cubosomes have cubic liquid crystalline D-type (Pn3m) structure, which provides good physicochemical stability and high encapsulation efficiency. Ex vivo corneal permeability experiments showed that the total amount of TM cubosomes penetrated was higher than the commercially available eye drops. In addition, in vivo studies revealed that TM cubosomes reduced the IOP in rabbits from 27.8 similar to 39.7 to 21.4 similar to 32.6 mmHg after 1-week administration and had a longer retention time and better lower-IOP effect than the commercial TM eye drops. Furthermore, neither cytotoxicity nor histological impairment in the rabbit corneas was observed. This study suggests that cubosomes are capable of increasing the corneal permeability and bioavailability of TM and have great potential for ocular disease treatment.
机译:青光眼是一种具有较高的眼内压(IOP)的眼部疾病,其主要治疗策略是通过药物降低IOP。当前眼镜药物递送治疗青光眼面临各种挑战,例如由于人眼的独特解剖结构,例如低角膜渗透性和生物利用度。为了解决这些挑战,在本研究中为蒂莫尔马来酸(TM)构建了一种青光眼处理的委托药物输送系统。通过高压均质化制备使用甘油单烯烃和泊洛膦酯407制备TM立方体(液晶纳米颗粒)。这些构造的纳米颗粒使用透射电子显微镜出现球形,平均粒度为142nm,Zeta电位为-6.27mV,封装效率超过85%。此外,使用偏振光显微镜和小角度X射线散射(SAX),示出了TM立方体具有立方液晶D型(PN3M)结构,可提供良好的物理化学稳定性和高封装效率。前体内角膜渗透性实验表明,穿透的TM缔约肌的总量高于市售的眼药水。此外,在体内研究表明,TM委员会将兔子的IOP降低27.8,类似于39.7至21.4,类似于39.7至21.4,在1周给药后的32.6mmHg,并且具有比商业TM滴眼液更长的保留时间和更好的降低IOP效果。此外,观察到兔角膜中的细胞毒性也不是组织学障碍。该研究表明,缔约肌能够增加TM的角膜渗透性和生物利用度,并且具有巨大的眼部疾病治疗潜力。

著录项

  • 来源
    《Journal of Turbulence》 |2017年第8期|共8页
  • 作者单位

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

    Univ Surrey Dept Chem &

    Proc Engn Guildford GU2 7XH Surrey England;

    Sun Yat Sen Univ Sch Pharmaceut Sci 132 Waihuan East Rd Higher Educ Mega Ctr Guangzhou 510006 Guangdong Peoples R China;

  • 收录信息
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类 流体力学;
  • 关键词

    cubosome; glaucoma; ocular drug delivery; timolol maleate;

    机译:卧牙;青光眼;眼药递送;蒂洛尔马来酸;

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