Characteristics and Transdermal Drug Delivery of Triamcinolone-Acetonide-Acetate-Loaded Solid Lipid Nanoparticles Carbomer Gel

Aim To prepare triamcinolone-acetonide-acetate (TAA)-loaded solid lipidnanoparticles (SLN) carbomer gel with tripalmitin glyceride (TPG), and investigate theircharacteristics and transdermal drug delivery. Methods SLN suspension was prepared by high-pressurehomogenization technique, and then mixed with carbomer gel matrix to get SLN gel. The morphology,particle size with polydispersi-ty index (PI) and zeta potential were examined by atomic forcemicroscopy (AFM) and photon correlation spectroscopy (PCS). The entrapment efficiency, stability andin vitro drug release were also studied. The transdermal drug delivery through porcine ear skin wasevaluated using modified Franz diffusion cells. Results The SLN had a spherical shape with theaverage size of (95.5 - 186.2) nm, the zeta potential of (-26.3- -15.7) mV and the entrapmentefficiency of 67.4%-90.3% for different TAA encapsulated compounds. TAA-SLN carbomer gel had goodstability, the release profile in vitro fitted Higuchi equation. In comparison with conventionalhydrogels, TAA-SLN carbomer gel resulted in higher drug permeation amount and drug deposition withinporcine ear skin after 24 h penetration experiment. Conclusion TAA-SLN carbomer gel is preparedwith stable physicochemical properties. The release profile and improved drug permeation into skinmake it be a promising vehicle for transdermal drug delivery.

Recent advances in arsenic trioxide encapsulated nanoparticles as drug delivery agents to solid cancers

Since arsenic trioxide was first approved as the front line therapy for acute promyelocytic leukemia 25 years ago,its anti-cancer properties for various malignancies have been under intense investigation.However,the clinical successes of arsenic trioxide in treating hematological cancers have not been translated to solid cancers.This is due to arsenic＇s rapid clearance by the body＇s immune system before reaching the tumor site.Several attempts have henceforth been made to increase its bioavailability toward solid cancers without increasing its dosage albeit without much success.This review summarizes the past and current utilization of arsenic trioxide in the medical field with primary focus on the implementation of nanotechnology for arsenic trioxide delivery to solid cancer cells.Different approaches that have been employed to increase arsenic＇s efficacy,specificity and bioavailability to solid cancer cells were evaluated and compared.The potential of combining different approaches or tailoring delivery vehicles to target specific types of solid cancers according to individual cancer characteristics and arsenic chemistry is proposed and discussed.

Preparation and evaluation of alpha-mangostin solid self-emulsifying drug delivery system

Alpha-mangostin(AMG),a natural xanthone extracted from Garcinia mangostana Linn,has a variety of pharmacological therapeutic effects such as antioxidant activity,antibacterial activity,anticancer,and anti-inflammatory[1].However,it has poor aqueous-solubility and dissolution,which results in low bioavailability.Solid self-emulsifying drug delivery system(solid-SEDDS),an effective pharmaceutical strategy,offers the potential for enhancing the oral bioavailability of poorly water-soluble drugs[2].Therefore,solid-SEDDS is of interest as a potential method for enhancing the solubility and dissolution of AMG.

Research progress of triptolide-loaded nanoparticles delivery systems

This paper reviewed the study of triptolide-loaded nano delivery systems (NDOS) in our group during the past. It was investigated for the preparation, characterization, pharmacology and toxicology of solid lipid nanoparticles (SLN), microemulsion and polymeric nanoparticles. The results indicated that the NDS presented more powerful activity and a lower toxicity in comparison with other drug carrier.

脂质纳米粒在经皮给药系统中治疗皮肤病的应用

经皮给药作为一种非侵入性给药方式,正逐渐受到广大医药工作者和患者的青睐。然而,皮肤角质层的屏障功能限制了药物的经皮吸收。脂质纳米粒作为一种新型的药物载体能够有效提高皮肤渗透性、减少药物相关副作用。本文就脂质纳米粒的特点、透皮作用机制以及在多种皮肤病中的应用做一综述,阐明脂质纳米粒在经皮给药领域的广阔发展前景,为脂质纳米粒的开发及临床应用提供参考。

Recent advances in drug delivery applications of cubosomes,hexosomes,and solid lipid nanoparticles

The use of lipid nanocarriers for drug delivery applications is an active research area,and a great interest has particularly been shown in the past two decades.Among different lipid nanocarriers,ISAsomes(Internally self-assembled somes or particles),including cubosomes and hexosomes,and solid lipid nanoparticles(SLNs)have unique structural features,making them attractive as nanocarriers for drug delivery.In this contribution,we focus exclusively on recent advances in formation and characterization of ISAsomes,mainly cubosomes and hexosomes,and their use as versatile nanocarriers for different drug delivery applications.Additionally,the advantages of SLNs and their application in oral and pulmonary drug delivery are discussed with focus on the biological fates of these lipid nanocarriers in vivo.Despite the demonstrated advantages in in vitro and in vivo evaluations including preclinical studies,further investigations on improved understanding of the interactions of these nanoparticles with biological fuids and tissues of the target sites is necessary for effcient designing of drug nanocarriers and exploring potential clinical applications.

固体脂质纳米粒作为药物载体

固体脂质纳米粒是一种新型的纳米给药系统。本文综述了固体脂质纳米粒作为药物载体的研究进展,包括固体脂质纳米粒的组分选择、制备方法、表面修饰,并且对物化性质分析、给药途径以及载药和释放进行了讨论。

固体脂质纳米粒的研究进展

目的综述固体脂质纳米粒的最新研究进展。方法以国内外大量有代表性的论文为依据,将固体脂质纳米粒的制备方法、特性分析、药物载入、药物释放及应用情况进行了概括,指出了发展前景和尚待解决的问题。结果固体脂质纳米粒的多种制备方法各有优、缺点,调整制备参数可调整药物的包封率和释药曲线。结论固体脂质纳米粒可供多途径给药,是极有发展前景的新型给药系统。

经内耳途径靶向脑给药的初步研究

本文探寻经内耳途径输送药物到脑部的可行性,为脑靶向给药提供一条崭新的研究思路。制备醋酸地塞米松(DA)固体脂质纳米粒(SLN),建立相应的HPLC含量测定方法。经静脉和鼓室注射DA-SLN,并与地塞米松磷酸钠(DSP)溶液相比较,测定药物在脑脊液(CSF)和内耳外淋巴液(PL)中的浓度及药代动力学参数。结果表明,与静脉注射比较,鼓室注射药物在CSF的局部生物利用度显著提高,鼓室注射DA-SLN比静脉注射高2.5倍,鼓室注射DSP溶液比静脉注射高4.3倍。与DSP溶液比较,鼓室注射DA-SLN能明显增加进入CSF的药量和延长药物的作用时间,AUC和MRT分别较前者高13和19倍;并且药物在PL中分布减少,其AUC低76%。提示经内耳途径给药有望成为一种新的脑靶向方法,值得进一步研究。

肝靶向氟尿嘧啶类脂纳米粒的研究

目的 为了提高氟尿嘧啶 (5 Fu)的疗效 ,降低其毒副作用 ,制备具肝靶向的 5 Fu类脂纳米粒。方法 利用氟尿嘧啶与硬脂酰氯进行反应 ,制备了 5 Fu前体药物N1 硬脂酰 5 Fu ,通过红外光谱及核磁共振谱对合成的目标化合物进行结构确认。同时研究了前体药物的性质及稳定性。采用物理凝聚法制备类脂纳米粒 ,并研究其形态、粒径及粒径分布、载药量、体外释药特征、动物体内分布与药代动力学参数等。结果 平均粒径dav=2 40 19nm ,载药量为 2 0 5 3 %。体外释药速率符合一级动力学模型。与 5 Fu水针剂比较 ,类脂纳米粒组在肝脏中药物含量平均增加了一倍以上。家兔体内主要药动学参数为 :Vc=0 0 4336L·kg-1,T1/ 2 β =1 2 834h ,CL =0 16 32L·h-1。结论 利用前体药物可提高药物的脂溶性 ,首次以物理凝聚法制备类脂纳米粒 ,小鼠体内分布研究表明类脂纳米粒有明显的肝靶向 。

肝靶向阿克拉霉素A固体脂质纳米粒质量考察及体内分布研究

目的为促进固体脂质纳米粒(SLN)的发展,提高阿克拉霉素A(ACM-A)的疗效,制备具有肝靶向的阿克拉霉素A固体脂质纳米粒(ACM-SLN)冻干针剂,并对其质量和体内组织分布进行研究。方法采用正交设计优化ACM-SLN及其冻干针剂的处方和制备工艺,并研究其形态、粒径及粒径分布、载药量,稳定性和动物体内分布。结果得到的ACM-SLN平均粒径为62 nm,平均载药量为4.41%,平均包封率为88.17%。体内分布研究结果表明,15,30和60 min时ACM-SLN冻干针剂在肝脏中的药物浓度分别为30.379,32.591和30.416 mg·L^-1而对应的ACM-A溶液剂的质量浓度分别为10.795,12.796和10.135 mg·L^-1结论得到的ACM-SLN冻干针剂基本稳定。与ACM-A溶液剂相比,ACM-SLN冻干针剂显著提高了ACM- A在靶器官肝脏中的药物水平。

十六酸拉米夫定酯固体脂质纳米粒的制备

目的 :为了提高拉米夫定 (lamivudine ,LA)的疗效 ,降低其毒副作用 ,制备十六酸拉米夫定酯固体脂质纳米粒(LAP SLN) .方法 :在二环己基碳二亚胺和 4 二甲氨基吡啶存在时 ,LA与十六酸反应 ,制备十六酸拉米夫定酯 (lamivudylpalmitate,LAP) ,并测定其核磁共振氢谱 .RP HPLC测定其在正辛醇和磷酸盐缓冲液中的分配系数及不同 pH缓冲液和组织匀浆中的稳定性 .采用薄膜分散法制备LAP SLN ;透射电镜研究其形态、粒径及粒径分布 ;RP HPLC测定载药量、包封率 .结果 :LAP在弱酸性溶液中较稳定 ,在弱碱性溶液中水解较快 ;在血清和组织匀浆中易水解 ,在肝匀浆中水解最快 ;LAP分配系数为 5 2 .2 .LAP SLN粒径为 (2 81± 98)nm ,载药量为 9.6 % ,包封率为 97.7% .结论 :LA转化成LAP后亲脂性增加 ;LAP SLN包封率较高 。

十六酸拉米夫定酯固体脂质纳米粒的肝靶向研究

目的 制备十六酸拉米夫定酯固体脂质纳米粒 (LAP -SLN)和半乳糖苷修饰的十六酸拉米夫定酯固体脂质纳米粒(LAP -GSLN) ,探讨并比较二者的肝靶向作用。方法 采用薄膜超声分散法制备LAP -SLN和LAP -GSLN ;透射电镜研究其形态、粒径及粒径分布 ;RP -HPLC测定载药量、包封率。小鼠尾静脉给药后 ,RP -HPLC测定拉米夫定 (Lamivudine ,LA)在血清及肝、肾、肺、脾中的浓度。结果 LAP -SLN和LAP -SLN的粒径分布分别为 2 80 .8± 98.2nm和 2 5 7.4± 92 .3nm ,载药量分别为 9.6 3%和 9.11% ,包封率分别为 97.6 9%和 95 .82 %。LA -sol,LAP -SLN和LAP -GSLN的靶向效率分别为 0 .89,1.2 6和 4 .6 6。结论 LAP -SLN和LAP -GSLN在体内具有良好的肝靶向性 ,对提高药物疗效 ,减少用量 ,降低毒副作用有一定意义。LAP -GSLN的靶向作用强于LAP -SLN。

固体脂质纳米粒和纳米结构脂质载体在经皮给药系统中的研究进展

目的介绍固体脂质纳米粒和纳米结构脂质载体在经皮给药系统中的应用与优势,为其开发利用提供参考。方法查阅国内外相关文献共30余篇,从固体脂质纳米粒和纳米结构脂质载体用于经皮给药系统的优势、药物在固体脂质纳米粒和纳米结构脂质载体中的分布形式及固体脂质纳米粒和纳米结构脂质载体在经皮给药领域中的应用等方面进行综述。结果固体脂质纳米粒和纳米结构脂质载体可以增强药物稳定性,能在皮肤表面产生包封效应,增加皮肤水合作用,具有药物靶向性。结论固体脂质纳米粒和纳米结构脂质载体是极有发展前景的新型经皮给药系统。

氟尿苷二乙酸酯固体脂质纳米粒的制备

目的为了提高氟尿苷(FUDR)的疗效,降低其毒副作用而制备氟尿苷二乙酸酯固体脂质纳米粒(FUDRA-SLN).方法在吡啶和4-二甲氨基吡啶存在时,FUDR与乙酸酐反应,制备氟尿苷二乙酸酯,并测定其核磁共振氢谱.RP-HPLC测定其在正辛醇和磷酸盐缓冲液中的分配系数及不同pH缓冲液和组织匀浆中的稳定性.采用薄膜分散法制备FUDRA-SLN;透射电镜研究其形态、粒径及粒径分布;RP-HPLC测定载药量、包封率.结果制备成的FUDRA在弱酸性溶液中较稳定,在弱碱性溶液中水解较快;在血清和组织匀浆中易水解,在肝匀浆中水解最快;FUDRA分配系数为58.13.FUDRA-SLN粒径为(208±53)nm,载药量为7.63%,包封率为94.21%.结论FUDR转化成FUDRA后亲脂性大大增加;FUDRA-SLN包封率较高,粒径分布较均匀.

生理参数及药物注射方式对球形实体肿瘤中药物输运的影响

目的研究球形实体肿瘤中生理参数对药物输运的影响,以及探讨有较好效果的药物注射方式。方法设肿瘤中毛细血管网成球对称分布,肿瘤中的毛细血管表面积和肿瘤体积之比为半径的函数。肿瘤间质为多孔介质,化学药物透过毛细血管壁进入肿瘤间质,在肿瘤间质中输运满足扩散方程。肿瘤外正常组织富含血管和淋巴,药物能被淋巴管吸收,药物输运采用改进的药代动力学模型。用肿瘤中各部位药物浓度维持在最小药物浓度MEC水平以上的时间曲线面积(AUC)来衡量药物的效果。结果增大肿瘤间质中毛细血管对药物的通透性P,提高药物在肿瘤间质的扩散系数D,AUC的值均增大。在给出的六种给药方式中,分时段连续滴注和等时间间隔一次性注射的给药方式,它们的AUC值最大。结论增大肿瘤间质中毛细血管对药物的通透性,提高药物在肿瘤间质的扩散系数,以及采用分时段连续滴注和等时间间隔一次性注射的给药方式,有利于肿瘤的治疗。

多西他赛自乳化固体分散体的制备及体外特性研究

目的制备多西他赛自乳化固体分散体(DTX-SESD),并考察其体外特性。方法以自乳化辅料和PEG6000为载体制备多西他赛固体分散体,进行溶解度、体外溶出度和稳定性实验,考察不同自乳化辅料、不同制备方法、不同介质对溶出度的影响。并采用差示扫描量热分析、X-射线粉末衍射分析以鉴别药物在载体中的存在状态。结果 DTX-SESD的溶解度和溶出度分别是原料药的约33.8倍和12.5(2 h)倍;自乳化辅料对药物溶出有显著影响;溶剂法和溶剂熔融法制备的自乳化固体分散体溶出度好于熔融法;溶出介质对溶出无显著影响;自乳化固体分散体中药物主要以分子状态存在。结论自乳化固体分散体能显著提高多西他赛的溶解度和溶出度。

实体肿瘤内微循环及药物传递的三维数值模拟

目的研究实体肿瘤内微环境流动特征及大分子药物在肿瘤组织内的输运过程。方法建立模拟肿瘤血液动力学及药物输运的三维模型。模拟肿瘤内的微循环以及两种大分子药物在肿瘤内的浓度分布。结果模拟结果很好地反映了肿瘤内异常的血液动力学特性,以及由此造成的药物输运屏障、浓度分布不均匀性等特征。研究还表明,分子量较小的药物更易在肿瘤组织内传递,也更易随着组织液流动向肿瘤外排出;分子量较大的药物较易在肿瘤内部积聚,从而能在较长时间内保持一定的有效药物浓度。结论本模型计算结果与生理实际相符,为研究肿瘤微环境,药物输运,以及制定药物治疗策略提供了可信的模型及数值研究手段。