Liposomal propranolol for treatment of infantile hemangioma at compounding pharmacies.

IF 3.6 4区 医学 Q2 BIOCHEMISTRY & MOLECULAR BIOLOGY Journal of Liposome Research Pub Date : 2024-12-01 Epub Date: 2024-02-09 DOI:10.1080/08982104.2024.2313452
Antigone Nifli, Aggeliki Liakopoulou, Elena Mourelatou, Konstantinos Avgoustakis, Sophia Hatziantoniou
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Abstract

Infantile hemangiomas (IH) are common benign soft tissue tumors, frequently affecting infants. While Propranolol Hydrochloride (Pro HCl) has emerged as a promising treatment for IH, its topical application remains challenging due to the need for stable and efficacious carriers. This study investigates the potential of preformulated liposomes as carriers for topical delivery of Pro HCl for the treatment of IH in compounding pharmacies. Liposomes loaded with Pro HCl were prepared using active pharmaceutical ingredient or commercially available propranolol tablets and various dilution media, including Water for Injection (WFI), Dextrose 5%, and NaCl 0.9%. The physicochemical properties of the liposomal formulations (Pro HCl content, encapsulation efficiency, loading capacity, and colloidal stability) were assessed over a 90-day storage at 4 °C. In vitro release kinetics and transdermal permeation of Pro HCl from liposomes were also evaluated. Liposome properties were influenced by the dilution medium. Pro HCl content remained stable in liposomes encapsulating API (Lipo-Pro), regardless of the dilution medium. Lipo-Pro showed sustained drug release over time, suggesting its potential for maintaining therapeutic levels. Pro HCl exhibited enhanced transdermal permeability from Lipo-Pro compared to aqueous solution, indicating its potential for topical IH treatment. Preformulated liposomes offer a stable and effective carrier for Pro HCl, potentially suitable for extemporaneous preparations in compounding pharmacies. Their enhanced transdermal permeability presents a promising alternative for topical IH treatment. This study provides valuable insights into the development of innovative and effective drug delivery strategies for managing IH, with future research focusing on in vivo applications and therapeutic potential.

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复方药房用于治疗婴儿血管瘤的普萘洛尔脂质体。
婴幼儿血管瘤(IH)是一种常见的良性软组织肿瘤,常累及婴儿。虽然盐酸普萘洛尔(Pro HCl)已成为治疗婴幼儿血管瘤的有效药物,但由于需要稳定而有效的载体,其局部应用仍具有挑战性。本研究探讨了预制脂质体作为载体在复方药房局部给药盐酸普萘洛尔治疗 IH 的潜力。使用活性药物成分或市售普萘洛尔片剂和各种稀释介质(包括注射用水(WFI)、5%葡萄糖和0.9%氯化钠)制备了负载盐酸丙卡特的脂质体。在 4 °C 下储存 90 天后,对脂质体制剂的理化性质(盐酸普萘洛尔含量、包封效率、负载能力和胶体稳定性)进行了评估。此外,还评估了盐酸原盐的体外释放动力学和脂质体的透皮渗透性。脂质体的特性受稀释介质的影响。无论稀释介质如何,盐酸原液在包裹原料药的脂质体(Lipo-Pro)中都保持稳定。Lipo-Pro 在一段时间内显示出持续的药物释放,这表明它具有维持治疗水平的潜力。与水溶液相比,Lipo-Pro 中盐酸原盐的透皮渗透性更强,这表明它具有局部 IH 治疗的潜力。预制脂质体为盐酸原氢大麻酚提供了一种稳定有效的载体,可能适用于复方药房的临时制剂。脂质体的透皮渗透性增强,为局部 IH 治疗提供了一种很有前景的选择。这项研究为开发治疗 IH 的创新有效的给药策略提供了宝贵的见解,未来的研究重点将放在体内应用和治疗潜力上。
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来源期刊
Journal of Liposome Research
Journal of Liposome Research 生物-生化与分子生物学
CiteScore
10.50
自引率
2.30%
发文量
24
审稿时长
3 months
期刊介绍: The Journal of Liposome Research aims to publish original, high-quality, peer-reviewed research on the topic of liposomes and related systems, lipid-based delivery systems, lipid biology, and both synthetic and physical lipid chemistry. Reviews and commentaries or editorials are generally solicited and are editorially reviewed. The Journal also publishes abstracts and conference proceedings including those from the International Liposome Society. The scope of the Journal includes: Formulation and characterisation of systems Formulation engineering of systems Synthetic and physical lipid chemistry Lipid Biology Biomembranes Vaccines Emerging technologies and systems related to liposomes and vesicle type systems Developmental methodologies and new analytical techniques pertaining to the general area Pharmacokinetics, pharmacodynamics and biodistribution of systems Clinical applications. The Journal also publishes Special Issues focusing on particular topics and themes within the general scope of the Journal.
期刊最新文献
Liposomal propranolol for treatment of infantile hemangioma at compounding pharmacies. Remote loading in liposome: a review of current strategies and recent developments. Targeting of M2 macrophages with IL-13-functionalized liposomal prednisolone inhibits melanoma angiogenesis in vivo. Design, optimization, characterization, and in vitro evaluation of metformin-loaded liposomes for triple negative breast cancer treatment. Review of recent preclinical and clinical research on ligand-targeted liposomes as delivery systems in triple negative breast cancer therapy.
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