皮肤病学研究中的脂质体。

D. Yarosh
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引用次数: 25

摘要

脂质体是微球,通常由两亲性磷脂组成。如果它们只是保护或隔离在制剂中不稳定的化合物,则它们可能在没有皮肤渗透的情况下是有用的。留在皮肤表面的脂质体是有用的光吸收剂,提供颜色或防晒霜的代理人,或作为定时释放的仓库。穿透角质层的脂质体具有与活组织相互作用的潜力。局部应用脂质体可以与角质层脂质基质混合或通过利用细胞间基质的脂水界面穿透角质层。至少有四种主要途径进入皮肤:毛孔、毛囊、柱状空隙和鳞片之间的脂质:水基质。驱动脂质体渗透的主要力量是水梯度,而柔性脂质体最能利用这些输送机会。有些脂质体在细胞外释放其内容物。光敏剂的局部应用可以通过脂质体的包封来增强。在局部皮肤区域,特别是在角质层和皮肤屏障功能被破坏的疾病部位,可能产生更高和更持久的药物浓度。脂质体膜应设计成能捕获膜内的亲脂性药物或膜内的亲水性药物。其他类型的脂质体可以被改造成被细胞吸收。一旦进入细胞,溶酶体囊和包覆网格蛋白的凹坑是脂质体的最终目的地,除非脂质体中有一条逃逸路径。已经开发出一种新的方法,允许通过从溶酶体囊中逃逸到皮肤细胞中。这些脂质体已被用于局部将活性DNA修复酶从脂质体输送到表皮细胞,并增强紫外线照射皮肤的DNA修复。从这些研究中,我们对DNA损伤和皮肤癌的关系有了大量的了解。突变和免疫抑制似乎都是皮肤癌的必要条件,两者都是由DNA损伤引起的。DNA损伤通过诱导细胞因子的表达产生直接影响,这意味着DNA损伤可以在邻近的未受损细胞中诱导信号传导。只有一小部分DNA损伤的修复会对生物反应产生不成比例的影响,这清楚地表明并非所有DNA损伤都是相同的。该技术证明了生物活性蛋白可以被输送到皮肤细胞中,为纠正或增强皮肤细胞代谢,改善人体健康开辟了新的领域。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Liposomes in investigative dermatology.
Liposomes are microscopic spheres, usually composed of amphiphilic phospholipids. They may be useful without skin penetration if they simply protect or sequester compounds that would otherwise be unstable in the formulation. Liposomes that remain on the skin surface are useful as light-absorbers, agents to deliver color or sunscreens, or as depots for timed-release. Liposomes that penetrate the stratum corneum have the potential to interact with living tissue. Topically applied liposomes can either mix with the stratum corneum lipid matrix or penetrate the stratum corneum by exploiting the lipid-water interface of the intercellular matrix. There are at least four major routes of entry into the skin: pores, hair follicles, columnular spaces and the lipid:water matrix between squames. A major force driving liposome penetration is the water gradient, and flexible liposomes are best able to exploit these delivery opportunities. Some liposomes release their contents extracellularly. Topical application of photosensitizers may be enhanced by encapsulation in liposomes. Higher and longer-lasting drug concentrations may be produced in localized areas of skin, particularly at disease sites where the stratum corneum and the skin barrier function are disrupted. The liposome membrane should be designed to capture lipophilic drugs in the membrane or hydrophilic drugs in the interior. Other types of liposomes can be engineered to be taken up by cells. Once inside cells, the lysosomal sac and clatherin-coated pit are the dead-end destinations for liposomes unless an escape path has been engineered into the liposome. A novel method has been developed to allow delivery into cells of the skin, by escape from the lysosomal sac. These liposomes have been used to topical deliver active DNA repair enzymes from liposomes into epidermal cells and to enhance DNA repair of UV-irradiated skin. From these studies a tremendous amount has been learned about the relationship of DNA damage and skin cancer. Both mutations and immunosuppression appear to be essential to skin cancer and both are induced by DNA damage. DNA damage produces immediate effects by inducing the expression of cytokines, which means that DNA damage can induce signaling in neighboring, undamaged cells. The repair of only a fraction of the DNA damage has a disproportionate effect on the biological responses, clearly demonstrating that not all DNA damage is equivalent. This technology demonstrates that biologically active proteins can be delivered into the cells of skin, and opens up a new field of correcting or enhancing skin cell metabolism to improve human health.
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