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用于卵清蛋白局部递送的超可变形古脂质体的结构特征

Structural features of ultradeformable archaeosomes for topical delivery of ovalbumin.

作者信息

Carrer Dolores C, Higa Leticia H, Tesoriero Maria Victoria Defain, Morilla Maria Jose, Roncaglia Diana I, Romero Eder Lilia

机构信息

Instituto Ferreyra, INIMEC-CONICET, casilla de correo 389, 5000 Cordoba, Argentina.

Programa de Nanomedicinas, Departamento de Ciencia y Tecnología, Universidad Nacional de Quilmes, Roque Saenz Peña 352, Bernal, B1876 BXD Buenos Aires, Argentina.

出版信息

Colloids Surf B Biointerfaces. 2014 Sep 1;121:281-9. doi: 10.1016/j.colsurfb.2014.05.015. Epub 2014 May 22.

Abstract

The ultradeformable archaeosomes (UDA, made of total polar archaeolipids (TPA) extracted from the extreme halophile archaea Halorubrum tebenquichense:soybean phosphatidylcholine (SPC):sodium cholate (NaChol), 3:3:1 w:w), are promising topical adjuvants showing high deformability, an essential property for intact skin penetration up to the viable epidermis/dermis. To gain insights on UDA structure, the interactions between TPA, SPC and the edge activator NaChol, were assessed by electrospray ionization mass spectroscopy (ESI-MS) and confocal fluorescence microscopy of giant unilamellar vesicles (GUV). The non covalent heterodimers NaChol-SPC, NaChol-phosphatidylglycerophosphate methyl ether (PGPMe), NaChol-sulfated diglycosyl diphytanyl-glycerol diether (SDGD5) and SPC-PGPMe detected in the gas phase by ESI-MS after direct infusion of UDA, together with the homogeneous partition of FASTDiO and DiIC18 in GUV suggested that in these proportions, lipids and NaChol were miscible. We propose therefore, a model where in UDA the SPC diluted sufficient enough in the rich PGPMe TPA, so as to the low lateral mobility of molecules (typical of rich in PGPMe bilayers) was no longer experienced. We also found that 50μm deep within in vitro human skin canyons, the fluorescence of Alexa fluor 647-ovalbumin in UDL was ∼1.5 folds higher than in UDA, indicating a potential steric hindrance of the voluminous structure of PGPMe UDA bilayer, to the penetration of a particulate cargo such as the 7nm diameter ovalbumin. According to these observations, a further reduction in PGPMe - a lipid playing no immune role - content could help to improve the performance of UDA as topical adjuvants.

摘要

超可变形古脂质体(UDA,由从嗜极嗜盐古菌嗜盐碱红菌中提取的总极性古菌脂质(TPA):大豆磷脂酰胆碱(SPC):胆酸钠(NaChol)按3:3:1 w:w比例制成)是很有前景的局部佐剂,具有高可变形性,这是完整皮肤穿透至活表皮/真皮的关键特性。为深入了解UDA的结构,通过电喷雾电离质谱(ESI-MS)和巨型单层囊泡(GUV)的共聚焦荧光显微镜评估了TPA、SPC与边缘活化剂NaChol之间的相互作用。在直接注入UDA后通过ESI-MS在气相中检测到的非共价异二聚体NaChol-SPC、NaChol-磷脂酰甘油磷酸甲酯(PGPMe)、NaChol-硫酸化二糖基二植烷酰甘油二醚(SDGD5)和SPC-PGPMe,以及FASTDiO和DiIC18在GUV中的均匀分布表明,在这些比例下,脂质和NaChol是可混溶的。因此,我们提出了一个模型,即在UDA中,SPC在富含PGPMe的TPA中充分稀释,以至于不再出现分子的低侧向流动性(这是富含PGPMe双层的典型特征)。我们还发现,在体外人皮肤峡谷50μm深处,UDL中Alexa fluor 647-卵清蛋白的荧光比UDA中的高约1.5倍,这表明PGPMe UDA双层的庞大结构可能对诸如直径7nm的卵清蛋白等颗粒货物的渗透存在空间位阻。根据这些观察结果,进一步降低PGPMe(一种不发挥免疫作用的脂质)的含量可能有助于提高UDA作为局部佐剂的性能。

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