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包裹于无定形Ca(2+)多聚磷酸盐纳米球中的视黄醇在MC3T3-E1细胞中发挥协同作用。

Retinol encapsulated into amorphous Ca(2+) polyphosphate nanospheres acts synergistically in MC3T3-E1 cells.

作者信息

Müller Werner E G, Tolba Emad, Schröder Heinz C, Diehl-Seifert Bärbel, Wang Xiaohong

机构信息

ERC Advanced Investigator Grant Research Group at the Institute for Physiological Chemistry, University Medical Center of the Johannes Gutenberg University, Duesbergweg 6, D-55128 Mainz, Germany.

ERC Advanced Investigator Grant Research Group at the Institute for Physiological Chemistry, University Medical Center of the Johannes Gutenberg University, Duesbergweg 6, D-55128 Mainz, Germany; Biomaterials Department, Inorganic Chemical Industries Division, National Research Center, Doki, 11884 Cairo, Egypt.

出版信息

Eur J Pharm Biopharm. 2015 Jun;93:214-23. doi: 10.1016/j.ejpb.2015.04.005. Epub 2015 Apr 18.

Abstract

Both the quality and quantity of collagen, the major structural component of the skin, decrease in aging skin. We succeeded to encapsulate retinol into amorphous inorganic polyphosphate (polyP) nanoparticles together with calcium ions ("aCa-polyP-NP"), under formation of amorphous Ca-polyP/retinol nanospheres ("retinol/aCa-polyP-NS"). The globular nanospheres are not cytotoxic, show an almost uniform size of ≈ 45 nm and have a retinol content of around 25%. Both components of those nanospheres, retinol and the aCa-polyP-NP, if administered together, caused a strong increase in proliferation of mouse calvaria MC3T3 cells. The expressions of collagen types I, II and III genes, but not the expression of collagen type V gene, were significantly enhanced if retinol is added together with aCa-polyP-NP. This synergistic effect was especially pronounced for the expression of the collagen type III gene. We propose that the synergistic effect of the retinol/aCa-polyP-NS on cell growth and collagen type III expression is induced via two routes, first through cellular uptake of the 45 nm nanospheres by clathrin-mediated endocytosis and second through extracellular disintegration of the nanospheres resulting in the release of retinol which is then taken up into the cells after binding to the retinal binding protein receptor.

摘要

胶原蛋白作为皮肤的主要结构成分,其质量和数量在皮肤老化过程中都会下降。我们成功地将视黄醇与钙离子一起封装到无定形无机聚磷酸盐(polyP)纳米颗粒中(“aCa-polyP-NP”),形成无定形Ca-polyP/视黄醇纳米球(“视黄醇/aCa-polyP-NS”)。球状纳米球无细胞毒性,尺寸几乎均匀,约为45nm,视黄醇含量约为25%。这些纳米球的两种成分,视黄醇和aCa-polyP-NP,如果一起给药,会使小鼠颅骨MC3T3细胞的增殖显著增加。如果将视黄醇与aCa-polyP-NP一起添加,I型、II型和III型胶原蛋白基因的表达会显著增强,但V型胶原蛋白基因的表达不会增强。这种协同效应在III型胶原蛋白基因的表达中尤为明显。我们认为,视黄醇/aCa-polyP-NS对细胞生长和III型胶原蛋白表达的协同效应是通过两条途径诱导的,首先是通过网格蛋白介导的内吞作用使45nm纳米球被细胞摄取,其次是通过纳米球的细胞外分解导致视黄醇释放,视黄醇与视网膜结合蛋白受体结合后再被细胞摄取。

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