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量子点在磷脂囊泡中的“捕获”会猝灭其光活性。

Entrapment in phospholipid vesicles quenches photoactivity of quantum dots.

机构信息

Department of Radiation Biology, Institute for Cancer Research, Norwegian Radium Hospital, Oslo University Hospital, Oslo, Norway.

出版信息

Int J Nanomedicine. 2011;6:1875-88. doi: 10.2147/IJN.S22953. Epub 2011 Sep 7.

Abstract

Quantum dots have emerged with great promise for biological applications as fluorescent markers for immunostaining, labels for intracellular trafficking, and photosensitizers for photodynamic therapy. However, upon entry into a cell, quantum dots are trapped and their fluorescence is quenched in endocytic vesicles such as endosomes and lysosomes. In this study, the photophysical properties of quantum dots were investigated in liposomes as an in vitro vesicle model. Entrapment of quantum dots in liposomes decreases their fluorescence lifetime and intensity. Generation of free radicals by liposomal quantum dots is inhibited compared to that of free quantum dots. Nevertheless, quantum dot fluorescence lifetime and intensity increases due to photolysis of liposomes during irradiation. In addition, protein adsorption on the quantum dot surface and the acidic environment of vesicles also lead to quenching of quantum dot fluorescence, which reappears during irradiation. In conclusion, the in vitro model of phospholipid vesicles has demonstrated that those quantum dots that are fated to be entrapped in endocytic vesicles lose their fluorescence and ability to act as photosensitizers.

摘要

量子点作为荧光标记物在免疫染色、细胞内运输标记和光动力治疗中的光敏剂方面具有很大的应用前景。然而,进入细胞后,量子点会被内吞小泡(如内体和溶酶体)捕获,其荧光会被猝灭。在这项研究中,研究了脂质体作为体外囊泡模型中量子点的光物理性质。量子点被包封在脂质体中会降低其荧光寿命和强度。与游离量子点相比,脂质体量子点产生自由基的能力受到抑制。然而,由于照射期间脂质体的光解,量子点的荧光寿命和强度增加。此外,蛋白质在量子点表面的吸附和囊泡的酸性环境也会导致量子点荧光猝灭,在照射过程中会重新出现。总之,磷脂囊泡的体外模型表明,那些注定要被内吞小泡捕获的量子点会失去其荧光和作为光敏剂的能力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/85e2/3173050/9081a63b7018/ijn-6-1875f1.jpg

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