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用二氢卟吩e6共轭微球处理的人膀胱癌细胞的光致敏破坏

Photosensitized destruction of human bladder carcinoma cells treated with chlorin e6-conjugated microspheres.

作者信息

Bachor R, Shea C R, Gillies R, Hasan T

机构信息

Department of Urology, Massachusetts General Hospital, Harvard Medical School, Boston 02114.

出版信息

Proc Natl Acad Sci U S A. 1991 Feb 15;88(4):1580-4. doi: 10.1073/pnas.88.4.1580.

Abstract

A photosensitizer conjugate, chlorin e6 (Ce6) covalently bound to 1-micron-diameter polystyrene microspheres, has been investigated in the photodynamic destruction of MGH-U1 human bladder carcinoma cells in vitro. The microspheres were taken up avidly by the carcinoma cells; confocal laser scanning fluorescence microscopy showed them to be localized in the cytoplasm, apparently within lysosomes, visualized by labeling with acridine orange. In contrast, fluorescence of unconjugated Ce6 was present within most cellular membranes. Use of Ce6-microsphere conjugates led to a 20-fold-higher mean intracellular concentration, compared with unconjugated Ce6. Cells incubated in the presence of Ce6-microsphere conjugates (0.43 microM equivalent) and subsequently irradiated at 659 nm with a dye laser pumped by an argon-ion laser showed dose-dependent phototoxicity, leading to total inhibition of colony formation at a radiant exposure of 5J/cm2; in contrast, cells incubated with either unconjugated Ce6 (0.43 microM) or unconjugated microspheres before laser irradiation were unaffected. Cells pretreated with Ce6-microsphere conjugates and irradiated in the presence of 90% 2H2O showed significantly increased phototoxicity, an effect consistent with an important role for excited-state singlet oxygen in the mechanism of injury. In solution, however, photosensitized generation of singlet oxygen with Ce6-microsphere conjugates was 9 times less efficient than with unconjugated Ce6. The markedly greater phototoxicity of Ce6-microsphere conjugates compared to unconjugated Ce6 was therefore a consequence of the high intracellular Ce6 concentration attained by phagocytosis of the conjugates and their particular sites of intracellular localization. Thus, these conjugates are an efficient system for the delivery of photosensitizing drugs to carcinoma cells.

摘要

一种将二氢卟吩e6(Ce6)共价结合到直径1微米的聚苯乙烯微球上的光敏剂共轭物,已在体外对MGH-U1人膀胱癌细胞的光动力破坏中进行了研究。癌细胞对这些微球有强烈摄取;共聚焦激光扫描荧光显微镜显示它们定位于细胞质中,显然在溶酶体内,通过吖啶橙标记可观察到。相比之下,未共轭的Ce6的荧光存在于大多数细胞膜内。与未共轭的Ce6相比,使用Ce6-微球共轭物导致细胞内平均浓度高出20倍。在Ce6-微球共轭物(0.43微摩尔当量)存在下孵育的细胞,随后用氩离子激光泵浦的染料激光在659纳米处照射,显示出剂量依赖性光毒性,在辐射暴露为5J/cm2时导致集落形成完全抑制;相比之下,在激光照射前用未共轭的Ce6(0.43微摩尔)或未共轭的微球孵育的细胞未受影响。用Ce6-微球共轭物预处理并在90% 2H2O存在下照射的细胞显示出明显增强的光毒性,这一效应与激发态单线态氧在损伤机制中的重要作用一致。然而,在溶液中,Ce6-微球共轭物产生单线态氧的光敏效率比未共轭的Ce6低9倍。因此,与未共轭的Ce6相比,Ce6-微球共轭物具有明显更强的光毒性,这是由于共轭物的吞噬作用及其细胞内特定定位位点所达到的高细胞内Ce6浓度所致。因此,这些共轭物是将光敏药物递送至癌细胞的有效系统。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/93f0/51063/ddbe022d440b/pnas01054-0507-a.jpg

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