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一种潜在光动力治疗剂在果蝇中的毒性和定位研究。

Toxicity and localization studies of a potential photodynamic therapy agent in Drosophila.

作者信息

Yoho Joshua, Stroh Colette, Swavey Shawn, Kango-Singh Madhuri

机构信息

Department of Chemistry, University of Dayton, Dayton, Ohio, 45469; Department of Biology, University of Dayton, Dayton, Ohio, 45469.

出版信息

Genesis. 2014 Apr;52(4):309-14. doi: 10.1002/dvg.22760. Epub 2014 Mar 12.

Abstract

Photodynamic therapy utilizes light, a photosensitizer, and molecular oxygen as a treatment modality for a variety of cancers. We have recently combined ruthenium(II) polypyridyl groups with a zinc(II) centered porphyrin as a new photosensitizer for the treatment of melanoma. In-vitro studies have indicated that this photosensitizer is toxic to melanoma cells when irradiated with low energy light; however, it is nontoxic to normal cells under similar conditions. To determine the toxicity and cell viability of this compound in-vivo we present, herein, a study using Drosophila melanogaster. In the absence of light, the new photosensitizer shows no discernible effects to fly larvae at various concentrations of compound and stages of larval development. When the larvae were fed the photosensitizer it was observed, by fluorescence microscopy, that the compound passes through the cell membrane and localizes in the cytosol at lower concentrations and the nucleus at slightly higher concentrations indicating that the compound is not immediately metabolized.

摘要

光动力疗法利用光、一种光敏剂和分子氧作为多种癌症的治疗方式。我们最近将钌(II)多吡啶基团与以锌(II)为中心的卟啉结合,作为一种治疗黑色素瘤的新型光敏剂。体外研究表明,这种光敏剂在低能量光照射下对黑色素瘤细胞有毒性;然而,在类似条件下对正常细胞无毒。为了确定该化合物在体内的毒性和细胞活力,我们在此展示一项使用黑腹果蝇的研究。在无光条件下,这种新型光敏剂在不同化合物浓度和幼虫发育阶段对果蝇幼虫均未显示出明显影响。当给幼虫喂食该光敏剂时,通过荧光显微镜观察到,该化合物穿过细胞膜,在较低浓度下定位在细胞质中,在稍高浓度下定位在细胞核中,这表明该化合物不会立即被代谢。

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