首页> 美国卫生研究院文献>British Journal of Cancer >Increased tumour dihydroceramide production after Photofrin-PDT alone and improved tumour response after the combination with the ceramide analogue LCL29. Evidence from mouse squamous cell carcinomas
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Increased tumour dihydroceramide production after Photofrin-PDT alone and improved tumour response after the combination with the ceramide analogue LCL29. Evidence from mouse squamous cell carcinomas

机译:单独使用Photofrin-PDT后增加了肿瘤二氢神经酰胺的产生并与神经酰胺类似物LCL29组合后改善了肿瘤反应。小鼠鳞状细胞癌的证据

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摘要

Photodynamic therapy (PDT) has been proven effective for treatment of several types of cancer. Photodynamic therapy alone, however, attains limited cures with some tumours and there is need for its improved efficacy in such cases. Sphingolipid (SL) analogues can promote tumour response in combination with anticancer drugs. In this study, we used mouse SCCVII squamous cell carcinoma tumours to determine the impact of Photofrin-PDT on the in vivo SL profile and the effect of LCL29, a C6-pyridinium ceramide, on PDT tumour response. Following PDT, the levels of dihydroceramides (DHceramides), in particular C20-DHceramide, were elevated in tumours. Similarly, increases in DHceramides, in addition to C20:1-ceramide, were found in PDT-treated SCCVII cells. These findings indicate the importance of the de novo ceramide pathway in Photofrin-PDT response not only in cells but also in vivo. Notably, co-exposure of SCCVII tumours to Photofrin-PDT and LCL29 led to enhanced tumour response compared with PDT alone. Thus, we show for the first time that Photofrin-PDT has a distinct signature effect on the SL profile in vitro and in vivo, and that the combined treatment advances PDT therapeutic gain, implying translational significance of the combination.
机译:光动力疗法(PDT)已被证明可有效治疗多种类型的癌症。然而,仅光动力疗法只能对某些肿瘤进行有限的治愈,因此在这种情况下需要提高疗效。鞘脂(SL)类似物可与抗癌药联合促进肿瘤反应。在这项研究中,我们使用了小鼠SCCVII鳞状细胞癌肿瘤来确定Photofrin-PDT对体内SL的影响以及LCL29(C6-吡啶神经酰胺)对PDT肿瘤反应的影响。 PDT后,肿瘤中的二氢神经酰胺(DHceramides),特别是C20-DHceramide的水平升高。类似地,在PDT处理的SCCVII细胞中,除C20:1-神经酰胺外,还发现DH神经酰胺的增加。这些发现表明,从头神经酰胺途径不仅在细胞中而且在体内在Photofrin-PDT应答中的重要性。值得注意的是,与单独的PDT相比,将SCCVII肿瘤与Photofrin-PDT和LCL29共同暴露可增强肿瘤反应。因此,我们首次证明Photofrin-PDT在体外和体内对SL谱具有明显的标志作用,并且联合治疗提高了PDT的治疗效果,这暗示了联合的翻译意义。

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