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Two course illuminating scheme improves aminolevulinic acid photodynamic therapy in cell cultures.

机译:两过程照明方案改善了细胞培养中氨基乙酰丙酸的光动力疗法。

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Photodynamic therapy with the pro-drug 5-aminolaevulinic acid (ALA-PDT) is being used for the treatment of Barrett's oesophagus. We postulated that a first early course of ALA-PDT would increase protoporphyrin IX (PPIX) accumulation and thus the efficacy of a second course of ALA-PDT, by manipulating ferrochelatase (FC) and porphobilinogen deaminase (PBG-d) activity. Human EBV-transformed lymphoblastoid cells were used as a model of human tumour cells for the ability to form haem is present in all cells. After a single course of illumination (633 nm, 100 mW/cm2) the FC activity decreased significantly whereas the PBG-d activity did not change. During continued incubation with ALA following the first illumination, cells accumulated up to four times more PPIX than non-illuminated controls [220% +/- 30% versus (vs) 55% +/- 5%; p<0.001]. Two illuminations resulted in more cell death than one illumination (97% +/- 1% vs 80% +/- 2%; p<0.001). Since a second course of ALA-PDT within 3 hr after the first course resulted in a four fold increase in PPIX accumulation and significantly more cell death, we propose that a two course ALA-PDT scheme might improve the efficacy of this treatment for Barrett's oesophagus.
机译:使用前药5-氨基戊酸(ALA-PDT)进行光动力疗法可治疗Barrett食道。我们推测,通过控制铁螯合酶(FC)和胆色素原脱氨酶(PBG-d)活性,ALA-PDT的第一个早期疗程将增加原卟啉IX(PPIX)的积累,从而增加第二个ALA-PDT疗程的功效。人类EBV转化的淋巴母细胞被用作人类肿瘤细胞的模型,因为形成血红素的能力存在于所有细胞中。经过一个单一的照射过程(633 nm,100 mW / cm2),FC活性显着下降,而PBG-d活性未改变。在第一次照射后继续与ALA孵育期间,细胞积累的PPIX最多是未照射对照的四倍[220%+/- 30%对(vs)55%+/- 5%; p <0.001]。两次照射比一次照射导致更多的细胞死亡(97%+/- 1%对80%+/- 2%; p <0.001)。由于第一疗程后3小时内进行第二疗程ALA-PDT会导致PPIX积累增加四倍,并且细胞死亡明显增加,因此我们建议采用两疗程ALA-PDT方案可能会改善这种治疗Barrett食道的疗效。

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