首页> 美国卫生研究院文献>Biochemical Journal >Ca(2+)-mediated prostaglandin E2 induction reduces haematoporphyrin-derivative-induced cytotoxicity of T24 human bladder transitional carcinoma cells in vitro.
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Ca(2+)-mediated prostaglandin E2 induction reduces haematoporphyrin-derivative-induced cytotoxicity of T24 human bladder transitional carcinoma cells in vitro.

机译:Ca(2+)介导的前列腺素E2诱导降低体外血红蛋白衍生物诱导的T24人膀胱移行癌细胞的细胞毒性。

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摘要

The effects of haematoporphyrin-derivative-mediated photodynamic treatment on arachidonic acid metabolism and its relation to clonogenicity have been studied in human bladder-tumour cells. Photodynamic treatment resulted in a transient release of arachidonic acid-derived compounds; prostaglandin E2 (PGE2) and thromboxane B2 (TXB2) especially were strongly increased. This release was reduced by chelation of intracellular Ca2+ with Quin-2 or by lowering the extracellular Ca2+ concentration in the medium with EGTA, presumably resulting in inhibition of phospholipase A2. A similar reduction was obtained when indomethacin, an inhibitor of the cyclo-oxygenase pathway, was added prior to light exposure. These three treatments enhanced the photosensitivity, as revealed by the clonogenicity assay. Incubation with PGE2 prior to light exposure, but not with TXB2, protected against reproductive-cell death. The results of these experiments suggest that Ca(2+)-mediated activation of cyclo-oxygenase, resulting in increased levels of PGE2, participates in a cellular-defence mechanism against photodynamic cell killing.
机译:在人膀胱肿瘤细胞中研究了血卟啉衍生物介导的光动力处理对花生四烯酸代谢的影响及其与克隆形成性的关系。光动力处理导致花生四烯酸衍生化合物的瞬时释放;前列腺素E2(PGE2)和血栓烷B2(TXB2)特别增加。通过用Quin-2螯合细胞内Ca2 +或通过用EGTA降低培养基中细胞外Ca2 +的浓度来减少这种释放,大概是导致磷脂酶A2的抑制。当在曝光前加入吲哚美辛(一种环加氧酶途径的抑制剂)时,得到类似的减少。如克隆形成测定所揭示的,这三种处理增强了光敏性。在曝光之前与PGE2一起孵育,但与TXB2一起孵育,可以防止生殖细胞死亡。这些实验的结果表明,Ca(2+)介导的环加氧酶激活,导致PGE2水平升高,参与了针对光动力细胞杀伤的细胞防御机制。

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