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细胞内pH值和热敏感性的改变。

Modification of intracellular pH and thermosensitivity.

作者信息

Lyons J C, Kim G E, Song C W

机构信息

Department of Therapeutic Radiology-Radiation Oncology, University of Minnesota Medical School, Minneapolis 55455.

出版信息

Radiat Res. 1992 Jan;129(1):79-87.

PMID:1728060
Abstract

The effects of amiloride (an inhibitor of Na+/H+ antiport), DIDS (an inhibitor of Na(+)-coupled and Na(+)-independent HCO3-/Cl- exchange) and nigericin (K+/H+ ionophore) alone and in various combinations on the intracellular pH (pHi) and thermosensitivity of SCK tumor cells were studied. Hyperthermia alone at 43 degrees C for 2 h decreased pHi of SCK cells by 0.15-0.20 pH units, as measured fluorometrically using the pH-sensitive dye BCECF. When the cells were treated with 0.5 mM amiloride at 37 degrees C, the pHi declined by 0.10-0.15 pH units at an extracellular pH (pHe) of both 7.2 and 6.6. Amiloride at 0.5 mM enhanced the thermal damage to SCK cells at pHe 6.6 but not at pHe 7.2. DIDS alone at 0.1 mM exerted no effect on pHi or cellular thermosensitivity. DIDS, however, enhanced the effects of amiloride in decreasing pHi and in increasing the thermoresponse of SCK cells, particularly at pHe 6.6. Treatment of the cells with nigericin at 0.1-1.0 micrograms/ml lowered the pHi and enhanced the thermosensitivity of the cells in a dose-dependent manner. Reductions in pHi and increases in thermosensitivity by nigericin at the lower concentration at pHe 6.6 were far greater than at pHe 7.2. When a mixture of 1.0 micrograms/ml nigericin, 0.5 mM amiloride, and 0.1 mM DIDS was present in the medium, the pHi rapidly decreased by about 0.3 and 0.4 pH units at pHe 7.2 and 6.6, respectively. This drug combination was also extremely effective in sensitizing SCK cells to heat, particularly at pHe 6.6. The fact that the thermosensitization by these drugs at pHe 6.6 is more pronounced than at pHe 7.2 and that intratumor environments are known to be acidic strongly suggested that it may then be possible to enhance the thermal damage with such drugs preferentially in tumors relative to normal tissues.

摘要

研究了氨氯吡咪(一种Na⁺/H⁺逆向转运抑制剂)、二碘水杨酸(一种Na⁺偶联和Na⁺非依赖性HCO₃⁻/Cl⁻交换抑制剂)和尼日利亚菌素(K⁺/H⁺离子载体)单独及各种组合对SCK肿瘤细胞细胞内pH值(pHi)和热敏感性的影响。单独在43℃进行2小时热疗会使SCK细胞的pHi通过使用pH敏感染料BCECF进行荧光测定降低0.15 - 0.20个pH单位。当细胞在37℃用0.5 mM氨氯吡咪处理时,在细胞外pH值(pHe)为7.2和6.6时,pHi分别下降0.10 - 0.15个pH单位。0.5 mM的氨氯吡咪在pHe 6.6时增强了对SCK细胞的热损伤,但在pHe 7.2时没有。单独0.1 mM的二碘水杨酸对pHi或细胞热敏感性没有影响。然而,二碘水杨酸增强了氨氯吡咪降低pHi和增加SCK细胞热反应的作用,特别是在pHe 6.6时。用0.1 - 1.0微克/毫升的尼日利亚菌素处理细胞会以剂量依赖的方式降低pHi并增强细胞的热敏感性。在较低浓度下,尼日利亚菌素在pHe 6.6时导致的pHi降低和热敏感性增加远大于在pHe 7.2时。当培养基中存在1.0微克/毫升尼日利亚菌素、0.5 mM氨氯吡咪和0.1 mM二碘水杨酸的混合物时,在pHe 7.2和6.6时,pHi分别迅速下降约0.3和0.4个pH单位。这种药物组合在使SCK细胞对热敏感方面也极其有效,特别是在pHe 6.6时。这些药物在pHe 6.6时的热致敏作用比在pHe 7.2时更明显,并且已知肿瘤内环境呈酸性,这强烈表明相对于正常组织,有可能优先在肿瘤中用此类药物增强热损伤。

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