Glutathione metabolism and glutathione S-conjugate export ATPase (MRP1/GS-X pump) activity in cancer. II. Cell-to-cell variability, relation with cellular activation state and functional absence of GS-X pump in lymphocytes.

P I de Bittencourt Júnior, S M Senna, A C Vidor, C K Miyasaka, R Curi, J F Williams
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Abstract

A severe complication in late-stage cancer patients is host immunosuppression. It is suggested that overproduction of the highly cytostatic and cytotoxic antiproliferative cyclopentenone prostaglandins (CP-PGs) within the plasma of cancer-bearing subjects may contribute to immunosuppression. Lymphoid tissues of Walker 256 tumor-bearing rats accumulate large amounts of CP-PGs while the tumor tissue itself does not. Moreover, tumor cells may present differential sensitivity to CP-PGs due to the expression of the multidrug resistance-associated protein (MRP1) gene product which shows a Mg(2+)-dependent vanadate-sensitive glutathione S-conjugate export ATPase (GS-X pump) activity that extrudes CP-PGs from cells as glutathione S-conjugates. In this study, the possibility that deficient GS-X pump activity in immune cells that may be involved in the accumulation of CP-PGs is investigated. Rat lymph node lymphocytes do not exhibit any notable activity even when mitogen-stimulated. Conversely, although rat peritoneal resident (quiescent) or thioglycollate-stimulated (inflammatory) macrophages exhibit low GS-X pump activity, Bacillus Calmette-Guérin (BCG)-activated macrophages show a notable rise in the activity of the ATPase, suggesting that the cellular activation state may modulate GS-X pump activity/expression and that, under appropriate stimuli (e.g., during immune response) macrophages may provide a self-defense against electrophilic CP-PGs by forming GS-conjugates that can be extruded from cells through the GS-X pump. ras oncogene expression may be linked with MRP1/GS-X pump expression/activity, since C2C12 promyoblasts transformed by v-H-ras transfection doubled GS-X pump activity. These results support the proposition that the accumulation of CP-PGs and the immunosuppression of tumor-bearing subjects may be attributed to a lack of GS-X pump activity/expression in lymphocytes.

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癌症中谷胱甘肽代谢和谷胱甘肽s偶联输出atp酶(MRP1/GS-X泵)活性。2细胞间变异,与细胞激活状态和淋巴细胞GS-X泵功能缺失的关系。
晚期癌症患者的一个严重并发症是宿主免疫抑制。这表明,高细胞抑制和细胞毒性的抗增殖环戊酮前列腺素(cp - pg)在癌症患者血浆中的过量产生可能有助于免疫抑制。Walker 256荷瘤大鼠淋巴组织积累了大量的cp - pg,而肿瘤组织本身没有。此外,由于多药耐药相关蛋白(MRP1)基因产物的表达,肿瘤细胞可能对cp - pg表现出不同的敏感性,该基因产物显示出Mg(2+)依赖的钒酸盐敏感谷胱甘肽s偶联物输出atp酶(GS-X泵)活性,该活性将cp - pg作为谷胱甘肽s偶联物从细胞中挤出。本研究探讨了免疫细胞中GS-X泵活性不足可能参与cp - pg积累的可能性。大鼠淋巴结淋巴细胞即使在有丝分裂原刺激下也不表现出任何显著的活性。相反,尽管大鼠腹膜内巨噬细胞(静止)或巯基乙酸刺激(炎症)表现出较低的GS-X泵活性,但卡介苗(BCG)激活的巨噬细胞显示出显著的atp酶活性升高,这表明细胞激活状态可能调节GS-X泵活性/表达,并且在适当的刺激下(例如,在免疫应答过程中,巨噬细胞可以通过形成GS-X泵从细胞中挤出的gs -偶联物来防御亲电性cp - pg。ras癌基因的表达可能与MRP1/GS-X泵的表达/活性有关,因为经v-H-ras转染转化的C2C12早肌母细胞使GS-X泵活性加倍。这些结果支持了cp - pg的积累和荷瘤受试者的免疫抑制可能归因于淋巴细胞中GS-X泵活性/表达的缺乏的观点。
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