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对具有缺陷的还原型叶酸载体功能的小鼠L1210白血病细胞中由低pH途径介导的叶酸转运的表征。

Characterization of folate transport mediated by a low pH route in mouse L1210 leukemia cells with defective reduced folate carrier function.

作者信息

Sierra E E, Goldman I D

机构信息

Albert Einstein College of Medicine, Comprehensive Cancer Center, Bronx, NY 10461, USA.

出版信息

Biochem Pharmacol. 1998 May 1;55(9):1505-12. doi: 10.1016/s0006-2952(97)00673-4.

Abstract

Folate influx at low pH was characterized in MTXrA cells, an L1210 mouse leukemia cell line with a functional defect in the reduced folate carrier. Folic acid influx in MTXrA cells was negligible at pH 7.5, increased 13-fold as the pH was decreased to 6.0, and was indistinguishable from that in L1210 cells. In contrast, while methotrexate (MTX) influx in MTXrA cells at pH 6.0 was 15-fold higher than at pH 7.5, in L1210 cells it was decreased by half. Influx of MTX, folic acid, 5-methyltetrahydrofolate and 5-formyltetrahydrofolate in MTXrA cells was increased at pH < 7.0, but their pH optima and profile differed substantially. Influx of MTX and 5-methyltetrahydrofolate at pH 6.0 showed saturability, with a Kt of 2.65 and 0.56 microM, and a Vmax of 0.45 and 0.083 nmol/g dry wt/min, respectively. MTX influx mediated by the low pH transporter was insensitive to the anionic composition of the transport buffer and affected minimally (approximately 20%) by Na+ substitution. The anion transport inhibitors sulfobromophthalein, diisothiocyanatostilbene disulfonic acid, and acetamidoisothiocyanatostilbene disulfonic acid were not effective inhibitors of the low pH route. MTX transport at low pH did not increase in MTXrA-R16 cells, an MTXrA derivative with 10-fold overexpression of the reduced folate carrier (RFC) due to transfection with RFC1 cDNA. Inhibition of reduced folate carrier activity with acetamidoisothiocyanatostilbene disulfonic acid resulted in identical MTX influx in L1210, MTXrA, and MTXrA-R16 cells at pH 5.5. Finally, low pH-mediated MTX influx was reduced by energy inhibitors and partially inhibited by ionophores (nigericin > monensin >> valinomycin). The data indicate that L1210 and MTXrA cells express similar activities of a low pH folate transporter that has properties distinct from, and independent of, the reduced folate carrier.

摘要

在MTXrA细胞中对低pH条件下的叶酸内流进行了表征,MTXrA细胞是一种L1210小鼠白血病细胞系,其还原型叶酸载体存在功能缺陷。在pH 7.5时,MTXrA细胞中的叶酸内流可忽略不计,当pH降至6.0时增加了13倍,且与L1210细胞中的情况无明显差异。相比之下,虽然在pH 6.0时MTXrA细胞中的甲氨蝶呤(MTX)内流比pH 7.5时高15倍,但在L1210细胞中却减少了一半。在pH < 7.0时,MTXrA细胞中MTX、叶酸、5-甲基四氢叶酸和5-甲酰四氢叶酸的内流增加,但其pH最佳值和变化曲线有很大不同。在pH 6.0时,MTX和5-甲基四氢叶酸的内流表现出饱和性,Kt分别为2.65和0.56 microM,Vmax分别为0.45和0.083 nmol/g干重/分钟。由低pH转运体介导的MTX内流对转运缓冲液的阴离子组成不敏感,并且受Na+替代的影响最小(约20%)。阴离子转运抑制剂磺溴酞、二异硫氰酸根合芪二磺酸和乙酰氨基异硫氰酸根合芪二磺酸不是低pH途径的有效抑制剂。在MTXrA-R16细胞(一种由于转染RFC1 cDNA而使还原型叶酸载体(RFC)过表达10倍的MTXrA衍生物)中,低pH条件下的MTX转运没有增加。用乙酰氨基异硫氰酸根合芪二磺酸抑制还原型叶酸载体活性导致在pH 5.5时L1210、MTXrA和MTXrA-R16细胞中的MTX内流相同。最后,能量抑制剂可降低低pH介导的MTX内流,离子载体(尼日利亚菌素>莫能菌素>>缬氨霉素)可部分抑制该内流。数据表明,L1210和MTXrA细胞表达一种低pH叶酸转运体的相似活性,该转运体具有与还原型叶酸载体不同且独立的特性。

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