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体内基因组筛选揭示了液泡H⁺-ATP酶和胞质酸化在对顺铂等DNA损伤剂敏感性中所起的作用。

Genomic screening in vivo reveals the role played by vacuolar H+ ATPase and cytosolic acidification in sensitivity to DNA-damaging agents such as cisplatin.

作者信息

Liao Chunyan, Hu Bin, Arno Matthew J, Panaretou Barry

机构信息

Pharmaceutical Science Research Division, King's College London, Franklin-Wilkins Building, 150 Stamford Street, London SE1 9NH, UK.

出版信息

Mol Pharmacol. 2007 Feb;71(2):416-25. doi: 10.1124/mol.106.030494. Epub 2006 Nov 8.

Abstract

Screening the Saccharomyces cerevisiae homozygous diploid deletion library against a sublethal concentration of cisplatin revealed 76 strains sensitive to the drug. As expected, the largest category of deletions, representing 40% of the sensitive strains, was composed of strains lacking genes involved in DNA replication and damage repair. Deletions lacking function of the highly conserved vacuolar H+ translocating ATPase (V-ATPase) composed the category representing the second largest number of sensitive strains. The effect on cell death exhibited by V-ATPase mutants was found to be a general response to various DNA damaging agents as opposed to being specific to cisplatin, as evidenced by sensitivity of the mutants to hydroxyurea (a DNA-alkylating agent) and UV irradiation. Loss of V-ATPase does not affect DNA repair, because double mutants defective for V-ATPase function and DNA repair pathways were more sensitive to cisplatin than the single mutants. V-ATPase mutants are more prone to DNA damage than wild-type cells, indicated by enhanced activation of the DNA damage checkpoint. Vacuole function per se is not cisplatin-sensitive, because vacuolar morphology and vacuolar acidification were unaffected by cisplatin in wild-type cells. V-ATPase also controls cytoplasmic pH, so the enhanced sensitivity to DNA damage may be associated with the drop in pHi associated with V-ATPase mutants. The increased loss in cell viability induced by cisplatin at lower pH in V-ATPase mutants supports this hypothesis. The loss in viability seen in wild-type cells under the same conditions was far less dramatic.

摘要

用亚致死浓度的顺铂筛选酿酒酵母纯合二倍体缺失文库,发现76个菌株对该药物敏感。正如预期的那样,缺失类型最多的一类(占敏感菌株的40%)是缺乏参与DNA复制和损伤修复基因的菌株。缺乏高度保守的液泡H⁺转运ATP酶(V-ATP酶)功能的缺失菌株构成了敏感菌株数量第二多的类别。发现V-ATP酶突变体对细胞死亡的影响是对各种DNA损伤剂的普遍反应,而不是对顺铂特异的反应,这一点由突变体对羟基脲(一种DNA烷化剂)和紫外线照射的敏感性所证明。V-ATP酶的缺失并不影响DNA修复,因为V-ATP酶功能和DNA修复途径有缺陷的双突变体比单突变体对顺铂更敏感。V-ATP酶突变体比野生型细胞更容易发生DNA损伤,这由DNA损伤检查点的增强激活所表明。液泡功能本身对顺铂不敏感,因为在野生型细胞中,液泡形态和液泡酸化不受顺铂影响。V-ATP酶还控制细胞质pH值,因此对DNA损伤的敏感性增强可能与V-ATP酶突变体相关的细胞内pH值下降有关。V-ATP酶突变体在较低pH值下由顺铂诱导的细胞活力损失增加支持了这一假设。在相同条件下野生型细胞中观察到的活力损失则要小得多。

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