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本文引用的文献

1
An in vitro assay to measure the viability of KHT tumor cells not previously exposed to culture conditions.一种用于测量此前未接触过培养条件的KHT肿瘤细胞活力的体外测定法。
Radiat Res. 1974 May;58(2):262-76.
2
Therapeutic potential of analogues of amiloride: inhibition of the regulation of intracellular pH as a possible mechanism of tumour selective therapy.阿米洛利类似物的治疗潜力:抑制细胞内pH调节作为肿瘤选择性治疗的一种可能机制。
Br J Cancer. 1993 Feb;67(2):297-303. doi: 10.1038/bjc.1993.56.
3
Transmembrane ion gradients and thermochemotherapy.
Prog Clin Biol Res. 1982;107:103-7.
4
Discrimination of three parallel pathways of lactate transport in the human erythrocyte membrane by inhibitors and kinetic properties.通过抑制剂和动力学特性区分人红细胞膜中乳酸转运的三条平行途径。
Biochim Biophys Acta. 1982 Jan 4;684(1):96-110. doi: 10.1016/0005-2736(82)90053-0.
5
Cytoplasmic pH and free Mg2+ in lymphocytes.淋巴细胞中的细胞质pH值和游离镁离子
J Cell Biol. 1982 Oct;95(1):189-96. doi: 10.1083/jcb.95.1.189.
6
The relevance of tumour pH to the treatment of malignant disease.肿瘤酸碱度与恶性疾病治疗的相关性。
Radiother Oncol. 1984 Dec;2(4):343-66. doi: 10.1016/s0167-8140(84)80077-8.
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Cytotoxicity of compounds that interfere with the regulation of intracellular pH: a potential new class of anticancer drugs.干扰细胞内pH调节的化合物的细胞毒性:一类潜在的新型抗癌药物。
Cancer Res. 1987 Mar 15;47(6):1497-504.
8
The Bacteroides by-product succinic acid inhibits neutrophil respiratory burst by reducing intracellular pH.拟杆菌的副产物琥珀酸通过降低细胞内pH值来抑制中性粒细胞的呼吸爆发。
Infect Immun. 1987 Apr;55(4):864-70. doi: 10.1128/iai.55.4.864-870.1987.
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Regulation of intracellular pH in eukaryotic cells.真核细胞内pH值的调节
Biochem J. 1988 Feb 15;250(1):1-8. doi: 10.1042/bj2500001.
10
Reduction of intracellular pH as a possible mechanism for killing cells in acidic regions of solid tumors: effects of carbonylcyanide-3-chlorophenylhydrazone.细胞内pH值降低作为实体瘤酸性区域细胞杀伤的一种可能机制:羰基氰化物-3-氯苯腙的作用
Cancer Res. 1989 Aug 15;49(16):4477-82.

酸性微环境中弱有机酸的选择性细胞酸化与毒性

Selective cellular acidification and toxicity of weak organic acids in an acidic microenvironment.

作者信息

Karuri A R, Dobrowsky E, Tannock I F

机构信息

Division of Experimental Therapeutics, Ontario Cancer Institute, Toronto, Canada.

出版信息

Br J Cancer. 1993 Dec;68(6):1080-7. doi: 10.1038/bjc.1993.485.

DOI:10.1038/bjc.1993.485
PMID:8260358
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1968646/
Abstract

The mean extracellular pH (pHe) within solid tumours has been found to be lower than in normal tissues. Agents which cause intracellular acidification at low pHe might have selective toxicity towards cells in tumours. Weak acids (or their anions) with pKa values in the range of 4-6 have a higher proportion of molecules in the uncharged form at low pHe and can diffuse more rapidly into cells. The effects of organic acids including succinate, monomethyl succinate and malonate to acidify cells have been evaluated under conditions of different pHe in the acidic range. These weak acids caused intracellular acidification of murine EMT-6 and human MGH-U1 cells in a concentration and pHe dependent fashion. At concentrations of 10 mM and above, these acids also caused in vitro cytotoxicity to these cells at low pHe (< 6.5). The rate and extent of cellular acidification caused by these weak acids, and their cytotoxicity at low pHe, were enhanced by exposure to amiloride and 5-(N-ethyl-N-isopropyl)amiloride (EIPA), agents which inhibit Na+/H+ exchange, and hence the regulation of intracellular pH. Acid dependent cytotoxicity was also investigated in a murine solid tumour using the endpoints of growth delay and colony formation in vitro following treatment in vivo. Agents were tested alone or with 15 Gy X-rays to select a population of hypoxic (and presumably acidic) cells. Achievable serum concentrations of succinate were about 1 mM and no antitumour activity of succinate was detected when used in this way. It is concluded that weak acids are selectively taken up into cells, and can cause selective cellular acidification and toxicity, at low pHe in culture. Weak acids that are normal cellular metabolites are not toxic in vivo, but weak acids carrying cytotoxic groups offer the potential for selective uptake and toxicity under the conditions of low pHe that exist in many solid tumours.

摘要

研究发现实体瘤内的平均细胞外pH值(pHe)低于正常组织。在低pHe条件下导致细胞内酸化的药物可能对肿瘤细胞具有选择性毒性。pKa值在4 - 6范围内的弱酸(或其阴离子)在低pHe时以不带电荷形式存在的分子比例更高,并且能够更快地扩散进入细胞。在酸性范围内不同pHe条件下,评估了包括琥珀酸、单甲基琥珀酸和丙二酸在内的有机酸使细胞酸化的作用。这些弱酸以浓度和pHe依赖的方式导致小鼠EMT - 6细胞和人MGH - U1细胞内酸化。在浓度为10 mM及以上时,这些酸在低pHe(< 6.5)条件下也对这些细胞产生体外细胞毒性。暴露于抑制Na⁺/H⁺交换从而调节细胞内pH的氨氯吡咪和5 -(N - 乙基 - N - 异丙基)氨氯吡咪(EIPA)后,这些弱酸引起的细胞酸化速率和程度及其在低pHe时的细胞毒性增强。还在小鼠实体瘤中研究了酸依赖性细胞毒性,采用体内治疗后体外生长延迟和集落形成的终点指标。单独或与15 Gy X射线联合测试药物,以选择一群缺氧(可能呈酸性)细胞。琥珀酸可达到的血清浓度约为1 mM,以这种方式使用时未检测到琥珀酸的抗肿瘤活性。结论是,在培养中低pHe条件下,弱酸可被选择性摄取到细胞中,并可导致选择性细胞酸化和毒性。作为正常细胞代谢产物的弱酸在体内无毒,但携带细胞毒性基团的弱酸在许多实体瘤存在的低pHe条件下具有选择性摄取和毒性的潜力。