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人骨髓性白血病细胞系中的核酸内切酶活性及DNA片段化诱导

Endonuclease activity and induction of DNA fragmentation in human myelogenous leukemic cell lines.

作者信息

Yanagisawa-Shiota F, Sakagami H, Kuribayashi N, Iida M, Sakagami T, Takeda M

机构信息

First Department of Biochemistry, School of Medicine, Showa University, Tokyo, Japan.

出版信息

Anticancer Res. 1995 Mar-Apr;15(2):259-65.

PMID:7762992
Abstract

When four human myelogenous leukemic cell lines (HL-60, ML-1, U-937, THP-1) were exposed to either ascorbic acid, hydrogen peroxide, etoposide, tumor necrosis factor, hyperthermia or UV irradiation, their growth inhibition and oligonucleosome-size DNA fragmentation were induced. Non-myelogenous leukemic cell lines (MOLT-4, K-562) were similarly sensitive to ascorbic acid and hydrogen peroxide, but relatively resistant to etoposide, TNF, hyperthermia and UV irradiation. Furthermore, these treatments except for UV irradiation, did not induce any apparent DNA fragmentation in MOLT-4 and K-562 cells. An autodigestion experiment revealed that all of these six cell lines contained divalent cation-independent endonuclease activity as a major endonuclease. The ability of this endonuclease to produce oligonucleosome-size DNA fragmentation was stimulated at acidic, but not at neutral pH. Since this enzyme activity was not detected in the lysosomal enzyme-free nuclei, prepared from all six cell lines, the cytoplasmic localization of this enzyme was suggested. The results suggest that the endonuclease activity might be differently regulated between myelogenous and non-myelogenous leukemic cell lines.

摘要

当四种人髓性白血病细胞系(HL - 60、ML - 1、U - 937、THP - 1)暴露于抗坏血酸、过氧化氢、依托泊苷、肿瘤坏死因子、热疗或紫外线照射时,它们的生长受到抑制并诱导出寡核小体大小的DNA片段化。非髓性白血病细胞系(MOLT - 4、K - 562)对抗坏血酸和过氧化氢同样敏感,但对依托泊苷、肿瘤坏死因子、热疗和紫外线照射相对耐药。此外,除紫外线照射外,这些处理在MOLT - 4和K - 562细胞中未诱导出任何明显的DNA片段化。自消化实验表明,这六种细胞系均含有一种以二价阳离子非依赖性核酸内切酶活性为主的核酸内切酶。该核酸内切酶产生寡核小体大小DNA片段化的能力在酸性pH条件下受到刺激,而在中性pH条件下则未受刺激。由于在从所有六种细胞系制备的无溶酶体酶的细胞核中未检测到这种酶活性,因此提示该酶定位于细胞质。结果表明,髓性和非髓性白血病细胞系之间核酸内切酶活性的调节可能存在差异。

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