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Enhancement of Lysosomal Enzyme Activity by Recombinant Human Tumor Necrosis Factor and Its Role in Tumor Cell Killing in vitro

机译:重组人肿瘤坏死因子增强溶酶体酶活性及其在体外杀死肿瘤细胞中的作用

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摘要

We investigated the effect of recombinant human tumor necrosis factor (TNF) on the lysosomal enzyme activity of various established cell lines in vitro. Incubation of 1 × 106TNF‐sensitive mouse tumorigenic fibroblasts (L‐M cells) in the presence of TNF (100 U/ml) for 48 h increased the total (the sum of the enzyme activities in the lysosomes and the cytoplasm) acid phosphatase and /9‐ghicuronidase activities by 3.7‐ and 4.2‐fold, respectively. The same increase was observed even when 1 U/ml of TNF was added to some cultures and no further augmentation occurred at 10 or 100 U/ml. Measurement of total and free enzyme activities showed that TNF stimulation not only enhanced the total intracellular enzyme activity but also accelerated the conversion into free (cytoplasmic) enzyme activity. Addition of a lysosomotropic agent (methylamine) suppressed both the enhancement of lysosomal enzyme activity and the cytotoxicity of TNF. A similar enhancement of lysosomal enzyme activities was also detected in various TNF‐sensitive tumor cell lines, and a strong correlation (acid phosphatase: r= 0.836, β‐glucuronidase: r=0.910) was observed between the enhancement of enzyme activity and sensitivity to TNF. No such increase was detected in TNF‐resistant human diploid cells. These results show that TNF induces the activation and release of lysosomal enzymes in TNF‐sensitive cells, and suggest that such events may play an important role in TNF‐mediated cytotoxicity.
机译:我们调查了重组人肿瘤坏死因子(TNF)对体外建立的各种细胞系的溶酶体酶活性的影响。在TNF(100 U / ml)存在下孵育1×10 6 TNF敏感的小鼠致瘤成纤维细胞(L-M细胞)48小时可增加总糖原酶活性溶酶体和细胞质的酸性磷酸酶和/ 9-葡糖醛酸苷酶的活性分别为3.7和4.2倍。即使在某些培养物中加入1 U / ml TNF,也观察到了相同的增加,而在10或100 U / ml下没有进一步的增加。对总和游离酶活性的测量表明,TNF刺激不仅增强了总细胞内酶活性,而且还加速了向游离(细胞质)酶活性的转化。加入溶溶同质剂(甲胺)既抑制了溶酶体酶活性的增强,又抑制了TNF的细胞毒性。在各种对TNF敏感的肿瘤细胞系中也检测到了类似的溶酶体酶活性增强,并且在酶活性增强和对TNF-α的敏感性之间观察到强相关性(酸性磷酸酶:r = 0.836,β-葡萄糖醛酸苷酶:r = 0.910)。肿瘤坏死因子在抗TNF的人类二倍体细胞中未检测到这种增加。这些结果表明TNF诱导TNF敏感细胞中溶酶体酶的激活和释放,并表明此类事件可能在TNF介导的细胞毒性中起重要作用。

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