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培养的恶性及腺苷环化3':5'-单磷酸诱导的“分化”神经母细胞瘤细胞中环状核苷酸与蛋白质的结合

Binding of cyclic nucleotides with proteins in malignant and adenosine cyclic 3':5'-monophosphate-induced "differentiated" neuroblastoma cells in culture.

作者信息

Prasad K N, Sinha P K, Sahu S K, Brown J L

出版信息

Cancer Res. 1976 Jul;36(7 PT 1):2290-6.

PMID:179701
Abstract

The binding of adenosine cyclic 3':5'-monophosphate (cyclic AMP) with soluble (100,000 X g supernatant), pellet, and total homogenate proteins from cyclic AMP-induced "differentiated" mouse neuroblastoma cells increased by about two-fold. The extent of binding with soluble proteins was higher than that with pellet proteins. The binding of cyclic AMP with soluble proteins from 5'-adenosine monophosphate-treated, serum-free medium-treated, sodium butyrate-treated, 6-thioguanine-treated, or X-irradiated neuroblastoma cells did not significantly change. When the soluble proteins containing bound cyclic [3H]AMP were filtered through a Sephadex G-25 column, the relative amount of protein-bound cyclic [3H]AMP in differentiated cells was greater than that in malignant cells, but the amount of free cyclic [3H]AMP was correspondingly less. The electrophoretic characteristics of cyclic AMP-binding proteins of differentiated and malignant cells were identical. There were two binding peaks, but the extent of binding at each peak was relatively high in differentiated neuroblastoma cells. An increase in cyclic AMP binding occurred 24 hr after treatment of neuroblastoma cells with prostaglandin E1. This increase was completely blocked by cycloheximide but not by actinomycin D. The binding was heat labile and sensitive to protease action. These data indicate that the increase in binding in differentiated cells is due to an elevation in the levels of binding proteins. The binding of cyclic AMP with soluble proteins from rat glial cells and mouse L-cells did not significantly change after treatment with prostaglandin E1 or an inhibitor of cyclic AMP phosphodiesterase. Cyclic AMP and guanosine cyclic 3':5'-monophosphate bind with the same proteins, but cyclic AMP has about 10-fold higher binding affinity than does guanosine cyclic 3':5'-monophosphate.

摘要

环磷腺苷(环磷酸腺苷,cyclic AMP)与环磷酸腺苷诱导的“分化”小鼠神经母细胞瘤细胞的可溶性蛋白(100,000×g 上清液)、沉淀蛋白和总匀浆蛋白的结合增加了约两倍。与可溶性蛋白的结合程度高于与沉淀蛋白的结合程度。环磷酸腺苷与经5'-单磷酸腺苷处理、无血清培养基处理、丁酸钠处理、6-硫鸟嘌呤处理或 X 射线照射的神经母细胞瘤细胞的可溶性蛋白的结合没有显著变化。当含有结合的环[3H]AMP 的可溶性蛋白通过 Sephadex G-25 柱过滤时,分化细胞中与蛋白结合的环[3H]AMP 的相对量大于恶性细胞中的相对量,但游离环[3H]AMP 的量相应较少。分化细胞和恶性细胞中环磷酸腺苷结合蛋白的电泳特性相同。有两个结合峰,但在分化的神经母细胞瘤细胞中每个峰的结合程度相对较高。用前列腺素 E1 处理神经母细胞瘤细胞 24 小时后,环磷酸腺苷结合增加。这种增加被放线菌酮完全阻断,但不被放线菌素 D 阻断。该结合对热不稳定且对蛋白酶作用敏感。这些数据表明分化细胞中结合的增加是由于结合蛋白水平的升高。用前列腺素 E1 或环磷酸腺苷磷酸二酯酶抑制剂处理后,环磷酸腺苷与大鼠神经胶质细胞和小鼠 L 细胞的可溶性蛋白的结合没有显著变化。环磷酸腺苷和环鸟苷酸(环磷鸟苷,guanosine cyclic 3':5'-monophosphate)与相同的蛋白结合,但环磷酸腺苷的结合亲和力比环鸟苷酸高约 10 倍。

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