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胰岛素和三碘甲状腺原氨酸对从胚胎小鼠大脑分离的细胞培养物中脑苷脂磺基转移酶合成的作用机制比较。

Comparison of the mechanisms of action of insulin and triiodothyronine on the synthesis of cerebroside sulfotransferase in cultures of cells dissociated from brains of embryonic mice.

作者信息

Ferret-Sena V, Sena A, Besnard F, Fressinaud C, Rebel G, Sarliève L L

机构信息

Centre de Neurochimie du CNRS, Strasbourg, France.

出版信息

Dev Neurosci. 1990;12(2):89-105. doi: 10.1159/000111838.

DOI:10.1159/000111838
PMID:2185927
Abstract

The effect of low (physiological) concentrations of insulin (2 and 20 ng/ml) and L-triiodothyronine (T3) were studied on two myelin-related enzymes: (1) the 3'-phosphoadenosine-5'-phosphosulfate:cerebroside sulfotransferase (CST, EC 2.8.2.11) catalyzing the production of sulfatide, and (2) the myelin enzyme, 2',3'-cyclic nucleotide 3'-phosphohydrolase (CNP, EC 3.1.4.3.7) in myelinogenic cultures of cells dissociated from embryonic mouse brain. Insulin treatment (20 ng/ml) of the cells in the presence of serum increased CST activity at 18 and 25 days in vitro (DIV) by 86 and 211%, respectively. At 18 DIV and under the same conditions, CNP was significantly stimulated (95%) by high doses of insulin (2,000 ng/ml) only, while arylsulfatase A (EC 3.1.6.1) or cerebroside sulfatase activities, both of which are involved in sulfatide degradation, were unchanged. Thus, it can be assumed that the observed increase of the incorporation of [35S]O4 into sulfatide after insulin treatment of mixed cell cultures is the result of CST induction rather than a decreased catabolism. The level of CST activity in insulin-treated cells (20 ng/ml) in serum-free medium was also increased at 18 and 25 DIV by about 50 and 70%, respectively. Conversely, none of the insulin concentrations used in the absence of serum (even at high doses) had any effect, either at 18 or 25 DIV on CNP and ASA activities. The involvement of insulin in the regulation of sulfatide synthesis was further confirmed by dose-response curves relating the activity of CST to hormone concentration in the medium. The increase in the activity of CST in insulin-treated cells was due only to the increase in the Vmax of this enzyme, suggesting that it may be attributed to enzyme induction. A study of kinetic parameters of CST indicated that there were no differences in pH optimum and Km values between control and induced enzyme. Further experiments using cycloheximide point to a direct effect of insulin on oligodendrocyte CST induction. Data similar to those described above for insulin were also obtained with T3. As for insulin, T3 stimulated the induction of CST but in serum-free medium only. This effect was prevented by cycloheximide. In addition, the induction of CST by T3 was blocked by actinomycin D. This was not the case for insulin. These results suggest that T3 and insulin act on CST by different mechanisms, i.e. at transcriptional and post-translational levels, respectively. Apart from this, the insulin effect on CST activity was additive to that of T3.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

研究了低(生理)浓度的胰岛素(2和20纳克/毫升)和L-三碘甲状腺原氨酸(T3)对两种髓鞘相关酶的影响:(1)3'-磷酸腺苷-5'-磷酸硫酸酯:脑苷脂磺基转移酶(CST,EC 2.8.2.11),催化硫脂的产生;(2)髓鞘酶2',3'-环核苷酸3'-磷酸水解酶(CNP,EC 3.1.4.3.7),在从胚胎小鼠脑部分离的细胞的髓鞘形成培养物中。在有血清存在的情况下,用胰岛素(20纳克/毫升)处理细胞,在体外培养18天和25天时,CST活性分别增加了86%和211%。在18天体外培养且相同条件下,只有高剂量胰岛素(2000纳克/毫升)能显著刺激CNP(95%),而参与硫脂降解的芳基硫酸酯酶A(EC 3.1.6.1)或脑苷脂硫酸酯酶活性未发生变化。因此,可以推测在混合细胞培养物中用胰岛素处理后观察到的[35S]O4掺入硫脂的增加是CST诱导的结果,而非分解代谢减少。在无血清培养基中用胰岛素(20纳克/毫升)处理的细胞,在18天和25天时CST活性水平也分别增加了约50%和70%。相反,在无血清情况下使用的任何胰岛素浓度(即使是高剂量),在18天或25天时对CNP和ASA活性均无影响。通过将CST活性与培养基中激素浓度相关的剂量反应曲线,进一步证实了胰岛素参与硫脂合成的调节。胰岛素处理细胞中CST活性的增加仅归因于该酶Vmax的增加,表明这可能归因于酶的诱导。对CST动力学参数的研究表明,对照酶和诱导酶在最适pH值和Km值上没有差异。使用放线菌酮的进一步实验表明胰岛素对少突胶质细胞CST诱导有直接作用。用T3也获得了与上述胰岛素类似的数据。与胰岛素一样,T3刺激CST的诱导,但仅在无血清培养基中。这种作用被放线菌酮阻止。此外,T3对CST的诱导被放线菌素D阻断。胰岛素则不然。这些结果表明,T3和胰岛素通过不同机制作用于CST,即分别在转录和翻译后水平。除此之外,胰岛素对CST活性的作用与T3的作用是相加的。(摘要截短至400字)

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