尿苷
醛固酮
蟾蜍
核糖核酸
核糖体RNA
脱氧胞苷
化学
分子生物学
生物化学
生物
内科学
内分泌学
医学
癌症
基因
吉西他滨
作者
Bernard C. Rossier,Peter A. Wilce,John F. Inciardi,Fayth K. Yoshimura,I. S. Edelman
出处
期刊:American Journal of Physiology-cell Physiology
[American Physiological Society]
日期:1977-05-01
卷期号:232 (5): C174-C179
被引量:10
标识
DOI:10.1152/ajpcell.1977.232.5.c174
摘要
Previous studies showed that aldosterone augments transepithelial active Na+ transport and the incorporation of [3H]uridine into polyadenylated RNA (poly(A)(+)-RNA) (putatively mRNA) early in the latent period. Soon thereafter, incorporation of [methyl-14C] groups, as well as [3H]uridine into rRNA is also increased. To evaluate the role of rRNA in mineralocorticoid action, the inhibitor 3'-deoxycytidine was used in studies on the urinary bladder of the toad Bufo marinus. 3'-deoxycytidine suppressed the incorporation of [methyl-14C] and [3H]uridine into nuclear precursors of rRNA and subunits of cytoplasmic rRNA. In contrast, 3'-deoxycytidine inhibited incorporation of ]3H]uridine into cytoplasmic poly(A)(+)-RNA minimally. In control experiments, 3'-deoxycytidine had no significant effect on Na+ transport, measured as the short-circuit current (scc), when given alone. 3'-Deoxycytidine also had no significant effect on the aldosterone-dependent increase in scc. In the presence of 3'-deoxycytidine, aldosterone enhanced both the scc and the incorporation of [3H]uridine into poly(A)(+)-RNA significantly. We conclude that during the first 3 h, the mineralocorticoid action of aldosterone is not sensitive to inhibition of rRNA synthesis. Previous studies, however, implicate mRNA synthesis in this early response.
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