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胚胎大鼠儿茶酚胺能细胞中酪氨酸羟化酶mRNA的调控:原位杂交分析

Regulation of tyrosine hydroxylase mRNA in catecholaminergic cells of embryonic rat: analysis by in situ hybridization.

作者信息

Jonakait G M, Rosenthal M, Morrell J I

机构信息

Department of Biological Sciences, Rutgers University, Newark, New Jersey 07102.

出版信息

J Histochem Cytochem. 1989 Jan;37(1):1-5. doi: 10.1177/37.1.2562802.

Abstract

In situ hybridization was used to examine the appearance of mRNA specific for tyrosine hydroxylase (TH), the rate-limiting enzyme in catecholamine (CA) biosynthesis, in neural crest derivatives of the rat embryo. These derivatives include sympathetic ganglia and transient catecholaminergic cells of embryonic intestine. Messenger RNA is first detected in sympathetic ganglia at E11.5, the age corresponding to the initial immunocytochemical expression of TH protein. In older embryos increased accumulation of TH-specific mRNA in sympathetic ganglia parallels the increase in TH immunoreactivity. By contrast, mRNA for TH is difficult to detect in embryonic intestines at E11.5 but is found instead in cells clustered at the dorsal boundaries of the pharynx and foregut. Cells expressing TH mRNA are infrequently found in embryonic intestines at any age, even though TH protein is immunohistochemically apparent. Treatment of pregnant rats with doses of reserpine, known to increase circulating levels of glucocorticoid hormones and prolong the expression of TH protein in embryonic gut cells, dramatically but transiently increases the number of gut cells at E12.5 with detectable TH mRNA. After E13.5 TH mRNA is undetectable even in reserpine-treated guts. Reserpine treatment also increases the labeling density in sympathetic ganglia. Taken together, these data are consistent with the hypothesis that the microenvironment of the embryonic intestine affects gene expression directly to alter phenotype. Moreover, although reserpine administration briefly increases TH mRNA levels, the effect is short-lived and does not alter neurotransmitter phenotypic conversion.

摘要

原位杂交技术用于检测大鼠胚胎神经嵴衍生物中酪氨酸羟化酶(TH)特异性mRNA的出现情况,TH是儿茶酚胺(CA)生物合成中的限速酶。这些衍生物包括交感神经节和胚胎肠道中的瞬时儿茶酚胺能细胞。在E11.5时首次在交感神经节中检测到信使RNA,这个时期与TH蛋白最初的免疫细胞化学表达相对应。在较大的胚胎中,交感神经节中TH特异性mRNA积累的增加与TH免疫反应性的增加平行。相比之下,在E11.5时,胚胎肠道中很难检测到TH的mRNA,而是在聚集于咽和前肠背侧边界的细胞中发现。尽管TH蛋白在免疫组织化学上很明显,但在任何年龄段的胚胎肠道中都很少发现表达TH mRNA的细胞。用已知能增加糖皮质激素循环水平并延长胚胎肠道细胞中TH蛋白表达的利血平剂量处理怀孕大鼠,在E12.5时可显著但短暂地增加可检测到TH mRNA的肠道细胞数量。在E13.5之后,即使在利血平处理的肠道中也检测不到TH mRNA。利血平处理还增加了交感神经节中的标记密度。综上所述,这些数据与胚胎肠道的微环境直接影响基因表达以改变表型的假设一致。此外,尽管给予利血平可短暂增加TH mRNA水平,但这种作用是短暂的,并且不会改变神经递质的表型转换。

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