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绒毛膜促性腺激素在人胎儿肾脏和肝脏中的细胞定位。

Cellular localization of chorionic gonadotropin in human fetal kidney and liver.

作者信息

Goldsmith P C, McGregor W G, Raymoure W J, Kuhn R W, Jaffe R B

出版信息

J Clin Endocrinol Metab. 1983 Sep;57(3):654-61. doi: 10.1210/jcem-57-3-654.

Abstract

Earlier, we reported that second trimester human fetal kidney and, to a much lesser extent, human fetal liver were capable of synthesizing and secreting the beta-subunit of hCG. Recently, we also have shown that these tissues, likewise, synthesize and secrete the alpha-subunit of hCG. The hCG produced is biologically active. To determine the cellular localization of these peptides, immunocytochemical studies were performed on human fetal tissues using antibodies against beta hCG, alpha hCG, and the intact hormone. Placental syncytiotrophoblast served as an immunopositive control. In the human fetal kidney, the ascending (thick) limb of the loop of Henle, distal convoluted tubule, and occasional cells in the collecting ducts were distinctly immunopositive for both beta hCG and the alpha-subunit. Small amounts of light positive staining occurred in only a few hepatocytes. Placental syncytiotrophoblast was routinely positive for both subunits, but fetal lung and striated muscle were negative. These immunocytochemical results indicate that immunoreactive beta hCG as well as the alpha-subunit are present in placental syncytiotrophoblast, in the distal renal nephron, and in a limited population of hepatocytes. The qualitative number and intensity of immunopositive cells closely correlate with the quantitative amounts of their hCG subunit synthesis. Taken together with our previous biosynthetic data, the immunocytochemical localization reported here indicates the probable cellular sites of alpha- and beta hCG synthesis in these tissues. The presence of comparable alpha- and beta-subunit staining in identical cell populations suggests that both hCG subunits and, therefore, perhaps intact hCG are produced at these same cellular sites during fetal life.

摘要

早些时候,我们报道了妊娠中期的人胎儿肾脏,以及程度小得多的人胎儿肝脏,能够合成并分泌人绒毛膜促性腺激素(hCG)的β亚基。最近,我们还表明,这些组织同样能合成并分泌hCG的α亚基。所产生的hCG具有生物活性。为了确定这些肽的细胞定位,我们使用抗β-hCG、α-hCG和完整激素的抗体,对人胎儿组织进行了免疫细胞化学研究。胎盘合体滋养层细胞作为免疫阳性对照。在人胎儿肾脏中,亨氏袢升支(厚段)、远曲小管以及集合管中偶尔出现的细胞,对β-hCG和α亚基均呈明显的免疫阳性。仅少数肝细胞出现少量轻度阳性染色。胎盘合体滋养层细胞对两个亚基均呈常规阳性,但胎儿肺和横纹肌呈阴性。这些免疫细胞化学结果表明,免疫反应性β-hCG以及α亚基存在于胎盘合体滋养层细胞、远端肾单位和有限数量的肝细胞中。免疫阳性细胞的定性数量和强度与它们hCG亚基合成的定量数量密切相关。结合我们之前的生物合成数据,此处报道的免疫细胞化学定位表明了这些组织中α-和β-hCG合成的可能细胞位点。在相同细胞群体中存在可比的α-和β-亚基染色,表明在胎儿期,这两个hCG亚基,因此可能还有完整的hCG,都是在这些相同的细胞位点产生的。

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