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生长激素和进食对生长板静止细胞及肝脏中快速信号转导子和转录激活子5磷酸化的调节

Regulation of rapid signal transducer and activator of transcription-5 phosphorylation in the resting cells of the growth plate and in the liver by growth hormone and feeding.

作者信息

Gevers Evelien F, Hannah Matthew J, Waters Michael J, Robinson Iain C A F

机构信息

Division of Molecular Neuroendocrinology, Medical Research Council National Institute for Medical Research, The Ridgeway, Mill Hill, London NW7 1AA, United Kingdom.

出版信息

Endocrinology. 2009 Aug;150(8):3627-36. doi: 10.1210/en.2008-0985. Epub 2009 Apr 9.

Abstract

GH has physiological functions in many tissues, but the cellular targets for direct effects of GH remain ill defined in complex tissues such as the growth plate in which the contribution of direct vs. indirect actions of GH remains controversial. The Janus kinase (Jak)-signal transducer and activator of transcription (STAT)-5 pathway is activated by GH, so we developed a method to visualize nuclear Stat5b and phosphorylated Stat5 in single cells in response to a pulse of GH. Hep2 cells did not show a Stat5 phosphorylation (pY-Stat5) response to GH except in cells transfected to express GH receptors. ATDC5 cells express GH receptors and showed GH-induced pY-Stat5 responses, which varied with their state of chondrocyte differentiation. In vivo, Stat5b(+ve) nuclei were seen in the resting and prehypertrophic chondrocytes of the growth plate. After a single ip pulse of human GH or mouse GH, but not prolactin, pY-Stat5 responses were visible in cells in the resting zone and groove of Ranvier, 10-45 min later. Prehypertrophic chondrocytes showed no pY-Stat5 response to GH. GH target cells were also identified in other tissues, and a marked variability in spatiotemporal pY-Stat5 responses was evident. Endogenous hepatic pY-Stat5 was detected in mice with intact GH secretion but only during a GH pulse. Fasting and chronic exposure to GH attenuated the pY-Stat5 response to an acute GH injection. In conclusion, pY-Stat5 responses to GH vary in time and space, are sensitive to nutritional status, and may be inhibited by prior GH exposure. In the growth plate, our data provide direct in vivo support for an early role of GH to regulate the fate of immature chondrocytes.

摘要

生长激素(GH)在许多组织中具有生理功能,但在诸如生长板等复杂组织中,GH直接作用的细胞靶点仍不清楚,在生长板中,GH直接作用与间接作用的贡献仍存在争议。Janus激酶(Jak)-信号转导子和转录激活子(STAT)-5途径可被GH激活,因此我们开发了一种方法来可视化单个细胞中核Stat5b和磷酸化Stat5对GH脉冲的反应。Hep2细胞对GH未表现出Stat5磷酸化(pY-Stat5)反应,除非在转染表达GH受体的细胞中。ATDC5细胞表达GH受体,并表现出GH诱导的pY-Stat5反应,该反应随软骨细胞分化状态而变化。在体内,在生长板的静止和前肥大软骨细胞中可见Stat5b(阳性)细胞核。在单次腹腔注射人GH或小鼠GH后,但不是催乳素,10-45分钟后在静止区和Ranvier沟的细胞中可见pY-Stat5反应。前肥大软骨细胞对GH未表现出pY-Stat5反应。在其他组织中也鉴定出了GH靶细胞,并且时空pY-Stat5反应存在明显差异。在GH分泌完整的小鼠中检测到内源性肝pY-Stat5,但仅在GH脉冲期间。禁食和长期暴露于GH会减弱对急性GH注射的pY-Stat5反应。总之,对GH的pY-Stat5反应在时间和空间上有所不同,对营养状况敏感,并且可能会被先前的GH暴露所抑制。在生长板中,我们的数据为GH在调节未成熟软骨细胞命运中的早期作用提供了直接的体内支持。

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