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p21/CIP1/WAF1(p21)在生长激素/生长激素受体及表皮生长因子/表皮生长因子受体通路的负调控中的作用,以及在生长激素转导缺陷中的作用。

The role of p21/CIP1/WAF1 (p21) in the negative regulation of the growth hormone/growth hormone receptor and epidermal growth factor/epidermal growth factor receptor pathways, in growth hormone transduction defect.

作者信息

Kostopoulou Eirini, Rojas Gil Andrea Paola, Spiliotis Bessie E

机构信息

Paediatric Endocrine Research Laboratory, Division of Paediatric Endocrinology and Diabetes, Department of Paediatrics, University of Patras School of Medicine, Patras, Greece.

Faculty of Human Movement and Quality of Life Sciences, Department of Nursing, University of Peloponnese, Sparta, Greece.

出版信息

Ann Pediatr Endocrinol Metab. 2018 Dec;23(4):204-209. doi: 10.6065/apem.2018.23.4.204. Epub 2018 Dec 31.

Abstract

PURPOSE

Growth hormone transduction defect (GHTD) is characterized by severe short stature, impaired STAT3 (signal transducer and activator of transcription-3) phosphorylation and overexpression of the cytokine inducible SH2 containing protein (CIS) and p21/CIP1/WAF1. To investigate the role of p21/CIP1/WAF1 in the negative regulation of the growth hormone (GH)/GH receptor and Epidermal Growth Factor (EGF)/EGF Receptor pathways in GHTD.

METHODS

Fibroblast cultures were developed from gingival biopsies of 1 GHTD patient and 1 control. The protein expression and the cellular localization of p21/CIP1/WAF1 was studied by Western immunoblotting and immunofluorescence, respectively: at the basal state and after induction with 200-μg/L human GH (hGH) (GH200), either with or without siRNA CIS (siCIS); at the basal state and after inductions with 200-μg/L hGH (GH200), 1,000-μg/L hGH (GH1000) or 50-ng/mL EGF.

RESULTS

After GH200/siCIS, the protein expression and nuclear localization of p21 were reduced in the patient. After successful induction of GH signaling (control, GH200; patient, GH1000), the protein expression and nuclear localization of p21 were reduced. After induction with EGF, p21 translocated to the cytoplasm in the control, whereas in the GHTD patient it remained located in the nucleus.

CONCLUSION

In the GHTD fibroblasts, when CIS is reduced, either after siCIS or after a higher dose of hGH (GH1000), p21's antiproliferative effect (nuclear localization) is also reduced and GH signaling is activated. There also appears to be a positive relationship between the 2 inhibitors of GH signaling, CIS and p21. Finally, in GHTD, p21 seems to participate in the regulation of both the GH and EGF/EGFR pathways, depending upon its cellular location.

摘要

目的

生长激素转导缺陷(GHTD)的特征为严重身材矮小、信号转导及转录激活因子3(STAT3)磷酸化受损以及细胞因子诱导含SH2结构域蛋白(CIS)和p21/CIP1/WAF1的过表达。旨在研究p21/CIP1/WAF1在GHTD中对生长激素(GH)/GH受体和表皮生长因子(EGF)/EGF受体通路负调控中的作用。

方法

从1例GHTD患者和1例对照者的牙龈活检组织中培养成纤维细胞。分别通过蛋白质免疫印迹法和免疫荧光法研究p21/CIP1/WAF1的蛋白表达和细胞定位:在基础状态下以及用200μg/L人GH(hGH)(GH200)诱导后,无论有无小干扰RNA CIS(siCIS);在基础状态下以及用200μg/L hGH(GH200)、1000μg/L hGH(GH1000)或50ng/mL EGF诱导后。

结果

在GH200/siCIS处理后,患者中p21的蛋白表达和核定位降低。在成功诱导GH信号传导后(对照,GH200;患者,GH1000),p21的蛋白表达和核定位降低。在用EGF诱导后,对照中p21转移至细胞质,而在GHTD患者中它仍位于细胞核中。

结论

在GHTD成纤维细胞中,当CIS减少时,无论是在siCIS处理后还是在更高剂量的hGH(GH1000)处理后,p21的抗增殖作用(核定位)也降低且GH信号传导被激活。GH信号传导的两种抑制剂CIS和p21之间似乎也存在正相关关系。最后,在GHTD中,p21似乎根据其细胞定位参与GH和EGF/EGFR通路的调控。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/84de/6312915/8617474433d0/apem-2018-23-4-204f1.jpg

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