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首页> 外文期刊>American Journal of Physiology >Developmental expression and biological activity of gastrin-releasing peptide and its receptors in the kidney.
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Developmental expression and biological activity of gastrin-releasing peptide and its receptors in the kidney.

机译:胃泌素释放肽及其受体在肾脏中的发育表达和生物学活性。

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摘要

Mammalian gastrin-releasing peptide (GRP) has a widespread distribution and multiple stimulating effects on metabolism, release of regulatory peptides, gastrointestinal and pancreatic secretions, and behavior. GRP is a potent mitogen for a number of tumor types, including colon and lung. Although GRP is known to stimulate the growth of renal tumors, little is known of its synthesis, distribution, and receptors in the developing and mature kidney. Both Northern blot analysis and RT-PCR revealed the presence of GRP mRNA in ovine kidney from midgestation through to adulthood. GRP mRNA was detected in rat kidney from embryonic day 19 to postnatal day 30 by RT-PCR. Sequence-specific radioimmunoassay demonstrated the presence of substantial amounts of fully processed amidated GRP in the ovine renal cortex and medulla. The mRNA for the major receptor subtype, GRP-R, was present in fetal and adult sheep and rat kidneys. The mRNA for the low-affinity GRP receptor, bombesin receptor subtype-3 (BRS-3), was only detected in the rat kidney. In the ovine kidney, immunohistochemistry localized GRP predominantly to the thick ascending limb of the loop of Henle. mRNAs for GRP, GRP-R, and BRS-3 were detected in the human embryonic kidney cell line HEK293, and radioimmunoassay of cell extracts and conditioned media revealed the presence of proGRP but not the amidated form. However, amidated GRP did stimulate the proliferation of these cells. These studies demonstrate that the developing and mature kidney may be previously unidentified sites of autocrine or paracrine action for GRP.
机译:哺乳动物胃泌素释放肽(GRP)对代谢,调节肽的释放,胃肠道和胰腺分泌以及行为具有广泛的分布和多种刺激作用。 GRP是多种肿瘤类型(包括结肠和肺)的有效促分裂原。尽管已知GRP会刺激肾肿瘤的生长,但对于发育中和成熟的肾脏中GRP的合成,分布和受体知之甚少。 Northern印迹分析和RT-PCR均显示,从妊娠中期到成年期,羊肾脏中存在GRP mRNA。通过RT-PCR从胚胎第19天至出生后第30天在大鼠肾脏中检测到GRP mRNA。序列特异性放射免疫分析表明,绵羊肾皮质和髓质中存在大量完全加工的酰胺化GRP。主要受体亚型GRP-R的mRNA存在于胎儿和成年绵羊及大鼠肾脏中。仅在大鼠肾脏中检测到了低亲和力GRP受体mRNA,即蛙蛙蛋白受体亚型3(BRS-3)。在绵羊肾脏中,免疫组织化学主要将GRP定位于Henle loop的厚上升肢。在人类胚胎肾细胞系HEK293中检测到GRP,GRP-R和BRS-3的mRNA,并且对细胞提取物和条件培养基进行放射免疫分析发现存在proGRP,但没有酰胺化形式。然而,酰胺化的GRP确实刺激了这些细胞的增殖。这些研究表明,发育中和成熟的肾脏可能是先前未确定的针对GRP的自分泌或旁分泌作用的部位。

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