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所有五个克隆的人类生长抑素受体(hSSTR1 - 5)在功能上都与腺苷酸环化酶偶联。

All five cloned human somatostatin receptors (hSSTR1-5) are functionally coupled to adenylyl cyclase.

作者信息

Patel Y C, Greenwood M T, Warszynska A, Panetta R, Srikant C B

机构信息

Fraser Laboratories, McGill University, Department of Medicine, Montreal, Quebec, Canada.

出版信息

Biochem Biophys Res Commun. 1994 Jan 28;198(2):605-12. doi: 10.1006/bbrc.1994.1088.

Abstract

Recent reports have suggested that only some of the cloned somatostatin receptors (SSTRs) are coupled to adenylyl cyclase. These studies have used both stable and transiently transfected cells or cells lacking appropriate Gi alpha and are controversial. To investigate SSTR signalling mechanisms, we have established stably transfected CHO-K1 cells expressing human genes for SSTR1-5. The effect of 0.1-100 nM SST-14 and SST-28 on forskolin (1 microM) stimulated cAMP accumulation was determined and compared to their receptor binding affinities. The 5 expressed hSSTRs bound SST-14 and SST-28 with high affinity (IC50 1.1-2.1 nM for SST-14; IC50 0.25-5.4 nM for SST-28). hSSTR1-4 bound SST-14 > SST-28 whereas hSSTR5 bound SST-28 > SST-14. Radioligand binding to hSSTR1-5 was significantly inhibited by GTP, GTP gamma S and pertussis toxin. Both SST-14 and SST-28 inhibited forskolin-induced cAMP stimulation with ED50 values which paralleled their binding affinities for the individual hSSTR subtypes. These results demonstrate that all 5 human SSTRs are functionally coupled to inhibition of adenylyl cyclase in CHO-K1 cells via pertussis toxin sensitive G proteins.

摘要

最近的报告表明,只有部分克隆的生长抑素受体(SSTRs)与腺苷酸环化酶偶联。这些研究使用了稳定转染和瞬时转染的细胞或缺乏适当Giα的细胞,存在争议。为了研究SSTR信号传导机制,我们建立了稳定转染的CHO-K1细胞,其表达人SSTR1-5基因。测定了0.1-100 nM的SST-14和SST-28对福斯可林(1 microM)刺激的cAMP积累的影响,并将其与其受体结合亲和力进行比较。5种表达的人SSTRs以高亲和力结合SST-14和SST-28(SST-14的IC50为1.1-2.1 nM;SST-28的IC50为0.25-5.4 nM)。hSSTR1-4结合SST-14 > SST-28,而hSSTR5结合SST-28 > SST-14。GTP、GTPγS和百日咳毒素显著抑制放射性配体与hSSTR1-5的结合。SST-14和SST-28均抑制福斯可林诱导的cAMP刺激,其ED50值与它们对各个hSSTR亚型的结合亲和力平行。这些结果表明,所有5种人SSTRs在CHO-K1细胞中通过百日咳毒素敏感的G蛋白在功能上与腺苷酸环化酶的抑制偶联。

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