Somatostatin and cortistatin exert multiple biological actions through five receptors (sst1-5); however, not all their effects can be explained by activation of sst1-5. Indeed, we recently identified novel truncated but functional human sst5-variants, present in normal and tumoral tissues. In this study, we identified and characterized three novel truncated sst5 variants in mice and one in rats displaying different numbers of transmembrane-domains [TMD; sst5TMD4, sst5TMD2, sst5TMD1 (mouse-variants) and sst5TMD1 (rat-variant)]. These sst5 variants: (1) are functional to mediate ligand-selective-induced variations in [Ca(2+)]i and cAMP despite being truncated; (2) display preferential intracellular distribution; (3) mostly share full-length sst5 tissue distribution, but exhibit unique differences; (4) are differentially regulated by changes in hormonal/metabolic environment in a tissue- (e.g., central vs. systemic) and ligand-dependent manner. Altogether, our results demonstrate the existence of new truncated sst5-variants with unique ligand-selective signaling properties, which could contribute to further understanding the complex, distinct pathophysiological roles of somatostatin and cortistatin.
Identification and characterization of new functional truncated variants of somatostatin receptor subtype 5 in rodents.
啮齿动物生长抑素受体亚型 5 的新型功能性截短变体的鉴定和表征
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作者:Córdoba-Chacón Jose, Gahete Manuel D, Duran-Prado Mario, Pozo-Salas Ana I, Malagón MarÃa M, Gracia-Navarro F, Kineman Rhonda D, Luque Raul M, Castaño Justo P
| 期刊: | Cellular and Molecular Life Sciences | 影响因子: | 6.200 |
| 时间: | 2010 | 起止号: | 2010 Apr;67(7):1147-63 |
| doi: | 10.1007/s00018-009-0240-y | ||
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