自发性高血压大鼠发育过程中D(1)多巴胺受体对NHE3的调节作用
D(1) dopamine receptor regulation of NHE3 during development in spontaneously hypertensive rats.
作者信息
Li X X, Xu J, Zheng S, Albrecht F E, Robillard J E, Eisner G M, Jose P A
机构信息
Department of Pediatrics, Georgetown University Medical Center, Washington, District of Columbia 20007, USA.
出版信息
Am J Physiol Regul Integr Comp Physiol. 2001 Jun;280(6):R1650-6. doi: 10.1152/ajpregu.2001.280.6.R1650.
To determine if the defective interactions among D(1)-like receptors, G proteins, and Na(+)/H(+) exchanger 3 (NHE3) are consequences of hypertension, we studied these interactions in rats, before (2--3 wk) and after (12 wk) the establishment of hypertension. To eliminate the confounding influence of second messenger action on D(1) receptor-NHE3 interaction, studies were performed in renal brush-border membranes (BBM) devoid of cytoplasmic second messengers. NHE3 activity increased with age in Wistar-Kyoto (WKY) rats (3 wk = 1.48 +/- 0.39, n = 13; 12 wk = 2.83 +/- 0.15, n = 16, P < 0.05) but not in spontaneously hypertensive rats (SHRs; 3 wk = 2.52 +/- 0.37, n = 11; 12 wk = 2.81 +/- 0.20, n = 16). D(1) receptor protein tended to decrease, whereas NHE3 protein tended to increase with age in both WKY and SHRs. However, the inhibitory effect of a D(1)-like agonist, SKF-81297, on NHE3 activity increased with age in WKY rats (3 wk = -40.7 +/- 5.3%, n = 10, 12 wk = -58.7 +/- 4.6%, n = 12, P < 0.05) but not in SHRs (3 wk = -27.6 +/- 5.9%, n = 11, 12 wk = -25.1 +/- 3.2%, n = 11). The decreased inhibitory effect of another D(1)-like agonist, fenoldopam, on NHE3 activity in SHRs was not caused by increased activity and binding of G beta gamma to NHE3 as has been reported in young WKY rats. G(s)alpha mediates, in part, the inhibitory effect of D(1)-like agonists on NHE3 activity. In WKY rats, fenoldopam increased G(s)alpha/NHE3 binding to the same extent in 2-wk-old (1.5-fold, n = 4) and adult (1.5-fold, n = 4) rats. In contrast, in SHRs, fenoldopam decreased the amount of G(s)alpha bound to NHE3 in 2-wk-old SHRs and had no effect in 4-wk-old and adult SHRs. These studies indicate that the decreased inhibitory effect of D(1)-like agonists on NHE3 activity in SHRs (compared with WKY rats) precedes the development of hypertension. This may be caused, in part, by a decreased interaction between G(s)alpha and NHE3 in BBM secondary to impaired D(1)-like receptor function.
为了确定D(1)样受体、G蛋白和钠/氢交换体3(NHE3)之间的缺陷性相互作用是否是高血压的后果,我们在高血压建立之前(2 - 3周)和之后(12周)对大鼠的这些相互作用进行了研究。为了消除第二信使作用对D(1)受体 - NHE3相互作用的混杂影响,研究在缺乏细胞质第二信使的肾刷状缘膜(BBM)中进行。Wistar - Kyoto(WKY)大鼠的NHE3活性随年龄增加(3周 = 1.48 ± 0.39,n = 13;12周 = 2.83 ± 0.15,n = 16,P < 0.05),但自发性高血压大鼠(SHR)中则不然(3周 = 2.52 ± 0.37,n = 11;12周 = 2.81 ± 0.20,n = 16)。在WKY大鼠和SHR中,D(1)受体蛋白随年龄有下降趋势,而NHE3蛋白随年龄有增加趋势。然而,D(1)样激动剂SKF - 81297对NHE3活性的抑制作用在WKY大鼠中随年龄增加(3周 = -40.7 ± 5.3%,n = 10;12周 = -58.7 ± 4.6%,n = 12,P < 0.05),但在SHR中并非如此(3周 = -27.6 ± 5.9%,n = 11;12周 = -25.1 ± 3.2%,n = 11)。另一种D(1)样激动剂非诺多泮对SHR中NHE3活性的抑制作用降低,并非如年轻WKY大鼠中所报道的那样是由于Gβγ与NHE3的活性和结合增加所致。G(s)α部分介导了D(1)样激动剂对NHE3活性的抑制作用。在WKY大鼠中,非诺多泮在2周龄(1.5倍,n = 4)和成年(同样1.5倍,n = 4)大鼠中增加G(s)α/NHE3结合的程度相同。相反,在SHR中,非诺多泮在2周龄SHR中减少了与NHE3结合的G(s)α量,而在4周龄和成年SHR中则无影响。这些研究表明,与WKY大鼠相比,SHR中D(1)样激动剂对NHE3活性的抑制作用降低在高血压发展之前就已出现。这可能部分是由于BBM中D(1)样受体功能受损继发的G(s)α与NHE3之间的相互作用减少所致。
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