近端肾单位中血管紧张素II对蛋白激酶C亚型的年龄依赖性激活。
Age-dependent activation of PKC isoforms by angiotensin II in the proximal nephron.
作者信息
Boesch D M, Garvin J L
机构信息
Division of Hypertension and Vascular Research, Henry Ford Hospital, 2799 West Grand Blvd., Detroit, MI 48202, USA.
出版信息
Am J Physiol Regul Integr Comp Physiol. 2001 Sep;281(3):R861-7. doi: 10.1152/ajpregu.2001.281.3.R861.
ANG II increases fluid absorption in proximal tubules from young rats more than those from adult rats. ANG II increases fluid absorption in the proximal nephron, in part, via activation of protein kinase C (PKC). However, it is unclear how age-related changes in ANG II-induced stimulation of the PKC cascade differ as an animal matures. We hypothesized that the response of the proximal nephron to ANG II decreases as rats mature due to a reduction in the amount and activation of PKC rather than a decrease in the number or affinity of ANG II receptors. Because PKC translocates from the cytosol to the membrane when activated, we first measured PKC activity in the soluble and particulate fractions of proximal tubule homogenates exposed to vehicle or 10(-10) M ANG II from young (26 +/- 1 days old) and adult rats (54 +/- 1 days old). ANG II increased PKC activity to the same extent in homogenates from young rats (from 0.119 +/- 0.017 to 0.146 +/- 0.015 U/mg protein) (P < 0.01) and adult rats (from 0.123 +/- 0.020 to 0.156 +/- 0.023 U/mg protein) (P < 0.01). Total PKC activity did not differ between groups (0.166 +/- 0.018 vs. 0.181 +/- 0.023). We next investigated whether activation of the alpha-, beta-, and gamma-PKC isoforms differed by Western blot. In homogenates from young rats, ANG II significantly increased activated PKC-alpha from 40.2 +/- 6.5 to 60.2 +/- 9.5 arbitrary units (AU) (P < 0.01) but had no effect in adult rats (46.1 +/- 5.1 vs. 48.5 +/- 8.2 AU). Similarly, ANG II increased activated PKC-gamma in proximal tubules from young rats from 47.9 +/- 13.2 to 65.6 +/- 16.7 AU (P < 0.01) but caused no change in adult rats. Activated PKC-beta, however, increased significantly in homogenates from both age groups. Specifically, activated PKC-beta increased from 8.6 +/- 1.4 to 12.2 +/- 2.1 AU (P < 0.01) in homogenates from nine young rats and from 19.0 +/- 5.5 to 25.1 +/- 7.1 AU (P < 0.01) in homogenates from 12 adult rats. ANG II did not alter the amount of soluble PKC-alpha, -beta, and -gamma significantly. The total amount of PKC-alpha and -gamma did not differ between homogenates from young and adult rats, whereas the total amount of PKC-beta was 59.7 +/- 10.7 and 144.9 +/- 41.8 AU taken from young and adult rats, respectively (P < 0.05). Maximum specific binding and affinity of ANG II receptors were not significantly different between young and adult rats. We concluded that the primary PKC isoform activated by ANG II changes during maturation.
血管紧张素II(ANG II)对幼鼠近端肾小管液体吸收的增加作用大于成年鼠。ANG II部分通过激活蛋白激酶C(PKC)增加近端肾单位的液体吸收。然而,尚不清楚随着动物成熟,ANG II诱导的PKC级联反应的年龄相关变化有何不同。我们推测,由于PKC数量和活性的降低而非ANG II受体数量或亲和力的下降,随着大鼠成熟,近端肾单位对ANG II的反应会降低。由于PKC激活时会从胞质溶胶转位到细胞膜,我们首先测量了来自幼鼠(26±1日龄)和成年鼠(54±1日龄)的近端肾小管匀浆的可溶性和颗粒部分中,在给予溶媒或10⁻¹⁰ M ANG II后PKC的活性。ANG II使幼鼠匀浆中的PKC活性增加程度与成年鼠相同(从0.119±0.017增至0.146±0.015 U/mg蛋白)(P<0.01)(成年鼠从0.123±0.020增至0.156±0.023 U/mg蛋白)(P<0.01)。两组间总PKC活性无差异(0.166±0.018对0.181±0.023)。接下来,我们通过蛋白质印迹法研究α-、β-和γ-PKC同工型的激活是否存在差异。在幼鼠匀浆中,ANG II使活化的PKC-α从40.2±6.5显著增加至60.2±9.5任意单位(AU)(P<0.01),但对成年鼠无影响(46.1±5.1对48.5±8.2 AU)。同样,ANG II使幼鼠近端肾小管中的活化PKC-γ从47.9±13.2增加至65.6±16.7 AU(P<0.01),但成年鼠无变化。然而,活化的PKC-β在两个年龄组的匀浆中均显著增加。具体而言,9只幼鼠匀浆中活化的PKC-β从8.6±1.4增加至12.2±2.1 AU(P<0.01),12只成年鼠匀浆中从19.0±5.5增加至25.1±7.1 AU(P<0.01)。ANG II未显著改变可溶性PKC-α、-β和-γ的量。幼鼠和成年鼠匀浆中PKC-α和-γ的总量无差异,而PKC-β的总量分别为59.7±10.7和144.9±41.8 AU(来自幼鼠和成年鼠)(P<0.05)。幼鼠和成年鼠之间ANG II受体的最大特异性结合和亲和力无显著差异。我们得出结论,ANG II激活的主要PKC同工型在成熟过程中发生变化。
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