速尿、曲弗罗辛和氰化物对肾小球滤过率反馈控制的干扰。
Interference with feedback control of glomerular filtration rate by furosemide, triflocin, and cyanide.
作者信息
Wright F S, Schnermann J
出版信息
J Clin Invest. 1974 Jun;53(6):1695-708. doi: 10.1172/JCI107721.
Microperfusion experiments have shown that increases in flow rate of tubule fluid through the loop of Henle are followed by reductions in single nephron glomerular filtration rate (SNGFR) and stop-flow pressure (SFP) measured in the proximal tubule of the same nephron. Because changes in luminal sodium concentration are not consistently related to changes in SNGFR and SFP, we explored the possibility that a transport step at a flow-dependent distal-sensing site might be involved in feedback control of SNGFR. Because the macula densa cells of the distal tubule are adjacent to the glomerular vessels of the same nephrons, they could be the distal-sensing mechanism. We perfused superficial loops of Henle from late proximal to early distal segments in three groups of rats while measuring SFP in the proximal tubule of the same nephron, SNGFR in the proximal tubule of the same nephron, or flow rates of fluid, Na, K, and Cl emerging from the perfused loops. Perfusion solutions used were 0.15 NaCl, Ringer or Ringer with one of several inhibitors of electrolyte transport. Perfusion rates were 10 or 40 nl/min (also, zero during measurements of SFP and SNGFR). With Ringer alone the loop-flow rate increased from 10 to 40 nl/min, caused a decrease in SFP from 37.6 to 32.1 mm Hg, and a decrease in SNGFR from 29.9 to 18.7 nl/min. Concentrations of Na, K, and Cl in early distal fluid and absorption of Na and Cl along the loop segment were also increased when loop perfusion rate was increased. Decreasing the perfusion rate to zero had little effect on SFP or SNGFR. The SFP response to increased flow rate did not occur when the perfusion solution contained furosemide (10(-4) M). No reduction of the SFP response was seen with other diuretics tested (amiloride, acetazolamide, ethacrynic acid, mercaptomerin) or with 0.15 M NaCl alone. The SNGFR response to increased perfusion rate was reduced by furosemide, triflocin, and cyanide but not by amiloride. Na and Cl absorption by the perfused segment were inhibited by furosemide, triflocin, cyanide, and amiloride. Amiloride and acetazolamide, probably do not act in the ascending limb. Ethacrynic acid and mercaptomerin are known to be ineffective in rat nephrons. Thus, agents that could have inhibited NaCl absorption by macula densa cells interfered with the feedback mechanism.
微量灌注实验表明,流经亨利袢的肾小管液流速增加后,同一肾单位近端小管测得的单肾单位肾小球滤过率(SNGFR)和停流压力(SFP)会降低。由于管腔钠浓度的变化与SNGFR和SFP的变化并非始终相关,我们探讨了流量依赖性远端传感部位的转运步骤可能参与SNGFR反馈控制的可能性。由于远端小管的致密斑细胞与同一肾单位的肾小球血管相邻,它们可能是远端传感机制。我们在三组大鼠中从近端晚期到远端早期灌注亨利袢浅环,同时测量同一肾单位近端小管的SFP、同一肾单位近端小管的SNGFR或从灌注环流出的液体、钠、钾和氯的流速。所用的灌注溶液为0.15 NaCl、林格液或含有几种电解质转运抑制剂之一的林格液。灌注速率为10或40 nl/min(在测量SFP和SNGFR时也为零)。仅用林格液时,环流量从10 nl/min增加到40 nl/min,导致SFP从37.6 mmHg降至32.1 mmHg,SNGFR从29.9 nl/min降至18.7 nl/min。当环灌注速率增加时,早期远端液中钠、钾和氯的浓度以及沿环段的钠和氯吸收也增加。将灌注速率降至零对SFP或SNGFR影响很小。当灌注溶液含有呋塞米(10⁻⁴ M)时,未出现SFP对流速增加的反应。在所测试的其他利尿剂(氨氯地平、乙酰唑胺、依他尼酸、汞撒利)或仅用0.15 M NaCl时,未观察到SFP反应的降低。呋塞米、三氟拉嗪和氰化物可降低SNGFR对灌注速率增加的反应,但氨氯地平不能。呋塞米、三氟拉嗪、氰化物和氨氯地平可抑制灌注段对钠和氯的吸收。氨氯地平和乙酰唑胺可能不在升支起作用。已知依他尼酸和汞撒利在大鼠肾单位中无效。因此,可能抑制致密斑细胞对NaCl吸收的药物会干扰反馈机制。
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