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首页> 外文期刊>Hypertension: An Official Journal of the American Heart Association >Gene transfer of eNOS to the thick ascending limb of eNOS-KO mice restores the effects of L-arginine on NaCl absorption.
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Gene transfer of eNOS to the thick ascending limb of eNOS-KO mice restores the effects of L-arginine on NaCl absorption.

机译:将eNOS基因转移到eNOS-KO小鼠的上肢粗大上肢恢复了L-精氨酸对NaCl吸收的影响。

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摘要

The thick ascending limb of the loop of Henle (THAL) plays an essential role in the regulation of sodium and water homeostasis by the kidney. l-Arginine, the substrate for nitric oxide synthase (NOS), decreases NaCl absorption by THALs. We hypothesized that eNOS produces the NO that regulates THAL NaCl transport and that selective expression of eNOS in the THAL of eNOS knockout(-/-) mice would restore the effects of l-arginine on NaCl absorption. eNOS-/- mice were anesthetized, the left kidney was exposed, and the renal interstitium was injected with recombinant adenoviral vectors that expressed green fluorescent protein (GFP) or eNOS driven by the promoter of the Na/K/2Cl cotransporter Ad-NKCC2GFP and Ad-NKCC2eNOS, respectively. In Ad-NKCC2eNOS-transduced kidneys, eNOS expression was detected 7 days after injection but was absent in Ad-NKCC2GFP-transduced kidneys. In THALs from eNOS-/- mice transduced with Ad-NKCC2eNOS, adding L-arginine increased DAF-2DA fluorescence, a measure of NO production, by 9.1+/-1.1% (P<0.05; n=5), but not in THALs transduced with Ad-NKCC2GFP. In THALs from eNOS-/- mice transduced with Ad-NKCC2eNOS, Cl absorption averaged 85.9+/-11.8 pmol/min per millimeter. Adding l-arginine (1 mmol/L) to the bath decreased Cl absorption to 59.7+/-11.0 pmol/min per millimeter (P<0.05; n=6). In THALs transduced with Ad-NKCC2GFP, Cl absorption averaged 96.0+/-21.0 pmol/min per millimeter. Adding L-arginine to the bath did not significantly affect Cl absorption (100.6+/-20.6 pmol/min per millimeter; n=4). We concluded that gene transfer of eNOS to the THAL of eNOS-/- mice restores L-arginine-induced inhibition of NaCl transport and NO production. These data indicate that eNOS is essential for the regulation of THAL NaCl transport by NO.
机译:Henle环的粗大上升肢(THAL)在肾脏调节钠和水稳态方面起着至关重要的作用。一氧化氮合酶(NOS)的底物1-精氨酸可降低THAL对NaCl的吸收。我们假设eNOS产生可调节THAL NaCl转运的NO,而在eNOS基因敲除(-/-)小鼠THAL中eNOS的选择性表达将恢复1-精氨酸对NaCl吸收的影响。麻醉eNOS-/-小鼠,裸露左肾,并向肾间质注射重组腺病毒载体,该载体表达由Na / K / 2Cl共转运蛋白Ad-NKCC2GFP和PC的启动子驱动的绿色荧光蛋白(GFP)或eNOS。 Ad-NKCC2eNOS。在Ad-NKCC2eNOS转导的肾脏中,注射后7天检测到eNOS表达,但在Ad-NKCC2GFP转导的肾脏中不存在。在用Ad-NKCC2eNOS转导的eNOS-/-小鼠的THAL中,添加L-精氨酸可使DAF-2DA荧光(NO生成量)增加9.1 +/- 1.1%(P <0.05; n = 5),但在用Ad-NKCC2GFP转导的THAL。在用Ad-NKCC2eNOS转导的eNOS-/-小鼠的THAL中,Cl吸收平均为85.9 +/- 11.8 pmol / min / mm。向浴中添加1-精氨酸(1 mmol / L)可使Cl吸收降至每毫米59.7 +/- 11.0 pmol / min(P <0.05; n = 6)。在用Ad-NKCC2GFP转导的THAL中,Cl吸收平均每毫米为96.0 +/- 21.0 pmol / min。向浴中添加L-精氨酸不会显着影响Cl的吸收(每毫米100.6 +/- 20.6 pmol / min; n = 4)。我们得出的结论是,将eNOS的基因转移至eNOS-/-小鼠的THAL可恢复L-精氨酸诱导的NaCl转运抑制和NO产生。这些数据表明,eNOS对于NO调节THAL NaCl转运至关重要。

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