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首页> 外文期刊>Investigative radiology >Effect of nitric oxide synthase inhibition on intrarenal oxygenation as evaluated by blood oxygenation level-dependent magnetic resonance imaging.
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Effect of nitric oxide synthase inhibition on intrarenal oxygenation as evaluated by blood oxygenation level-dependent magnetic resonance imaging.

机译:一氧化氮合酶抑制对肾内氧合的影响,通过血液氧合水平依赖性磁共振成像评估。

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OBJECTIVE: To investigate the feasibility of studying renal effects of nitric oxide synthase inhibition (NOSi) in humans by blood oxygenation level-dependent (BOLD) MRI. Nitric oxide (NO) is known to play a key role in the pathophysiology of hypertension and previous reports suggest reduced bioavailability of NO in the kidneys of hypertensive rats and hence show reduced response to NOSi using BOLD MRI. Ability to perform similar studies in humans could potentially lead to detection of early changes before development of symptoms, and to monitor novel interventions targeted toward improved NO bioavailability. The specific goals for this study were: (1) to examine whether lower doses and dose rate of administration of NOSi such as those previously used in humans can be detected by BOLD MRI in rat kidneys, (2) to compare changes in R2* to direct measures of renal medullary oxygen levels and blood flow using invasive probes (OxyLite/OxyFlo), and (3) to examine for the first time the effect of NOSi on intrarenal oxygenation in humans. MATERIAL AND METHODS: In rat kidneys, acute changes in renal tissue oxygenation induced by different doses (2, 4, and 10 mg/kg) of N-nitro-L-arginine methyl ester were studied in 36 Sprague Dawley rats, which were equally divided into BOLD MRI and OxyLite/OxyFlo groups. Similarly in humans, acute changes in renal oxygenation were induced by 2 different NOS inhibitors NG-monomethyl-L-arginine (4.25 mg/kg) in 7 volunteers and N-nitro-L-arginine methyl ester (2 mg/kg and 4 mg/kg) in 6 healthy young volunteers. A multiple gradient echo sequence was used in both rats (TE = 4.4-57.8 milliseconds with 3.6 milliseconds interecho spacing) and humans (TE = 6.4-40.8 milliseconds with a 2.3 milliseconds interecho spacing) to acquire 16 T2*-weighted images. R2* maps were constructed by fitting a single exponential decay to the image data on pixel by pixel basis. R2* measurements in the cortex and medulla were performed by regions of interest analysis. Measurements were performed before and during infusion of NOSi. RESULTS: In rats, NOSi decreased medullary pO2 and blood flow in a dose-dependent manner, and BOLD MRI showed an increase in medullary R2* consistent with the invasive pO2 measurements. In humans, BOLD MRI similarly showed an increase in medullary and cortical R2* after NOSi in a dose-dependent manner. In both rats and humans, the R2* values fell back toward baseline before the end of the infusion period. CONCLUSION: Comparison of BOLD MRI measurements with those using invasive probes suggests that changes in blood flow are at least partly responsible for observed changes with BOLD MRI. Monitoring changes after NOSi by renal BOLD MRI in vivo in human kidneys are feasible, and preliminary findings are consistent with observations in rat kidneys. Future studies are warranted to fully understand the apparent reversal in R2* changes during the infusion of NOSi.
机译:目的:通过血液氧合水平依赖性(BOLD)MRI研究研究一氧化氮合酶抑制(NOSi)对人肾脏的影响的可行性。一氧化氮(NO)在高血压的病理生理中起着关键作用,以前的报道表明一氧化氮在高血压大鼠肾脏中的生物利用度降低,因此使用BOLD MRI显示对NOSi的反应降低。在人类中进行相似研究的能力可能潜在地导致在症状发展之前及早发现变化,并监测针对改善NO生物利用度的新干预措施。这项研究的具体目标是:(1)检查是否可以通过BOLD MRI在大鼠肾脏中检测出较低剂量和较低剂量的NOSi,例如以前在人体内使用的剂量,(2)比较R2 *与使用侵入性探针(OxyLite / OxyFlo)直接测量肾脏髓质氧水平和血流量,以及(3)首次检查NOSi对人肾内氧合的影响。材料与方法:在大鼠肾脏中,对36只Sprague Dawley大鼠进行了研究,研究了不同剂量(2、4和10 mg / kg)的N-硝基-L-精氨酸甲酯引起的肾脏组织氧合的急性变化。分为BOLD MRI和OxyLite / OxyFlo组。同样,在人类中,由7种志愿者中的2种不同的NOS抑制剂NG-单甲基-L-精氨酸(4.25 mg / kg)和N-硝基-L-精氨酸甲酯(2 mg / kg和4 mg / kg)在6名健康的年轻志愿者中。在大鼠(TE = 4.4-57.8毫秒,回声间隔为3.6毫秒)和人类(TE = 6.4-40.8毫秒,回声间隔为2.3毫秒)中均使用了多重梯度回波序列,以获取16张T2 *加权图像。 R2 *映射是通过将单个指数衰减按像素逐个拟合到图像数据而构建的。皮质和髓质中的R2 *测量通过感兴趣区域分析进行。在注入NOSi之前和之中进行测量。结果:在大鼠中,NOSi以剂量依赖的方式降低了髓质pO2和血流量,BOLD MRI显示髓质R2 *的增加与侵入性pO2测量一致。在人类中,BOLD MRI同样显示NOSi后髓样和皮质R2 *呈剂量依赖性增加。在大鼠和人类中,R2 *值在输液期结束前均回落至基线。结论:将BOLD MRI测量结果与使用侵入性探头的测量结果进行比较,表明血流变化至少部分负责观察到的BOLD MRI变化。在人肾脏中通过肾脏BOLD MRI体内监测NOSi后的变化是可行的,初步发现与在大鼠肾脏中观察到的一致。有必要进行进一步的研究,以充分了解注入NOSi期间R2 *变化的明显逆转。

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