Ferrazzano Peter, Shi Yejie, Manhas Namratta, Wang Yanping, Hutchinson Beth, Chen Xinzhi, Chanana Vishal, Gerdts Josiah, Meyerand Mary Elizabeth, Sun Dandan
Department of Pediatrics, University of Wisconsin, Madison, WI 53792, USA.
Front Biosci (Elite Ed). 2011 Jan 1;3(1):81-8. doi: 10.2741/e222.
We used magnetic resonance imaging (MRI) to assess the efficacy of Na+/H+ exchanger isoform 1 (NHE-1) inhibition following cerebral ischemia. Transient focal cerebral ischemia was induced in wild-type controls (NHE-1(+/+)), NHE-1 genetic knockdown mice (NHE-1(+/-)), and NHE-1(+/+) mice treated with the selective NHE-1 inhibitor HOE642. Diffusion weighted imaging (DWI) revealed a brain lesion as early as 1 hour following reperfusion and illustrated significant protection in NHE-1(+/-) mice (16.2 +/- 7.9 mm3 in NHE-1(+/-) mice vs. 47.5 +/- 16.6 mm3 in NHE-1(+/+) mice). Knockdown of NHE-1 showed significantly smaller infarct at 72 hours on T2 imaging (21.2 +/- 12.6 mm3 in NHE-1(+/-) mice vs. 64.6 +/- 2.5 mm3 in NHE-1(+/+) mice). Administration of HOE642 prior to reperfusion or during early reperfusion reduced ischemic damage. Thus, high resolution T2 images can be used for consistent and precise calculation of lesion volumes, while changes of DWI are a sensitive early marker of ischemic injury. The results of this study demonstrate the therapeutic potential for inhibition of NHE-1 in treating cerebral ischemia.
我们使用磁共振成像(MRI)来评估脑缺血后钠氢交换体1(NHE-1)抑制的效果。在野生型对照小鼠(NHE-1(+/+))、NHE-1基因敲低小鼠(NHE-1(+/-))以及用选择性NHE-1抑制剂HOE642处理的NHE-1(+/+)小鼠中诱导短暂性局灶性脑缺血。弥散加权成像(DWI)显示再灌注后1小时就出现脑损伤,并表明NHE-1(+/-)小鼠有显著的保护作用(NHE-1(+/-)小鼠为16.2±7.9立方毫米,而NHE-1(+/+)小鼠为47.5±16.6立方毫米)。NHE-1基因敲低显示在T2成像上72小时时梗死灶明显更小(NHE-1(+/-)小鼠为21.2±12.6立方毫米,而NHE-1(+/+)小鼠为64.6±2.5立方毫米)。在再灌注前或早期再灌注期间给予HOE642可减少缺血损伤。因此,高分辨率T2图像可用于一致且精确地计算损伤体积,而DWI的变化是缺血性损伤的敏感早期标志物。本研究结果证明了抑制NHE-1在治疗脑缺血方面的治疗潜力。