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通过靶向对比超声心动图对P-选择素进行分子成像检测近期心肌缺血

Detection of recent myocardial ischaemia by molecular imaging of P-selectin with targeted contrast echocardiography.

作者信息

Kaufmann Beat A, Lewis Christopher, Xie Aris, Mirza-Mohd Ayoub, Lindner Jonathan R

机构信息

Cardiovascular Division, UHN-62, Oregon Health and Sciences University, 3181 SW Sam Jackson Park Road, Portland, OR 97239, USA.

出版信息

Eur Heart J. 2007 Aug;28(16):2011-7. doi: 10.1093/eurheartj/ehm176. Epub 2007 May 26.

DOI:10.1093/eurheartj/ehm176
PMID:17526905
Abstract

AIMS

We hypothesized that molecular imaging of endothelial P-selectin expression with targeted myocardial contrast echocardiography (MCE) could identify recently ischaemic myocardium without infarction.

METHODS AND RESULTS

The microvascular behaviour of P-selectin-targeted (MB(p)) and control (MB(c)) microbubbles was assessed by intravital microscopy of the cremaster muscle in mice. Targeted MCE imaging with MB(p) and MB(c) was performed in mice after brief left anterior descending (LAD) occlusion and reperfusion and in open- and closed-chest controls. Regional wall motion and perfusion by MCE were assessed during occlusion and after reperfusion. On intravital microscopy, ischaemia-reperfusion produced a 10-fold increase (P < 0.01) in venular attachment for MB(p). Attachment for MB(c) was rare. With myocardial ischaemia-reperfusion, LAD occlusion produced hypoperfusion and wall motion abnormalities that resolved after 45 min of reperfusion. At 45 min, signal enhancement in the post-ischaemic region was four-fold greater (P < 0.05) for MB(p) vs. MB(c). MB(p) produced low-level enhancement in non-ischaemic myocardium in all open-chest animals, suggesting P-selectin expression from surgical cardiac exposure.

CONCLUSION

Molecular imaging of P-selectin with targeted MCE can identify the presence of recently ischaemic myocardium in the absence of necrosis and after resolution of hypoperfusion and post-ischaemic stunning. This technique can potentially provide a method for risk stratifying patients with acute chest pain.

摘要

目的

我们假设通过靶向心肌对比超声心动图(MCE)对内皮P-选择素表达进行分子成像能够识别近期发生缺血但未梗死的心肌。

方法与结果

通过对小鼠提睾肌进行活体显微镜检查,评估靶向P-选择素的微泡(MB(p))和对照微泡(MB(c))的微血管行为。在短暂左前降支(LAD)闭塞和再灌注后,以及在开胸和闭胸对照小鼠中,使用MB(p)和MB(c)进行靶向MCE成像。在闭塞期间和再灌注后,通过MCE评估局部室壁运动和灌注情况。在活体显微镜下,缺血-再灌注使MB(p)的静脉附着增加了10倍(P<0.01)。MB(c)的附着很少见。心肌缺血-再灌注时,LAD闭塞导致灌注不足和室壁运动异常,再灌注45分钟后恢复。在45分钟时,缺血后区域MB(p)的信号增强比MB(c)大四倍(P<0.05)。在所有开胸动物中,MB(p)在非缺血心肌中产生低水平增强,提示手术心脏暴露导致P-选择素表达。

结论

用靶向MCE对P-选择素进行分子成像可识别近期缺血心肌的存在,且不存在坏死,同时可在灌注不足和缺血后心肌顿抑恢复后进行识别。该技术可能为急性胸痛患者的风险分层提供一种方法。

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