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A fluorogenic near-infrared imaging agent for quantifying plasma and local tissue renin activity in vivo and ex vivo

机译:一种荧光的近红外成像剂用于定量体内和离体血浆和局部组织肾素的活性

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摘要

The renin-angiotensin system (RAS) is well studied for its regulation of blood pressure and fluid homeostasis, as well as for increased activity associated with a variety of diseases and conditions, including cardiovascular disease, diabetes, and kidney disease. The enzyme renin cleaves angiotensinogen to form angiotensin I (ANG I), which is further cleaved by angiotensin-converting enzyme to produce ANG II. Although ANG II is the main effector molecule of the RAS, renin is the rate-limiting enzyme, thus playing a pivotal role in regulating RAS activity in hypertension and organ injury processes. Our objective was to develop a near-infrared fluorescent (NIRF) renin-imaging agent for noninvasive in vivo detection of renin activity as a measure of tissue RAS and in vitro plasma renin activity. We synthesized a renin-activatable agent, ReninSense 680 FAST (ReninSense), using a NIRF-quenched substrate derived from angiotensinogen that is cleaved specifically by purified mouse and rat renin enzymes to generate a fluorescent signal. This agent was assessed in vitro, in vivo, and ex vivo to detect and quantify increases in plasma and kidney renin activity in sodium-sensitive inbred C57BL/6 mice maintained on a low dietary sodium and diuretic regimen. Noninvasive in vivo fluorescence molecular tomographic imaging of the ReninSense signal in the kidney detected increased renin activity in the kidneys of hyperreninemic C57BL/6 mice. The agent also effectively detected renin activity in ex vivo kidneys, kidney tissue sections, and plasma samples. This approach could provide a new tool for assessing disorders linked to altered tissue and plasma renin activity and to monitor the efficacy of therapeutic treatments.
机译:肾素-血管紧张素系统(RAS)对血压和体液稳态的调节以及与包括心血管疾病,糖尿病和肾脏疾病在内的多种疾病和状况相关的活动增加,都得到了充分研究。肾素酶裂解血管紧张素原形成血管紧张素I(ANG I),再由血管紧张素转化酶裂解产生ANG II。尽管ANG II是RAS的主要效应分子,但肾素是限速酶,因此在高血压和器官损伤过程中调节RAS活性起着关键作用。我们的目标是开发一种近红外荧光(NIRF)肾素成像剂,用于无创体内检测肾素活性,作为组织RAS和体外血浆肾素活性的量度。我们使用源自血管紧张素原的NIRF淬灭底物合成了一种肾素激活剂ReninSense 680 FAST(ReninSense),该底物被纯化的小鼠和大鼠肾素酶特异性裂解以产生荧光信号。在体外,体内和离体评估该药物,以检测和定量维持低饮食钠和利尿方案的钠敏感性近交C57BL / 6小鼠血浆和肾脏肾素活性的增加。肾脏中ReninSense信号的无创体内荧光分子断层显像检测到高肾素C57BL / 6小鼠肾脏中的肾素活性增加。该试剂还可以有效检测离体肾脏,肾脏组织切片和血浆样品中的肾素活性。这种方法可以提供一种新的工具,用于评估与组织和血浆肾素活性改变有关的疾病,并监测治疗效果。

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