Experimental Imaging/Advanced Technology, Global Pharmaceutical Research and Development, Abbott Laboratories, Abbott Park, IL 60064, USA.
Neurobiol Aging. 2012 May;33(5):933-44. doi: 10.1016/j.neurobiolaging.2010.08.005. Epub 2010 Oct 18.
With 90% of neuroscience clinical trials failing to see efficacy, there is a clear need for the development of disease biomarkers that can improve the ability to predict human Alzheimer's disease (AD) trial outcomes from animal studies. Several lines of evidence, including genetic susceptibility and disease studies, suggest the utility of fluorodeoxyglucose positron emission tomography (FDG-PET) as a potential biomarker with congruency between humans and animal models. For example, early in AD, patients present with decreased glucose metabolism in the entorhinal cortex and several regions of the brain associated with disease pathology and cognitive decline. While several of the commonly used AD mouse models fail to show all the hallmarks of the disease or the limbic to cortical trajectory, there has not been a systematic evaluation of imaging-derived biomarkers across animal models of AD, contrary to what has been achieved in recent years in the Alzheimer's Disease Neuroimaging Initiative (ADNI) (Miller, 2009). If animal AD models were found to mimic endpoints that correlate with the disease onset, progression, and relapse, then the identification of such markers in animal models could afford the field a translational tool to help bridge the preclinical-clinical gap. Using a combination of FDG-PET and functional magnetic resonance imaging (fMRI), we examined the Tg2576 mouse for global and regional measures of brain glucose metabolism at 7 and 19 months of age. In experiment 1 we observed that at younger ages, when some plaque burden and cognitive deficits have been reported, Tg2576 mice showed hypermetabolism as assessed with FDG-PET. This hypermetabolism decreased with age to levels similar to wild type (WT) counterparts such that the 19-month-old transgenic (Tg) mice did not differ from age matched WTs. In experiment 2, using cerebral blood volume (CBV) fMRI, we demonstrated that the hypermetabolism observed in Tg mice at 7 months could not be explained by changes in hemodynamic parameters as no differences were observed when compared with WTs. Taken together, these data identify brain hypermetabolism in Tg2576 mice which cannot be accounted for by changes in vascular compliance. Instead, the hypermetabolism may reflect a neuronal compensatory mechanism. Our data are discussed in the context of disease biomarker identification and target validation, suggesting little or no utility for translational based studies using Tg2576 mice.
90%的神经科学临床试验未能显示出疗效,因此显然需要开发能够提高从动物研究中预测人类阿尔茨海默病 (AD) 试验结果的疾病生物标志物的能力。包括遗传易感性和疾病研究在内的几条证据表明,氟脱氧葡萄糖正电子发射断层扫描 (FDG-PET) 作为一种潜在的生物标志物具有实用性,其在人类和动物模型之间具有一致性。例如,在 AD 早期,患者的内嗅皮层和与疾病病理和认知能力下降相关的大脑的几个区域的葡萄糖代谢降低。虽然几种常用的 AD 小鼠模型未能显示出疾病的所有特征或边缘到皮质的轨迹,但与近年来在阿尔茨海默病神经影像学倡议 (ADNI) 中所取得的成果相反,尚未对 AD 动物模型中的成像衍生生物标志物进行系统评估 (米勒,2009 年)。如果发现动物 AD 模型模拟与疾病发作、进展和复发相关的终点,那么在动物模型中识别此类标志物可以为该领域提供一种转化工具,帮助弥合临床前-临床差距。我们使用 FDG-PET 和功能磁共振成像 (fMRI) 的组合,在 7 个月和 19 个月大时检查了 Tg2576 小鼠的大脑葡萄糖代谢的整体和区域测量值。在实验 1 中,我们观察到,在较年轻的年龄时,当已经报道了一些斑块负担和认知缺陷时,Tg2576 小鼠表现出 FDG-PET 评估的代谢亢进。这种代谢亢进随着年龄的增长而降低,达到与野生型 (WT) 对应物相似的水平,以至于 19 个月大的转基因 (Tg) 小鼠与年龄匹配的 WT 没有区别。在实验 2 中,我们使用脑血容量 (CBV) fMRI 证明,在 7 个月大的 Tg 小鼠中观察到的代谢亢进不能用血液动力学参数的变化来解释,因为与 WT 相比,没有观察到差异。总之,这些数据确定了 Tg2576 小鼠的大脑代谢亢进,这种亢进不能用血管顺应性的变化来解释。相反,代谢亢进可能反映了神经元的代偿机制。我们的数据在疾病生物标志物识别和目标验证的背景下进行了讨论,表明使用 Tg2576 小鼠进行基于转化的研究几乎没有或没有用处。
