Kung Mei-Ping, Hou Catherine, Zhuang Zhi-Ping, Skovronsky Daniel, Kung Hank F
Department of Radiology, University of Pennsylvania, 3700 Market Street, Room 305 Philadelphia, PA 19104, United States.
Brain Res. 2004 Oct 29;1025(1-2):98-105. doi: 10.1016/j.brainres.2004.08.004.
In vivo imaging of amyloid plaques may be useful for evaluation and diagnosis of Alzheimer's disease (AD) patients. Towards that end, we have developed 6-iodo-2-(4'-dimethylamino-)phenyl-imidazo[1,2]pyridine (IMPY), and 4-N-methylamino-4'-hydroxystilbene (SB-13) as ligands for specifically targeting amyloid plaques. These ligands can be readily radiolabeled with I-123 or C-11, for in vivo imaging using single photon emission computerized tomography (SPECT) or positron emission tomography (PET), respectively. However, in order to be useful in vivo, probes must show selective high affinity binding to a sufficiently abundant binding site on amyloid plaques. Therefore, as a prelude to in vivo imaging studies, we evaluated the binding properties of these two potential imaging agents to amyloid plaques present in human brain tissues. In vitro binding studies were carried out with [(125)I]IMPY and [(3)H]SB-13 in homogenates prepared from postmortem samples of affected cortex and cerebellum of pathologically confirmed AD patients and age-matched controls. Binding parameters such as K(d) and B(max) were estimated. Competition study was designed to evaluate the amyloid plaque binding specificity using human brain tissues. Plaque binding was confirmed by thioflavin-S staining. Specific [(125)I]IMPY or [(3)H]SB-13 binding can be clearly measured in the cortical gray matter, but not in the white matter of AD cases. There was a very low specific binding in cortical tissue homogenates of control brains. Cerebellar homogenates prepared from either AD or control brains did not show any specific [(125)I]IMPY or [(3)H]SB-13 binding. The K(d) values of AD cortical homogenates were 5.3+/-1.0 and 2.4+/-0.2 nM for [(125)I]IMPY and [(3)H]SB-13, respectively. High binding capacity and comparable values were observed for both ligands (14-45 pmol/mg protein). The location and density of specific signal detected by [(125)I]IMPY or [(3)H]SB-13 correlated with the distribution of amyloid plaques in these brain specimens, as confirmed by thioflavin-S staining. Competition profiles of known ligands suggest that the binding is highly selective and comparable to that reported by using preformed Abeta peptide aggregates. [(125)I]IMPY and [(3)H]SB-13 show an abundant binding capacity with high binding affinities for amyloid plaques in affected cortical regions of AD brains. These properties suggest that when labeled with I-123 or C-11, these two ligands may be useful to quantitate amyloid plaque burdens in the living AD patients.
淀粉样斑块的体内成像可能有助于阿尔茨海默病(AD)患者的评估和诊断。为此,我们已开发出6-碘-2-(4'-二甲基氨基-)苯基-咪唑并[1,2]吡啶(IMPY)和4-N-甲基氨基-4'-羟基芪(SB-13)作为特异性靶向淀粉样斑块的配体。这些配体可以很容易地用I-123或C-11进行放射性标记,分别用于单光子发射计算机断层扫描(SPECT)或正电子发射断层扫描(PET)的体内成像。然而,为了在体内发挥作用,探针必须对淀粉样斑块上足够丰富的结合位点表现出选择性高亲和力结合。因此,作为体内成像研究的前奏,我们评估了这两种潜在成像剂与存在于人类脑组织中的淀粉样斑块的结合特性。用[(125)I]IMPY和[(3)H]SB-13在由经病理证实的AD患者和年龄匹配对照的受影响皮质和小脑的死后样本制备的匀浆中进行体外结合研究。估计了诸如解离常数(K(d))和最大结合量(B(max))等结合参数。设计竞争研究以使用人类脑组织评估淀粉样斑块结合特异性。通过硫黄素-S染色证实斑块结合。在AD病例的皮质灰质中可以清楚地测量到特异性[(125)I]IMPY或[(3)H]SB-13结合,但在白质中则不然。对照脑的皮质组织匀浆中特异性结合非常低。从AD或对照脑制备的小脑匀浆未显示任何特异性[(125)I]IMPY或[(3)H]SB-13结合。[(125)I]IMPY和[(3)H]SB-13在AD皮质匀浆中的解离常数(K(d))值分别为5.3±1.0和2.4±0.2 nM。两种配体均观察到高结合能力和相当的值(14 - 45 pmol/mg蛋白质)。如硫黄素-S染色所证实,[(125)I]IMPY或[(3)H]SB-13检测到的特异性信号的位置和密度与这些脑标本中淀粉样斑块的分布相关。已知配体的竞争曲线表明结合具有高度选择性,并且与使用预先形成的β-淀粉样肽聚集体报道的情况相当。[(125)I]IMPY和[(3)H]SB-13对AD脑受影响皮质区域中的淀粉样斑块表现出丰富的结合能力和高结合亲和力。这些特性表明,当用I-123或C-11标记时,这两种配体可能有助于定量活体AD患者中的淀粉样斑块负荷。
