Muhsin Sura A, Abdullah Amjed, Kobashigawa Estela, Al-Amidie Muthana, Russell Sherri, Zhang Michael Z, Zhang Shuping, Almasri Mahmoud
University of Missouri-Columbia, Electrical Engineering and Computer Science, Columbia, MO USA.
University of Missouri-Columbia, College of Veterinary Medicine, Veterinary Medical Diagnostic Laboratory, Columbia, MO USA.
Microsyst Nanoeng. 2023 Aug 21;9:104. doi: 10.1038/s41378-023-00569-1. eCollection 2023.
Cervids are affected by a neurologic disease that is always fatal to individuals and has population effects. This disease is called chronic wasting disease (CWD) and is caused by a misfolded prion protein. The disease is transmitted via contact with contaminated body fluids and tissue or exposure to the environment, such as drinking water or food. Current CWD diagnosis depends on ELISA screening of cervid lymph nodes and subsequent immunohistochemistry (IHC) confirmation of ELISA-positive results. The disease has proven to be difficult to control in part because of sensitivity and specificity issues with the current test regimen. We have investigated an accurate, rapid, and low-cost microfluidic microelectromechanical system (MEMS) biosensing device for the detection of CWD pathologic prions in retropharyngeal lymph nodes (RLNs), which is the current standard type of CWD diagnostic sample. The device consists of three novel regions for concentrating, trapping, and detecting the prion. The detection region includes an array of electrodes coated with a monoclonal antibody against pathologic prions. The experimental conditions were optimized using an engineered prion control antigen. Testing could be completed in less than 1 hour with high sensitivity and selectivity. The biosensor detected the engineered prion antigen at a 1:24 dilution, while ELISA detected the same antigen at a 1:8 dilution. The relative limit of detection (rLOD) of the biosensor was a 1:1000 dilution of a known strong positive RLN sample, whereas ELISA showed a rLOD of 1:100 dilution. Thus, the biosensor was 10 times more sensitive than ELISA, which is the currently approved CWD diagnostic test. The biosensor's specificity and selectivity were confirmed using known negative RPLN samples, a negative control antibody (monoclonal antibody against bovine coronavirus BCV), and two negative control antigens (bluetongue virus and Epizootic hemorrhagic disease virus). The biosensor's ability to detect pathogenic prions was verified by testing proteinase-digested positive RLN samples.
鹿类动物会感染一种神经系统疾病,这种疾病对个体来说总是致命的,并且会对种群产生影响。这种疾病被称为慢性消耗病(CWD),由错误折叠的朊病毒蛋白引起。该疾病通过接触受污染的体液和组织或暴露于环境(如饮用水或食物)传播。目前,CWD的诊断依赖于对鹿类动物淋巴结进行酶联免疫吸附测定(ELISA)筛查,随后通过免疫组织化学(IHC)对ELISA阳性结果进行确认。事实证明,这种疾病难以控制,部分原因是当前检测方案存在灵敏度和特异性问题。我们研究了一种准确、快速且低成本的微流体微机电系统(MEMS)生物传感装置,用于检测咽后淋巴结(RLN)中的CWD病理性朊病毒,咽后淋巴结是目前CWD诊断样本的标准类型。该装置由用于浓缩、捕获和检测朊病毒的三个新区域组成。检测区域包括涂有针对病理性朊病毒的单克隆抗体的电极阵列。使用工程化朊病毒对照抗原对实验条件进行了优化。检测可在不到1小时内完成,具有高灵敏度和选择性。生物传感器能在1:24稀释度下检测到工程化朊病毒抗原,而ELISA在1:8稀释度下才能检测到相同抗原。生物传感器的相对检测限(rLOD)为已知强阳性RLN样本的1:1000稀释度,而ELISA的rLOD为1:100稀释度。因此,生物传感器的灵敏度比目前批准的CWD诊断测试ELISA高10倍。使用已知的阴性RPLN样本、阴性对照抗体(抗牛冠状病毒BCV的单克隆抗体)和两种阴性对照抗原(蓝舌病毒和流行性出血病病毒)确认了生物传感器的特异性和选择性。通过检测蛋白酶消化后的阳性RLN样本,验证了生物传感器检测致病性朊病毒的能力。
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