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Coordination‐Responsive Longitudinal Relaxation Tuning as a Versatile MRI Sensing Protocol for Malignancy Targets

机译:协调响应的纵向弛豫调整作为针对恶性肿瘤目标的多功能MRI传感方案

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摘要

Biomarkers (e.g., acidity, H2O2, hypoxia, and specific molecules) as one primary component of tumor microenvironments are closely associated with occurrence, invasion, and metastasis of malignancy, thus can act as biological targets. However, their monitoring remains a challenging task. Herein, a coordination‐dependent longitudinal relaxation tuning (CLRT) that occurs between a Mn2+ “donor” and a Mn2+ “acceptor” is established to enable biological target sensing. Relying on the differences of coordination ability and spatial structure between donors and acceptors, the biological targets as Mn2+ acceptor can take Mn2+ away from the donors (i.e., modified ligands) in nanoscale probes, which consequently varies T1‐weighted (T1W) magnetic resonance imaging (MRI) signal. The coordination ability and spatial structure of the modified Mn2+ “donor” and the pore diameter of donor carrier are demonstrated to determine the feasibility, specificity, and generality of CLRT. With CLRT, this MRI‐based ruler is demonstrated for the successful specific detection of biological targets (i.e., hyaluronic acid and glutathione) of malignancy, and its potential in quantitative measurement of hyaluronic acid is further demonstrated. CLRT can serve as a novel and general sensing principle to augment the exploration of a wide range of biological systems.
机译:作为肿瘤微环境的主要组成部分的生物标志物(例如酸度,H2O2,低氧和特定分子)与恶性肿瘤的发生,侵袭和转移密切相关,因此可以作为生物学靶标。但是,对其进行监视仍然是一项艰巨的任务。在本文中,建立了Mn 2 + “供体”和Mn 2 + “受体”之间发生的依赖于坐标的纵向弛豫调谐(CLRT)以实现生物学靶​​标感应。依靠供体和受体之间的协调能力和空间结构的差异,作为Mn 2 + 受体的生物靶标可以使Mn 2 + 脱离供体(即修饰配体),因此会改变T1加权(T1W)磁共振成像(MRI)信号。通过修饰的Mn 2 + “供体”的配位能力和空间结构以及供体载体的孔径,确定了CLRT的可行性,特异性和通用性。借助CLRT,这种基于MRI的标尺可成功成功地特异性检测恶性生物靶标(即透明质酸和谷胱甘肽),并进一步证明了其在定量测量透明质酸中的潜力。 CLRT可以作为一种新颖的通用感测原理,以增强对多种生物系统的探索。

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