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Multiple Kernel Learning Captures a Systems-Level Functional Connectivity Biomarker Signature in Amyotrophic Lateral Sclerosis

机译:多核学习捕获肌萎缩性侧索硬化症的系统级功能连接性生物标志物签名。

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摘要

There is significant clinical and prognostic heterogeneity in the neurodegenerative disorder amyotrophic lateral sclerosis (ALS), despite a common immunohistological signature. Consistent extra-motor as well as motor cerebral, spinal anterior horn and distal neuromuscular junction pathology supports the notion of ALS a system failure. Establishing a disease biomarker is a priority but a simplistic, coordinate-based approach to brain dysfunction using MRI is not tenable. Resting-state functional MRI reflects the organization of brain networks at the systems-level, and so changes in of motor functional connectivity were explored to determine their potential as the substrate for a biomarker signature. Intra- as well as inter-motor functional networks in the 0.03–0.06 Hz frequency band were derived from 40 patients and 30 healthy controls of similar age, and used as features for pattern detection, employing multiple kernel learning. This approach enabled an accurate classification of a group of patients that included a range of clinical sub-types. An average of 13 regions-of-interest were needed to reach peak discrimination. Subsequent analysis revealed that the alterations in motor functional connectivity were widespread, including regions not obviously clinically affected such as the cerebellum and basal ganglia. Complex network analysis showed that functional networks in ALS differ markedly in their topology, reflecting the underlying altered functional connectivity pattern seen in patients: 1) reduced connectivity of both the cortical and sub-cortical motor areas with non motor areas 2)reduced subcortical-cortical motor connectivity and 3) increased connectivity observed within sub-cortical motor networks. This type of analysis has potential to non-invasively define a biomarker signature at the systems-level. As the understanding of neurodegenerative disorders moves towards studying pre-symptomatic changes, there is potential for this type of approach to generate biomarkers for the testing of neuroprotective strategies.
机译:尽管有共同的免疫组织学特征,但神经退行性疾病肌萎缩性侧索硬化症(ALS)仍存在明显的临床和预后异质性。一致的运动外以及运动性脑,脊髓前角和远端神经肌肉接头病理学支持ALS的概念,即系统衰竭。建立疾病生物标记是一个优先事项,但是使用MRI解决基于脑部功能障碍的简单,基于坐标的方法并不可行。静止状态功能MRI反映了系统级别的大脑网络的组织,因此研究了运动功能连接性的变化,以确定它们作为生物标志物标记底物的潜力。 0.03-0.06 Hz频带内的以及电动机内部的功能网络来自40位患者和30位年龄相似的健康对照,并用作模式检测的特征,并采用了多核学习。这种方法可以对包括一系列临床亚型的一组患者进行准确分类。平均需要13个感兴趣的区域才能达到最高的区分度。随后的分析表明,运动功能连接性的改变普遍存在,包括未受到临床明显影响的区域,例如小脑和基底神经节。复杂的网络分析表明,ALS中的功能网络在拓扑结构上有显着差异,反映出患者体内功能连接模式的潜在变化:1)皮质和皮质下运动区与非运动区的连通性降低2)皮质下皮质降低马达连接性; 3)皮质下马达网络中的连接性增强。这种类型的分析具有潜在地在系统级别非侵入式定义生物标记签名的潜力。随着对神经退行性疾病的了解逐渐转向研究症状前的变化,这种方法有可能产生用于测试神经保护策略的生物标志物。

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