12 research outputs found
Injury induced neuroplasticity and cell specific targeting of the lumbar enlargement for gene therapy.
This dissertation is an examination of spinal cord injury induced neuroplasticity and tests whether noninvasive gene therapy can successfully target neurons in the lumbar spinal cord. It begins with an overview of neural control of locomotion and a brief summary of therapeutics that are used and/or in development for treating spinal anatomically characterize s subset of neurons in the spinal cord, long ascending propriospinal neurons, that are involved in interlimb coordination. Characterization of these neurons allows for subsequent evaluation of their potential involvement in injury induced neuroplasticity. This dissertation is divided into five chapters, covering spinal cord injury and therapeutics. Chapter One gives background on locomotor control, propriospinal neurons, spinal cord injury, and therapeutics. Chapter Two develops and characterizes viral tracing methods for spinal cord anatomy. Chapter Three then uses these methods to characterize long ascending propriospinal neurons and evaluate their involvement in injury induced plasticity. Chapter Four then focuses on the development of noninvasive delivery of gene transfer to the lumbar enlargement. This involves optimizing focused ultrasound and intravenous microbubble delivery to focally and transiently permeabilize the blood spinal cord barrier of the lumbar spinal cord. This optimization then allows for successful gene transfer in neurons in the lumbar spinal cord following intravenous delivery of viral vector. Lasty, Chapter Five discusses the implications for all of these findings and how these findings have contributed to our understanding spinal cord anatomy and injury, and how the proof-of-concept in Chapter 4 provides a promising new avenue for spinal cord injury therapeutics
Explainable AI: A review of applications to neuroimaging data
Deep neural networks (DNNs) have transformed the field of computer vision and currently constitute some of the best models for representations learned via hierarchical processing in the human brain. In medical imaging, these models have shown human-level performance and even higher in the early diagnosis of a wide range of diseases. However, the goal is often not only to accurately predict group membership or diagnose but also to provide explanations that support the model decision in a context that a human can readily interpret. The limited transparency has hindered the adoption of DNN algorithms across many domains. Numerous explainable artificial intelligence (XAI) techniques have been developed to peer inside the “black box” and make sense of DNN models, taking somewhat divergent approaches. Here, we suggest that these methods may be considered in light of the interpretation goal, including functional or mechanistic interpretations, developing archetypal class instances, or assessing the relevance of certain features or mappings on a trained model in a post-hoc capacity. We then focus on reviewing recent applications of post-hoc relevance techniques as applied to neuroimaging data. Moreover, this article suggests a method for comparing the reliability of XAI methods, especially in deep neural networks, along with their advantages and pitfalls
Metabolic and Blood Flow Properties of Functional Brain Networks Using Human Multimodal Neuroimaging
The brain has a high energetic cost to support neuronal activity, requiring both oxygen and glucose supply from the cerebral vascular system. Additionally, the brain functions through complex patterns of interconnectivity between neuronal assemblies giving rise to functional network architectures that can be investigated across multiple spatial scales. Different brain regions have different roles and importance within these network architectures, with some regions exhibiting more global importance by being involved in cross-network communication while other being predominantly involved in local connections. There are indications that regions exhibiting a more global role in inter networks connectivity are characterized by a higher and more efficient metabolic profile, leading to differences in metabolic properties when compared to more locally connected regions. Understanding the link between oxygen/glucose metabolism and functional features of brain network architectures, across different spatial scales, is of primary importance.
This thesis consists of three original studies combining human brain resting-state multimodal neuroimaging and transcriptional data to investigate the glucose/oxygen metabolic costs of brain functional connectivity. We quantified glucose metabolism from positron emission tomography, and oxygen metabolism and functional connectivity from magnetic resonance imaging. In the first study, we highlight how the oxygen/glucose metabolism of brain regions can non-linearly relate to their functional hubness, within the resting-state networks of the brain across a nested hierarchy. We found that an increase in oxygen/glucose metabolism is associated with a non-linear increase in functional hubness where increase rates are both network- and scale-dependent. In the second study, we show specific transcriptional signatures that characterize the oxygen/glucose metabolic costs of regions involved in network global versus local centrality. This study highlights the different metabolic profiles of local and global regions, with gene expression related to oxidative metabolism and synaptic pathways being enriched in association with spatial patterns in common with resting blood flow and metabolism (oxygen and glucose) and globally-connected regions. In the third study, we demonstrate that there are oxygen/glucose metabolic costs to the functional integration and segregation of resting-state networks. We highlight that the metabolic costs of functional integration could reflect the hierarchical organization of the brain from unimodal to transmodal regions
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Application of Deep Learning to Brain Connectivity Classification in Large MRI Datasets
The use of machine learning for whole-brain classification of magnetic resonance imaging (MRI) data is of clear interest, both for understanding phenotypic differences in brain structure and function and for diagnostic applications. Developments of deep learning models in the past decade have revolutionized photographic image and speech recognition, bringing promise to do the same to other fields of science. However, there are many practical and theoretical challenges in the translation of such methods to the unique context of MRIs of the brain. This thesis presents a theoretical underpinning for whole-brain classification of extremely large datasets of multi-site MRIs, including machine learning model architecture, dataset curation methods, machine learning visualization methods, encoding of MRI data, and feature extraction. To replicate large sample sizes typically applied to deep learning models, a dataset of over 50,000 functional and structural MRIs was amassed from nine different databases, and the undertaken analyses were conducted on three covariates commonly found across these collections: sex, resting state/task, and autism spectrum disorder. I find that deep learning is not only a method that has promise for clinical application in the future, but also a powerful statistical tool for analyzing complex, nonlinear relationships in brain data where conventional statistics may fail. However, results are also dependent on factors such as dataset imbalances, confounding factors such as motion and head size, selected methods of encoding MRI data, variability of machine learning models and selected methods of visualizing the machine learning results. In this thesis, I present the following methodological innovations: (1) a method of balancing datasets as a means of regressing out measurable confounding factors; (2) a means of removing spatial biases from deep learning visualization methods; (3) methods of encoding functional and structural datasets as connectivity matrices; (4) the use of ensemble models and convolutional neural network architectures to improve classification accuracy and consistency; (5) adaptation of deep learning visualization methods to study brain connections utilized in the classification process. Additionally, I discuss interpretations, limitations, and future directions of this research.Gates Cambridge Scholarshi
Dynamical complexity of large-scale neurocognitive networks in healthy and pathological brain states
Joint Exploration and Mining of Memory-Relevant Brain Anatomic and Connectomic Patterns via a Three-Way Association Model
Early change in memory performance is a key symptom of many brain diseases, but its underlying mechanism remains largely unknown. While structural MRI has been playing an essential role in revealing potentially relevant brain regions, increasing availability of diffusion MRI data (e.g., Human Connectome Project (HCP)) provides excellent opportunities for exploration of their complex coordination. Given the complementary information held in these two imaging modalities, we hypothesize that studying them as a whole, rather than individually, and exploring their association will provide us valuable insights of the memory mechanism. However, many existing association methods, such as sparse canonical correlation analysis (SCCA), only manage to handle two-way association and thus cannot guarantee the selection of biomarkers and associations to be memory relevant. To overcome this limitation, we propose a new outcome-relevant SCCA model (OSCCA) together with a new algorithm to enable the three-way associations among brain connectivity, anatomic structure and episodic memory performance. In comparison with traditional SCCA, we demonstrate the effectiveness of our model with both synthetic and real data from the HCP cohort