Publications by authors named "Kristen Maynard"

Over the past decade, single-cell genomics technologies have allowed scalable profiling of cell-type-specific features, which has substantially increased our ability to study cellular diversity and transcriptional programs in heterogeneous tissues. Yet our understanding of mechanisms of gene regulation or the rules that govern interactions between cell types is still limited. The advent of new computational pipelines and technologies, such as single-cell epigenomics and spatially resolved transcriptomics, has created opportunities to explore two new axes of biological variation: cell-intrinsic regulation of cell states and expression programs and interactions between cells.

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  • - Maternal smoking during pregnancy has notable negative effects on the cognitive and behavioral development of offspring, with this study specifically comparing the impacts of nicotine and cigarette smoke on gene expression in developing brains.
  • - Researchers found a significant number of differentially expressed genes (1,010 for nicotine and 4,165 for smoking) linked to prenatal exposure, indicating different neurodevelopmental pathways affected by each substance.
  • - The findings suggest that while both prenatal nicotine exposure and maternal smoking have specific and overlapping effects on the developing brain, these effects are not replicated in the adult brain, highlighting developmental-stage sensitivity to smoke-related changes.
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  • The study investigates how neurodegenerative disorders, particularly Alzheimer's disease, affect brain microenvironments by analyzing brain tissue lesions associated with amyloid-β and hyperphosphorylated tau.
  • Researchers used the advanced 10x Genomics Visium Spatial Proteogenomics platform to explore gene expression changes in post-mortem human brains, specifically in the inferior temporal cortex during late-stage Alzheimer's.
  • The findings offer insights into molecular processes linked to brain pathology, provide a framework for analyzing spatial gene expression, and deliver accessible interactive resources for the scientific community to explore related datasets.
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Drugs of abuse activate defined neuronal ensembles in brain reward structures such as the nucleus accumbens (NAc), which are thought to promote the enduring synaptic, circuit, and behavioral consequences of drug exposure. While the molecular and cellular effects arising from experience with drugs like cocaine are increasingly well understood, the mechanisms that sculpt NAc ensemble participation are largely unknown. Here, we leveraged unbiased single-nucleus transcriptional profiling to identify expression of the secreted glycoprotein Reelin (encoded by the gene) as a marker of cocaine-activated neuronal ensembles within the rat NAc.

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  • The study focuses on the molecular organization of the human neocortex, particularly the dorsolateral prefrontal cortex, using advanced spatial transcriptomic technologies.
  • Researchers created a detailed neuroanatomical atlas that highlights different spatial domains based on gene expression patterns, moving beyond traditional histological layers.
  • By integrating data from various sources, the team identified specific cell types and interactions linked to neuropsychiatric disorders, showing how these relate to spatial domains in the brain.
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  • - The study investigates the unique cell types within the human hippocampus, focusing on their roles in learning, memory, and cognition, using advanced methods like spatially-resolved transcriptomics (SRT) and single-nucleus RNA-sequencing (snRNA-seq) on tissue from ten neurotypical adults.
  • - Researchers employed non-negative matrix factorization (NMF) to analyze gene expression patterns across different neuronal cell types, discovering variations in excitatory and inhibitory responses within distinct spatial regions of the hippocampus.
  • - The findings include the identification of molecular profiles for various hippocampal cell types and suggest these profiles’ relevance to learning capabilities, while making the resulting data publicly available for further research.
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Relative cell type fraction estimates in bulk RNA-sequencing data are important to control for cell composition differences across heterogenous tissue samples. Current computational tools estimate relative RNA abundances rather than cell type proportions in tissues with varying cell sizes, leading to biased estimates. We present , a computational tool to accurately deconvolute cell types with varying sizes.

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Spatially resolved transcriptomics (SRT) is a growing field that links gene expression to anatomical context. SRT approaches that use next-generation sequencing (NGS) combine RNA sequencing with histological or fluorescent imaging to generate spatial maps of gene expression in intact tissue sections. These technologies directly couple gene expression measurements with high-resolution histological or immunofluorescent images that contain rich morphological information about the tissue under study.

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  • High-resolution imaging techniques are enhancing our ability to observe biological systems in detail, but sharing and customizing these images can be challenging.
  • Samui is a new web-based tool designed for fast and interactive visualization and annotation of large multidimensional images.
  • The tool is compatible with images from Vizgen MERFISH and 10x Genomics Visium Spatial Gene Expression, and it's available for use at https://samuibrowser.com.
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  • - The study investigates the habenula (Hb) in relation to schizophrenia (SCZD) by examining its cell types and how their transcriptomic profiles differ in individuals with SCZD compared to healthy controls.
  • - Researchers used advanced techniques like single nucleus RNA-sequencing and fluorescent hybridization to identify 17 distinct cell types in the human Hb and validated these findings.
  • - They discovered 45 genes that are differentially expressed in the Hb of SCZD individuals, revealing significant genetic changes and providing new insights into the molecular basis of neuropsychiatric disorders.
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  • - The study focuses on improving the cellular deconvolution of bulk RNA-seq data using single-cell RNA-seq data to estimate cell type composition in diverse tissues, particularly in the human brain.
  • - Researchers created a detailed multi-assay dataset from 22 postmortem human brain samples, employing various RNA-seq methods and comparing estimated cell proportions with actual measurements from other techniques.
  • - The analysis identified specific deconvolution algorithms that performed best, revealing that factors like cell size and differences in gene quantification can impact the accuracy of these methods in reflecting true tissue composition.
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Norepinephrine (NE) neurons in the locus coeruleus (LC) make long-range projections throughout the central nervous system, playing critical roles in arousal and mood, as well as various components of cognition including attention, learning, and memory. The LC-NE system is also implicated in multiple neurological and neuropsychiatric disorders. Importantly, LC-NE neurons are highly sensitive to degeneration in both Alzheimer's and Parkinson's disease.

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Deconvolution of cell mixtures in "bulk" transcriptomic samples from homogenate human tissue is important for understanding disease pathologies. However, several experimental and computational challenges impede transcriptomics-based deconvolution approaches using single-cell/nucleus RNA-seq reference atlases. Cells from the brain and blood have substantially different sizes, total mRNA, and transcriptional activities, and existing approaches may quantify total mRNA instead of cell type proportions.

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The dentate gyrus of the hippocampus is important for many cognitive functions, including learning, memory, and mood. Here, we investigated age-associated changes in transcriptome-wide spatial gene expression in the human dentate gyrus across the lifespan. Genes associated with neurogenesis and the extracellular matrix were enriched in infants, while gene markers of inhibitory neurons and cell proliferation showed increases and decreases in post-infancy, respectively.

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We define and identify a new class of control genes for next-generation sequencing called total RNA expression genes (TREGs), which correlate with total RNA abundance in cell types of different sizes and transcriptional activity. We provide a data-driven method to identify TREGs from single-cell RNA sequencing data, allowing the estimation of total amount of RNA when restricted to quantifying a limited number of genes. We demonstrate our method in postmortem human brain using multiplex single-molecule fluorescent in situ hybridization and compare candidate TREGs against classic housekeeping genes.

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Aims: The harms arising from psychoactive drug use are complex, and harm reduction strategies should be informed by a detailed understanding of the extent and nature of that harm. Drug harm is also context specific, and so any comprehensive assessment of drug harm should be relevant to the characteristics of the population in question. This study aimed to evaluate and rank drug harms within Aotearoa New Zealand using a multi-criteria decision analysis (MCDA) framework, and to separately consider harm within the total population, and among youth.

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Activity-regulated gene (ARG) expression patterns in the hippocampus (HPC) regulate synaptic plasticity, learning, and memory, and are linked to both risk and treatment responses for many neuropsychiatric disorders. The HPC contains discrete classes of neurons with specialized functions, but cell type-specific activity-regulated transcriptional programs are not well characterized. Here, we used single-nucleus RNA-sequencing (snRNA-seq) in a mouse model of acute electroconvulsive seizures (ECS) to identify cell type-specific molecular signatures associated with induced activity in HPC neurons.

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Deconvolution of cell mixtures in "bulk" transcriptomic samples from homogenate human tissue is important for understanding the pathologies of diseases. However, several experimental and computational challenges remain in developing and implementing transcriptomics-based deconvolution approaches, especially those using a single cell/nuclei RNA-seq reference atlas, which are becoming rapidly available across many tissues. Notably, deconvolution algorithms are frequently developed using samples from tissues with similar cell sizes.

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Generation of a molecular neuroanatomical map of the human prefrontal cortex reveals novel spatial domains and cell-cell interactions relevant for psychiatric disease. The molecular organization of the human neocortex has been historically studied in the context of its histological layers. However, emerging spatial transcriptomic technologies have enabled unbiased identification of transcriptionally-defined spatial domains that move beyond classic cytoarchitecture.

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Article Synopsis
  • High-resolution imaging techniques are improving our ability to observe biological systems, but sharing and customizing these large image datasets can be difficult.
  • Samui is a new web-based tool designed for fast and interactive visualization and annotation of these images, allowing users to quickly explore their features.
  • The tool has been tested with images from Vizgen MERFISH and 10x Genomics Visium platforms, and it's available for use with example datasets at https://samuibrowser.com.
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Background: Multispectral fluorescence imaging coupled with linear unmixing is a form of image data collection and analysis that allows for measuring multiple molecular signals in a single biological sample. Multiple fluorescent dyes, each measuring a unique molecule, are simultaneously measured and subsequently "unmixed" to provide a read-out for each molecular signal. This strategy allows for measuring highly multiplexed signals in a single data capture session, such as multiple proteins or RNAs in tissue slices or cultured cells, but can often result in mixed signals and bleed-through problems across dyes.

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  • - The lateral septum (LS) is a critical area in the brain for regulating social novelty, but how it interacts with other brain regions and signaling pathways is not fully understood.
  • - Brain-derived neurotrophic factor (BDNF) and its receptor TrkB play vital roles in social behavior, with most LS GABAergic neurons expressing TrkB, although BDNF itself is not produced in the LS.
  • - Disruption of inputs to LS from the basolateral amygdala (BLA) significantly impairs social novelty recognition, suggesting that BLA-LS projection neurons are essential sources of BDNF that activate TrkB signaling in the LS for managing social behaviors.
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Objective: Posttraumatic stress disorder (PTSD) is a debilitating neuropsychiatric disease that is highly comorbid with major depressive disorder (MDD) and bipolar disorder. The overlap in symptoms is hypothesized to stem from partially shared genetics and underlying neurobiological mechanisms. To delineate conservation between transcriptional patterns across PTSD and MDD, the authors examined gene expression in the human cortex and amygdala in these disorders.

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Background: Spatially-resolved transcriptomics has now enabled the quantification of high-throughput and transcriptome-wide gene expression in intact tissue while also retaining the spatial coordinates. Incorporating the precise spatial mapping of gene activity advances our understanding of intact tissue-specific biological processes. In order to interpret these novel spatial data types, interactive visualization tools are necessary.

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