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1. High-resolution spatiotemporal analysis of single serotonergic axons in an in vitro system

   https://doi.org/10.3389/fnins.2022.994735  

   Hingorani, Melissa; Viviani, Adele M.; Sanfilippo, Jenna E.; Janušonis, Skirmantas (October 2022, Frontiers in Neuroscience)

   Vertebrate brains have a dual structure, composed of ( i ) axons that can be well-captured with graph-theoretical methods and ( ii ) axons that form a dense matrix in which neurons with precise connections operate. A core part of this matrix is formed by axons (fibers) that store and release 5-hydroxytryptamine (5-HT, serotonin), an ancient neurotransmitter that supports neuroplasticity and has profound implications for mental health. The self-organization of the serotonergic matrix is not well understood, despite recent advances in experimental and theoretical approaches. In particular, individual serotonergic axons produce highly stochastic trajectories, fundamental to the construction of regional fiber densities, but further advances in predictive computer simulations require more accurate experimental information. This study examined single serotonergic axons in culture systems (co-cultures and monolayers), by using a set of complementary high-resolution methods: confocal microscopy, holotomography (refractive index-based live imaging), and super-resolution (STED) microscopy. It shows that serotonergic axon walks in neural tissue may strongly reflect the stochastic geometry of this tissue and it also provides new insights into the morphology and branching properties of serotonergic axons. The proposed experimental platform can support next-generation analyses of the serotonergic matrix, including seamless integration with supercomputing approaches. 

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2. Serotonergic neurons in 3D-hydrogels: Tunable environments to study axon dynamics

   Haiman, Justin H.; Hingorani, Melissa; Dunn, Geneva; Janusonis, S. (November 2022, Abstracts Society for Neuroscience)

   Serotonergic axons (fibers) have a ubiquitous distribution in vertebrate brains, where they form meshworks with well-defined, regionally-specific densities. In humans, perturbations of these densities have been associated with abnormal neural processes, including neuropsychiatric conditions. The self-organization of serotonergic meshworks depends on the cumulative behavior of many serotonergic axons, each one of which has a virtually unpredictable trajectory. In order to bridge the high stochasticity at the microscopic level and the regional stability at the mesoscopic level, we are developing tunable hydrogel systems that can support causal modeling of these processes. These same systems can support future restorative efforts in neural tissue because serotonergic axons are nearly unique in their ability to robustly regenerate in the adult brain. In the study, we extended our research in 2D-primary brainstem cultures (Hingorani et al., 2022) to 3D-hydrogels. Tunable hydrogel scaffolds can closely mimic the mechanical and biochemical properties of actual neural tissue in all three dimensions and are therefore qualitatively different from 2D-environments. However, the integration of these scaffolds with highly sensitive neurons poses unique challenges. As the first step in building a hydrogel-based platform for the bioengineering of serotonergic axons, we studied primary brainstem neurons in several commercially available hydrogel platforms. The viability and dynamics of serotonergic somata and neurites were analyzed at different days in vitro with immunocytochemistry and high-resolution confocal microscopy. In addition, live imaging of neuron growth cones was performed, and the observed dynamics was compared to our extensive database of holotomographic (refractive index-based) recordings in 2D-cultures. The progress and key problems will be discussed. This research was funded by NSF CRCNS (#1822517 and #2112862), NIMH (#MH117488), and the California NanoSystems Institute. 

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3. The Self-Organization of the Brain Serotonergic Matrix: From Stochastic Axon Paths to Regional Densities

   Janusonis, Skirmantas; Vojta, Thomas; Metzler, Ralf; Haiman, Justin H.; Wang, Wei (January 2022, NSF CRCNS PI Meeting)

   The neighborhood of virtually every brain neuron contains thin, meandering axons that release serotonin (5-HT). These axons, also referred to as serotonergic fibers, are present in all vertebrate species (from fish to mammals) and are an essential component of biological neural networks. In the mammalian brain, they create dense meshworks that are macroscopically described by densities. It is not known how these densities arise from the trajectories of individual fibers, each of which resembles a unique random-walk path. Solving this problem will advance our understanding of the fundamental structure of neural tissue, including its plasticity and regeneration. Our interdisciplinary program investigates the stochastic structure of serotonergic fibers, by employing a range of experimental, computational, and theoretical methods. Transgenic mouse models (e.g., Brainbow) and brainstem cell cultures are used with advanced microscopy (3D-confocal imaging, STED super-resolution microscopy, holotomography) to visualize individual serotonergic fibers and their trajectories. Serotonergic fibers are modeled as paths of a superdiffusive stochastic process, with a focus on fractional Brownian motion (FBM). The formation of regional fiber densities is tested with supercomputer modeling in neuroanatomically accurate 2D- and 3D-brain-like shapes. Within the same framework, we are developing the mathematical theory of the reflected, branching, and spatially heterogenous FBM. 

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4. An experimental toolbox for the analysis of single serotonergic axons in the mouse brain

   Mays, Kasie C.; Haiman, Justin H.; Janusonis, Skirmantas. (November 2022, Abstracts Society for Neuroscience)

   The self-organization of the serotonergic matrix in the brain is a key unsolved problem in neuroscience. This matrix is composed of extremely long axons (fibers) that originate in the brainstem, invade nearly all brain regions, and accumulate in remarkably high densities in many of them. Serotonergic fibers possess a number of intriguing properties, including the ability to robustly regenerate in the adult brain, the strongly stochastic trajectories, and the poorly understood but consistent association with neural plasticity. We developed several experimental methods that can be used to capture the individual trajectories of serotonergic fibers in the mouse brain, including regions with high fiber densities. These data are essential for stochastic modeling efforts that currently utilize two different frameworks (a step-wise random walk based on the von Mises-Fisher directional distribution and the superdiffusive fractional Brownian motion). In one approach, we show that serotonergic fibers can be experimentally isolated by using transgenic mice with the inducible Cre (under the Tph2-promoter), crossed with a Cre reporter line. While the overall labeling intensity falls below that of the best constitutive model in the field (Migliarini et al., 2013), the inducible Cre allows for control over how many fibers are labeled in high-density regions, thus facilitating their semi-automated tracing. A particularly powerful approach is based on the Brainbow toolbox (Cai et al., 2013) which can be used to randomly “color-code” individual axons. We have developed the first implementation of Brainbow-tagging in the serotonergic system (based on intracranial AAV-injections) and demonstrate its potential in downstream stochastic analyses. In particular, we show that some apparent branching points are different fibers crossing at distances below the limit of optical resolution (even in high-power confocal imaging). Finally, we demonstrate the feasibility of imaging single serotonergic fibers with CUBIC-based tissue clearing and high-resolution light-sheet microscopy (with a 20X objective). This experimental toolbox, integrated with stochastic modeling, can advance the current understanding of the dynamics, robustness, and plasticity of the brain serotonergic system. This research was funded by NSF CRCNS (#1822517 and #2112862), NIMH (#MH117488), and the California NanoSystems Institute. 

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5. Qualitative Observations of Transgenically Individualized Serotonergic Fibers in the Mouse Telencephalon

   https://doi.org/10.1101/2023.11.25.568688  

   Haiman, Justin H; Mays, Kasie C; Roostaeyan, Helen A; Elyasi, Nasim; Janušonis, Skirmantas (November 2023, bioRxiv)

   ABSTRACT The matrix of serotonergic axons (fibers) is a constant feature of neural tissue in vertebrate brains. Its fundamental role appears to be associated with the spatiotemporal control of neuroplasticity. The densities of serotonergic fibers vary across brain regions, but their development and maintenance remain poorly understood. A specific fiber concentration is achieved as the result of the dynamics of a large number of individual fibers, each of which can make trajectory decisions independently of other fibers. Bridging these processes, operating on very different spatial scales, remains a challenge in neuroscience. The study provides the first qualitative description of individually-tagged serotonergic axons in four selected telencephalic regions (cortical and subcortical) of the mouse brain. Based on our previous implementation of the Brainbow toolbox in this system, serotonergic fibers were labeled with random intensity combinations of three fluorophores and imaged with high-resolution confocal microscopy. All examined regions contained serotonergic fibers of diverse identities and morphologies, often traveling in close proximity to one another. Some fibers transitioned among several morphologies in the same imaged volume. High fiber densities appeared to be associated with highly tortuous fiber segments produced by some individual fibers. This study supports efforts to predictively model the self-organization of the serotonergic matrix in all vertebrates, including regenerative processes in the adult human brain. 

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