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ABSTRACT Achieving targeted perturbations of neural activity is essential for dissecting the causal architecture of brain circuits. A crucial challenge in targeted manipulation experiments is the identification ofhigh efficacyperturbation sites whose stimulation exerts desired effects, currently done with costly trial-and-error procedures. Can one predict stimulation effects solely based on observations of the circuit activity, in the absence of perturbation? We answer this question in dissociated neuronal cultures on High-Density Microelectrode Arrays (HD-MEAs), which, compared toin vivopreparations, offer a controllablein vitroplatform that enables precise stimulation and full access to network dynamics. We first reconstruct theperturbome- the full map of network responses to focal electrical stimulation - by sequentially activating individual single sites and quantifying their network-wide effects. The measured perturbome patterns cluster into functional modules, with limited spread across clusters. We then demonstrate that the perturbome can be predicted from spontaneous activity alone. Using short baseline recordings in the absence of perturbations, we estimate Effective Connectivity (EC) and show that it predicts the spatial organization of the perturbome, including spatial clusters and local connectivity. Our results demonstrate that spontaneous dynamics encode the latent causal structure of neural circuits and that EC metrics can serve as effective, model-free proxies for stimulation outcomes. This framework enables data-driven targeting and causal inferencein vitro, with potential applications to more complex preparations such as human iPSC-derived neurons and brain organoids, with implications for both basic research and therapeutic strategies targeting neurological disorders. Significance StatementNeuronal cultures are increasingly used as controllable platforms to study neuronal network dynamics, neuromodulation, and brain-inspired therapies. To fully exploit their potential, we need robust methods to probe and interpret causal interactions. Here, we develop a framework to reconstruct the perturbome—the network-wide map of responses to localized electrical stimulation—and show that it can be predicted from spontaneous activity alone. Using simple, model-free metrics of Effective Connectivity, we reveal that ongoing activity encodes causal structure and provides reliable proxies for stimulation outcomes. This validates EC as a practical measure of causal influence in vitro. Our methodology refines the use of neuronal cultures for brain-on-a-chip approaches, and paves the way for data-driven neuromodulation strategies in human stem cell–derived neurons and brain organoids.
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Multiscale Cloud-Based Pipeline for Neuronal Electrophysiology Analysis and Visualization
SUMMARY Electrophysiology offers a high-resolution method for real-time measurement of neural activity. Longitudinal recordings from high-density microelectrode arrays (HD-MEAs) can be of considerable size for local storage and of substantial complexity for extracting neural features and network dynamics. Analysis is often demanding due to the need for multiple software tools with different runtime dependencies. To address these challenges, we developed an open-source cloud-based pipeline to store, analyze, and visualize neuronal electrophysiology recordings from HD-MEAs. This pipeline is dependency agnostic by utilizing cloud storage, cloud computing resources, and an Internet of Things messaging protocol. We containerized the services and algorithms to serve as scalable and flexible building blocks within the pipeline. In this paper, we applied this pipeline on two types of cultures, cortical organoids andex vivobrain slice recordings to show that this pipeline simplifies the data analysis process and facilitates understanding neuronal activity.
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- PAR ID:
- 10569009
- Publisher / Repository:
- bioRxiv
- Date Published:
- Format(s):
- Medium: X
- Sponsoring Org:
- National Science Foundation
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Accepted Manuscript1.0
- Posted Content:
- https://doi.org/10.1101/2024.11.14.623530
