Evaluating Methods for the Prediction of Cell Type-Specific Enhancers in the Mammalian Cortex

Author:

Johansen Nelson J.ORCID,Kempynck NiklasORCID,Zemke Nathan R.ORCID,Somasundaram SarojaORCID,Winter Seppe DeORCID,Hooper MarcusORCID,Dwivedi DeepanjaliORCID,Lohia RuchiORCID,Wehbe FabienORCID,Li Bocheng,Abaffyová DarinaORCID,Armand Ethan J.ORCID,Man Julie DeORCID,Eksi Eren CanORCID,Hecker NikolaiORCID,Hulselmans GertORCID,Konstantakos VasilisORCID,Mauduit DavidORCID,Mich John K.ORCID,Partel GabrieleORCID,Daigle Tanya L.ORCID,Levi Boaz P.ORCID,Zhang KaiORCID,Tanaka YoshiakiORCID,Gillis JesseORCID,Ting Jonathan T.ORCID,Ben-Simon YoavORCID,Miller JeremyORCID,Ecker Joseph R.ORCID,Ren BingORCID,Aerts SteinORCID,Lein Ed S.ORCID,Tasic BosiljkaORCID,Bakken Trygve E.ORCID

Abstract

SummaryIdentifying cell type-specific enhancers in the brain is critical to building genetic tools for investigating the mammalian brain. Computational methods for functional enhancer prediction have been proposed and validated in the fruit fly and not yet the mammalian brain. We organized the ‘Brain Initiative Cell Census Network (BICCN) Challenge: Predicting Functional Cell Type-Specific Enhancers from Cross-Species Multi-Omics’ to assess machine learning and feature-based methods designed to nominate enhancer DNA sequences to target cell types in the mouse cortex. Methods were evaluated based onin vivovalidation data from hundreds of cortical cell type-specific enhancers that were previously packaged into individual AAV vectors and retro-orbitally injected into mice. We find that open chromatin was a key predictor of functional enhancers, and sequence models improved prediction of non-functional enhancers that can be deprioritized as opposed to pursued forin vivotesting. Sequence models also identified cell type-specific transcription factor codes that can guide designs of in silico enhancers. This community challenge establishes a benchmark for enhancer prioritization algorithms and reveals computational approaches and molecular information that are crucial for the identification of functional enhancers for mammalian cortical cell types. The results of this challenge bring us closer to understanding the complex gene regulatory landscape of the mammalian brain and help us design more efficient genetic tools and potential gene therapies for human neurological diseases.

Publisher

Cold Spring Harbor Laboratory

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