Mapping the transcriptional diversity of genetically and anatomically defined cell populations in the mouse brain

Author:

Sugino Ken1ORCID,Clark Erin2ORCID,Schulmann Anton1,Shima Yasuyuki2,Wang Lihua1,Hunt David L1,Hooks Bryan M1ORCID,Tränkner Dimitri1,Chandrashekar Jayaram1ORCID,Picard Serge1,Lemire Andrew L1,Spruston Nelson1ORCID,Hantman Adam W1,Nelson Sacha B2ORCID

Affiliation:

1. Janelia Research Campus, Ashburn, United States

2. Brandeis University, Waltham, United States

Abstract

Understanding the principles governing neuronal diversity is a fundamental goal for neuroscience. Here, we provide an anatomical and transcriptomic database of nearly 200 genetically identified cell populations. By separately analyzing the robustness and pattern of expression differences across these cell populations, we identify two gene classes contributing distinctly to neuronal diversity. Short homeobox transcription factors distinguish neuronal populations combinatorially, and exhibit extremely low transcriptional noise, enabling highly robust expression differences. Long neuronal effector genes, such as channels and cell adhesion molecules, contribute disproportionately to neuronal diversity, based on their patterns rather than robustness of expression differences. By linking transcriptional identity to genetic strains and anatomical atlases, we provide an extensive resource for further investigation of mouse neuronal cell types.

Funder

Howard Hughes Medical Institute

National Eye Institute

National Institute of Mental Health

National Institute of Neurological Disorders and Stroke

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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