Abstract

Somatic mutations, present in some but not all cells of the brain, are increasingly implicated in neurological and psychiatric diseases. Somatic mutations that arise during the cell divisions of prenatal brain development are inherited in clonal fashion and can cause neurodevelopmental diseases such as epilepsy and intellectual disability, even when present at low levels of mosaicism. The previous funding period of this grant developed new methods and algorithms to analyze somatic mutations in postmortem human brain, and technologies to sequence the genomes of single neurons, and has shown that each neuron has a unique genome, with hundreds of developmental mutations present at birth, and dozens more mutations being added each year of life. During prenatal life, 2-3 mutations mark each cell division, so that mutations make in principal a permanent record of each cell division. Integrating the analysis of DNA marks of cell lineage with patterns of gene expression that identify the different neural types in human brain potentially now enables the discovery of the first systematic picture of the pattern of cell divisions that generates the cells of the human brain. In this project, we will apply our existing methods to provide several scientific discoveries not otherwise attainable, providing tools of widespread utility to the genetics and neuroscience communities. Our three Specific Aims will be to 1) use simultaneous analysis of DNA mutations and RNA gene expression to map the lineage of neural cell types in cerebral cortex; 2) map clonal patterns across the surface of the human cerebral cortex to see how they relate to functional subdivisions of the cortex; and 3) focus on the analysis of development of human temporal lobe, which is subject to many unique conditions like temporal lobe epilepsy. These data provide three major discoveries which have all been major goals of neuroscience and which are not presently obtainable by other means: 1) the first direct cell lineage data from the adult human brain, 2) a preliminary lineage map connecting neuronal cell classes, and 3) unique insight into temporal lobe development.

Public Health Relevance

Every cell in the human body contains many somatic DNA mutations, and these mutations have an impact of human development, diseases such as cancer and epilepsy, and aging. We have shown that studying these mutations also provide key insights into the development of the human brain, which is a fundamental question of neuroscience. This proposal aims to analyze the somatic mutations in the human brain that occur during development to create a developmental map of the human brain.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
2R01NS032457-22
Application #
10052369
Study Section
Neurogenesis and Cell Fate Study Section (NCF)
Program Officer
Lavaute, Timothy M
Project Start
1994-12-16
Project End
2025-06-30
Budget Start
2020-09-15
Budget End
2021-06-30
Support Year
22
Fiscal Year
2020
Total Cost
Indirect Cost

  Institution

Name
Boston Children's Hospital
Department
Type
DUNS #
076593722
City
Boston
State
MA
Country
United States
Zip Code
02115

  Publications

Sherman, Maxwell A; Barton, Alison R; Lodato, Michael A et al. (2018) PaSD-qc: quality control for single cell whole-genome sequencing data using power spectral density estimation. Nucleic Acids Res 46:e20
Rodin, Rachel E; Walsh, Christopher A (2018) Somatic Mutation in Pediatric Neurological Diseases. Pediatr Neurol 87:20-22
Walsh, Christopher A (2018) Rainer W. Guillery and the genetic analysis of brain development. Eur J Neurosci :
Dou, Yanmei; Gold, Heather D; Luquette, Lovelace J et al. (2018) Detecting Somatic Mutations in Normal Cells. Trends Genet 34:545-557
Johnson, Matthew B; Sun, Xingshen; Kodani, Andrew et al. (2018) Aspm knockout ferret reveals an evolutionary mechanism governing cerebral cortical size. Nature 556:370-375
Lodato, Michael A; Rodin, Rachel E; Bohrson, Craig L et al. (2018) Aging and neurodegeneration are associated with increased mutations in single human neurons. Science 359:555-559
Smith, Richard S; Kenny, Connor J; Ganesh, Vijay et al. (2018) Sodium Channel SCN3A (NaV1.3) Regulation of Human Cerebral Cortical Folding and Oral Motor Development. Neuron 99:905-913.e7
Woodworth, Mollie B; Girskis, Kelly M; Walsh, Christopher A (2017) Building a lineage from single cells: genetic techniques for cell lineage tracking. Nat Rev Genet 18:230-244
Jamuar, Saumya S; Schmitz-Abe, Klaus; D'Gama, Alissa M et al. (2017) Biallelic mutations in human DCC cause developmental split-brain syndrome. Nat Genet 49:606-612
Oaks, Adam W; Zamarbide, Marta; Tambunan, Dimira E et al. (2017) Cc2d1a Loss of Function Disrupts Functional and Morphological Development in Forebrain Neurons Leading to Cognitive and Social Deficits. Cereb Cortex 27:1670-1685

Showing the most recent 10 out of 55 publications