Minor spliceosome inactivation causes microcephaly, owing to cell cycle defects and death of self-amplifying radial glial cells

Marybeth Baumgartner; Anouk M Olthof; Gabriela S Aquino; Katery C Hyatt; Christopher Lemoine; Kyle Drake; Nikita Sturrock; Nhut Nguyen; Sahar Al Seesi; Rahul N Kanadia

doi:10.1242/dev.166322

Minor spliceosome inactivation causes microcephaly, owing to cell cycle defects and death of self-amplifying radial glial cells

Development. 2018 Aug 28;145(17):dev166322. doi: 10.1242/dev.166322.

Authors

Marybeth Baumgartner^{1

2}, Anouk M Olthof¹, Gabriela S Aquino¹, Katery C Hyatt¹, Christopher Lemoine^{1

3}, Kyle Drake¹, Nikita Sturrock^{1

4}, Nhut Nguyen¹, Sahar Al Seesi⁵, Rahul N Kanadia^{6

7}

Affiliations

¹ Physiology and Neurobiology Department, University of Connecticut, Storrs, CT 06269, USA.
² Connecticut Institute for the Brain and Cognitive Sciences, University of Connecticut, Storrs, CT 06269, USA.
³ College of Medicine, University of Illinois, Chicago, IL 60612, USA.
⁴ Biological and Biomedical Sciences Program, Harvard Medical School, Boston, MA 02115, USA.
⁵ Computer Science Engineering Department, University of Connecticut, Storrs, CT 06269, USA.
⁶ Physiology and Neurobiology Department, University of Connecticut, Storrs, CT 06269, USA rahul.kanadia@uconn.edu.
⁷ Institute of Systems Genomics, University of Connecticut, Storrs, CT 06269, USA.

Abstract

Mutation in minor spliceosome components is linked to the developmental disorder microcephalic osteodysplastic primordial dwarfism type 1 (MOPD1). Here, we inactivated the minor spliceosome in the developing mouse cortex (pallium) by ablating Rnu11, which encodes the crucial minor spliceosome small nuclear RNA (snRNA) U11. Rnu11 conditional knockout mice were born with microcephaly, which was caused by the death of self-amplifying radial glial cells (RGCs), while intermediate progenitor cells and neurons were produced. RNA sequencing suggested that this cell death was mediated by upregulation of p53 (Trp53 - Mouse Genome Informatics) and DNA damage, which were both observed specifically in U11-null RGCs. Moreover, U11 loss caused elevated minor intron retention in genes regulating the cell cycle, which was consistent with fewer RGCs in S-phase and cytokinesis, alongside prolonged metaphase in RGCs. In all, we found that self-amplifying RGCs are the cell type most sensitive to loss of minor splicing. Together, these findings provide a potential explanation of how disruption of minor splicing might cause microcephaly in MOPD1.

Keywords: Cell cycle; Cortical development; Microcephaly; Minor spliceosome; Radial glial cells; U11 snRNA.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Base Sequence
Cell Cycle / genetics*
Cell Death / physiology*
Dwarfism / genetics*
Ependymoglial Cells / metabolism*
Fetal Growth Retardation / genetics*
Mice
Mice, Inbred C57BL
Mice, Knockout
Microcephaly / genetics*
Neural Stem Cells / cytology*
Osteochondrodysplasias / genetics*
RNA Splicing / genetics*
RNA, Small Nuclear / genetics*
Spliceosomes / genetics*
Spliceosomes / metabolism
Tumor Suppressor Protein p53 / biosynthesis

Minor spliceosome inactivation causes microcephaly, owing to cell cycle defects and death of self-amplifying radial glial cells

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