RP58 Represses Transcriptional Programs Linked to Nonneuronal Cell Identity and Glioblastoma Subtypes in Developing Neurons

• Published in: Molecular and cellular biology Vol. 41; no. 7; p. e0052620
• Main Authors: Xiang, Chaomei, Frietze, Karla K., Bi, Yingtao, Li, Yanwen, Dal Pozzo, Valentina, Pal, Sharmistha, Alexander, Noah, Baubet, Valerie, D'Acunto, Victoria, Mason, Christopher E., Davuluri, Ramana V., Dahmane, Nadia
• Format: Journal Article
• Language: English
• Published: United States Taylor & Francis 23.06.2021; American Society for Microbiology
• Subjects: aging; Animals; BTB/POZ; Cell Differentiation - genetics; Cell Movement - genetics; cerebral cortex; Gene Expression Regulation, Developmental - physiology; glioblastoma; Glioblastoma - metabolism; glioma; Mice; microcephaly; neurodegenerative diseases; Neurogenesis - physiology; Neuroglia - metabolism; neuronal differentiation; neuronal identity; Neurons - metabolism; Repressor Proteins - genetics; Repressor Proteins - metabolism; Research Article; RP58; Spotlight; transcription factor; transcriptomics; ZBTB18; ZBTB18; microcephaly; cerebral cortex; glioblastoma; neuronal identity; BTB/POZ; RP58; transcriptomics; glioma; transcription factor, aging, neurodegenerative diseases; neuronal differentiation
• ISSN: 0270-7306; 1098-5549; 1098-5549
• DOI: 10.1128/MCB.00526-20

How mammalian neuronal identity is progressively acquired and reinforced during development is not understood. We have previously shown that loss of RP58 (ZNF238 or ZBTB18), a BTB/POZ-zinc finger-containing transcription factor, in the mouse brain leads to microcephaly, corpus callosum agenesis, and cerebellum hypoplasia and that it is required for normal neuronal differentiation. The transcriptional programs regulated by RP58 during this process are not known. Here, we report for the first time that in embryonic mouse neocortical neurons a complex set of genes normally expressed in other cell types, such as those from mesoderm derivatives, must be actively repressed in vivo and that RP58 is a critical regulator of these repressed transcriptional programs. Importantly, gene set enrichment analysis (GSEA) analyses of these transcriptional programs indicate that repressed genes include distinct sets of genes significantly associated with glioma progression and/or pluripotency. We also demonstrate that reintroducing RP58 in glioma stem cells leads not only to aspects of neuronal differentiation but also to loss of stem cell characteristics, including loss of stem cell markers and decrease in stem cell self-renewal capacities. Thus, RP58 acts as an in vivo master guardian of the neuronal identity transcriptome, and its function may be required to prevent brain disease development, including glioma progression.