| Literature DB >> 28126843 |
Alba Redo Riveiro1,2, Luca Mariani1,2, Emily Malmberg1,2, Pier Giorgio Amendola1,2, Juhani Peltonen3, Garry Wong4, Anna Elisabetta Salcini5,2.
Abstract
Components of the KDM7 family of histone demethylases are implicated in neuronal development and one member, PHF8, is often found to be mutated in cases of X-linked mental retardation. However, how PHF8 regulates neurodevelopmental processes and contributes to the disease is still largely unknown. Here, we show that the catalytic activity of a PHF8 homolog in Caenorhabditis elegans, JMJD-1.2, is required non-cell-autonomously for proper axon guidance. Loss of JMJD-1.2 dysregulates transcription of the Hedgehog-related genes wrt-8 and grl-16, the overexpression of which is sufficient to induce the axonal defects. Deficiency of either wrt-8 or grl-16, or reduced expression of homologs of genes promoting Hedgehog signaling, restores correct axon guidance in jmjd-1.2 mutants. Genetic and overexpression data indicate that Hedgehog-related genes act on axon guidance through actin remodelers. Thus, our study highlights a novel function of jmjd-1.2 in axon guidance that might be relevant for the onset of X-linked mental retardation and provides compelling evidence of a conserved function of the Hedgehog pathway in C. elegans axon migration.Entities:
Keywords: Axon guidance; C. elegans; Epigenetics; Hedgehog signaling; Histone demethylase; Neuronal development
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Year: 2017 PMID: 28126843 DOI: 10.1242/dev.142695
Source DB: PubMed Journal: Development ISSN: 0950-1991 Impact factor: 6.868