A Biallelic Variant of the RNA Exosome GeneEXOSC4Causes Translational Defects Associated with a Neurodevelopmental Disorder

Author:

Fasken Milo B.ORCID,Leung Sara W.,Cureton Lauryn A.ORCID,Al-Awadi Maha,Al-Kindy Adila,Khoshnevis SohailORCID,Ghalei HomaORCID,Al-Maawali AlmundherORCID,Corbett Anita H.ORCID

Abstract

ABSTRACTThe RNA exosome is an evolutionarily conserved complex required for both precise RNA processing and decay. Mutations inEXOSCgenes encoding structural subunits of the complex are linked to several autosomal recessive disorders. Here, we describe a missense allele of theEXOSC4gene, which causes a collection of clinical features in two affected siblings. This missense mutation (NM_019037.3: exon3:c.560T>C), changes a leucine residue within a highly conserved region of EXOSC4 to proline (p.Leu187Pro). The two affected individuals presented with prenatal growth restriction, failure to thrive, global developmental delay, intracerebral and basal ganglia calcifications, and kidney failure. Homozygosity for the damaging variant was identified through exome sequencing and Sanger sequencing confirmed segregation. To explore the functional consequences of this amino acid change, we modeled EXOSC4-L187P in the corresponding budding yeast protein, Rrp41 (Rrp41-L187P). Cells that express Rrp41-L187P as the sole copy of the essential Rrp41 protein show significant growth defects. The steady-state level of both the Rrp41-L187P and the EXOSC4-L187P proteins is significantly decreased compared to control Rrp41/EXOSC4. Consistent with this observation, targets of the RNA exosome accumulate inrrp41-L187Pcells, including the 7S precursor of 5.8S rRNA. Polysome profiles show a significant decrease in translation inrrp41-L187Pcells as compared to control cells with apparent incorporation of 7S pre-rRNA into polysomes. Taken together, this work adds the EXOSC4 subunit of the RNA exosome to the structural subunits of this complex that have been linked to human disease and defines foundational molecular defects that could contribute to the adverse growth phenotypes caused by this novel EXOSC4 pathogenic variant.

Publisher

Cold Spring Harbor Laboratory

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