Impaired protein hydroxylase activity causes replication stress and developmental abnormalities in humans
Sally C. Fletcher, … , Katrin Õunap, Mathew L. Coleman
Sally C. Fletcher, … , Katrin Õunap, Mathew L. Coleman
Published February 16, 2023
Citation Information: J Clin Invest. 2023;133(7):e152784. https://doi.org/10.1172/JCI152784.
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Impaired protein hydroxylase activity causes replication stress and developmental abnormalities in humans

Abstract

Although protein hydroxylation is a relatively poorly characterized posttranslational modification, it has received significant recent attention following seminal work uncovering its role in oxygen sensing and hypoxia biology. Although the fundamental importance of protein hydroxylases in biology is becoming clear, the biochemical targets and cellular functions often remain enigmatic. JMJD5 is a “JmjC-only” protein hydroxylase that is essential for murine embryonic development and viability. However, no germline variants in JmjC-only hydroxylases, including JMJD5, have yet been described that are associated with any human pathology. Here we demonstrate that biallelic germline JMJD5 pathogenic variants are deleterious to JMJD5 mRNA splicing, protein stability, and hydroxylase activity, resulting in a human developmental disorder characterized by severe failure to thrive, intellectual disability, and facial dysmorphism. We show that the underlying cellular phenotype is associated with increased DNA replication stress and that this is critically dependent on the protein hydroxylase activity of JMJD5. This work contributes to our growing understanding of the role and importance of protein hydroxylases in human development and disease.

Authors

Sally C. Fletcher, Charlotte Hall, Tristan J. Kennedy, Sander Pajusalu, Monica H. Wojcik, Uncaar Boora, Chan Li, Kaisa Teele Oja, Eline Hendrix, Christian A.E. Westrip, Regina Andrijes, Sonia K. Piasecka, Mansi Singh, Mohammed E. El-Asrag, Anetta Ptasinska, Vallo Tillmann, Martin R. Higgs, Deanna A. Carere, Andrew D. Beggs, John Pappas, Rachel Rabin, Stephen J. Smerdon, Grant S. Stewart, Katrin Õunap, Mathew L. Coleman

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Figure 1

Heritable JMJD5 pathogenic variants are carried by 2 patients with a novel developmental disorder.

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Heritable JMJD5 pathogenic variants are carried by 2 patients with a nov...
(A) Photographs of 2 affected individuals (Sib4In/CY and Sib5In/CY) demonstrating common phenotypes including relative macrocephaly and facial dysmorphism (also see Supplemental Figure 1 and Supplemental Patient Case Reports). Top: Affected male Sib4In/CY at age 3 years and 3 months (left) and age 10 years (middle and right). Bottom: Affected female Sib5In/CY at ages 2 months (left), 15 months (middle), and 7 years (right). (B) Pedigree of the family. The JMJD5 genotype is annotated for each individual (In, intronic variant; CY, C123Y variant; Mat, maternal; Pat, paternal; Sib, sibling). (C) Graphical representation of the JMJD5 gene structure and the position of the 2 variants. The C123Y variant is localized within exon 2, which encodes most of the N-terminus (Figure 2). The intronic deletion is located between exons 7 and 8.