| Autor: |
Aagaard Nolting, Line, Holling, Tess, Nishimura, Gen, Ek, Jakob, Bak, Mads, Ljungberg, Merete, Kutsche, Kerstin, Hove, Hanne |
| Předmět: |
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| Zdroj: |
Clinical Genetics; Sep2024, Vol. 106 Issue 3, p360-366, 7p |
| Abstrakt: |
Biallelic variants in PISD cause a phenotypic spectrum ranging from short stature with spondyloepimetaphyseal dysplasia (SEMD) to a multisystem disorder affecting eyes, ears, bones, and brain. PISD encodes the mitochondrial‐localized enzyme phosphatidylserine decarboxylase. The PISD precursor is self‐cleaved to generate a heteromeric mature enzyme that converts phosphatidylserine to the phospholipid phosphatidylethanolamine. We describe a 17‐year‐old male patient, born to unrelated healthy parents, with disproportionate short stature and SEMD, featuring platyspondyly, prominent epiphyses, and metaphyseal dysplasia. Trio genome sequencing revealed compound heterozygous PISD variants c.569C>T; p.(Ser190Leu) and c.799C>T; p.(His267Tyr) in the patient. Investigation of fibroblasts showed similar levels of the PISD precursor protein in both patient and control cells. However, patient cells had a significantly higher proportion of fragmented mitochondria compared to control cells cultured under basal condition and after treatment with 2‐deoxyglucose that represses glycolysis and stimulates respiration. Structural data from the PISD orthologue in Escherichia coli suggest that the amino acid substitutions Ser190Leu and His267Tyr likely impair PISD's autoprocessing activity and/or phosphatidylethanolamine biosynthesis. Based on the data, we propose that the novel PISD p.(Ser190Leu) and p.(His267Tyr) variants likely act as hypomorphs and underlie the pure skeletal phenotype in the patient. [ABSTRACT FROM AUTHOR] |
| Databáze: |
Complementary Index |
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