The homozygous variant c.797G>A/p.(Cys266Tyr) in PISD is associated with a Spondyloepimetaphyseal dysplasia with large epiphyses and disturbed mitochondrial function

Girisha, Katta M.; von Elsner, Leonie; Neethukrishna, Kausthubham; Muranjan, Mamta; Shukla, Anju; Bhavani, Gandham SriLakshmi; Nishimura, Gen; Kutsche, Kerstin; Mortier, Geert

doi:10.1002/HUMU.23693

Title

The homozygous variant c.797G>A/p.(Cys266Tyr) in PISD is associated with a Spondyloepimetaphyseal dysplasia with large epiphyses and disturbed mitochondrial function

Author

Girisha, Katta M.

von Elsner, Leonie

Neethukrishna, Kausthubham

Muranjan, Mamta

Shukla, Anju

Bhavani, Gandham SriLakshmi

Nishimura, Gen

Kutsche, Kerstin

Mortier, Geert

Abstract

Spondyloepimetaphyseal dysplasias (SEMD) are a group of genetically heterogeneous skeletal disorders characterized by abnormal vertebral bodies and epimetaphyseal abnormalities. We investigated two families with a new SEMD type with one proband each. They showed mild facial dysmorphism, flat vertebral bodies (platyspondyly), large epiphyses, metaphyseal dysplasia, and hallux valgus as common clinical features. By trio-exome sequencing, the homozygous missense variant c.797G>A/p.(Cys266Tyr) in PISD was found in both affected individuals. Based on exome data analyses for homozygous regions, the two patients shared a single homozygous block on chromosome 22 including PISD, indicating their remote consanguinity. PISD encodes phosphatidylserine (PS) decarboxylase that is localized in the inner mitochondrial membrane and catalyzes the decarboxylation of PS to phosphatidylethanolamine (PE) in mammalian cells. PE occurs at high abundance in mitochondrial membranes. Patient-derived fibroblasts showed fragmented mitochondrial morphology. Treatment of patient cells with MG-132 or staurosporine to induce activation of the intrinsic apoptosis pathway revealed significantly decreased cell viability with increased caspase-3 and caspase-7 activation. Remarkably, ethanolamine (Etn) supplementation largely restored cell viability and enhanced apoptosis in MG-132-stressed patient cells. Our data demonstrate that the biallelic hypomorphic PISD variant p.(Cys266Tyr) is associated with a novel SEMD form, which may be treatable with Etn administration.

Language

English

Source (journal)

Human mutation. - New York, N.Y.

Publication

New York, N.Y. : 2019

ISSN

1059-7794

DOI

10.1002/HUMU.23693

Volume/pages

40 :3 (2019) , p. 299-309

ISI

000458333600006

Pubmed ID

30488656

Full text (Publisher's DOI)

https://doi.org/10.1002/HUMU.23693

Full text (open access)

https://repository.uantwerpen.be/docman/irua/e6ef85/157478_2019_05_29.pdf

Full text (publisher's version - intranet only)

https://repository.uantwerpen.be/docman/iruaauth/5a5fa6/157478.pdf

Faculty/Department				Faculty of Medicine and Health Sciences

Research group
Project info				GENOMED - Genomics in Medicine.
Publication type				A1 Journal article

Subject				Human medicine

Affiliation				Publications with a UAntwerp address

Web of Science

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Identifier

Creation

01.03.2019

Last edited

12.11.2024

To cite this reference

https://hdl.handle.net/10067/1574780151162165141