| Literature DB >> 34800363 |
Zheng Yie Yap1, Stephanie Efthymiou2, Simone Seiffert3, Karen Vargas Parra1, Sukyeong Lee4, Alessia Nasca5, Reza Maroofian2, Isabelle Schrauwen6, Manuela Pendziwiat7, Sunhee Jung8, Elizabeth Bhoj9, Pasquale Striano10, Kshitij Mankad11, Barbara Vona12, Sanmati Cuddapah9, Anja Wagner13, Javeria Raza Alvi14, Elham Davoudi-Dehaghani15, Mohammad-Sadegh Fallah16, Srinitya Gannavarapu17, Costanza Lamperti5, Andrea Legati5, Bibi Nazia Murtaza18, Muhammad Shahid Nadeem19, Mujaddad Ur Rehman20, Kolsoum Saeidi21, Vincenzo Salpietro10, Sarah von Spiczak22, Abigail Sandoval1, Sirous Zeinali15, Massimo Zeviani23, Adi Reich24, Cholsoon Jang8, Ingo Helbig25, Tahsin Stefan Barakat26, Daniele Ghezzi27, Suzanne M Leal28, Yvonne Weber29, Henry Houlden2, Wan Hee Yoon30.
Abstract
The 2-oxoglutarate dehydrogenase-like (OGDHL) protein is a rate-limiting enzyme in the Krebs cycle that plays a pivotal role in mitochondrial metabolism. OGDHL expression is restricted mainly to the brain in humans. Here, we report nine individuals from eight unrelated families carrying bi-allelic variants in OGDHL with a range of neurological and neurodevelopmental phenotypes including epilepsy, hearing loss, visual impairment, gait ataxia, microcephaly, and hypoplastic corpus callosum. The variants include three homozygous missense variants (p.Pro852Ala, p.Arg244Trp, and p.Arg299Gly), three compound heterozygous single-nucleotide variants (p.Arg673Gln/p.Val488Val, p.Phe734Ser/p.Ala327Val, and p.Trp220Cys/p.Asp491Val), one homozygous frameshift variant (p.Cys553Leufs∗16), and one homozygous stop-gain variant (p.Arg440Ter). To support the pathogenicity of the variants, we developed a novel CRISPR-Cas9-mediated tissue-specific knockout with cDNA rescue system for dOgdh, the Drosophila ortholog of human OGDHL. Pan-neuronal knockout of dOgdh led to developmental lethality as well as defects in Krebs cycle metabolism, which was fully rescued by expression of wild-type dOgdh. Studies using the Drosophila system indicate that p.Arg673Gln, p.Phe734Ser, and p.Arg299Gly are severe loss-of-function alleles, leading to developmental lethality, whereas p.Pro852Ala, p.Ala327Val, p.Trp220Cys, p.Asp491Val, and p.Arg244Trp are hypomorphic alleles, causing behavioral defects. Transcript analysis from fibroblasts obtained from the individual carrying the synonymous variant (c.1464T>C [p.Val488Val]) in family 2 showed that the synonymous variant affects splicing of exon 11 in OGDHL. Human neuronal cells with OGDHL knockout exhibited defects in mitochondrial respiration, indicating the essential role of OGDHL in mitochondrial metabolism in humans. Together, our data establish that the bi-allelic variants in OGDHL are pathogenic, leading to a Mendelian neurodevelopmental disease in humans.Entities:
Keywords: CRISPR-Cas9 gene editing; DEE; Drosophila; OGDHL; bi-allelic; developmental and epileptic encephalopathy; exome sequencing; mitochondria; neurodevelopmental disease; α-ketoglutarate
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Year: 2021 PMID: 34800363 PMCID: PMC8715183 DOI: 10.1016/j.ajhg.2021.11.003
Source DB: PubMed Journal: Am J Hum Genet ISSN: 0002-9297 Impact factor: 11.043