ME2 Deficiency Is Associated With Recessive Neurodevelopmental Disorder

Naif A M Almontashiri¹, Essa Alharby¹, Mohammed Saleh², Mohamed Abu-Farha³, Ali Alasmari², Marinella Gebbia^{4

5}, Charlotte Hiesl⁶, Roy W A Peake⁷, Sami Samir Amr^{8

9}, Eckhard Boles⁶, Frederick P Roth^{4

10}, Jehad Abubaker³

Affiliations

¹ Center for Genetics and Inherited Diseases, Taibah University, Almadinah Almunwarah, Saudi Arabia.
² Section of Medical Genetics, Children's Specialist Hospital, King Fahad Medical City, Saudi Arabia.
³ Biochemistry and Molecular Biology Department, Dasman Diabetes Institute, Kuwait City, Kuwait.
⁴ Lunenfeld-Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada.
⁵ Donnelly Centre and Department of Molecular Genetics, University of Toronto, Toronto, Ontario, Canada.
⁶ Institute for Molecular Bioscience, Goethe University, Frankfurt, Germany.
⁷ Department of Laboratory Medicine, Boston Children's Hospital, Boston, Massachusetts, USA.
⁸ Department of Pathology, Brigham and Women's Hospital, Harvard Medical School, Cambridge, Massachusetts, USA.
⁹ Laboratory for Molecular Medicine, Personalized Medicine, Mass General Brigham, Cambridge, Massachusetts, USA.
¹⁰ Department of Computational and Systems Biology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.

PMID: 39401966
DOI: 10.1111/cge.14632

Case Reports

ME2 Deficiency Is Associated With Recessive Neurodevelopmental Disorder

Naif A M Almontashiri et al. Clin Genet. 2025 Feb.

. 2025 Feb;107(2):201-207.

doi: 10.1111/cge.14632. Epub 2024 Oct 14.

Authors

Affiliations

¹ Center for Genetics and Inherited Diseases, Taibah University, Almadinah Almunwarah, Saudi Arabia.
² Section of Medical Genetics, Children's Specialist Hospital, King Fahad Medical City, Saudi Arabia.
³ Biochemistry and Molecular Biology Department, Dasman Diabetes Institute, Kuwait City, Kuwait.
⁴ Lunenfeld-Tanenbaum Research Institute, Mount Sinai Hospital, Toronto, Ontario, Canada.
⁵ Donnelly Centre and Department of Molecular Genetics, University of Toronto, Toronto, Ontario, Canada.
⁶ Institute for Molecular Bioscience, Goethe University, Frankfurt, Germany.
⁷ Department of Laboratory Medicine, Boston Children's Hospital, Boston, Massachusetts, USA.
⁸ Department of Pathology, Brigham and Women's Hospital, Harvard Medical School, Cambridge, Massachusetts, USA.
⁹ Laboratory for Molecular Medicine, Personalized Medicine, Mass General Brigham, Cambridge, Massachusetts, USA.
¹⁰ Department of Computational and Systems Biology, University of Pittsburgh School of Medicine, Pittsburgh, Pennsylvania, USA.

PMID: 39401966
DOI: 10.1111/cge.14632

Abstract

Malate is an important dicarboxylic acid produced from fumarate in the tricarboxylic acid cycle. Deficiencies of fumarate hydrolase (FH) and malate dehydrogenase (MDH), responsible for malate formation and metabolism, respectively, are known to cause recessive forms of neurodevelopmental disorders (NDDs). The malic enzyme isoforms, malic enzyme 1 (ME1) and 2 (ME2), are required for the conversion of malate to pyruvate. To date, there have been no reports linking deficiency of either malic enzyme isoforms to any Mendelian disease in humans. We report a patient presenting with NDD, subtle dysmorphic features, resolved dilated cardiomyopathy, and mild blood lactate elevation. Whole exome sequencing (WES) revealed a homozygous frameshift variant (c.1379_1380delTT, p.Phe460fs*22) in the malic enzyme 2 (ME2) gene resulting in truncated and unstable ME2 protein in vitro. Subsequent deletion of the yeast ortholog of human ME2 (hME2) resulted in growth arrest, which was rescued by overexpression of hME2, strongly supporting an important role of ME2 in mitochondrial function. Our results also support the pathogenicity and candidacy of the ME2 gene and variant in association with NDD. To our knowledge, this is the first report of a Mendelian human disease resulting from a biallelic variant in the ME encoding gene. Future studies are warranted to confirm ME2-associated recessive NDD.

Keywords: ME2; Krebs cycle; NDD; loss of function; malate; recessive.

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References

1. G. Loeber, A. A. Infante, I. Maurer‐Fogy, E. Krystek, and M. B. Dworkin, “Human NAD(+)‐Dependent Mitochondrial Malic Enzyme. cDNA Cloning, Primary Structure, and Expression in Escherichia coli ,” Journal of Biological Chemistry 266 (1991): 3016–3021.
1. R. L. Pongratz, R. G. Kibbey, G. I. Shulman, and G. W. Cline, “Cytosolic and Mitochondrial Malic Enzyme Isoforms Differentially Control Insulin Secretion,” Journal of Biological Chemistry 282 (2007): 200–207.
1. P. Jiang, W. Du, A. Mancuso, K. E. Wellen, and X. Yang, “Reciprocal Regulation of p53 and Malic Enzymes Modulates Metabolism and Senescence,” Nature 493 (2013): 689–693.
1. J.‐Y. Hsieh, K. C. Chen, C. H. Wang, et al., “Suppression of the Human Malic Enzyme 2 Modifies Energy Metabolism and Inhibits Cellular Respiration,” Communications Biology 6 (2023): 548.
1. B. Hassel, “Pyruvate Carboxylation in Neurons,” Journal of Neuroscience Research 66 (2001): 755–762.

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ME2 Deficiency Is Associated With Recessive Neurodevelopmental Disorder

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ME2 Deficiency Is Associated With Recessive Neurodevelopmental Disorder

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