Loss of PYCR2 Causes Neurodegeneration by Increasing Cerebral Glycine Levels via SHMT2

Nathalie Escande-Beillard; Abigail Loh; Sahar N Saleem; Kohei Kanata; Yui Hashimoto; Umut Altunoglu; Artina Metoska; Joanes Grandjean; Fui Mee Ng; Oz Pomp; Nithya Baburajendran; Joyner Wong; Jeffrey Hill; Emmanuel Beillard; Patrick Cozzone; Maha Zaki; Hülya Kayserili; Hiroshi Hamada; Hidetaka Shiratori; Bruno Reversade

doi:10.1016/j.neuron.2020.03.028

Loss of PYCR2 Causes Neurodegeneration by Increasing Cerebral Glycine Levels via SHMT2

Neuron. 2020 Jul 8;107(1):82-94.e6. doi: 10.1016/j.neuron.2020.03.028. Epub 2020 Apr 23.

Authors

Nathalie Escande-Beillard¹, Abigail Loh², Sahar N Saleem³, Kohei Kanata⁴, Yui Hashimoto⁵, Umut Altunoglu⁶, Artina Metoska⁷, Joanes Grandjean⁸, Fui Mee Ng⁹, Oz Pomp², Nithya Baburajendran⁹, Joyner Wong⁹, Jeffrey Hill⁹, Emmanuel Beillard¹⁰, Patrick Cozzone⁸, Maha Zaki¹¹, Hülya Kayserili⁶, Hiroshi Hamada⁴, Hidetaka Shiratori¹², Bruno Reversade¹³

Affiliations

¹ Institute of Medical Biology, Human Genetics and Embryology Laboratory, A(∗)STAR, Singapore 138648, Singapore; Genome Institute of Singapore, A∗STAR, Singapore 138672, Singapore; Department of Medical Genetics, Koç University, School of Medicine, 34010 Istanbul, Turkey. Electronic address: nathalie.escande@reversade.com.
² Institute of Medical Biology, Human Genetics and Embryology Laboratory, A(∗)STAR, Singapore 138648, Singapore; Institute of Molecular and Cellular Biology, A(∗)STAR, Singapore 138673, Singapore.
³ Radiology Department, Kasr Al Ainy Faculty of Medicine - Cairo University, El Manial, Cairo 11956, Egypt.
⁴ Developmental Genetics Group, Graduate School of Frontier Biosciences, Osaka University, Suita, Osaka 565-0871, Japan.
⁵ Division of Life Sciences, Kyoto Sangyo University, Kyoto 603-8555, Japan.
⁶ Department of Medical Genetics, Koç University, School of Medicine, 34010 Istanbul, Turkey.
⁷ Institute of Medical Biology, Human Genetics and Embryology Laboratory, A(∗)STAR, Singapore 138648, Singapore.
⁸ Singapore Bioimaging Consortium, Biomedical Sciences Institutes, A(∗)STAR, Singapore 138667, Singapore.
⁹ Experimental Drug Development Centre, A(∗)STAR, Singapore 138669, Singapore.
¹⁰ Institut Pasteur, 97306 Cayenne, French Guiana.
¹¹ Human Genetics and Genome Research Division, National Research Centre, Cairo 12311, Egypt.
¹² Developmental Genetics Group, Graduate School of Frontier Biosciences, Osaka University, Suita, Osaka 565-0871, Japan; Division of Life Sciences, Kyoto Sangyo University, Kyoto 603-8555, Japan. Electronic address: shiratori@cc.kyoto-su.ac.jp.
¹³ Institute of Medical Biology, Human Genetics and Embryology Laboratory, A(∗)STAR, Singapore 138648, Singapore; Genome Institute of Singapore, A∗STAR, Singapore 138672, Singapore; Institute of Molecular and Cellular Biology, A(∗)STAR, Singapore 138673, Singapore; Department of Medical Genetics, Koç University, School of Medicine, 34010 Istanbul, Turkey; Department of Paediatrics, National University of Singapore, Singapore 119260, Singapore. Electronic address: bruno@reversade.com.

PMID: 32330411
DOI: 10.1016/j.neuron.2020.03.028

Abstract

Patients lacking PYCR2, a mitochondrial enzyme that synthesizes proline, display postnatal degenerative microcephaly with hypomyelination. Here we report the crystal structure of the PYCR2 apo-enzyme and show that a novel germline p.Gly249Val mutation lies at the dimer interface and lowers its enzymatic activity. We find that knocking out Pycr2 in mice phenocopies the human disorder and depletes PYCR1 levels in neural lineages. In situ quantification of neurotransmitters in the brains of PYCR2 mutant mice and patients revealed a signature of encephalopathy driven by excessive cerebral glycine. Mechanistically, we demonstrate that loss of PYCR2 upregulates SHMT2, which is responsible for glycine synthesis. This hyperglycemia could be partially reversed by SHMT2 knockdown, which rescued the axonal beading and neurite lengths of cultured Pycr2 knockout neurons. Our findings identify the glycine metabolic pathway as a possible intervention point to alleviate the neurological symptoms of PYCR2-mutant patients.

Keywords: HLD10; MRS; PYCR1; PYCR2; SHMT2; cerebral glycine; hypomyelination; microcephaly; mouse models; neurodegeneration.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adolescent
Animals
Cerebral Cortex / metabolism*
Cerebral Cortex / pathology
Child, Preschool
Female
Glycine / metabolism*
Glycine Hydroxymethyltransferase / metabolism*
Hereditary Central Nervous System Demyelinating Diseases / genetics
Hereditary Central Nervous System Demyelinating Diseases / metabolism
Hereditary Central Nervous System Demyelinating Diseases / pathology*
Humans
Infant
Male
Mice
Mice, Knockout
Nerve Degeneration / genetics
Nerve Degeneration / metabolism
Nerve Degeneration / pathology
Pedigree
Pyrroline Carboxylate Reductases / deficiency
Pyrroline Carboxylate Reductases / genetics*

Substances

PYCR2 protein, human
Pyrroline Carboxylate Reductases
Glycine Hydroxymethyltransferase
SHMT protein, human
Glycine