Homozygous variants in <i>pyrroline‐5‐carboxylate reductase 2</i> (<i>PYCR2</i>) in patients with progressive microcephaly and hypomyelinating leukodystrophy

Meng, Linyan; Donti, Taraka; Xia, Fan; Niu, Zhiyv; Shamsi, Aisha Al; Hertecant, Jozef; Al-Jasmi, Fatma; Gibson, James B.; Nagakura, Honey; Zhang, Jing; He, Weimin; Eng, Christine M.; Yang, Yaping; Elsea, Sarah H.

doi:10.1002/ajmg.a.38049

Cited by 22 publications

(28 citation statements)

References 25 publications

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“…Hypomyelinating leucodystrophies (HLD) are clinically overlapping, genetically heterogeneous disorders. Homozygous variants in the PYCR2 gene (pyrroline-5-carboxylase reductase 2) cause HLD10 [1,2]: failure to thrive, microcephaly, dysmorphisms, progressive psychomotor disability, axial hypotonia with limb spasticity, death within the first decade [3].…”

Section: Dear Editormentioning

confidence: 99%

Prolonged survival in a patient with a novel pyrroline‐5‐carboxylase reductase 2 genetic variant

Spagnoli

Pavlidis

Salerno

et al. 2019

Euro J of Neurology

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Section: Dear Editormentioning

confidence: 99%

Prolonged survival in a patient with a novel pyrroline‐5‐carboxylase reductase 2 genetic variant

Spagnoli

Pavlidis

Salerno

et al. 2019

Euro J of Neurology

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“…This is yet another illustrative example of phenotype expansion. PYCR2 , in turn, which is a mitochondrial enzyme that catalyzes the final step of proline biosynthesis and reduces pyrroline-5-carboxylate (P5C) to L-proline, was found to be involved in the development of hypomyelinating leukodystrophy 10 [ 133 ].…”

Section: Introduction: Advances In the Field Of Rare Diseases Reachedmentioning

confidence: 99%

NGS Technologies as a Turning Point in Rare Disease Research , Diagnosis and Treatment

Fernández–Marmiesse

Gouveia

Couce

2018

CMC

129

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Approximately 25-50 million Americans, 30 million Europeans, and 8% of the Aus-tralian population have a rare disease. Rare diseases are thus a common problem for clini-cians and account for enormous healthcare costs worldwide due to the difficulty of establish-ing a specific diagnosis. In this article, we review the milestones achieved in our understanding of rare diseases since the emergence of next-generation sequencing (NGS) technologies and analyze how these advances have influenced research and diagnosis. The first half of this review describes how NGS has changed diagnostic workflows and provided an unprecedent-ed, simple way of discovering novel disease-associated genes. We focus particularly on meta-bolic and neurodevelopmental disorders. NGS has enabled cheap and rapid genetic diagnosis, highlighted the relevance of mosaic and de novo mutations, brought to light the wide pheno-typic spectrum of most genes, detected digenic inheritance or the presence of more than one rare disease in the same patient, and paved the way for promising new therapies. In the sec-ond part of the review, we look at the limitations and challenges of NGS, including determina-tion of variant causality, the loss of variants in coding and non-coding regions, and the detec-tion of somatic mosaicism variants and epigenetic mutations, and discuss how these can be overcome in the near future.

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“…The PYCR2 p.Arg266* variant has been reported in the five nonrelated Egyptian families and a Moroccan family. 4,5 This variant could be a founder variant in the north African population.…”

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confidence: 99%

“…We listed demographics, birth history, detailed clinical features including dysmorphic features, skeletal and ophthalmological features of 25 patients with pyrroline-5-carboxylate reductase 2 deficiency in Supplemental Table 1. [3][4][5][6] Twelve PYCR2 variants in 18 families were identified and 7 of them (58%) were missense and 5 of them (42%) were truncating. Eight patients had a homozygous known p.Arg266* variant in PYCR2.…”

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confidence: 99%

“…Pyrroline-5-carboxylate reductase 2 deficiency is classified as hypomyelinating leukodystrophy-10 (OMIM#616420) by Nakayama et al 3 Delayed myelination, demyelination, cerebral atrophy, thin corpus callosum, and cerebellar atrophy in brain MRI were also reported in patients. [4][5][6] Hypomyelination and delayed myelination have a similar appearance on a single MRI. The diagnosis of hypomyelination requires another MRI at least 6 months apart from the first MRI to see if myelin content has been increasing.…”

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confidence: 99%

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Pyrroline-5-Carboxylate Reductase 2 Deficiency: A New Case and Review of the Literature

Afroze

Mercimek‐Andrews

2020

Can. J. Neurol. Sci.

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Pyrroline-5-carboxylate reductase 2 (EC 1.5.1.2) is involved in the endogenous proline synthesis from glutamate and pyrroline-5-carboxylate. 1,2 Its deficiency (MIM#616420) is caused by biallelic variants in PYCR2. Proline is an important amino acid for central nervous system and connective tissues. 2 Less than 30 patients have been reported in the literature. 3-6 The clinical features include global developmental delay, acquired microcephaly, movement disorder, seizures, and failure to thrive. 3-6 We report a new patient with a known pathogenic homozygous PYCR2 variant who presented with early infantile onset severe global developmental delay, acquired microcephaly, failure to thrive, and delayed myelination in brain magnetic resonance imaging (MRI). Additionally, we summarized all patients published in the literature for their phenotype and genotype in this case report. This 2-year 2-month-old girl was born to healthy consanguineous Egyptian parents. The pregnancy was remarkable for maternal hypothyroidism and thyroid hormone treatment. She was delivered by an elective caesarian section at 37 weeks of gestation. Birth weight was at the 3rd percentile. Her apgars were 9 and 10 at 1 and 5 minutes, respectively. She was formula-fed due to lack of breast milk production. There was persistent vomiting and failure to thrive from the first few months of life. She was started on oral ranitidine at 4 months of age and vomiting was improved, but not failure to thrive. Developmental delay was noted from the first few months of age. She had her first generalized tonic seizure lasting 1 minute at the age of 7 months. Her electroencephalography (EEG) showed intermittent diffuse 2-3 Hz delta slowing indicating cortical encephalopathy with no epileptogenic discharges at the age of 8 months. She underwent video EEG recording, which showed four brief myoclonic jerks during drowsiness and wakefulness with generalized 2.5-3 Hz spike-and polyspike-and-wave complexes. There was intermittent sharply contoured slow-wave activity over bilateral temporal head region during sleep. She was started on levetiracetam. At the age of 18 months, she was attempting to reach objects, roll from prone to supine, and was babbling. She did not achieve unsupported sitting or acquired any words at the age of 26 months. Her weight, height, and head circumference were below the 3rd percentile. She had full eyebrows, upslanting palpebral fissures, long eyelashes, bulbous nasal tip, absent antihelix bilaterally and plagiocephaly. She had central hypotonia. Muscle stretch reflexes were +2 and symmetrical. Chromosomal microarray, ammonia, lactate, acylcarnitine profile, plasma amino acids, total and free carnitine, total homocysteine, very long chain fatty acids, transferrin isoelectric focusing, urine organic acids, urine oligosaccharides and urine Hmz c.751C>T (p.Arg251Cys) in PYCR2 4 b /7.6 3 GDD, nonambulatory, dysmorphic features, microcephaly, FTT, muscle wasting Hypomyelination, thin corpus callosum, thin brain stem Hmz c.751C>T (p.Arg251Cys) in PYCR2...

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Homozygous variants in pyrroline‐5‐carboxylate reductase 2 (PYCR2) in patients with progressive microcephaly and hypomyelinating leukodystrophy

Cited by 22 publications

References 25 publications

Prolonged survival in a patient with a novel pyrroline‐5‐carboxylase reductase 2 genetic variant

Prolonged survival in a patient with a novel pyrroline‐5‐carboxylase reductase 2 genetic variant

NGS Technologies as a Turning Point in Rare Disease Research , Diagnosis and Treatment

Pyrroline-5-Carboxylate Reductase 2 Deficiency: A New Case and Review of the Literature

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