# Myoclonus in Pediatric Metabolic Diseases: Clinical Spectrum, Mechanisms, and Treatable Causes—A Systematic Review

**Authors:** Elżbieta Majewska, Zofia Zdort, Aleksandra Ochocka, Justyna Paprocka

PMC · DOI: 10.3390/metabo16020098 · 2026-01-28

## TL;DR

This paper reviews how myoclonus, a sudden involuntary movement, is a symptom of metabolic diseases in children and highlights treatable causes.

## Contribution

The paper systematically summarizes the clinical spectrum, mechanisms, and treatable causes of metabolic myoclonus in pediatric patients.

## Key findings

- Myoclonus is associated with six categories of inherited metabolic disorders.
- Conditions like GLUT1 deficiency and folate receptor α deficiency are treatable with dietary or pharmacological interventions.
- Metabolic screening is recommended for unexplained myoclonus, especially with developmental delay or systemic issues.

## Abstract

Background: Myoclonus, a sudden brief shock-like involuntary movement, represents a common yet under-recognized manifestation across many inherited metabolic disorders. Although its occurrence has been reported in case series and small cohorts, the overall spectrum, pathophysiological mechanisms, and therapeutic relevance of metabolic myoclonus have not been systematically summarized. Methods: A systematic search of PubMed was conducted for English-language publications from 2014 to 2025 using predefined MeSH terms related to myoclonus, movement disorders, and inborn errors of metabolism. Titles and abstracts were screened independently by three reviewers. After removal of duplicates, 27 articles were included, complemented by 65 additional references addressing individual disorders. Data were organized according to the International Classification of Inherited Metabolic Disorders (ICIMD). Results: Myoclonus was documented across six ICIMD categories, including intermediary metabolism, mitochondrial energy metabolism, lipid metabolism, disorders of complex molecules and organelles, cofactor and mineral metabolism, and metabolic cell signaling disorders. Clinical presentation ranged from isolated jerks to progressive myoclonic epilepsies. Several conditions—such as GLUT1 deficiency, cerebrotendinous xanthomatosis, and folate receptor α deficiency—are treatable through dietary or pharmacological interventions. Conclusions: Recognition of myoclonus as a presenting feature of inherited errors of metabolism (IEMs) is critical for timely diagnosis and treatment. Metabolic screening should be considered in all unexplained cases of myoclonus, particularly when accompanied by developmental delay or systemic abnormalities.

## Linked entities

- **Diseases:** cerebrotendinous xanthomatosis (MONDO:0008948)

## Full-text entities

- **Genes:** CP (ceruloplasmin) [NCBI Gene 1356] {aka AB073614, CP-2}, PIGA (phosphatidylinositol glycan anchor biosynthesis class A) [NCBI Gene 5277] {aka GPI3, MCAHS2, NEDEPH, PIG-A, PNH1}, FOSL1 (FOS like 1, AP-1 transcription factor subunit) [NCBI Gene 8061] {aka FRA, FRA1, fra-1}, NPC1 (NPC intracellular cholesterol transporter 1) [NCBI Gene 4864] {aka NPC, POGZ, SLC65A1}, POLG (DNA polymerase gamma, catalytic subunit) [NCBI Gene 5428] {aka MIRAS, MTDPS4A, MTDPS4B, PEO, POLG1, POLGA}, PCCB (propionyl-CoA carboxylase subunit beta) [NCBI Gene 5096], ALDH5A1 (aldehyde dehydrogenase 5 family member A1) [NCBI Gene 7915] {aka SSADH, SSDH}, PEX13 (peroxisomal biogenesis factor 13) [NCBI Gene 5194] {aka NALD, PBD11A, PBD11B, ZWS}, PCCA (propionyl-CoA carboxylase subunit alpha) [NCBI Gene 5095], PEX1 (peroxisomal biogenesis factor 1) [NCBI Gene 5189] {aka HMLR1, PBD1A, PBD1B, ZWS, ZWS1}, NPC2 (NPC intracellular cholesterol transporter 2) [NCBI Gene 10577] {aka EDDM1, HE1}, ATP7A (ATPase copper transporting alpha) [NCBI Gene 538] {aka DSMAX, HMNX, MK, MNK, SMAX3}, GCDH (glutaryl-CoA dehydrogenase) [NCBI Gene 2639] {aka ACAD5, GCD}, FOLR1 (folate receptor alpha) [NCBI Gene 2348] {aka FBP, FOLR, FR-alpha, FRalpha, NCFTD}, SLC2A1 (solute carrier family 2 member 1) [NCBI Gene 6513] {aka CSE, DYT17, DYT18, DYT9, EIG12, GLUT}, TRNK (tRNA-Lys) [NCBI Gene 4566] {aka MTTK}, PIGN (phosphatidylinositol glycan anchor biosynthesis class N) [NCBI Gene 23556] {aka GPI-ETI, MCAHS, MCAHS1, MCD4, MDC4, PIG-N}, TF (transferrin) [NCBI Gene 7018] {aka HEL-S-71p, PRO1557, PRO2086, TFQTL1}, ALG13 (ALG13 UDP-N-acetylglucosaminyltransferase subunit) [NCBI Gene 79868] {aka CDG1S, CXorf45, DEE36, EIEE36, GLT28D1, MDS031}, PEX19 (peroxisomal biogenesis factor 19) [NCBI Gene 5824] {aka D1S2223E, HK33, PBD12A, PMP1, PMPI, PXF}, CYP27A1 (cytochrome P450 family 27 subfamily A member 1) [NCBI Gene 1593] {aka CP27, CTX, CYP27}, PMM2 (phosphomannomutase 2) [NCBI Gene 5373] {aka CDG1, CDG1a, CDGS, PMI, PMI1, PMM 2}, PEX26 (peroxisomal biogenesis factor 26) [NCBI Gene 55670] {aka PBD7A, PBD7B, PEX26M1T, Pex26pM1T}, ALG11 (ALG11 alpha-1,2-mannosyltransferase) [NCBI Gene 440138] {aka CDG1P, GT8}, NGLY1 (N-glycanase 1) [NCBI Gene 55768] {aka CDDG, CDG1V, PNG-1, PNG1, PNGase}
- **Diseases:** microcephaly (MESH:D008831), stroke (MESH:D020521), retinopathy (MESH:D058437), chronic diarrhea (MESH:D003967), Gaucher disease type III (MESH:D005776), DRD (MESH:C538007), nystagmus (MESH:D009759), dysarthria (MESH:D004401), disorders of creatine (MESH:C535598), dentate (MESH:D002527), lesions (MESH:D009059), gait abnormalities (MESH:D020233), CDG (MESH:D018981), white matter abnormalities (MESH:D056784), leukodystrophy (MESH:D007966), myoclonic, focal, and atypical absence seizures (MESH:D004828), CTX (MESH:D019294), speech and language impairment (MESH:D001072), disorders of branched-chain amino (MESH:D008375), disorders of trace element and metal metabolism (MESH:D008664), gangliosidosis type 1 and 2 (MESH:D012497), blindness (MESH:D001766), disorders (MESH:D009358), NPC (MESH:D052556), storage disorders (MESH:D006432), status epilepticus (MESH:D013226), Wilson disease (MESH:D006527), purine metabolism disorders (MESH:D011686), PED (MESH:C564288), SSADH (MESH:C535803), progressive ataxia (MESH:C580388), fever (MESH:D005334), cerebellar and cortical atrophy (MESH:D002526), Myoclonic seizures (MESH:D012640), sensorineural hearing loss (MESH:D006319), Metabolic Diseases (MESH:D008659), inherited metabolic diseases (MESH:D030342), AHS (MESH:D002549), neurotransmitter-related diseases (MESH:D000077733), neurological decline (MESH:D009461), Glutaric aciduria type I (MESH:C536833), Mitochondrial Disorders (MESH:D028361), autonomic disturbances (MESH:D014832), neocortical dysplasia (MESH:D015792), tendon xanthomas (MESH:D014973), muscle (MESH:D019042), PDE (MESH:C536254), X-linked cobalamin disorder (MESH:C564747), encephalopathic crises (MESH:D013224), tunnel vision (MESH:D014786), sterol metabolism disorders (MESH:C537345), Menkes disease (MESH:D007706), Sleep disturbances (MESH:D012893), autism spectrum disorder (MESH:D000067877), red fibres (MESH:D000071075), dystonia (MESH:D004421), neurodegeneration (MESH:D019636), injury to (MESH:D014947), biotinidase deficiency (MESH:D028921), anxiety (MESH:D001007)
- **Chemicals:** propionic acid (MESH:C029658), 5-formyltetrahydrofolate (MESH:D002955), biperiden (MESH:D001712), phenobarbital (MESH:D010634), cholesterol (MESH:D002784), benzhexol (MESH:D014282), oxysterol (MESH:D000072376), copper (MESH:D003300), noradrenaline (MESH:D009638), GABA (MESH:D005680), miglustat (MESH:C059896), pyridoxine (MESH:D011736), pyruvate (MESH:D019289), alpha-AASA (MESH:C000061), coenzyme Q10 (MESH:C024989), DHPG (MESH:C010117), DOPAC (MESH:D015102), glycosphingolipid (MESH:D006028), homovanillic acid (MESH:D006719), lactate (MESH:D019344), carbidopa (MESH:D002230), arimoclomol (MESH:C486387), sterol (MESH:D013261), carbamazepine (MESH:D002220), Lipid (MESH:D008055), very long-chain fatty acids (MESH:C017364), benserazide (MESH:D001545), selegiline (MESH:D012642), ATP (MESH:D000255), folate (MESH:D005492), perampanel (MESH:C551441), glucose (MESH:D005947), PLP (MESH:D011732), vigabatrin (MESH:D020888), dopamine (MESH:D004298), Vitamin B6 (MESH:D025101), lysine (MESH:D008239), L-carnitine (MESH:D002331), 5-methyltetrahydrofolate (MESH:C005984), cholestanol (MESH:D004083), bile acid (MESH:D001647), levodopa (MESH:D007980), pterins (MESH:D011622), AMPA receptor antagonists (-), fatty acid (MESH:D005227), arginine (MESH:D001120), gamma-hydroxybutyric acid (MESH:C111420), CDCA (MESH:D002635), acylcarnitine (MESH:C116917), copper-histidine (MESH:C098468), valproate (MESH:D014635), amino acid (MESH:D000596), phenytoin (MESH:D010672), catecholamine (MESH:D002395), triheptanoin (MESH:C531010), idebenone (MESH:C036619)
- **Species:** Homo sapiens (human, species) [taxon 9606]
- **Mutations:** A467T, Phe/Tyr, m.8344A > G

## Figures

1 figure with captions in the complete paper: https://tomesphere.com/paper/PMC12942292/full.md

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Source: https://tomesphere.com/paper/PMC12942292