JOURNAL OF THE CZECH PEDIATRIC SOCIETY AND THE SLOVAK PEDIATRIC SOCIETY

Čes-slov Pediat 2022, 77(6):370-382 | DOI: 10.55095/CSPediatrie2022/066

Inborn errors of amino acid, organic acid metabolism and disorders of the urea cycleKapitoly k atestaci z pediatrie

Tomáš Honzík, Jiří Zeman
Klinika pediatrie a dědičných poruch metabolismu 1. LF UK a VFN, Praha

Introduction: Inborn errors of amino acid (AA), organic acid (OA) metabolism and disorders of the urea cycle (UCD) represent a heterogeneous group of 135 different diseases caused by impaired synthesis, transport or degradation of AA, OA and ammonia. Individual diseases are rare, but the overall incidence in the population is 1: 3000-4000.

Methodology: The work summarizes the clinical, diagnostic and therapeutic aspects of the most common inborn errors of AA, OA metabolism and UCD. Eight diseases are part of laboratory neonatal screening, diagnosis of other IEMs depends on clinical suspicion, determination of ammonia in the blood and rapid indication of selective metabolic screening.

Results: Inborn errors of AA, OA metabolism and UCD are clinically manifested by acute or subacute metabolic disruption with metabolic alkalosis or acidosis and subsequent hepatic, renal and / or cerebral impairment or slowly progressive brain impairment with developmental delay and cognitive decline. The first group includes OA, tyrosinemia type 1, leucinosis and UCD, which are manifested by the accumulat ion of toxic metabolites arising from amino acid degradation. The second group includes phenylketonuria and homocystinuria, which are associated with eye, bone and / or thromboembolic events.

Conclusion: Adequate therapy depends on early diagnosis. Elimination methods are used in patients with acute brain involvement, such as severe hyperammonaemia. In patients with chronic disease, a lifelong low-protein diet supplemented with foods for special medical purposes, vitamin therapy and chaperone therapy supporting the ac tivities of affected enzymes and efforts to block or activate alternative metabolic pathways are used. The number of diseases in which enzyme replacement therapy or liver or kidney transplantation is used is increasing. Trials with gene therapy are underway.

Keywords: inborn errors of metabolism, phenylketonuria, homocystinuria, tyrosinemia, leucinosis, glycine encephalopathy, organic acidurias, urea cycle disorders

Published: December 8, 2022  Show citation

ACS AIP APA ASA Harvard Chicago Chicago Notes IEEE ISO690 MLA NLM Turabian Vancouver
Honzík T, Zeman J. Inborn errors of amino acid, organic acid metabolism and disorders of the urea cycle. Ces-slov Pediat. 2022;77(6):370-382. doi: 10.55095/CSPediatrie2022/066.
Share...
Download citation
  • BibTeX (.bib)
  • Bookends (.ris)
  • EasyBib (.ris)
  • EndNote (.enw)
  • EndNote 8 (.xml)
  • ISI WoS (.isi)
  • Medlars (.medlars)
  • Mendeley (.ris)
  • MODS (.xml)
  • Papers (.ris)
  • RefWorks (.txt)
  • RefManager (.ris)
  • RIS (.ris)
  • MS Word (.xml)
  • Zotero (.ris)
    • Open full article

    References

    1. Honzík T, Kožich V, Pešková K, Votava F. Laboratorní novorozenecký screening. Ces-slov Pediat 2022; 77(1): 12-18. Go to original source...
    2. Saudubray JM, Baumgartner MR, Walter JH. Inborn metabolic diseases: diagnosis and treatment. 6th ed. Heidelberg: Springer 2016: 4-5. Go to original source...
    3. Honzík T, Zeman J, et al. Dědičné poruchy metabolismu v kazuistikách. Praha: Mladá fronta 2016.
    4. Kolářová H, Honzík T. Charakteristické klinické příznaky a laboratorních odchylky dědičných poruch metabolismu. Čes-slov Pediat 2018; 73(6): 348-364.
    5. Honzík T, Zeman J. Výživa u dědičných metabolických poruch. In: Kohout P, et al. Klinická výživa. Praha: Galén 2021: 779-798.
    6. Blau N, Duran M, Gibson KM, et al. Physician's guide to the diagnosis, treatment, and follow-up of inherited metabolic diseases. Heidelberg: Springer 2014. Go to original source...
    7. van Wegberg AMJ, MacDonald A, Ahring K, et al. The complete European guidelines on phenylketonuria: diagnosis and treatment. Orphanet J Rare Dis 2017; 12(1): 162. Go to original source... Go to PubMed...
    8. Zemanova M, Chrastina P, Sebron V, et al. Extremely low birthweight neonates with phenylketonuria require special dietary management. Acta Paediatr 2021; 110(11): 2994-2999. Go to original source... Go to PubMed...
    9. Mayorandan S, Meyer U, Gokcay G, et al. Cross-sectional study of 168 patients with hepatorenal tyrosinemia and implication for clinical practice. Orphanet J Rare Dis 2014; 9: 107. Go to original source... Go to PubMed...
    10. Frazier DM, Allgeier C, Homer C, et al. Nutrition management guideline for maple sirup urine disease: an evidence and consensus-based approach. Mol Genet Metab 2014; 12(3): 210-217. Go to original source... Go to PubMed...
    11. Morris A, Kožich V, Santra S, et al. Guidelines for the diagnosis and management of cystathionine beta-synthase deficiency. J Inherit Metab Dis 2017; 40(1): 49-74. Go to original source... Go to PubMed...
    12. Hoover-Fong JE, Shah S, van Hove JL, et al. Natural history of nonketotic hyperglycinemia in 65 patients. Neurology 2004; 63: 1847-1853. Go to original source... Go to PubMed...
    13. Forny P, Hörster F, Ballhausen D, et al. Guidelines for the diagnosis and management of methylmalonic acidaemia and propionic acidaemia: first revision. J Inherit Metab Dis 2021; 44(3): 566-592. Go to original source... Go to PubMed...
    14. Boy N, Mühlhausen Ch, Maier EM, et al. Proposed recommedations for diagnosing and managing individuals with glutaric aciduria type I: second revision. J Inherit Metab Dis 2007; 30(1): 5-22. Go to PubMed...
    15. Häberle J, Burlina A, Chakrapani A, et al. Suggested guidelines for the diagnosis and management of urea cycle disorders: first revision. J Inherit Metab Dis 2019; 42(6): 1192-1230. Go to original source... Go to PubMed...

    This is an open access article distributed under the terms of the Creative Commons Attribution 4.0 International License (CC BY 4.0), which permits use, distribution, and reproduction in any medium, provided the original publication is properly cited. No use, distribution or reproduction is permitted which does not comply with these terms.


    Return to the content