Inborn Errors of Metabolism 229
3
olism and, as a consequence, the reversal of the
breakdown of endogenous protein [3].
Treatment strategies include: (1) natural pro-
tein restriction of precursor amino acids (aiming
to provide safe levels of protein intake [6] ); (2)
maintaining an optimal energy intake; and (3)
use of adjunctive compounds to dispose of toxic
metabolites (e.g. carnitine) or to increase activity
of deficient enzymes (e.g. vitamin B 12 in MMA).
Some inherited metabolic disease centres pre-
scribe precursor-free amino acids to supplement
natural protein intake, although the long-term
value of these supplements remains uncertain. In
MMA and PA, to reduce the production of pro-
pionate, it is also necessary to avoid prolonged
fasting (with the use of overnight tube feeding) in
order to limit oxidation of odd-chain fatty acids
liberated from triglyceride stores during lipoly-
sis. Also in MMA/PA, metronidazole is given to
reduce intestinal production of propionate. Met-
abolic decompensation caused by catabolic stress
(e.g. from vomiting and decreased oral intake) re-
quires prompt intervention with an emergency
regimen.Urea Cycle DisordersUCD are rare defects in waste nitrogen metabo-
lism associated with the breakdown of protein
and other nitrogen-containing molecules [7].
Partial deficiency or total absence of any of the
enzyme activities in the urea cycle (including car-
bamoyl-phosphate synthetase 1, ornithine car-
bamoyltransferase, argininosuccinate synthetase,
argininosuccinate lyase and arginase) causes ac-
cumulation of ammonia and glutamine, and nor-
mal arginine biosynthesis is interrupted. The re-
sulting hyperammonaemia and central nervous
system dysfunction is associated with high mor-
tality and morbidity. Although symptoms mainly
develop in the neonatal period, patients differ in
age at presentation, in the character and severity
Table 1 of symptoms and in their susceptibility to meta-(continued)ConditionIncidenceClassificationSymptoms in untreated patientsTreatmentHCU1 in 344,000Pyridoxine responsiveDislocation of the optic lens, myopiaClassic HCU onlyin classicNon-pyridoxine responsiveand glaucomaLow-methionine diet (classic HCU tolerates aHCUOsteoporosis, scoliosis, thinning andmedian of 230 mg/day)(varies fromlengthening of the long bonesMethionine-freeL-amino acid supplement1 in 65,000 toLearning difficulties, developmental delay,Cystine supplements if blood levels low1 in 900,000)psychiatric problems, EEG abnormalities(dosage titrated according to blood levels)and epilepsyUse of low-protein foods (special and natural) to maintainThromboembolism‘normal’ energy requirementsVitamin/minerals/essential and LC PUFAFolic acid supplementationBetaine supplementationBCKD = Branched-chain α-keto acid dehydrogenase; BCAA = branched-chain amino acids; LC PUFA = long-chain polyunsaturated fattyacids.Koletzko B, et al. (eds): Pediatric Nutrition in Practice. World Rev Nutr Diet. Basel, Karger, 2015, vol 113, pp 226–233
DOI: 10.1159/000360344