Argininosuccinic aciduria: Recent pathophysiological insights and therapeutic prospects.
Julien BaruteauCarmen Diez-FernandezShaul LernerGiusy RanucciPaul GissenCarlo Dionisi-ViciSandesh NagamaniAyelet ErezJohannes HäberlePublished in: Journal of inherited metabolic disease (2019)
The first patients affected by argininosuccinic aciduria (ASA) were reported 60 years ago. The clinical presentation was initially described as similar to other urea cycle defects, but increasing evidence has shown overtime an atypical systemic phenotype with a paradoxical observation, that is, a higher rate of neurological complications contrasting with a lower rate of hyperammonaemic episodes. The disappointing long-term clinical outcomes of many of the patients have challenged the current standard of care and therapeutic strategy, which aims to normalize plasma ammonia and arginine levels. Interrogations have raised about the benefit of newborn screening or liver transplantation on the neurological phenotype. Over the last decade, novel discoveries enabled by the generation of new transgenic argininosuccinate lyase (ASL)-deficient mouse models have been achieved, such as, a better understanding of ASL and its close interaction with nitric oxide metabolism, ASL physiological role outside the liver, and the pathophysiological role of oxidative/nitrosative stress or excessive arginine treatment. Here, we present a collaborative review, which highlights these recent discoveries and novel emerging concepts about ASL role in human physiology, ASA clinical phenotype and geographic prevalence, limits of current standard of care and newborn screening, pathophysiology of the disease, and emerging novel therapies. We propose recommendations for monitoring of ASA patients. Ongoing research aims to better understand the underlying pathogenic mechanisms of the systemic disease to design novel therapies.
Keyphrases
- nitric oxide
- end stage renal disease
- ejection fraction
- newly diagnosed
- healthcare
- chronic kidney disease
- prognostic factors
- endothelial cells
- risk factors
- patient reported outcomes
- peritoneal dialysis
- cerebral blood flow
- mouse model
- chronic pain
- patient reported
- health insurance
- current status
- smoking cessation
- amino acid