HPRT - (Hypoxanthine phosphoribosyltransferase)
Description:
HPRT catalyses the salvage of hypoxanthine to form IMP and guanine to form GMP. The enzyme is assayed in red cell lysates as the formation of IMP from the substrates hypoxanthine and phosphoribosylpyrophosphate using an HPLC based method.
This test is not currently included in the laboratory's UKAS scope of accreditation to ISO15189:2022.
This test is not currently included in the laboratory's UKAS scope of accreditation to ISO15189:2022.
Clinical details:
HPRT deficiency either partial or complete, results in hyperuricaemia due to uric acid overproduction. It is an X-linked disorder. Complete HPRT deficiency results in Lesch-Nyhan Disease (LND), characterised by hyperuricaemia, choreoathetosis, spasticity, and difficulties with speech and feeding. The hallmark of the condition is compulsive self-mutilation and aggression. There is a phenotypic spectrum with residual enzyme activity protecting against some or all neurological abnormalities including self-injurious behaviour. Patients with partial HPRT deficiency may present with gout as teenagers. Biochemical markers for HPRT are purine over production seen as an increased uric acid/creatinine ratio in urine, a raised plasma uric acid, and raised NAD levels in the red cell nucleotide profile.
Reference range:
80 - 130
Units:
nmol/h/mgHb
Department:
Location:
Sample type and Volume required:
4 mL blood EDTA (purple top)
Turnaround time:
1 week
Storage and transport:
Store in fridge, ( don’t freeze)to laboratory within 3 days/1st class pos
Contacts:
Inherited Metabolic Diseases Unit at Blackfriars Hub
07592 502653
Reference Chemistry, 1st Floor Blackfriars Hub
Friars Bridge Court
Blackfriars Road
London
SE1 8NZ
Friars Bridge Court
Blackfriars Road
London
SE1 8NZ
Laboratory:
Last updated: 08/10/2025
