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Endocrine Abstracts (2011) 27 P33

1University of of Sheffield, Sheffield, UK; 2Sheffield Children’s NHS Foundation Trust, Sheffield, UK; 3Sheffield Teaching Hospitals NHS Foundation Trust, Sheffield, UK.


Introduction: A 2009 BSPED survey revealed that 90% use a low dose Synacthen test (LDST) and 44% had noticed increased referrals of asthmatic children prescribed inhaled corticosteroids (ICS). Approximately 21% of UK children have asthma of whom 70% are prescribed ICS (10% at ‘high dose’). There is an increasing need for a simple, less invasive, alternative to the LDST to evaluate their adrenal function. We are developing a non-invasive LDST, with Synacthen administered nasally and cortisol measured in saliva.

Methods: We performed three Synacthen tests on 12 healthy, adult males. On the first visit volunteers received 1 μg i.v. Synacthen, the second and third visits 100 and 25 μg intranasal Synacthen respectively. During a 3 h test 14-paired samples of blood and saliva were taken. All volunteers were dexamethasone suppressed enabling us to measure Synacthen on an ACTH RIA.

Results: We achieved a median AUC0–180 min with 100 μg intranasal Synacthen, 20% of that following a 1 μg i.v. dose, (6% with 25 μg), this gave a bioavailability of 0.2–0.24%. The Cmax was 17.9 and 11 pg/ml respectively compared with 169 pg/ml i.v. Tmax was 17.5 and 10 min respectively compared with 5 min i.v. On analysis of the 1 μg i.v. data we observed considerable variability in mean peak plasma Synacthen (261.6 pg/ml S.D. 104.9). The timing of the peak cortisol varied, occurring at 30 min in 50%. There was no relationship between peak Synacthen and peak cortisol, despite correction for BMI and BSA. None of our participants achieved a cortisol above 450 nmol/l, which we believe is a blunting effect of dexamethasone.

Conclusion: We have shown considerable variability in the 1 μg i.v. LDST. The doses of intranasal Synacthen chosen in our study did not reach bioequivalence with the 1 μg LDST. However the test was well tolerated and easy to administer and so with increased dose holds considerable promise.

Volume 27

39th Meeting of the British Society for Paediatric Endocrinology and Diabetes

British Society for Paediatric Endocrinology and Diabetes 

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