Abstract
PurposeGrowth hormone deficiency (GHD) must be confirmed before starting treatment in adults with Prader-Willi syndrome (PWS). Most studies use the growth-hormone-releasing hormone plus arginine (GHRH-arginine) test. No data are available on the glucagon stimulation test (GST) in PWS. We compared the utility of fixed-dose (1 mg) GST versus GHRH-arginine test in diagnosing GHD.MethodsAdults and late adolescents with PWS underwent both tests on separate days. In the GHRH-arginine test, GHD was defined according to body mass index. In the GST, two cutoffs were analyzed: peak GH concentration < 3 ng/mL and < 1 ng/mL. For analyses, patients were divided into two groups according to body weight (≤ 90 kg and > 90 kg).ResultsWe analyzed 34 patients: 22 weighing ≤ 90 kg and 12 weighing > 90 kg. In patients weighing ≤ 90 kg, the two tests were concordant in 16 (72.72%) patients (k = 0.476, p = 0.009 with GST cutoff < 3 ng/mL, and k = 0.450, p = 0.035 with GST cutoff < 1 ng/mL). In patients weighing > 90 kg, the two tests were not concordant with GST cutoff < 3 ng/mL, but were concordant in 11 (91.6%) patients (k = 0.833, p = 0.003) with GST cutoff < 1 ng/mL. GH peaks on the two tests correlated (r = 0.725, p = 0.008).ConclusionFixed-dose (1 mg) GST using a peak GH cutoff of < 3 ng/mL or < 1 ng/mL promises to be useful for screening for GHD in adults and late adolescents with PWS. However, in those weighing > 90 kg, the < 1 ng/mL cutoff seems better. Larger studies are necessary to establish definitive glucagon doses and cutoffs, especially in extremely obese patients.
Highlights
Prader-Willi syndrome (PWS) is the most common syndromic form of obesity, occurring in approximately one in 10,000–30,000 live births, without sex differences in prevalence
We evaluated 22 patients with PWS who weighed ≤ 90 kg [18 adults and 4 late adolescents; 5 male and 17 female; median age, 23.5 y (IQR: 19.7–36.2), range 15–47 y; median body mass index (BMI), 30.7 kg/m2 (IQR: 24.8–34.0)]
We aimed to evaluate the utility of a glucagon stimulation test (GST) using a fixeddose (1 mg) of glucagon administered intramuscularly in diagnosing growth hormone deficiency (GHD) in adults and late adolescents with PWS by comparing the results with those achieved with the GHRHarginine test
Summary
Prader-Willi syndrome (PWS) is the most common syndromic form of obesity, occurring in approximately one in 10,000–30,000 live births, without sex differences in prevalence. PWS is characterized by hypotonia, high adiposity, low lean mass, hypogonadism, and growth hormone deficiency (GHD) [1, 2]. In children with PWS, it is widely accepted that treatment with growth hormone (GH) can be started without provocative tests to demonstrate GHD. GH treatment usually ends when the growth plates close and longitudinal bone growth finishes. After growth and body development, GHD can cause a wide variety of physical and psychological problems that can dramatically worsen quality of life. In early adolescence and adulthood, GH treatment can only be started if GHD is demonstrated by GH provocative tests [3]
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