Prader-Willi Syndrome Clinical Trial
Official title:
Effect of Somatostatin on Ghrelin Concentrations, Food Seeking Behaviour and Weight in Patients With Prader-Willi Syndrome
Excessive weight gain is a cardinal feature of Prader-Willi syndrome (PWS) for which there is presently no effective treatment. It is caused by increased appetite, decreased perception of satiety and obsessive and compulsive behaviour towards food. Ghrelin is a powerful appetite-stimulating hormone. Patients with PWS have markedly elevated ghrelin levels, suggesting that it may be responsible for the increased food intake. The goal of the study is to determine whether treatment with somatostatin (Sandostatin), a hormone that inhibits ghrelin, is an effective treatment for the prevention and treatment of weight excess in patients with PWS.
Prader-Willi Syndrome and Obesity:
Prader-Willi syndrome (PWS) is a genetic disorder occurring in 1/10,000 to 1/15,000 live
births. Clinical characteristics include neonatal and infantile central hypotonia with
feeding problems and poor weight gain followed after 1-3 years by hyperphagia and excessive
weight gain. Patients also have characteristic facial features, short stature (possibly due
to growth hormone [GH] deficiency of hypothalamic origin), hypogonadism, increased pain
threshold, global developmental delay and variable mental retardation.
Obesity is clearly one of the cardinal features of PWS. It can result in tremendous distress
for both the parents and the affected child and is a significant health problem with
complications that include hypertension, sleep apneas and diabetes. More than 1/3 of
patients with PWS weigh more than 200% of their ideal body weight. Obesity is thought to
result mainly from hyperphagia, persistent hunger with increased caloric intake, decreased
perception of satiety and obsessive and compulsive behaviours that are primarily food
related. Decreased physical activity associated with hypotonia and/or decreased energy
expenditure is also thought to play a role in the pathophysiology of obesity.
The treatment of obesity in PWS is very difficult and requires constant involvement of the
parents or caregivers with establishment of rigid structures around the young patient:
increased physical activity, hiding food, locking fridges etc. Recently, studies on the
effects of growth hormone (GH) treatment (now an approved indication in most patients with
PWS in the US irrespective of their GH status) on body composition in PWS have been
performed. While GH, among other favourable effects, significantly improves body composition
(increased lean mass and decreased fat mass), the long-term effects on body mass index are
modest and variable.
Thus, obesity is clearly one of the greatest challenges faced by parents of patients with
PWS and treatment modalities are presently not successful.
Ghrelin:
Ghrelin is a recently discovered peptide that stimulates appetite and GH secretion. Ghrelin
increases with fasting and decreases following a meal, and is thought to play a role in meal
initiation in humans. In obese adult and young patients (without PWS), ghrelin is decreased
compared to control, lean subjects suggesting that it does not play a causal role in the
development of obesity. In contrast, PWS patients are characterized by extremely high
circulating ghrelin levels (3 to 10 times higher compared to controls). The mechanisms
underlying ghrelin increase in PWS are unclear. The gene encoding ghrelin is located on
chromosome 3 in humans while PWS is associated with the functional loss of paternally
expressed genes located on chromosome 15 (most patients affected with PWS present with a
deletion in the area of 15q11-13 [70%] or a uniparental disomy for maternal chromosome 15
[30%]). A logical hypothesis is that these missing genes may be part of a pathway regulating
ghrelin expression.
Thus, the elevated ghrelin concentrations observed in PWS at the very least raise the
possibility that ghrelin may play an etiological role in the food-seeking behaviour reported
in these patients. In support of this hypothesis, a significant correlation between hunger
sensation and ghrelin concentrations has recently been reported in a combined group of 6
lean controls and 7 patients with PWS.
Somatostatin and Somatostatin Analogues:
Somatostatin is a hormone that circulates under 2 main forms: a 14 amino acid peptide
(SST-14, mainly in the brain, including the hypothalamus) and a 28 amino acid peptide
(SST-28, mainly in the gastrointestinal tract). Somatostatin inhibits GH and insulin
secretion. Somatostatin is also a powerful regulator of gastric activity that decreases
gastrin release, acid output and gastric motility.
The somatostatin analogue octreotide (Sandostatin®, Novartis) contains 8 amino acids and is
very similar to SST-14. It is an effective treatment of neonatal hyperinsulinism (a
condition characterized by excessive and inappropriate secretion of insulin that causes
severe hypoglycemia in infants) and acromegaly (a condition characterized by excessive GH
production by the pituitary). Sandostatin LAR® is a recent long-acting analogue of
somatostatin that is used for the treatment of acromegaly and less often in children's
hyperinsulinism.
Sandostatin LAR® therapy may be associated with significant side-effects):
- Reduction of bile production and gallbladder contractility and increased risk of
cholesterol gallstones. However, these tend to resolve either spontaneously when
therapy is discontinued or with ursodiol despite remaining on therapy. Therefore,
gallbladder ultrasound is part of the routine follow-up of all patients receiving
octreotide for prolonged periods.
- Decreased height velocity secondary to inhibition of GH secretion. This effect is
variable in intensity but present and will need to be taken into account in case of
prolonged octreotide treatment. In the proposed study, 12 weeks of octreotide treatment
are not expected to have a significant long-term effect on longitudinal growth.
Octreotide should not interfere with GH action in PWS subjects receiving concomitant
exogenous human GH.
- Glucose intolerance. Prolonged octreotide treatment has been associated with impaired
glucose tolerance secondary to a decrease in insulin secretion. However, when
octreotide treatment results in weight loss, an improvement in glucose tolerance is
observed. Therefore, parameters reflecting glucose tolerance must be followed as part
of Sandostatin LAR® therapy.
Other side effects include nausea, abdominal cramps, diarrhea and flatulence that usually
subside after 2 weeks of treatment.
Effect of Somatostatin Analogues on Ghrelin and Weight Gain:
Somatostatin has been shown to decrease ghrelin concentrations in normal subjects as well as
in patients with PWS and with acromegaly. In nine lean young men, continuous SC infusion of
octreotide (600 microg/24 hours) caused a 50% decrease in ghrelin concentrations. In
patients with PWS, using the dose of 5 microg Sandostatin/kg body weight, SC, three times a
day, Hacqq et al observed a 67% drop in ghrelin concentrations. The study was of short
duration (1 week) but the results suggest that somatostatin may indeed be helpful in
decreasing ghrelin concentrations in patients with PWS. There were no complications. In
adults with acromegaly (aged 25-59 years, mean BMI 28.9 kg/m2), fasting ghrelin
concentrations decreased in all patients (mean 54%, range 30-74) following treatment with
Sandostatin LAR® (10 to 30 mg/4-6 weeks) for 3-29 months. Finally, Lustig et al reported the
effects of daily injections of octreotide for 6 months in a group of children with severe
hypothalamic obesity due to brain tumor treatment and/or cranial irradiation. They observed
that the weight gain in octreotide-treated patients was minimal (+ 1.2 kg/6 mo) compared to
the placebo group (+ 9.2 kg/6 mo). Bile sludging and/or gallstones were observed in 44% of
the patients but resolved with ursodiol therapy. Ghrelin concentrations were not measured in
that study.
Thus, somatostatin analogues cause a marked decrease in ghrelin concentrations in control
subjects as well as in patients with PWS. Whether they are associated with a sustained
decrease in ghrelin concentrations and whether the decrease in ghrelin is associated with a
decrease in appetite is unknown and will be studied in the present project.
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Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double-Blind, Primary Purpose: Treatment
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