Michael Brändle

The Cost-Effectiveness of Lifestyle Modification or Metformin in Preventing Type 2 Diabetes in Adults with Impaired Glucose Tolerance

Context The Diabetes Prevention Program (DPP) showed that lifestyle changes or metformin effectively decreased the development of type 2 diabetes in adults with impaired glucose tolerance. The economics of these interventions is important to policymakers. Contribution This cost-effectiveness model estimates that the DPP life-style intervention would cost society about

Glucagon-like peptide-1 receptor imaging for localization of insulinomas.

8800 and metformin would cost about

Glucagon-Like Peptide-1 Versus Somatostatin Receptor Targeting Reveals 2 Distinct Forms of Malignant Insulinomas

29900 per quality-adjusted life-year saved. While lifestyle intervention had a favorable cost-effectiveness profile at any adult age, metformin was not cost-effective after age 65 years. Implications The cost-effectiveness of lifestyle intervention to prevent type 2 diabetes in high-risk individuals is within the range that American society typically finds acceptable for health care interventions. The Editors During the past half century, the number of persons with diagnosed diabetes in the United States has increased 4- to 6-fold (1). Recent large clinical trials from Asia, Europe, and North America have demonstrated that behavioral and medication interventions can delay or prevent the development of type 2 diabetes in persons with impaired glucose tolerance, which is defined by a plasma glucose level between 7.77 mmol/L (140 mg/dL) and 11.04 mmol/L (199 mg/dL) 2 hours after a 75-g oral glucose load (2-6). The Diabetes Prevention Program (DPP) randomly assigned 3234 nondiabetic persons 25 years of age or older with impaired glucose tolerance and fasting glucose levels between 5.27 mmol/L (95 mg/dL) and 6.94 mmol/L (125 mg/dL) to placebo; a lifestyle-modification program with the goals of at least a 7% weight loss and 150 minutes of physical activity per week; or metformin, 850 mg twice daily (4). The mean age of participants was 51 years, and the mean body mass index was 34.0 kg/m2; 68% were women and 45% were members of minority groups (4). The average follow-up was 2.8 years. Compared with the placebo intervention, the lifestyle intervention reduced the incidence of type 2 diabetes by 58% and the metformin intervention reduced the incidence of type 2 diabetes by 31% (4). We have previously described the costs of the DPP interventions and their cost-effectiveness within the 3-year trial period (7, 8). In this analysis, we project the costs, health outcomes, and cost-effectiveness of the DPP lifestyle and metformin interventions over a lifetime relative to the placebo intervention. Methods Clinical Trial The lifestyle intervention involved a healthy, low-calorie, low-fat diet and moderate physical activity, such as brisk walking. The lifestyle intervention was implemented with a 16-lesson core curriculum covering diet, exercise, and behavior modification that was taught by case managers on a one-on-one basis, followed by individual sessions (usually monthly) and group sessions with case managers (9). At the end of the study, 38% of participants in the lifestyle intervention group had lost at least 7% of their initial body weight. The metformin and placebo interventions were initiated at a dosage of 850 mg once a day. At 1 month, the dosage of metformin or placebo was increased to 850 mg twice daily. Case managers reinforced adherence during individual quarterly sessions (10). At the end of the study, 72% of participants in the metformin intervention group and 77% of participants in the placebo intervention group took at least 80% of the prescribed dose. All participants received standard lifestyle recommendations through written information and an annual 20- to 30-minute individual session that emphasized the importance of a healthy lifestyle (10). Simulation Model We assessed the progression from impaired glucose tolerance to onset of diabetes to clinically diagnosed diabetes to diabetes with complications and death by using a lifetime simulation model originally developed by the Centers for Disease Control and Prevention and Research Triangle Institute International. The model has a Markov structure and includes annual transition probabilities between disease states (11). In addition to disease progression, the model tracks costs and quality-adjusted life-years (QALYs). The model has been described elsewhere (11). For our analyses, we modified the model to include data from the DPP on progression, costs, and quality of life associated with impaired glucose tolerance, data from the United Kingdom Prospective Diabetes Study (UKPDS) on diabetes progression and complications, and new data on cost and quality of life associated with diabetes. A technical report describing the model is available. Supplement. Technical Report Disease Progression, Complications, and Comorbid Conditions Impaired Glucose Tolerance to Onset of Type 2 Diabetes We analyzed data from the DPP to assess the annual hazard of diabetes onset in the lifestyle, metformin, and placebo intervention groups. For patients receiving the placebo intervention, the annual hazard of diabetes onset was 10.8 per 100 person-years. At 3 years of follow-up, the risk reductions for the lifestyle and metformin interventions were 55.8% and 29.9%, respectively. In the base-case analysis, we assumed that the lifestyle and metformin interventions would be applied until diabetes onset and that the health and quality-of-life benefits associated with the interventions persisted until diabetes onset. Complications and Comorbid Conditions Associated with Impaired Glucose Tolerance We analyzed data from the DPP and other published sources to assess the prevalence of complications and comorbid conditions in participants with impaired glucose tolerance. At baseline, 6.0% of DPP participants had microalbuminuria and 0.4% had nephropathy. The DPP did not measure peripheral neuropathy, but previous studies found that the prevalence of neuropathy in persons with impaired glucose tolerance was 74% of that in persons with newly diagnosed type 2 diabetes (12) and 12.3% of persons with newly diagnosed type 2 diabetes have neuropathy (13). Therefore, we assumed that at baseline, 8.5% of DPP participants had clinical neuropathy. At baseline, 28% of DPP participants had hypertension, 45% had dyslipidemia, 7% were smokers, 1.1% had a history of cerebrovascular disease, and 2.0% had a history of myocardial infarction. No other complications were present. We assumed that during impaired glucose tolerance, microvascular or neuropathic complications would not progress. We assumed that hypertension and dyslipidemia developed at the rates observed in the DPP. On the basis of 2 large studies (14, 15), we assumed that the incidences of coronary heart disease and cerebrovascular disease in patients with impaired glucose tolerance were 58% and 56%, respectively, of those observed in patients with type 2 diabetes. We further assumed that nondiabetes-related mortality for persons with impaired glucose tolerance was the same as for persons with diabetes (16). Onset of Type 2 Diabetes to Clinical Diagnosis of Type 2 Diabetes In the DPP, participants were tested for diabetes every 6 months; diabetes was diagnosed at onset. In routine clinical practice, type 2 diabetes is estimated to develop 8 to 12 years before its clinical diagnosis (17, 18). In our base-case analysis, we therefore assumed that a 10-year delay occurred between the onset and clinical diagnosis of diabetes. Participants in the DPP had a mean hemoglobin A1c level of 6.4% at the onset of diabetes. Participants in the UKPDS had a mean hemoglobin A1c of 7.1% after a dietary run-in period but before randomization (13). Both DPP placebo participants and UKPDS participants received standard lifestyle recommendations. Accordingly, we assumed that during the 10-year interval between onset and clinical diagnosis of diabetes, patients were treated for type 2 diabetes and that hemoglobin A1c level increased at 0.07% per year from 6.4% to 7.1%. Complications and Comorbid Conditions Associated with Undiagnosed Diabetes We further assumed that between onset and clinical diagnosis of diabetes, microvascular and neuropathic complications progressed slowly, such that by clinical diagnosis of type 2 diabetes, their prevalence reached the level observed in the UKPDS cohort at randomization (13, 19, 20). We assumed that blood pressure and lipid levels progressed as they did in DPP participants and that cardiovascular complications occurred as they would in type 2 diabetes according to risk factors and hemglobin A1c level (21, 22). Clinical Diagnosis of Type 2 Diabetes to Diabetes with Complications and Death We assumed that after clinical diagnosis, all persons with type 2 diabetes received intensive glycemic management as described in the UKPDS (13). We modeled changes in hemoglobin A1c and diabetes treatments to reflect those observed in the UKPDS intensive therapy group. We based risk for retinopathy progression on UKPDS 38 (23), risk for nephropathy progression on UKPDS 64 (20), and risk for neuropathy progression on UKPDS 33 (13). We based risk for cerebrovascular disease on UKPDS 60 (22) and risk for coronary heart disease on UKPDS 56 (21). Costs Costs of Impaired Glucose Tolerance To estimate the total direct medical costs of impaired glucose tolerance, we considered the costs of the DPP interventions (the cost of identifying participants, implementing and maintaining the interventions, and monitoring and treating the side effects of the interventions) and the costs of the medical care outside the DPP (7). In analyses from the perspective of society, we included both direct medical costs and direct nonmedical costs. We did not include indirect costs because they are captured in the assessment of QALYs (24). Table 1 shows the total direct medical costs by treatment group, sex, and year in the DPP (7). Costs were higher in the lifestyle and metformin interventions than in the placebo intervention and higher in women than in men. Costs decreased over time in all 3 intervention groups but after year 1 tended to decrease more in the lifestyle than t

Glucagon-like peptide-1 receptor imaging for the localisation of insulinomas: a prospective multicentre imaging study

CONTEXT The surgical removal of insulinomas is hampered by difficulties to localize it using conventional radiological procedures. Recently these tumors were shown to exhibit a very high density of glucagon-like peptide-1 receptors (GLP-1R) in vitro that may be used as specific targets for in vivo receptor radiolabeling. OBJECTIVE The objective of the study was to test the 111In-labeled GLP-1R agonist 111In-DOTA-exendin-4 in localizing insulinomas using single photon emission computed tomography in combination with computed tomography images. DESIGN This was a prospective open-label investigation. SETTING The study was conducted at three tertiary referral centers in Switzerland. PATIENTS Patients included six consecutive patients with proven clinical and biochemical endogenous hyperinsulinemic hypoglycemia. INTERVENTION (111)In-DOTA-exendin-4 was administered iv at a dose of about 90 MBq (30 microg peptide) over 5 min. Whole-body planar images of the abdomen were performed at 20 min, 4 h, 23 h, 96 h, and up to 168 h after injection. After surgical removal of the insulinomas, GLP-1R expression was assessed in the tumor tissue in vitro by GLP-1R autoradiography. MAIN OUTCOME MEASURE The detection rate of insulinomas was measured. RESULTS In all six cases, the GLP-1R scans successfully detected the insulinomas identified using conventional methods in four cases. By using a gamma-probe intraoperatively, GLP-1R detection permitted a successful surgical removal of the tumors in all patients, diagnosed histopathologically as five pancreatic and one extrapancreatic insulinomas. In vitro GLP-1R autoradiography showed a high density of GLP-1R in all tested insulinomas. CONCLUSION In vivo GLP-1R imaging is an innovative, noninvasive diagnostic approach that successfully localizes small insulinomas pre- and intraoperatively and that may in the future affect the strategy of insulinoma localization.

Assessment of selective arterial calcium stimulation and hepatic venous sampling to localize insulin-secreting tumours.

Glucagon-like peptide-1 (GLP-1) receptor imaging is superior to somatostatin receptor subtype 2 (sst2) imaging in localizing benign insulinomas. Here, the role of GLP-1 and sst2 receptor imaging in the management of malignant insulinoma patients was investigated. Methods: Eleven patients with malignant insulinoma were prospectively included. 111In-[Lys40(Ahx-diethylenetriaminepentaacetic acid [DTPA])NH2]-exendin-4 SPECT/CT, 68Ga- DOTATATE PET/CT, and in vitro receptor autoradiography were performed to assess the receptor status and to evaluate the detection rate. Results: GLP-1 receptor targeting was positive in 4 of 11 patients, and sst2 receptor expression was positive in 8 of 11. In only 1 patient were both receptors expressed. In 1 patient, GLP-1 receptor imaging was the only method that successfully localized the primary tumor in the pancreas. In 3 patients with sst2-expressing tumors, DOTATATE radiotherapy was effectively applied. Conclusion: As opposed to benign insulinomas, malignant insulinomas often lack GLP-1 receptors. Conversely, malignant insulinomas often express sst2, which can be targeted therapeutically.

PITUITARY APOPLEXY: RE-EVALUATION OF RISK FACTORS FOR BLEEDING INTO PITUITARY ADENOMAS AND IMPACT ON OUTCOME

BACKGROUND Small benign insulinomas are hard to localise, leading to difficulties in planning of surgical interventions. We aimed to prospectively assess the insulinoma detection rate of single-photon emission CT in combination with CT (SPECT/CT) with a glucagon-like peptide-1 receptor avid radiotracer, and compare detection rates with conventional CT/MRI techniques. METHODS In our prospective imaging study, we enrolled adults aged 25-81 years at centres in Germany, Switzerland, and the UK. Eligible patients had proven clinical and biochemical endogenous hyperinsulinaemic hypoglycaemia and no evidence for metastatic disease on conventional imaging. CT/MRI imaging was done at referring centres according to standard protocols. At three tertiary nuclear medicine centres, we used whole body planar images and SPECT/CT of the abdomen up to 168 h after injection of (111)In-[Lys40(Ahx-DTPA-(111)In)NH2]-exendin-4 ((111)In-DTPA-exendin-4) to identify insulinomas. Consenting patients underwent surgery and imaging findings were confirmed histologically. FINDINGS Between Oct 1, 2008, and Dec 31, 2011, we recruited 30 patients. All patients underwent (111)In-DTPA-exendin-4 imaging, 25 patients underwent surgery (with histological analysis), and 27 patients were assessed with CT/MRI. (111)In-DTPA-exendin-4 SPECT/CT correctly detected 19 insulinomas and four additional positive lesions (two islet-cell hyperplasia and two uncharacterised lesions) resulting in a positive predictive value of 83% (95% CI 62-94). One true negative (islet-cell hyperplasia) and one false negative (malignant insulinoma) result was identified in separate patients by (111)In-DTPA-exendin-4 SPECT/CT. Seven patients (23%) were referred to surgery on the basis of (111)In-DTPA-exendin-4 imaging alone. For 23 assessable patients, (111)In-DTPA-exendin-4 SPECT/CT had a higher sensitivity (95% [95% CI 74-100]) than did CT/MRI (47% [27-68]; p=0.011). INTERPRETATION (111)In-DTPA-exendin-4 SPECT/CT could provide a good second-line imaging strategy for patients with negative results on initial imaging with CT/MRI. FUNDING Oncosuisse, the Swiss National Science Foundation, and UK Department of Health.

Glycemia and the Quality of Well-Being in Patients with Diabetes

OBJECTIVE Non‐invasive localization modalities such as ultrasound, computed tomography (CT) or magnetic resonance imaging (MRI) often fail to localize insulinomas smaller than 2 cm in diameter. Recent studies have shown that the selective arterial stimulation and hepatic venous sampling (ASVS) technique using intra‐arterial calcium as the insulin secretagogue facilitates the regionalization of such occult insulinomas. This study assesses the sensitivity of ASVS in localizing insulin‐secreting tumours.

Randomized controlled trial of bilateral superficial cervical plexus block versus placebo in thyroid surgery.

OBJECTIVE To assess frequency, symptoms and outcome of pituitary apoplexy (PA) among pituitary adenoma patients, to gain better insight into risk factors for bleeding into pituitary adenoma and to estimate the sequelae of PA by means of a matched control group. METHOD By reviewing charts of 574 patients with pituitary adenoma, we analysed incidence, symptoms and outcome of PA and potential risk factors for developing PA by means of a control group (patients with pituitary adenoma without PA). RESULTS In total, 42 suffered from PA, all had macroadenomas; 30/217 male (14%) and 12/179 female (7%) macroadenoma patients, 32/194 patients with clinically non-functioning (16.5%) and 10/202 with clinically active (5.0%) macroadenoma were affected. Antithrombotic therapy predisposed patients to PA (P=0.026), diabetes mellitus and hypertension did not (P=1.00). Patients with PA and pituitary adenoma patients without PA had similar frequencies of hypopituitarism (45 vs 48%, P>0.05) and visual field defects (38 vs 55%, P>0.05), but ophthalmoplegia was significantly more common (76 vs 5%, P<0.001) in patients with PA. Nearly all patients were treated by surgery; most recovered from ophthalmoplegia, whereas visual function improved only moderately. Endocrine outcome was worse in patients with PA than in patients without PA. CONCLUSIONS Male sex and characteristics of the adenoma itself (especially tumour size and tumour type) rather than patients cardiovascular risk factors such as diabetes and hypertension seem to predispose to PA; antithrombotic therapy may also be important.

Effect of thyroxine replacement on serum IGF‐I, IGFBP‐3 and the acid‐labile subunit in patients with hypothyroidism and hypopituitarism

Objectives: To investigate the cross-sectional relationships among self-reported frequencies of symptomatic hyperglycemia and hypoglycemia, HbA1c, and symptoms in the Quality of Well-Being Self-Administered (QWB-SA), and to examine the associations among these measures of glycemia and health utility scores. Research design and methods: The study group included 1522 patients with diabetes who attended University of Michigan Health System clinics. Published studies were reviewed to identify symptoms in the QWB-SA that might be associated with measures of glycemia. Linear regression analyses were performed to evaluate the strength of the associations among the frequency of self-reported measures of glycemia, QWB-SA symptoms, and QWB-SA-derived health utility scores. Results: Frequency of hyperglycemic symptoms was associated with 3% of the variance in the QWB-SA-derived health utility score in type 1 diabetes and with 5% of the variance in type 2 diabetes. Frequency of hypoglycemic symptoms was not associated with the QWB-SA-derived health utility score in type 1 diabetes but was associated with 1% of the variance in type 2 diabetes. HbA1c levels were not significantly associated with QWB-SA-derived health utility scores. After controlling for age, gender, and complications, frequency of hyperglycemic symptoms was significantly associated with QWB-SA-derived health utility scores in type 1 and type 2 diabetes. Conclusions: Reported frequency of hyperglycemic symptoms is associated with symptoms included in the QWB-SA and with QWB-SA-derived health utility scores. The QWB-SA may be an appropriate measure to assess the health burden of hyperglycemia.

Management of von Hippel-Lindau Disease: An Interdisciplinary Review

Bilateral superficial cervical block during thyroid surgery can reduce postoperative pain but its value is unclear. This randomized clinical trial assessed the efficacy of such regional anaesthesia on postoperative pain after thyroid surgery performed under general anaesthesia.