Prognostic relevance of hypoglycemia following an oral glucose challenge for cystic fibrosis–related diabetes
K Radike, K Molz, RW Holl, B Poeter, H Hebestreit… - Diabetes …, 2011 - ncbi.nlm.nih.gov
K Radike, K Molz, RW Holl, B Poeter, H Hebestreit, M Ballmann
Diabetes Care, 2011•ncbi.nlm.nih.govWe retrospectively analyzed data collected between 2001 and 2009 from 1,779 patients
who participated in a longitudinal prospective study on “Early Diagnosis of Diabetes Mellitus
in Patients with Cystic Fibrosis.” All patients were 10 years of age or older and performed
standardized OGTTs (5), at least on an annual basis. OGTT results were categorized
following the World Health Organization guidelines (5). All patients included into the current
analysis (n 5 841) had at least two valid OGTTs each and a normal glucose tolerance to the …
who participated in a longitudinal prospective study on “Early Diagnosis of Diabetes Mellitus
in Patients with Cystic Fibrosis.” All patients were 10 years of age or older and performed
standardized OGTTs (5), at least on an annual basis. OGTT results were categorized
following the World Health Organization guidelines (5). All patients included into the current
analysis (n 5 841) had at least two valid OGTTs each and a normal glucose tolerance to the …
We retrospectively analyzed data collected between 2001 and 2009 from 1,779 patients who participated in a longitudinal prospective study on “Early Diagnosis of Diabetes Mellitus in Patients with Cystic Fibrosis.” All patients were 10 years of age or older and performed standardized OGTTs (5), at least on an annual basis. OGTT results were categorized following the World Health Organization guidelines (5). All patients included into the current analysis (n 5 841) had at least two valid OGTTs each and a normal glucose tolerance to the first challenge. The patients with normal glucose tolerance were divided into two subgroups: one group with an entirely normal, nonhypoglycemic plasma glucose level 2 h after the challenge (3.3–7.7 mmol/L; 60–139 mg/dL) and one group with a hypoglycemic 2-h plasma glucose level (, 3.3 mmol/L;, 60 mg/dL). The groups were compared regarding the incidence of IGT and CFRD at the last available OGTT using χ2 statistics. A hypoglycemic response to the first oral glucose challenge was observed in 53 of the 841 participants (6.3%). There was no difference between patients with an entirely normal, nonhypoglycemic response (n 5 788) and those with a hypoglycemic response to the first OGTT in the incidence of CFRD (10.3 vs. 13.2%) or IGT (12.9 vs. 11.3%) at the last OGTT 3.5 6 1.8 years later. Likewise, groups did not differ in age, sex distribution, BMI, and time interval between first and last OGTT.
The 7% incidence of hypoglycemia observed in our study was lower than the 15% previously reported for CF patients (2). A hypoglycemic response to an OGTT does not indicate a risk for future CFRD or IGT, at least not in the following 3.5 years. This finding is in contrast to our hypothesis. We had expected that a dysregulation of insulin secretion in CF would be responsible for reactive hypoglycemia and also—at least in part—for glucose intolerance and overt diabetes in this disease. Our data indicate that the mechanisms underlying reactive hypoglycemia are different from those involved in glucose intolerance or CFRD in CF.
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