UKPDS 26: sulphonylurea failure in non-insulin-dependent diabetic patients over six years
UKPDS 26: sulphonylurea failure in non-insulin-dependent diabetic patients over six years
Patients with Type 2 (non-insulin-dependent) diabetes mellitus (DM) on sulphonylurea therapy convert to insulin progressively as the sulphonylureas 'fail'. The rate of failure and the features of those who fail have been poorly described. To assess secondary failure rates of sulphonylureas, we report on the responses in 1305 patients with newly diagnosed Type 2 DM randomly allocated to therapy with either chlorpropamide or glibenclamide in the UK Prospective Diabetes Study (UKPDS). These patients were initially treated by diet for 3 months and had a fasting plasma glucose >6 mmol l-1; mean age 53 (SD 9) years; BMI 26.8 (SD 5.0) kg m-2; and median fasting plasma glucose 9.1 (7.6-12.5 quartiles) mmol l-1. If their fasting plasma glucose subsequently rose above 15.0 mmol l-1, or they developed hyperglycaemic symptoms, additional hypoglycaemic therapy was given: metformin, ultratard insulin, and soluble insulin as required. By 6 years, 44 % had required additional therapy. Of those randomized to glibenclamide, 48 % required additional therapy by 6 years, compared with 40 % of those allocated to chlorpropamide (p < 0.01). Sixty-one per cent, 39 %, and 23 %, respectively, of patients with fasting plasma glucose ≤10.0 mmol-1, ≤7.8 mmol-1 to <10.0 mmol-1 and <7.8 mmol-1 at randomization required additional therapy (p < 0.001). In the initial 3 years, non-obese subjects (BMI <30 kg m-2) were more likely to require additional therapy than obese patients (BMI ≤30 kgm-2) (43 % vs 53 % at 6 years; p < 0.001). Modelled beta-cell function showed that those with lower function were more likely to fail (p < 0.0001). Thus sulphonylureas fail as a therapeutic agent at rates which are dependent both on the phenotype at presentation and perhaps on the agent used initially. Higher failure rates were found in those with higher glucose concentrations, those who were younger, those with lower beta-cell reserve and those randomized to glibenclamide compared with chlorpropamide.
Chlorpropramide, Glibenclamide, Non-insulin-dependent diabetes, Sulphonylurea therapy
297-303
Matthews, D.R.
e33af8f8-c64f-4d4c-bb9f-f99d99aa513b
Cull, C.A.
ae95233f-ce25-4c32-a5b9-368419e07826
Stratton, I.M.
772f25b9-23c0-4240-a3f6-1e76b03b172f
Holman, R.R.
336fb2f7-edb5-4d65-a7b0-465111cbd047
Turner, R.C.
dd017b41-5773-419b-aeba-c00bebb70c18
April 1998
Matthews, D.R.
e33af8f8-c64f-4d4c-bb9f-f99d99aa513b
Cull, C.A.
ae95233f-ce25-4c32-a5b9-368419e07826
Stratton, I.M.
772f25b9-23c0-4240-a3f6-1e76b03b172f
Holman, R.R.
336fb2f7-edb5-4d65-a7b0-465111cbd047
Turner, R.C.
dd017b41-5773-419b-aeba-c00bebb70c18
Matthews, D.R., Cull, C.A., Stratton, I.M., Holman, R.R. and Turner, R.C.
(1998)
UKPDS 26: sulphonylurea failure in non-insulin-dependent diabetic patients over six years.
Diabetic Medicine, 15 (4), .
(doi:10.1002/(SICI)1096-9136(199804)15:4<297::AID-DIA572>3.0.CO;2-W).
Abstract
Patients with Type 2 (non-insulin-dependent) diabetes mellitus (DM) on sulphonylurea therapy convert to insulin progressively as the sulphonylureas 'fail'. The rate of failure and the features of those who fail have been poorly described. To assess secondary failure rates of sulphonylureas, we report on the responses in 1305 patients with newly diagnosed Type 2 DM randomly allocated to therapy with either chlorpropamide or glibenclamide in the UK Prospective Diabetes Study (UKPDS). These patients were initially treated by diet for 3 months and had a fasting plasma glucose >6 mmol l-1; mean age 53 (SD 9) years; BMI 26.8 (SD 5.0) kg m-2; and median fasting plasma glucose 9.1 (7.6-12.5 quartiles) mmol l-1. If their fasting plasma glucose subsequently rose above 15.0 mmol l-1, or they developed hyperglycaemic symptoms, additional hypoglycaemic therapy was given: metformin, ultratard insulin, and soluble insulin as required. By 6 years, 44 % had required additional therapy. Of those randomized to glibenclamide, 48 % required additional therapy by 6 years, compared with 40 % of those allocated to chlorpropamide (p < 0.01). Sixty-one per cent, 39 %, and 23 %, respectively, of patients with fasting plasma glucose ≤10.0 mmol-1, ≤7.8 mmol-1 to <10.0 mmol-1 and <7.8 mmol-1 at randomization required additional therapy (p < 0.001). In the initial 3 years, non-obese subjects (BMI <30 kg m-2) were more likely to require additional therapy than obese patients (BMI ≤30 kgm-2) (43 % vs 53 % at 6 years; p < 0.001). Modelled beta-cell function showed that those with lower function were more likely to fail (p < 0.0001). Thus sulphonylureas fail as a therapeutic agent at rates which are dependent both on the phenotype at presentation and perhaps on the agent used initially. Higher failure rates were found in those with higher glucose concentrations, those who were younger, those with lower beta-cell reserve and those randomized to glibenclamide compared with chlorpropamide.
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Accepted/In Press date: 15 November 1997
Published date: April 1998
Keywords:
Chlorpropramide, Glibenclamide, Non-insulin-dependent diabetes, Sulphonylurea therapy
Identifiers
Local EPrints ID: 487030
URI: http://eprints.soton.ac.uk/id/eprint/487030
ISSN: 0742-3071
PURE UUID: 0aa302f6-116e-4c64-8377-70cc05cfe529
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Date deposited: 09 Feb 2024 17:47
Last modified: 18 Mar 2024 04:01
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Contributors
Author:
D.R. Matthews
Author:
C.A. Cull
Author:
I.M. Stratton
Author:
R.R. Holman
Author:
R.C. Turner
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