Microalbuminuria prevalence varies with age, sex, and puberty in children with type 1 diabetes followed from diagnosis in a longitudinal study
Microalbuminuria prevalence varies with age, sex, and puberty in children with type 1 diabetes followed from diagnosis in a longitudinal study
OBJECTIVE - The predictive value of microalbuminuria (MA) in children with type 1 diabetes has not been defined. We describe the natural history of MA in a large cohort of children recruited at diagnosis of type 1 diabetes. RESEARCH DESIGN AND METHODS - Between 1985 and 1996, 514 children (279 male) who developed type 1 diabetes before the age of 16 years (91% of those eligible from a region where ascertainment of new cases is 95%) were recruited for a longitudinal study with central annual assessment of HbA(1c) and albumin excretion (three urine samples). Dropout rates have been <1% per year, and 287 children have been followed for >4.5 years. RESULTS - MA (defined as albumin-to-creatinine ratio ≥3.5 and ≥4.0 mg/mmol in boys and girls, respectively) developed in 63 (12.8%) and was persistent in 22 (4.8%) of the subjects. The cumulative probability (based on the Kaplan-Meier method) for developing MA was 40% after 11 years. HbA(1c), was worse in those who developed MA than in others (mean difference ± SEM: 1.1% ± 0.2, P < 0.001). In subjects who had been 5-11 years of age when their diabetes was diagnosed, the appearance of MA was delayed until puberty, whereas of those whose age was <5 years at diagnosis of diabetes, 5 of 11 (45%) developed MA before puberty. The adjusted proportional probability (Cox model) of MA was greater for female subjects (200%), after pubertal onset (310%), and with greater HbA(1c) (36% increase for every 1% increase in HbA(1c)). Despite earlier differences based on age at diagnosis of diabetes (<5, 5-11, and >11 years), the overall cumulative risks in these groups were similar (38 vs. 29 vs. 39%, respectively) after 10 years' duration of diabetes. CONCLUSIONS - Prepubertal duration of diabetes and prepubertal hyperglycemia contribute to the risk of postpubertal MA. The differences in rates of development of MA relating to HbA(1c), sex, and age at diagnosis relative to puberty may have long-term consequences for the risk of subsequent nephropathy and for cardiovascular risk.
495-502
Schultz, Carl J.
11997a8c-f4af-4493-9b50-63077dee5fdc
Konopelska-Bahu, Teresa
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Dalton, R. N.
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Carroll, Tina A.
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Stratton, Irene
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Gale, Edwin A.M.
b819dcfa-423c-4f10-95cc-7e7c2c061b39
Neil, Andrew
bd810992-d0a4-440e-b0d9-a71176e2a385
Dunger, David B.
5b4c17b6-7f65-424f-9d1d-17c4331a4b9c
March 1999
Schultz, Carl J.
11997a8c-f4af-4493-9b50-63077dee5fdc
Konopelska-Bahu, Teresa
a9b9c678-d30d-40b7-ab4d-27e2b3f0c497
Dalton, R. N.
760a08d2-324f-4373-aaca-ca20844ca24f
Carroll, Tina A.
fd995ce2-c75f-4846-9c4d-4695efebe877
Stratton, Irene
772f25b9-23c0-4240-a3f6-1e76b03b172f
Gale, Edwin A.M.
b819dcfa-423c-4f10-95cc-7e7c2c061b39
Neil, Andrew
bd810992-d0a4-440e-b0d9-a71176e2a385
Dunger, David B.
5b4c17b6-7f65-424f-9d1d-17c4331a4b9c
Schultz, Carl J., Konopelska-Bahu, Teresa, Dalton, R. N., Carroll, Tina A., Stratton, Irene, Gale, Edwin A.M., Neil, Andrew and Dunger, David B.
(1999)
Microalbuminuria prevalence varies with age, sex, and puberty in children with type 1 diabetes followed from diagnosis in a longitudinal study.
Diabetes Care, 22 (3), .
(doi:10.2337/diacare.22.3.495).
Abstract
OBJECTIVE - The predictive value of microalbuminuria (MA) in children with type 1 diabetes has not been defined. We describe the natural history of MA in a large cohort of children recruited at diagnosis of type 1 diabetes. RESEARCH DESIGN AND METHODS - Between 1985 and 1996, 514 children (279 male) who developed type 1 diabetes before the age of 16 years (91% of those eligible from a region where ascertainment of new cases is 95%) were recruited for a longitudinal study with central annual assessment of HbA(1c) and albumin excretion (three urine samples). Dropout rates have been <1% per year, and 287 children have been followed for >4.5 years. RESULTS - MA (defined as albumin-to-creatinine ratio ≥3.5 and ≥4.0 mg/mmol in boys and girls, respectively) developed in 63 (12.8%) and was persistent in 22 (4.8%) of the subjects. The cumulative probability (based on the Kaplan-Meier method) for developing MA was 40% after 11 years. HbA(1c), was worse in those who developed MA than in others (mean difference ± SEM: 1.1% ± 0.2, P < 0.001). In subjects who had been 5-11 years of age when their diabetes was diagnosed, the appearance of MA was delayed until puberty, whereas of those whose age was <5 years at diagnosis of diabetes, 5 of 11 (45%) developed MA before puberty. The adjusted proportional probability (Cox model) of MA was greater for female subjects (200%), after pubertal onset (310%), and with greater HbA(1c) (36% increase for every 1% increase in HbA(1c)). Despite earlier differences based on age at diagnosis of diabetes (<5, 5-11, and >11 years), the overall cumulative risks in these groups were similar (38 vs. 29 vs. 39%, respectively) after 10 years' duration of diabetes. CONCLUSIONS - Prepubertal duration of diabetes and prepubertal hyperglycemia contribute to the risk of postpubertal MA. The differences in rates of development of MA relating to HbA(1c), sex, and age at diagnosis relative to puberty may have long-term consequences for the risk of subsequent nephropathy and for cardiovascular risk.
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Published date: March 1999
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Local EPrints ID: 486958
URI: http://eprints.soton.ac.uk/id/eprint/486958
ISSN: 0149-5992
PURE UUID: 1e8caa76-f62f-42a7-95cd-12fc1021588b
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Date deposited: 08 Feb 2024 17:46
Last modified: 18 Mar 2024 04:01
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Author:
Carl J. Schultz
Author:
Teresa Konopelska-Bahu
Author:
R. N. Dalton
Author:
Tina A. Carroll
Author:
Irene Stratton
Author:
Edwin A.M. Gale
Author:
Andrew Neil
Author:
David B. Dunger
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