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Diabetologia

Erschienen in:

01.10.2003 | Article

Three generations of autoimmune diabetes: an extended family study

verfasst von: I. F. Douek, K. M. Gillespie, R. J. Dix, P. J. Bingley, Prof. E. A. M. Gale

Erschienen in: Diabetologia | Ausgabe 10/2003

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Abstract

Aims/hypothesis

One in four children with Type 1 diabetes in a population-based family study has an affected grandparent. We set out to study the clinical and immune features of diabetes in the grandparents' generation, and to examine sharing of HLA class II susceptibility haplotypes between grandparent and grandchild.

Methods

Of 5855 grandparents in the Bart's-Oxford family study, 428 (7.3%) were known to have diabetes. Clinical data and samples were collected from 115 of 213 surviving affected grandparents and from 219 unaffected grandparents within the same families. Samples were tested for ICA and autoantibodies to GAD and IA-2, and typed for HLA-DRB1-DQA1-DQB1. Transmission of HLA class II haplotype from affected and unaffected grandparents to the diabetic proband was compared.

Results

Of 115 affected grandparents studied, the median age at diagnosis was 61 years and at analysis was 73 years; 70% were diet or tablet treated and 30% were on insulin. One or more islet autoantibodies were found in 26% and 66% had one or both of the high risk HLA class II susceptibility haplotypes DRB1*03-DQA1*0501-DQB1*0201 or DRB1*04-DQA1*0301-DQB1*0302. In 79 informative families the HLA class II haplotype of the affected grandparent was transmitted to the proband more frequently than expected overall (59%, p=0.02), and in the insulin-treated subgroups (65%, p=0.03).

Conclusion/interpretation

A total of 7.3% of grandparents reported a clinical diagnosis of diabetes and 2.2% had features of Type 1 diabetes. Genetic susceptibility was shared between grandparents with diabetes and their affected grandchildren. Diabetes in the grandparents of children with Type 1 diabetes often has an autoimmune basis, even when it presents late in life and does not require insulin treatment.

Alberti KGMM, Zimmet PZ (1998) Definition, diagnosis and classification of diabetes mellitus and its complications part 1: diagnosis and classification of diabetes mellitus. Provisional report of a WHO consultation. Diabet Med 15:539–553PubMed

Douek IF, Gillespie KM, Bingley PJ, Gale EAM (2002) Diabetes in the parents of children with type 1 diabetes. Diabetologia 45:495–501CrossRefPubMed

Onkamo P, Väänänen S, Karvonen M, Tuomilehto J (1999) Worldwide increase in incidence of Type 1 diabetes—the analysis of the data on published incidence trends. Diabetologia 42:1395–1403PubMed

EURODIAB ACE Study Group (2000) Variation and trends in incidence of childhood diabetes in europe. Lancet 355:873–876PubMed

Fagot-Campagna A, Narayan KMV, Imperatore G (2001) Type 2 diabetes in children. BMJ 322:377–378CrossRefPubMed

Bingley PJ, Gale EAM (1989) Incidence of insulin dependent diabetes in England: a study in the Oxford region, 1985–1986. BMJ 298:558–560PubMed

Bingley PJ, Bonifacio E, Williams AJK, Genovese S, Bottazzo GF, Gale EAM (1997) Prediction of IDDM in the General Population. Strategies based on combinations of autoantibody markers. Diabetes 46:1701–1710PubMed

Verge CF, Stenger D, Bonifacio E et al. (1998) Combined use of autoantibodies (IA-2 autoantibody, GAD autoantibody, insulin autoantibody, cytoplasmic islet cell antibodies) in type 1 diabetes. Combinatorial islet autoantibody workshop. Diabetes 47:1857–1866PubMed

Gillespie KM, Valovin SJ, Saunby J et al. (2000) HLA class II typing of whole genome amplified mouth swab DNA. Tissue Antigens 56:530–538CrossRefPubMed

10.

Bunce M, O'Neill CM, Barnado MCNM, Krausa P, Morris PJ, Welsh KI (1995) Phototyping: comprehensive DNA typing for HLA-A, B, C, DRB1, DRB3, DRB4, DRB5 and DQB1 by PCR with 144 primer mixes utilising sequence-specific primers (PCR-SSP). Tissue Antigens 46:355–367PubMed

11.

Lawrence JM, Bennett P, Young A, Robinson AM (2001) Screening for diabetes in general practice: cross sectional population study. BMJ 323:548–551CrossRefPubMed

12.

Croxson SC, Burden AC, Bodington M, Botha JL (1991) The prevalence of diabetes in elderly people. Diabet Med 8:28–31PubMed

13.

Kilpatrick ES, Maylor PW, Keevil BG (1998) Biological variance of glycated hemoglobin. Diabetes Care 21:261–264PubMed

14.

Gatling W, Budd S, Walters D, Mullee MA, Goddard JR, Hill RD (1998) Evidence of an increasing prevalence of diagnosed diabetes mellitus in the Poole area from 1983 to 1996. Diabet Med 15:1015–1021CrossRefPubMed

15.

Morris AD, Boyle DIR, MacAlpine R et al. (1997) The diabetes audit and research in Tayside Scotland (DARTS) study: electronic record linkage to create a diabetes register. BMJ 315:524–528PubMed

16.

Verge CF, Howard NJ, Rowley MJ et al. (1994) Anti-glutamate decarboxylase and other antibodies at the onset of childhood IDDM: a population based study. Diabetologia 37:1113–1120PubMed

17.

Vandewalle CL, Falorni A, Svanholm S et al. (1995) High diagnostic sensitivity of glutamate decarboxylase autoantibodies in insulin-dependent diabetes mellitus with clinical onset between age 20 and 40 years. J Clin Endocrinol Metab 80:846–851

18.

Gorus FK, Goubert P, Semakula C et al. (1997) IA-2-autoantibodies complement GAD₆₅-autoantibodies in new-onset IDDM patients and help predict impending diabetes in their siblings. Diabetologia 40:95–99PubMed

19.

Li H, Isomaa B, Taskinen MR, Groop L, Tuomi T (2000) Consequences of a family history of type 1 and type 2 diabetes on the phenotype of patients with type 2 diabetes. Diabetes Care 23:589–594PubMed

20.

Savola K, Sabbah E, Kulmala P, Vähäsalo P, Ilonen J, Knip M (1998) Autoantibodies associated with type 1 diabetes mellitus persist after diagnosis in children. Diabetologia 41:1293–1297PubMed

21.

Decochez K, Tits J, Coolens JL et al. (2000) High frequency of persisting or increasing islet-specific autoantibody levels after diagnosis of type 1 diabetes presenting before 40 years of age. Diabetes Care 23:838–844PubMed

22.

Dromey JA, Mijovic CH, Christie MR et al. (2000) HLA linked persistence of antibodies to GAD 65 in patients with 50 years of type 1 diabetes. Diabet Med 17: A73

23.

Gale EAM (2002) The rise of childhood Type 1 diabetes in the twentieth century. Diabetes 51:3353–3361PubMed

Titel: Three generations of autoimmune diabetes: an extended family study
verfasst von: I. F. Douek
K. M. Gillespie
R. J. Dix
P. J. Bingley
Prof. E. A. M. Gale
Publikationsdatum: 01.10.2003
Verlag: Springer-Verlag
Erschienen in: Diabetologia / Ausgabe 10/2003
Print ISSN: 0012-186X
Elektronische ISSN: 1432-0428
DOI: https://doi.org/10.1007/s00125-003-1186-5

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