ISLET AUTOANTIBODY MARKERS IN IDDM - RISK ASSESSMENT STRATEGIES YIELDING HIGH-SENSITIVITY

被引:183
作者
BONIFACIO, E
GENOVESE, S
BRAGHI, S
BAZZIGALUPPI, E
LAMPASONA, V
BINGLEY, PJ
ROGGE, L
PASTORE, MR
BOGNETTI, E
BOTTAZZO, GF
GALE, EAM
BOSI, E
机构
[1] ST BARTHOLOMEWS HOSP,COLL MED,DEPT DIABET & METAB,LONDON,ENGLAND
[2] ROCHE MILANO RIC,MILAN,ITALY
[3] LONDON HOSP,COLL MED,DEPT IMMUNOL,LONDON,ENGLAND
关键词
ISLET CELL ANTIBODIES; GLUTAMIC ACID DECARBOXYLASE(65) ANTIBODIES; ISLET AUTOANTIGENS; INSULIN-DEPENDENT DIABETES MELLITUS PREDICTION; CARBOXYPEPTIDASE-H; ICA69;
D O I
10.1007/s001250050358
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Identification of islet autoantigens offers the possibility that antibody tests other than islet cell antibodies may be used for assessing risk of insulin-dependent diabetes mellitus (IDDM). The aim of this study was to determine the combination of islet autoantibody markers that could identify most future cases of IDDM. Islet cell antibodies, antibodies to glutamic acid decarboxylase (GAD)(65), 37,000/40,000 M(r) islet tryptic fragments, carboxypeptidase-H, and islet cell autoantigen (ICA)69 were measured in sera from 100 newly-diagnosed IDDM patients, 27 individuals prior to onset of IDDM, and 83 control subjects. Islet cell antibodies were detected in 88 % of IDDM patients and 81 % with pre-IDDM, GAD(65) antibodies in 70 % of IDDM patients and 89 % with pre-IDDM, and antibodies to 37,000/40,000 M(r) islet tryptic fragments in 54 % of IDDM patients and in 48 % with pre-IDDM. The latter were found only in conjunction with islet cell antibodies and were more frequent in young onset cases. All 20 IDDM patients and the 3 pre-IDDM subjects who had islet cell anti-bodies without GAD(65) antibodies had antibodies to 37,000/40,000 M(r) islet tryptic fragments, and all but one had disease onset before age 15 years. No sera strongly immunoprecipitated in vitro translated ICA69 or carboxypeptidase-H; 4 % of patients had anti-ICA69 and 11 % anti-carboxypeptidase-H levels above those of the control subjects. The findings suggest that none of the single antibody specificities are as sensitive as islet cell antibodies, but that a combination of GAD(65) antibodies and antibodies to 37,000/40,000 M(r) islet tryptic fragments has the potential to identify more than 90 % of future cases of IDDM. Such a strategy could eventually replace islet cell antibodies in population screening for IDDM risk assessment.
引用
收藏
页码:816 / 822
页数:7
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