TY - JOUR
T1 - Validity of screening for individuals at risk for type I diabetes by combined analysis of antibodies to recombinant proteins
AU - Christie, Michael R.
AU - Roll, Ursula
AU - Payton, Mark A.
AU - Hatfield, Emma C.I.
AU - Ziegler, Anette G.
PY - 1997/6
Y1 - 1997/6
N2 - OBJECTIVE - To determine whether screening for the presence of multiple antibody markers for IDDM is effective at identifying individuals with high risk for disease development. RESEARCH DESIGN AND METHODS - Antibodies to GAD and the tyrosine phosphatase-like protein IA-2 were determined in sequential serum samples from 44 first-degree relatives of IDDM patients, identified as possessing islet cell antibody (ICA) and/or insulin autoantibody (IAA), who were followed prospectively for IDDM development. ICA, IAA, and antibodies to GAD and IA-2 were also determined in 93 cases of new-onset nonfamilial IDDM. RESULTS - The presence of two or more antibodies in addition to ICA or IAA conferred high risk (61%) for development of IDDM within 5 years of entry into the study and identified 89% of those who have developed IDDM on current follow-up. None of the relatives positive for ICA or IAA alone, in the absence of other antibody markers, have developed IDDM. Antibodies to islet antigens could both appear and disappear in follow-up samples obtained after entry into the study. The majority (60%) of young (< 16 years), sporadic cases of IDDM had multiple antibodies to islet antigens, but this proportion was lower in older patients (37%). CONCLUSIONS - A screening strategy based on die analysis of antibodies to multiple islet antigens can predict IDDM at high sensitivity and specificity in families, and such a strategy may also be applicable to identify young individuals in the general population with high disease risk. Since appearance of antibodies to different antigens occurs sequentially rather than simultaneously, accurate assessment of diabetes risk based on the presence of multiple antibodies will require follow-up over a number of years after the first evidence islet autoimmunity.
AB - OBJECTIVE - To determine whether screening for the presence of multiple antibody markers for IDDM is effective at identifying individuals with high risk for disease development. RESEARCH DESIGN AND METHODS - Antibodies to GAD and the tyrosine phosphatase-like protein IA-2 were determined in sequential serum samples from 44 first-degree relatives of IDDM patients, identified as possessing islet cell antibody (ICA) and/or insulin autoantibody (IAA), who were followed prospectively for IDDM development. ICA, IAA, and antibodies to GAD and IA-2 were also determined in 93 cases of new-onset nonfamilial IDDM. RESULTS - The presence of two or more antibodies in addition to ICA or IAA conferred high risk (61%) for development of IDDM within 5 years of entry into the study and identified 89% of those who have developed IDDM on current follow-up. None of the relatives positive for ICA or IAA alone, in the absence of other antibody markers, have developed IDDM. Antibodies to islet antigens could both appear and disappear in follow-up samples obtained after entry into the study. The majority (60%) of young (< 16 years), sporadic cases of IDDM had multiple antibodies to islet antigens, but this proportion was lower in older patients (37%). CONCLUSIONS - A screening strategy based on die analysis of antibodies to multiple islet antigens can predict IDDM at high sensitivity and specificity in families, and such a strategy may also be applicable to identify young individuals in the general population with high disease risk. Since appearance of antibodies to different antigens occurs sequentially rather than simultaneously, accurate assessment of diabetes risk based on the presence of multiple antibodies will require follow-up over a number of years after the first evidence islet autoimmunity.
UR - http://www.scopus.com/inward/record.url?scp=0030960386&partnerID=8YFLogxK
U2 - 10.2337/diacare.20.6.965
DO - 10.2337/diacare.20.6.965
M3 - Article
C2 - 9167107
AN - SCOPUS:0030960386
SN - 0149-5992
VL - 20
SP - 965
EP - 970
JO - Diabetes Care
JF - Diabetes Care
IS - 6
ER -