Temporal Trends in the Incidence of Childhood Diabetes
4.2.3.1.
Type 1 Diabetes
The majority of epidemiological data on T1D are based on a clinical definition
including physician diagnosis of diabetes and daily insulin injections
(36)
. In addition,
most studies have limited the age range of populations to < 14 years, to avoid
misclassification of diabetes type. It has been assumed, but not confirmed via
measured diabetes autoantibodies (DA), that “type 1” diabetes is autoimmune
mediated diabetes. SEARCH for Diabetes in Youth is unique in that it extends the
surveillance effort to youth age < 20 years, and it collects data on DA close to the
time of diagnosis, to validate the clinical assessment of diabetes type.
The majority of epidemiological data on T1D are based on data on populations of
European origin. SEARCH demonstrated that in 2002-2003 the incidence of T1D
was highest in non-Hispanic whites (NHW), followed by African Americans (AA)
and Hispanics, and it was lowest in Asian/Pacific Islanders (API) and American
Indians (AI)
(5)
. SEARCH for Diabetes in Youth is the only registry effort to include
a comprehensive assessment of T1D burden and risk across all major racial/ethnic
groups.
4.2.3.1.1.
Incidence Trends
Most
(10, 37 - 41)
but not all
(42 - 46)
population-based registries showed an increasing
incidence of T1D over time. An updated report from the DIAMOND project
examined the trends in incidence of T1D from 1990-1999 in 114 populations from
57 countries. Based on 43,013 cases of T1D from a study population of 84
million children ≤14 years
(2)
, the average annual increase in incidence over this
time period was 2.8% (95% CI 2.4-3.2%). Similarly, the EURODIAB study, a
large European survey including
20 population-based registries in 17 countries
showed a 3.2% (95% CI 2.7-3.7) annual increase for the period 1989-1998
(4)
, and
a more recent 3.9% (95% CI 3.6-4.2)
increase
from 1989-2003
(8)
. Interestingly,
the observed incidence rates confirmed, and in fact exceeded, the incidence
predicted for 2010 by earlier projections
(47)
. In EURODIAB
(8)
, estimates of the
Section 4A - Study Objectives/Background and Significance (Phase 3 - 11/2010)
Section 4A - Page 7
Registry
Study
rates of increase were highest in the youngest age-group [
5.4% (4.8–6.1)
for
children age 0-4 years].
Recent data from the U.S., where registry efforts have been less coordinated,
suggest similar trends. While the U.S. stood apart from other parts of the world in
reporting a stable incidence of childhood T1D in the 1970’s through the 1990s
(48)
,
SEARCH recently reported that the 2002-05 incidence of T1D in NHW youth
aged ≤ 14 years was 27.5 per 100 000 per year
(49)
a rate that exceeds the
incidence predicted for 2010 from older data from Allegheny County
(47)
. Using
data from the Colorado IDDM registry and the SEARCH-Colorado site the
incidence of T1D was shown to increase in youth age ≤ 17 years over the past 3
decades
(9)
. During a 26 year period, the incidence of T1D increased by 2.3%
(95% CI 1.6-3.1) per year and was much higher than predicted from earlier
Colorado data
(47)
. Of note, the increase was significant for both NHW (2.7%;
95% CI 1.9 - 3.6 per year, P < 0.0001) and Hispanic youth (1.6%; 0.2-3.1 per
year, P < 0.013). Similar to the EURODIAB data, in Colorado, the increase in
incidence was highest among the 0- to 4-year age-group (3.5%; 95% CI 2.1-4.9
per year). Additional suggestions of increasing incidence of T1D come from
registries in Philadelphia
(50, 51)
, Chicago
(52)
and Allegheny County
(53)
, reporting
mainly an increase among AA, but also Hawaii, reporting a four-fold overall
increase (1980 to 1989)
(54)
.
4.2.3.2.
Trends in Genetic Susceptibility to T1D
Genetic susceptibility plays a large role in T1D with the human leukocyte antigen
(HLA) genotypes (DR and DQ genes) explaining approximately 40-50% of T1D risk
(55)
. The genetic variation can explain the variation in incidence across racial/ethnic
groups, but it is unlikely to explain the rapid increase in the incidence of T1D.
Recent studies have suggested that the contribution of high risk HLA genotype DR3,4
has been relatively stable or has decreased over time
(56 – 58)
. Of note, one of these
studies was conducted in Colorado, based on the prior Colorado IDDM and the
current SEARCH data, and found a significant decrease in the proportion of cases of
T1D with the high risk HLA genotype in the last two decades among both NHW and
Hispanic participants
(59)
. These data suggest that the increase in T1D over the past
half century is likely not due to increased incidence among those at the highest
genetic risk in the HLA region, and must rather be explained by an increase in
environmental factors, increased penetrance of low/moderate HLA genotypes or other
genetic loci, or interactions between environmental risk factors and non-HLA genes.
Section 4A - Study Objectives/Background and Significance (Phase 3 - 11/2010)
Section 4A - Page 8
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4.2.3.3.
Trends in Clinical Presentation
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