Microsoft Word search phase 3 Title Page Amendment
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Severity at Onset of T1D: The onset of T1D is heterogeneous, ranging from severe
diabetic ketoacidosis (DKA) requiring hospitalization to a relatively gradual onset. Younger age at onset is usually associated with a more severe onset, more need for hospitalization, a greater chance of DKA, lower C peptide levels and higher HbA 1c . As onset age is decreasing, the presentation of diabetes in very young children is increasing, and can be particularly difficult for parents to recognize (65) . SEARCH found an increasing prevalence of DKA at onset of T1D with younger age: 15% of children 15-19; 27% of children 5-9; 25% of children 10-14; and 37% of children age 0-4 (19) . This study also revealed that the incidence of DKA at diagnosis of T1D has not changed significantly over the past two decades, despite efforts to improve awareness regarding diabetes symptoms to facilitate the earlier diagnosis and treatment of diabetes in children. By continuing to assess the presence of DKA at onset of T1D, SEARCH will be positioned to document potential temporal trends in the severity of T1D onset and to explore potential determinants of such trends. Other characteristics which differ by age at onset include fasting C peptide (FCP) levels, and level and type of autoantibodies. A study examining FCP at diagnosis of T1D found that higher levels were associated with older age at onset, less hyperglycemia, and a reduced insulin requirement (60) . SEARCH also found that, among youth with T1D and positive DA, older onset age and lower HbA 1c levels were associated with preservation of FCP within the first year of diagnosis (17) . It is not known if the percent of youth with T1D and preserved beta cell function is changing over time. Such knowledge may have important implications for clinical care and clinical trials. The presence of islet cell (ICA), insulin (IAA), 65-kDa isoform of glutamic acid decarboxylase (GAD65), insulinoma-associated protein 2 (IA-2) or islet zinc transporter (ZnT8) autoantibodies is highly predictive of T1D risk. It is believed that Section 4A - Study Objectives/Background and Significance (Phase 3 - 11/2010) Section 4A - Page 9 Registry Study seroconversion occurs early in life (66) ; however, autoimmunity can occur at any age (67) . The Diabetes Prevention Trial - Type 1 recently confirmed that not only presence, but number of DA, type and titers are also predictive for T1D risk (67) . Differences in the levels of DA have also been reported by onset age. Zimmet et al reported a higher frequency of GAD65 positive antibodies among patients who were diagnosed with T1D at age 10+ compared to those diagnosed before age 10 (68) . Similarly, SEARCH reported a higher prevalence of GAD65 antibodies in T1D youth age 10+ compared with those < 10 years old at diagnosis (65.6% vs. 56.4%) (5) . Data on trends in autoimmunity at presentation with T1D are very limited. It is unknown if autoimmunity is shifting to younger ages over time as seen with T1D onset age. Such knowledge of a potential shift in DA seroconversion would narrow the exposure window and help in identifying potential environmental triggers. Yüklə 1,48 Mb. Dostları ilə paylaş:
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