Immunogenetic and clinical characterization of slowly progressive IDDM
Immunogenetic and clinical characterization of slowly progressive IDDM. T Kobayashi , K Tamemoto , K Nakanishi , N Kato , M Okubo , H Kajio , T Sugimoto , T Murase and K Kosaka Department of Endocrinology and Metabolism, Toranomon Hospital, Tokyo, Japan. Abstract OBJECTIVE--To examine the clinical a...
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| Published in | Diabetes care Vol. 16; no. 5; pp. 780 - 788 |
|---|---|
| Main Authors | , , , , , , , , |
| Format | Journal Article |
| Language | English |
| Published |
Alexandria, VA
American Diabetes Association
01.05.1993
|
| Subjects | |
| Online Access | Get full text |
| ISSN | 0149-5992 1935-5548 |
| DOI | 10.2337/diacare.16.5.780 |
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| Abstract | Immunogenetic and clinical characterization of slowly progressive IDDM.
T Kobayashi ,
K Tamemoto ,
K Nakanishi ,
N Kato ,
M Okubo ,
H Kajio ,
T Sugimoto ,
T Murase and
K Kosaka
Department of Endocrinology and Metabolism, Toranomon Hospital, Tokyo, Japan.
Abstract
OBJECTIVE--To examine the clinical and immunogenetic heterogeneity of IDDM. RESEARCH DESIGN AND METHODS--We divided 207 IDDM
patients into groups based on the interval from clinical onset to initiation of insulin therapy: group A (< 3 mo, acute clinical-onset
group, n = 134), group B (3-12 mo, intermediate group, n = 31), and group C (> or = 13 mo, slowly progressive group, n = 42).
Immunogenetic and clinical markers were compared between group A and group C. RESULTS--The mode age of onset was higher in
group C (52 yr) than group A (10 yr). Group C had a higher prevalence of islet cell antibodies (42.9%, 18 of 42) than group
A (25.4%, 34 of 134, P = 0.05). Serum C-peptide immunoreactivity assayed by radioimmunoassay in response to a 100-g oral glucose
tolerance test was significantly higher in group C than in group A. Group C patients were also more likely to have a family
history of NIDDM (26.1%, 11 of 42) among their first-degree relatives than group A patients (11.2%, 15 of 134, P = 0.039).
The prevalences of family history of IDDM and endocrine autoimmune diseases were not different between groups C and A. The
frequency of complications of endocrine autoimmune disease was not different between group A (6.7%, 9 of 134) and group C
(2.3%, 1 of 42). Significant associations with two class I major histocompatibility complex antigens (HLA-A24 and -Bw54) and
one class II antigen (HLA-DR4) were observed in group A. Group A patients were associated with three diabetogenic HLA-DQ haplotypes
including DQA1*0301-DQB1*0401, DQA1*0301-DQB1*0302, and DQA1*0301-DQB1*0303. In contrast, group C lacked the association with
class I antigens, although HLA-DR4 and HLA-DQA1*0301-DQB1*0401 were more common in this group than in control subjects. CONCLUSIONS--These
results indicate that the clinical subtype with slowly progressive course (slowly progressive IDDM) has distinct findings
including late-age onset, high prevalence of islet cell antibodies, preserved beta-cell function, and high family history
of NIDDM. An additive effect of class I and class II major histocompatibility complex antigens is suggested as an explanation
for the acute clinical manifestations and more severe beta-cell destruction in group A patients. |
|---|---|
| AbstractList | To examine the clinical and immunogenetic heterogeneity of IDDM.OBJECTIVETo examine the clinical and immunogenetic heterogeneity of IDDM.We divided 207 IDDM patients into groups based on the interval from clinical onset to initiation of insulin therapy: group A (< 3 mo, acute clinical-onset group, n = 134), group B (3-12 mo, intermediate group, n = 31), and group C (> or = 13 mo, slowly progressive group, n = 42). Immunogenetic and clinical markers were compared between group A and group C.RESEARCH DESIGN AND METHODSWe divided 207 IDDM patients into groups based on the interval from clinical onset to initiation of insulin therapy: group A (< 3 mo, acute clinical-onset group, n = 134), group B (3-12 mo, intermediate group, n = 31), and group C (> or = 13 mo, slowly progressive group, n = 42). Immunogenetic and clinical markers were compared between group A and group C.The mode age of onset was higher in group C (52 yr) than group A (10 yr). Group C had a higher prevalence of islet cell antibodies (42.9%, 18 of 42) than group A (25.4%, 34 of 134, P = 0.05). Serum C-peptide immunoreactivity assayed by radioimmunoassay in response to a 100-g oral glucose tolerance test was significantly higher in group C than in group A. Group C patients were also more likely to have a family history of NIDDM (26.1%, 11 of 42) among their first-degree relatives than group A patients (11.2%, 15 of 134, P = 0.039). The prevalences of family history of IDDM and endocrine autoimmune diseases were not different between groups C and A. The frequency of complications of endocrine autoimmune disease was not different between group A (6.7%, 9 of 134) and group C (2.3%, 1 of 42). Significant associations with two class I major histocompatibility complex antigens (HLA-A24 and -Bw54) and one class II antigen (HLA-DR4) were observed in group A. Group A patients were associated with three diabetogenic HLA-DQ haplotypes including DQA1*0301-DQB1*0401, DQA1*0301-DQB1*0302, and DQA1*0301-DQB1*0303. In contrast, group C lacked the association with class I antigens, although HLA-DR4 and HLA-DQA1*0301-DQB1*0401 were more common in this group than in control subjects.RESULTSThe mode age of onset was higher in group C (52 yr) than group A (10 yr). Group C had a higher prevalence of islet cell antibodies (42.9%, 18 of 42) than group A (25.4%, 34 of 134, P = 0.05). Serum C-peptide immunoreactivity assayed by radioimmunoassay in response to a 100-g oral glucose tolerance test was significantly higher in group C than in group A. Group C patients were also more likely to have a family history of NIDDM (26.1%, 11 of 42) among their first-degree relatives than group A patients (11.2%, 15 of 134, P = 0.039). The prevalences of family history of IDDM and endocrine autoimmune diseases were not different between groups C and A. The frequency of complications of endocrine autoimmune disease was not different between group A (6.7%, 9 of 134) and group C (2.3%, 1 of 42). Significant associations with two class I major histocompatibility complex antigens (HLA-A24 and -Bw54) and one class II antigen (HLA-DR4) were observed in group A. Group A patients were associated with three diabetogenic HLA-DQ haplotypes including DQA1*0301-DQB1*0401, DQA1*0301-DQB1*0302, and DQA1*0301-DQB1*0303. In contrast, group C lacked the association with class I antigens, although HLA-DR4 and HLA-DQA1*0301-DQB1*0401 were more common in this group than in control subjects.These results indicate that the clinical subtype with slowly progressive course (slowly progressive IDDM) has distinct findings including late-age onset, high prevalence of islet cell antibodies, preserved beta-cell function, and high family history of NIDDM. An additive effect of class I and class II major histocompatibility complex antigens is suggested as an explanation for the acute clinical manifestations and more severe beta-cell destruction in group A patients.CONCLUSIONSThese results indicate that the clinical subtype with slowly progressive course (slowly progressive IDDM) has distinct findings including late-age onset, high prevalence of islet cell antibodies, preserved beta-cell function, and high family history of NIDDM. An additive effect of class I and class II major histocompatibility complex antigens is suggested as an explanation for the acute clinical manifestations and more severe beta-cell destruction in group A patients. To examine the clinical and immunogenetic heterogeneity of IDDM. We divided 207 IDDM patients into groups based on the interval from clinical onset to initiation of insulin therapy: group A (< 3 mo, acute clinical-onset group, n = 134), group B (3-12 mo, intermediate group, n = 31), and group C (> or = 13 mo, slowly progressive group, n = 42). Immunogenetic and clinical markers were compared between group A and group C. The mode age of onset was higher in group C (52 yr) than group A (10 yr). Group C had a higher prevalence of islet cell antibodies (42.9%, 18 of 42) than group A (25.4%, 34 of 134, P = 0.05). Serum C-peptide immunoreactivity assayed by radioimmunoassay in response to a 100-g oral glucose tolerance test was significantly higher in group C than in group A. Group C patients were also more likely to have a family history of NIDDM (26.1%, 11 of 42) among their first-degree relatives than group A patients (11.2%, 15 of 134, P = 0.039). The prevalences of family history of IDDM and endocrine autoimmune diseases were not different between groups C and A. The frequency of complications of endocrine autoimmune disease was not different between group A (6.7%, 9 of 134) and group C (2.3%, 1 of 42). Significant associations with two class I major histocompatibility complex antigens (HLA-A24 and -Bw54) and one class II antigen (HLA-DR4) were observed in group A. Group A patients were associated with three diabetogenic HLA-DQ haplotypes including DQA1*0301-DQB1*0401, DQA1*0301-DQB1*0302, and DQA1*0301-DQB1*0303. In contrast, group C lacked the association with class I antigens, although HLA-DR4 and HLA-DQA1*0301-DQB1*0401 were more common in this group than in control subjects. These results indicate that the clinical subtype with slowly progressive course (slowly progressive IDDM) has distinct findings including late-age onset, high prevalence of islet cell antibodies, preserved beta-cell function, and high family history of NIDDM. An additive effect of class I and class II major histocompatibility complex antigens is suggested as an explanation for the acute clinical manifestations and more severe beta-cell destruction in group A patients. Immunogenetic and clinical characterization of slowly progressive IDDM. T Kobayashi , K Tamemoto , K Nakanishi , N Kato , M Okubo , H Kajio , T Sugimoto , T Murase and K Kosaka Department of Endocrinology and Metabolism, Toranomon Hospital, Tokyo, Japan. Abstract OBJECTIVE--To examine the clinical and immunogenetic heterogeneity of IDDM. RESEARCH DESIGN AND METHODS--We divided 207 IDDM patients into groups based on the interval from clinical onset to initiation of insulin therapy: group A (< 3 mo, acute clinical-onset group, n = 134), group B (3-12 mo, intermediate group, n = 31), and group C (> or = 13 mo, slowly progressive group, n = 42). Immunogenetic and clinical markers were compared between group A and group C. RESULTS--The mode age of onset was higher in group C (52 yr) than group A (10 yr). Group C had a higher prevalence of islet cell antibodies (42.9%, 18 of 42) than group A (25.4%, 34 of 134, P = 0.05). Serum C-peptide immunoreactivity assayed by radioimmunoassay in response to a 100-g oral glucose tolerance test was significantly higher in group C than in group A. Group C patients were also more likely to have a family history of NIDDM (26.1%, 11 of 42) among their first-degree relatives than group A patients (11.2%, 15 of 134, P = 0.039). The prevalences of family history of IDDM and endocrine autoimmune diseases were not different between groups C and A. The frequency of complications of endocrine autoimmune disease was not different between group A (6.7%, 9 of 134) and group C (2.3%, 1 of 42). Significant associations with two class I major histocompatibility complex antigens (HLA-A24 and -Bw54) and one class II antigen (HLA-DR4) were observed in group A. Group A patients were associated with three diabetogenic HLA-DQ haplotypes including DQA1*0301-DQB1*0401, DQA1*0301-DQB1*0302, and DQA1*0301-DQB1*0303. In contrast, group C lacked the association with class I antigens, although HLA-DR4 and HLA-DQA1*0301-DQB1*0401 were more common in this group than in control subjects. CONCLUSIONS--These results indicate that the clinical subtype with slowly progressive course (slowly progressive IDDM) has distinct findings including late-age onset, high prevalence of islet cell antibodies, preserved beta-cell function, and high family history of NIDDM. An additive effect of class I and class II major histocompatibility complex antigens is suggested as an explanation for the acute clinical manifestations and more severe beta-cell destruction in group A patients. |
| Author | T Murase K Nakanishi K Kosaka T Sugimoto N Kato K Tamemoto M Okubo H Kajio T Kobayashi |
| Author_xml | – sequence: 1 givenname: Tetsuro surname: Kobayashi fullname: Kobayashi, Tetsuro organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 2 givenname: Koji surname: Tamemoto fullname: Tamemoto, Koji organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 3 givenname: Koji surname: Nakanishi fullname: Nakanishi, Koji organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 4 givenname: Norihiro surname: Kato fullname: Kato, Norihiro organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 5 givenname: Minoru surname: Okubo fullname: Okubo, Minoru organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 6 givenname: Hiroshi surname: Kajio fullname: Kajio, Hiroshi organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 7 givenname: Tadao surname: Sugimoto fullname: Sugimoto, Tadao organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 8 givenname: Toshio surname: Murase fullname: Murase, Toshio organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan – sequence: 9 givenname: Kinori surname: Kosaka fullname: Kosaka, Kinori organization: Department of Endocrinology and Metabolism, Toranomon Hospital; the Okinaka Memorial Institute for Medical Research Toranomon, Minato-Ku; and the Institute for Diabetes Care and Research, Asahi Life Foundation Marunouchi, Chiyoda-Ku, Tokyo, Japan |
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| DOI | 10.2337/diacare.16.5.780 |
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| Issue | 5 |
| Keywords | Endocrinopathy Human Immunopathology Histocompatibility system Immunological investigation Insulin dependent diabetes Clinical form Autoimmune disease Evolution |
| Language | English |
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| PublicationPlace | Alexandria, VA |
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| PublicationTitle | Diabetes care |
| PublicationTitleAlternate | Diabetes Care |
| PublicationYear | 1993 |
| Publisher | American Diabetes Association |
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| Snippet | Immunogenetic and clinical characterization of slowly progressive IDDM.
T Kobayashi ,
K Tamemoto ,
K Nakanishi ,
N Kato ,
M Okubo ,
H Kajio ,
T Sugimoto ,
T... To examine the clinical and immunogenetic heterogeneity of IDDM. We divided 207 IDDM patients into groups based on the interval from clinical onset to... To examine the clinical and immunogenetic heterogeneity of IDDM.OBJECTIVETo examine the clinical and immunogenetic heterogeneity of IDDM.We divided 207 IDDM... |
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| SubjectTerms | Adolescent Adult Autoantibodies - blood Base Sequence Biological and medical sciences C-Peptide - blood C-Peptide - urine Child Child, Preschool Diabetes Mellitus, Type 1 - genetics Diabetes Mellitus, Type 1 - immunology Diabetes Mellitus, Type 1 - physiopathology Diabetes. Impaired glucose tolerance Endocrine pancreas. Apud cells (diseases) Endocrinopathies Etiopathogenesis. Screening. Investigations. Target tissue resistance Female Gene Frequency Glycated Hemoglobin A - analysis Haplotypes - genetics Histocompatibility Testing HLA-A Antigens - genetics HLA-B Antigens - genetics HLA-DQ Antigens - genetics HLA-DR Antigens - genetics Humans Islets of Langerhans - immunology Male Medical sciences Middle Aged Molecular Sequence Data Oligodeoxyribonucleotides Polymerase Chain Reaction Polymorphism, Restriction Fragment Length Reference Values |
| Title | Immunogenetic and clinical characterization of slowly progressive IDDM |
| URI | http://care.diabetesjournals.org/content/16/5/780.abstract https://www.ncbi.nlm.nih.gov/pubmed/8098691 https://www.proquest.com/docview/75741126 |
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