Search

Your search keyword '"McIndoe, Richard A."' showing total 6 results
Start Over Author "McIndoe, Richard A." Publisher wiley-blackwell
6 results on '"McIndoe, Richard A."'

1. Possible heterogeneity of initial pancreatic islet beta‐cell autoimmunity heralding type 1 diabetes.

Author

Lernmark, Åke, Akolkar, Beena, Hagopian, William, Krischer, Jeffrey, McIndoe, Richard, Rewers, Marian, Toppari, Jorma, Vehik, Kendra, and Ziegler, Anette‐G.

Subjects
TYPE 1 diabetes, ISLANDS of Langerhans, AUTOIMMUNITY, GLUTAMATE decarboxylase, PANCREATIC beta cells, AUTOIMMUNE diseases
Abstract

The etiology of type 1 diabetes (T1D) foreshadows the pancreatic islet beta‐cell autoimmune pathogenesis that heralds the clinical onset of T1D. Standardized and harmonized tests of autoantibodies against insulin (IAA), glutamic acid decarboxylase (GADA), islet antigen‐2 (IA‐2A), and ZnT8 transporter (ZnT8A) allowed children to be followed from birth until the appearance of a first islet autoantibody. In the Environmental Determinants of Diabetes in the Young (TEDDY) study, a multicenter (Finland, Germany, Sweden, and the United States) observational study, children were identified at birth for the T1D high‐risk HLA haploid genotypes DQ2/DQ8, DQ2/DQ2, DQ8/DQ8, and DQ4/DQ8. The TEDDY study was preceded by smaller studies in Finland, Germany, Colorado, Washington, and Sweden. The aims were to follow children at increased genetic risk to identify environmental factors that trigger the first‐appearing autoantibody (etiology) and progress to T1D (pathogenesis). The larger TEDDY study found that the incidence rate of the first‐appearing autoantibody was split into two patterns. IAA first peaked already during the first year of life and tapered off by 3–4 years of age. GADA first appeared by 2–3 years of age to reach a plateau by about 4 years. Prior to the first‐appearing autoantibody, genetic variants were either common or unique to either pattern. A split was also observed in whole blood transcriptomics, metabolomics, dietary factors, and exposures such as gestational life events and early infections associated with prolonged shedding of virus. An innate immune reaction prior to the adaptive response cannot be excluded. Clarifying the mechanisms by which autoimmunity is triggered to either insulin or GAD65 is key to uncovering the etiology of autoimmune T1D. [ABSTRACT FROM AUTHOR]

Published
2023
Full Text
View/download PDF

3. Molecular Pathways Altered by Insulin B9-23 Immunization.

Author

ECKENRODE, SARAH E., RUAN, QING‐GUO, COLLINS, CHRISTIN D., YANG, PING, MCINDOE, RICHARD A., MUIR, ANDREW, and SHE, JIN‐XIONG

Subjects
DIABETES, IMMUNOGLOBULINS, INSULIN, PANCREATIC secretions, DIABETIC acidosis
Abstract

Type 1 diabetes (T1D) in the nonobese diabetic (NOD) mouse can be delayed by administration of insulin or specific insulin peptides. To better understand how insulin treatment delays diabetes development, NOD mice treated with an insulin peptide (B9-23) were compared with age-matched NOD and NOD congenic mice for gene expression changes in spleen using cDNA microarray. Fifty genes were identified that were significantly altered by B9-23 treatment. Thirty-three of these genes are downregulated by the treatment while they are upregulated during the natural disease progression in NOD from immature (3-4 weeks) to mature (10 weeks) stages. Taken together, our data suggest that the B9-23 treatment, like the protective genes in NOD congenic strains, reduces pro-inflammatory activation of lymphocytes that normally occurs in NOD mice. Furthermore, our studies discovered two genes (Irf4 and Tra1) with increased expression in B9-23-treated mice that promote the Th2 response, providing a molecular basis for the B9-23-protective therapy. [ABSTRACT FROM AUTHOR]

Published
2004
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results