Your search keyword '"McDaniel, Kristen"' showing total 3 results

1. Failed Genetic Protection: Type 1 Diabetes in the Presence of .

Author

Simmons, Kimber M., Mitchell, Angela M., Alkanani, Aimon A., McDaniel, Kristen A., Baschal, Erin E., Armstrong, Taylor, Pyle, Laura, Yu, Liping, and Michels, Aaron W.

Subjects

TYPE 1 diabetes, T cells, AUTOANTIBODIES, RESEARCH, HLA-B27 antigen, RESEARCH methodology, ALLELES, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, HAPLOTYPES, RESEARCH funding

Abstract

Certain HLA class II genes increase the risk for type 1 diabetes (T1D) development while others provide protection from disease development. HLA class II alleles encode MHC proteins on antigen-presenting cells, which function to present peptides and activate CD4 T cells. The DRB1*15:01 (DR15)-DQA1*01:02-DQB1*06:02 (DQ6) haplotype provides dominant protection across all stages of T1D and is a common haplotype found in Caucasians. However, it is present in <1% of people with T1D. Knowing which metabolic, immunologic, and genetic features are unique to individuals who fail genetic protection and develop T1D is important for defining the underlying mechanisms of DQB1*06:02-mediated protection. We describe a T1D cohort with DQB1*06:02 (n = 50) and compare them to individuals with T1D and without DQB1*06:02 (n = 2,759) who were identified over the last 26 years at the Barbara Davis Center for Diabetes. The age at diagnosis was similar between the cohorts and normally distributed throughout childhood and early adulthood. The average hemoglobin A1c was 10.8 ± 2.8% (95 ± 7 mmol/mol) at diagnosis in those DQB1*06:02 positive. The majority of T1D DQB1*06:02+ individuals were positive for one or more islet autoantibodies; however, there was a greater proportion who were islet autoantibody negative compared with those T1D DQB1*06:02- individuals. Interestingly, DQB1*03:02, which confers significant T1D risk, was present in only those DQB1*06:02+ individuals with islet autoantibodies. This is one of the largest studies examining patients presenting with clinical T1D in the presence of DQB1*06:02, which provides a population to study the mechanisms of failed genetic protection against T1D. [ABSTRACT FROM AUTHOR]

Published

2020

2. Islet-Derived CD4 T Cells Targeting Proinsulin in Human Autoimmune Diabetes.

Author

Michels, Aaron W., Landry, Laurie G., McDaniel, Kristen A., Liping Yu, Martha Campbell-Thompson, Kwok, William W., Jones, Kenneth L., Gottlieb, Peter A., Kappler, John W., Qizhi Tang, Roep, Bart O., Atkinson, Mark A., Mathews, Clayton E., Maki Nakayama, Yu, Liping, Campbell-Thompson, Martha, Tang, Qizhi, and Nakayama, Maki

Subjects

TYPE 1 diabetes, AUTOIMMUNE diseases, INSULIN, ISLANDS of Langerhans, ANTIGENS, ANIMAL models in research, DIAGNOSIS, C-peptide, CELL receptors, PEPTIDES, PROINSULIN, PROTEIN precursors, RESEARCH funding, T cells, HLA-B27 antigen

Abstract

Type 1 diabetes results from chronic autoimmune destruction of insulin-producing β-cells within pancreatic islets. Although insulin is a critical self-antigen in animal models of autoimmune diabetes, due to extremely limited access to pancreas samples, little is known about human antigenic targets for islet-infiltrating T cells. Here we show that proinsulin peptides are targeted by islet-infiltrating T cells from patients with type 1 diabetes. We identified hundreds of T cells from inflamed pancreatic islets of three young organ donors with type 1 diabetes with a short disease duration with high-risk HLA genes using a direct T-cell receptor (TCR) sequencing approach without long-term cell culture. Among 85 selected CD4 TCRs tested for reactivity to preproinsulin peptides presented by diabetes-susceptible HLA-DQ and HLA-DR molecules, one T cell recognized C-peptide amino acids 19-35, and two clones from separate donors responded to insulin B-chain amino acids 9-23 (B:9-23), which are known to be a critical self-antigen-driving disease progress in animal models of autoimmune diabetes. These B:9-23-specific T cells from islets responded to whole proinsulin and islets, whereas previously identified B:9-23 responsive clones from peripheral blood did not, highlighting the importance of proinsulin-specific T cells in the islet microenvironment. [ABSTRACT FROM AUTHOR]

Published

2017

3. Methyldopa blocks MHC class II binding to disease-specific antigens in autoimmune diabetes.

Author

Ostrov, David A., Alkanani, Aimon, McDaniel, Kristen A., Case, Stephanie, Baschal, Erin E., Pyle, Laura, Ellis, Sam, Pöllinger, Bernadette, Seidl, Katherine J., Shah, Viral N., Garg, Satish K., Atkinson, Mark A., Gottlieb, Peter A., and Michels, Aaron W.

Subjects

*AUTOIMMUNE diseases, *DIABETES, *AUTOIMMUNITY, *CARBOHYDRATE intolerance, *IMMUNOGLOBULINS, *ANIMAL experimentation, *AUTOANTIBODIES, *CELLULAR immunity, *COMPARATIVE studies, *TYPE 1 diabetes, *RESEARCH methodology, *MEDICAL cooperation, *MICE, *RESEARCH, *T cells, *HLA-B27 antigen, *EVALUATION research, *METHYLDOPA, *ANTIBODY formation, *PHARMACODYNAMICS

Abstract

Major histocompatibility (MHC) class II molecules are strongly associated with many autoimmune disorders. In type 1 diabetes (T1D), the DQ8 molecule is common, confers significant disease risk, and is involved in disease pathogenesis. We hypothesized that blocking DQ8 antigen presentation would provide therapeutic benefit by preventing recognition of self-peptides by pathogenic T cells. We used the crystal structure of DQ8 to select drug-like small molecules predicted to bind structural pockets in the MHC antigen-binding cleft. A limited number of the predicted compounds inhibited DQ8 antigen presentation in vitro, with 1 compound preventing insulin autoantibody production and delaying diabetes onset in an animal model of spontaneous autoimmune diabetes. An existing drug with a similar structure, methyldopa, specifically blocked DQ8 in patients with recent-onset T1D and reduced inflammatory T cell responses to insulin, highlighting the relevance of blocking disease-specific MHC class II antigen presentation to treat autoimmunity. [ABSTRACT FROM AUTHOR]

Published

2018