Human immune phenotyping reveals accelerated aging in type 1 diabetes

被引:20
作者
Shapiro, Melanie R. [1 ,2 ]
Dong, Xiaoru [2 ,3 ]
Perry, Daniel J. [1 ,2 ]
McNichols, James M. [1 ,2 ]
Thirawatananond, Puchong [1 ,2 ]
Posgai, Amanda L. [1 ,2 ]
Peters, Leeana D. [1 ,2 ]
Motwani, Keshav [1 ,2 ]
Musca, Richard S. [1 ,2 ]
Muir, Andrew [4 ]
Concannon, Patrick [1 ,2 ,5 ]
Jacobsen, Laura M. [1 ,2 ,6 ]
Mathews, Clayton E. [1 ,2 ]
Wasserfall, Clive H. [1 ,2 ]
Haller, Michael J. [2 ,6 ]
Schatz, Desmond A. [2 ,6 ]
Atkinson, Mark A. [1 ,2 ,6 ]
Brusko, Maigan A. [1 ,2 ]
Bacher, Rhonda L. [2 ,3 ]
Brusko, Todd M. [1 ,2 ,6 ]
机构
[1] Univ Florida, Coll Med, Dept Pathol Immunol & Lab Med, Gainesville, FL USA
[2] Univ Florida, Diabet Inst, Coll Publ Hlth & Hlth Profess, Gainesville, FL USA
[3] Univ Florida, Coll Publ Hlth & Hlth Profess, Dept Biostat, Gainesville, FL USA
[4] Emory Univ, Dept Pediat, Atlanta, GA USA
[5] Univ Florida, Genet Inst, Coll Med, Gainesville, FL USA
[6] Univ Florida, Coll Med, Dept Pediat, Gainesville, FL USA
关键词
GENETIC RISK; PD-1; GENE; T-CELLS; CHILDREN; ASSOCIATION; MELLITUS; SYSTEM; TIME; HLA; AUTOANTIBODIES;
D O I
10.1172/jci.insight.170767
中图分类号
R-3 [医学研究方法]; R3 [基础医学];
学科分类号
1001 ;
摘要
The proportions and phenotypes of immune cell subsets in peripheral blood undergo continual and dramatic remodeling throughout the human life span, which complicates efforts to identify disease-associated immune signatures in type 1 diabetes (T1D). We conducted cross-sectional flow cytometric immune profiling on peripheral blood from 826 individuals (stage 3 T1D, their first-degree relatives, those with >= 2 islet autoantibodies, and autoantibody-negative unaffected controls). We constructed an immune age predictive model in unaffected participants and observed accelerated immune aging in T1D. We used generalized additive models for location, shape, and scale to obtain age-corrected data for flow cytometry and complete blood count readouts, which can be visualized in our interactive portal (ImmScape); 46 parameters were significantly associated with age only, 25 with T1D only, and 23 with both age and T1D. Phenotypes associated with accelerated immunological aging in T1D included increased CXCR3(+) and programmed cell death 1-positive (PD-1(+)) frequencies in naive and memory T cell subsets, despite reduced PD-1 expression levels on memory T cells. Phenotypes associated with T1D after age correction were predictive of T1D status. Our findings demonstrate advanced immune aging in T1D and highlight disease-associated phenotypes for biomarker monitoring and therapeutic interventions.
引用
收藏
页数:20
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