Cell-Surface Autoantibody Targets Zinc Transporter-8 (ZnT8) for In Vivo β-Cell Imaging and Islet-Specific Therapies

被引:3
|
作者
Guo, Zheng [1 ]
Kasinathan, Devi [1 ]
Merriman, Chengfeng [1 ]
Nakayama, Maki [2 ]
Li, Hua [3 ]
Li, Huilin [3 ]
Xu, Cheng [1 ]
Wong, G. William [1 ]
Yu, Liping [2 ]
Golson, Maria L. [4 ]
Fu, Dax [1 ]
机构
[1] Johns Hopkins Sch Med, Dept Physiol, Baltimore, MD 21205 USA
[2] Univ Colorado, Barbara Davis Ctr Diabet, Aurora, CO USA
[3] Van Andel Inst, Dept Biol Struct, Grand Rapids, MI USA
[4] Johns Hopkins Sch Med, Div Endocrinol Diabet & Metab, Baltimore, MD USA
基金
美国国家卫生研究院;
关键词
GLUCOSE-HOMEOSTASIS; DOUBLE-BLIND; NOD MICE; B-CELLS; ANTIGEN; ANTIBODIES; INSULITIS; MASS;
D O I
10.2337/db22-0477
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Type 1 diabetes (T1D) is a disease in which autoimmune attacks are directed at the insulin-producing beta-cell in the pancreatic islet. Autoantigens on the beta-cell surface membrane are specific markers for molecular recognition and targets for engagement by autoreactive B lymphocytes, which produce islet cell surface autoantibody (ICSA) upon activation. We report the cloning of an ICSA (mAb43) that recognizes a major T1D autoantigen, ZnT8, with a subnanomolar binding affinity and conformation specificity. We demonstrate that cell-surface binding of mAb43 protects the extracellular epitope of ZnT8 against immunolabeling by serum ICSA from a patient with T1D. Furthermore, mAb43 exhibits in vitro and ex vivo specificity for islet cells, mirroring the exquisite specificity of islet autoimmunity in T1D. Systemic administration of mAb43 yields a pancreas-specific biodistribution in mice and islet homing of an mAb43-linked imaging payload through the pancreatic vasculature, thereby validating the in vivo specificity of mAb43. Identifying ZnT8 as a major antigenic target of ICSA allows for research into the molecular recognition and engagement of autoreactive B cells in the chronic phase of T1D progression. The in vivo islet specificity of mAb43 could be further exploited to develop in vivo imaging and islet-specific immunotherapies.
引用
收藏
页码:184 / 195
页数:12
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