| Literature DB >> 28127566 |
Zhiyuan Zhao1, Dongmei Miao2, Kathleen Waugh2, Iman Taki2, Fran Dong2, Edwin Liu3, Marian Rewers2, Yu Liu4, Liping Yu2.
Abstract
Higher sensitive transglutaminase autoantibody (TGA) assay will detect the onset of celiac disease (CD) autoimmunity earlier. In developing a nonradioactive assay for TGA, we utilized electrochemiluminescence (ECL) technology and compared it to a high-performance radioimmunoassay (RIA) currently being used to screen patients with type 1 diabetes (T1D) and genetically at-risk individuals for CD. We selected 183 T1D patients with 60 patients having received biopsy and analyzed 396 sequential samples from 73 young children longitudinally followed up with TGA seroconversion, with 27 undergoing biopsy. In addition, 112 age-matched healthy control subjects were included in the study. With the 99th percentile of specificity, the ECL assay detected significantly more TGA positivity among patients with T1D (133/183) than RIA (114/183) and more of the sequential samples (34%) from 73 children than RIA (18%). The TGA assay performed by ECL was positive in all 59 subjects with villous atrophy. Among 73 longitudinally followed up children, ECL assay had earlier detection of TGA on 34 children by a mean of 2.5 years. In conclusion, the new TGA assay by ECL has a higher sensitivity than the current RIA assay and may better predict the onset of CD.Entities:
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Year: 2016 PMID: 28127566 PMCID: PMC5239972 DOI: 10.1155/2016/2904563
Source DB: PubMed Journal: J Immunol Res ISSN: 2314-7156 Impact factor: 4.818
Figure 1Titration of TGA by both RIA and ECL assay using a TGA positive sample from six of T1D patients studied with confirmed clinical CD by biopsy (marked patient 1, patient 2, patient 3, patient 4, patient 5, and patient 6, respectively). The samples were in a serial of 1 : 1 dilution with a normal control serum to a maximum of 1 : 4096 dilutions. The solid curves were TGA levels from ECL assay and the dotted curves with gray color were TGA levels from RIA. A horizontal dotted line represents assay cut-offs for both ECL and RIA at 3 standard deviation (SD) scores. The SD scores are calculated with the following formula: (index value − mean index of controls)/SD.
Figure 2TGA levels from ECL assay and our current standard RIA were compared among 183 patients with type 1 diabetes. The cases without or with biopsy+ or − are shown in different markers. Four cases from biopsy group that became TGA negative by RIA were pointed by arrows.
Figure 3TGA levels from ECL assay and our current standard RIA were compared on 396 sequential samples from 73 children who were confirmed TGA positive seroconversion during the longitudinal follow-up.
Figure 4TGA were detected earlier in age in 34 children with ECL assay than RIA. The beginning of each line is TGA detecting age with ECL assay for a child and the end of line is TGA detecting age with RIA.