| Literature DB >> 29856484 |
Qiong Jiang1, Tingting Zhao1, Wenhong Zheng2, Jijun Zhou3, Haoliang Wang1, Hui Dong1, Yongwen Chen1, Xiaoqin Tang1, Cong Liu1, Lilin Ye1, Qing Mao3, Chunlin Wang4, Jian Han5, Xiaoyun Shang1, Yuzhang Wu1.
Abstract
The presence of shared T-cell clonotypes was found in several different diseases, but its relationship with the progression of disease remains unclear. By sequencing the complementary determining region 3 of T-cell receptor (TCR) β chains from the purified antigen-experienced CD8+ T cells, we characterized the T-cell repertoire in a prospective cohort study among 75 patients with chronic hepatitis B in China, as well as a healthy control and a validation cohort. We found that most T-cell clones from patients harbored the "patient-specific" TCR sequences. However, "patient-shared" TCR clonotypes were also widely found, which correlated with the favorable turnover of disease. Interestingly, the frequency of the "patient-shared" clonotypes can serve as a biomarker for favorable prognosis. Based on the clonotypes in those patients with favorable outcomes, we created a database including several clusters of protective anti-HBV CD8+ T-cell clonotypes that might be a reasonable target for therapeutic vaccine development or adoptive cell transfer therapy. These findings were validated in an additional independent cohort of patients. These results suggest that the "patient-shared" TCR clonotypes may serve as a valuable prognostic tool in the treatment of chronic hepatitis B and possibly other chronic viral diseases.Entities:
Keywords: Antigen specific T cells; Chronic viral infection; Hepatitis B virus infection; High throughput sequencing; T-cell repertoire
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Year: 2018 PMID: 29856484 DOI: 10.1002/eji.201747327
Source DB: PubMed Journal: Eur J Immunol ISSN: 0014-2980 Impact factor: 5.532