| Literature DB >> 30700589 |
Wei Zhang1,2, Xinyue Li1,2, Longlong Wang1,2, Jianxiang Deng1,2, Liya Lin1,2, Lei Tian1,2, Jinghua Wu1,2, Chenling Tang1,2, Huanming Yang1,2, Jian Wang1,2, Ping Qiu3, Tong-Ming Fu3, Nitin K Saksena1,2, I-Ming Wang4, Xiao Liu5,2.
Abstract
The rhesus macaque is a valuable preclinical animal model to estimate vaccine effectiveness and is also important for understanding Ab maturation and B cell repertoire evolution responding to vaccination. However, incomplete mapping of rhesus Ig germline genes hinders the research efforts. To address this deficiency, we sequenced the BCR repertoires of 75 Indian rhesus macaques. Using a bioinformatic method that has been validated with BCR repertoire analysis of three human donors, we were able to infer rhesus variable (V) and joint (J) germline alleles. We identified a total of 122 V and 20 J germline alleles, of which 91 V and 13 J alleles were novel, with 40 V novel genes, of which 8 were located at a novel genomic region not, to our knowledge, previously recorded. The novelty of these newly identified alleles was supported by two observations. First, the 50 V and 5 J novel alleles were observed in the whole genome sequencing data of 10 rhesus macaques. Second, using alignment reference including the novel alleles, the mutation rate of the rearranged repertoires significantly declined in nine other irrelevant samples, and all our identified novel V and J alleles were 100%-identity mapped by rearranged repertoire data. These identified novel alleles, along with the previously reported alleles, provide an important reference for future investigations of rhesus immune repertoire evolution in response to vaccination or infection. In addition, the method outlined in our study offers a powerful foundation for the identification of novel Ig alleles in the future.Entities:
Mesh:
Substances:
Year: 2019 PMID: 30700589 DOI: 10.4049/jimmunol.1800342
Source DB: PubMed Journal: J Immunol ISSN: 0022-1767 Impact factor: 5.422