AI Article Synopsis
- B cells in the mucosal area play a crucial role in maintaining balance with various antigens, and tumor-infiltrating lymphocytes could be important for cancer prognosis and treatment.
- This study introduced a new method for analyzing the immunoglobulin heavy chain (IgH) repertoire using high-throughput sequencing from biopsies across different intestinal areas, showing significant similarities within the large intestine but notable differences between the terminal ileum and large intestine.
- Results indicated distinct IgH profiles between colorectal cancer (CRC) tumors, advanced adenomas (AD), and normal mucosa, identifying 1445 public clones for normal mucosa and 22 for CRC tumors, which may aid in improving clinical approaches to CRC diagnosis and treatment.
Article Abstract
The B cells inhabited in mucosa play a vital role in mediating homeostasis with autoantigens and external Ags. Tumor-infiltrating lymphocytes are potential prognostic markers and therapeutic agents for cancer. However, the spatial heterogeneity of the B cell repertoire in intestinal mucosa and the tumor-infiltrating lymphocytes in colorectal cancer (CRC) remain poorly understood. In this study, we developed an unbiased method to amplify the IgH repertoire, as well as a bioinformatic pipeline to process these high-throughput sequencing data. With biopsies from seven intestinal mucosal segments, we uncovered their strong spatial homogeneity among the large intestine, where the clone overlap rate was up to 62.21%. The heterogeneity between terminal ileum and large intestine was also observed, including discrepant isotype distribution and low clone overlap rate. With tumor and adjacent normal mucosal tissues from CRC and colorectal advanced adenoma (AD) patients, we observed a similar IgH profile between tumor and adjacent normal mucosal tissues in AD, as well as a slight difference in CRC. Interestingly, we found distinct repertoire properties in the CRC tumor from AD and normal mucosa. Finally, we identified 1445 public clones for the normal mucosa, and 22 public clones for the CRC tumor with characteristic features. These data may be of potential use in clinical prognosis, diagnosis, and treatment of CRC.
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| http://dx.doi.org/10.4049/jimmunol.1602039 | DOI Listing |
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