BMC Cancer (Oct 2018)

Profiling the B/T cell receptor repertoire of lymphocyte derived cell lines

  • Kar-Tong Tan,
  • Ling-Wen Ding,
  • Qiao-Yang Sun,
  • Zhen-Tang Lao,
  • Wenwen Chien,
  • Xi Ren,
  • Jin-Fen Xiao,
  • Xin Yi Loh,
  • Liang Xu,
  • Michael Lill,
  • Anand Mayakonda,
  • De-Chen Lin,
  • Henry Yang,
  • H. Phillip Koeffler

DOI
https://doi.org/10.1186/s12885-018-4840-5
Journal volume & issue
Vol. 18, no. 1
pp. 1 – 13

Abstract

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Abstract Background Clonal VDJ rearrangement of B/T cell receptors (B/TCRs) occurring during B/T lymphocyte development has been used as a marker to track the clonality of B/T cell populations. Methods We systematically profiled the B/T cell receptor repertoire of 936 cancer cell lines across a variety of cancer types as well as 462 Epstein-Barr Virus (EBV) transformed normal B lymphocyte lines using RNA sequencing data. Results Rearranged B/TCRs were readily detected in cell lines derived from lymphocytes, and subclonality or potential biclonality were found in a number of blood cancer cell lines. Clonal BCR/TCR rearrangements were detected in several blast phase CML lines and unexpectedly, one gastric cancer cell line (KE-97), reflecting a lymphoid origin of these cells. Notably, clonality was highly prevalent in EBV transformed B lymphocytes, suggesting either transformation only occurred in a few B cells or those with a growth advantage dominated the transformed population through clonal evolution. Conclusions Our analysis reveals the complexity and heterogeneity of the BCR/TCR rearrangement repertoire and provides a unique insight into the clonality of lymphocyte derived cell lines.

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