2016
DOI: 10.1038/srep30064
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Immune DNA signature of T-cell infiltration in breast tumor exomes

Abstract: Tumor infiltrating lymphocytes (TILs) have been associated with favorable prognosis in multiple tumor types. The Cancer Genome Atlas (TCGA) represents the largest collection of cancer molecular data, but lacks detailed information about the immune environment. Here, we show that exome reads mapping to the complementarity-determining-region 3 (CDR3) of mature T-cell receptor beta (TCRB) can be used as an immune DNA (iDNA) signature. Specifically, we propose a method to identify CDR3 reads in a breast tumor exom… Show more

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Cited by 31 publications
(21 citation statements)
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“…In other two studies, the immune signature predicted benefit from trastuzumab in adjuvant (Perez et al 2015) or neoadjuvant (Varadan et al 2016) settings. Interestingly, in these and other studies (Levy et al 2016, Heimes et al 2017, Kim et al 2017, when immunological signature was associated with immune function and immune response, it directly correlated with a better clinical outcome. Moreover, epigenetic alterations, in addition to the genetic alterations, of immune genes with prognostic impact have been increasingly reported in different types of cancers, including breast cancer.…”
Section: Immune Signatures and Prognosismentioning
confidence: 49%
“…In other two studies, the immune signature predicted benefit from trastuzumab in adjuvant (Perez et al 2015) or neoadjuvant (Varadan et al 2016) settings. Interestingly, in these and other studies (Levy et al 2016, Heimes et al 2017, Kim et al 2017, when immunological signature was associated with immune function and immune response, it directly correlated with a better clinical outcome. Moreover, epigenetic alterations, in addition to the genetic alterations, of immune genes with prognostic impact have been increasingly reported in different types of cancers, including breast cancer.…”
Section: Immune Signatures and Prognosismentioning
confidence: 49%
“…Finding biophysicochemical TCRb motifs that, within a cancer type, are shared across the TILs repertoires of all patients but are largely absent from healthy tissue repertoires is consistent with the hypothesis that we are detecting TCR with specificity for a tumorassociated antigen that is shared between patients. We are not the first to hypothesize that patients may have shared TCRs responding to a common antigen, nor are we the first to look for the corresponding TCRs in colorectal and breast cancer TILs (7,10,25,26,41,42). To address this hypothesis, other investigators have searched for CDR3 amino acid sequences that were shared between multiple patient TILs repertoires (7,10,25,26,41,42).…”
Section: Discussionmentioning
confidence: 99%
“…None of the studies found sequences shared across all patients in a study, and the degree of sharing varied tremendously. In the breast cancer studies, it was concluded that the shared TCRb CDR3 sequences most likely correspond to public clones rather than receptors responding to common cancer antigens, because the same TCRb CDR3 sequences were frequently found in databases of TCRb repertoires from presumed healthy individuals (7,25,41,42). In addition, Beausang and colleagues analyzed the sequence properties of the shared sequences and found that they had many features in common with the TCRb CDR3 sequences of public clones, such as being shorter in length and having few insertions (25).…”
Section: Discussionmentioning
confidence: 99%
“…After capture of the whole-exome by hybrid selection, the DNA libraries were amplified and sequenced. The performance was evaluated in comparison to whole exome data generated from 200 ng of DNA extracted from a mirrored frozen tissue specimen [38]. Libraries generated from 200 or 50 ng FFPE DNA achieved reasonable coverage, with nearly all targeted bases covered at least 20-fold (referred to as Cov20).…”
Section: Evaluation Of Targeted Sequencing Approaches For Low Input Fmentioning
confidence: 99%