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通过Ion Torrent S5新一代测序技术进行IGH和TCR克隆性检测在B细胞和T细胞癌症诊断及疾病监测中的验证与解读

Validation and interpretation of IGH and TCR clonality testing by Ion Torrent S5 NGS for diagnosis and disease monitoring in B and T cell cancers.

作者信息

Lay Lindsay, Stroup Brooke, Payton Jacqueline E

机构信息

Barnes-Jewish Hospital, St. Louis, MO, USA.

Washington University School of Medicine, St. Louis, MO, USA.

出版信息

Pract Lab Med. 2020 Nov 25;22:e00191. doi: 10.1016/j.plabm.2020.e00191. eCollection 2020 Nov.

Abstract

Cancers of B and T lymphocytes are the most common hematologic malignancies in the US. Molecular assays for assessing clonal rearrangements of the immunoglobulin receptor (IGH) and T-cell receptor (TCR), commonly referred to as B- and T-cell clonality, as well as determination of IGH somatic mutation status, enables improved diagnostic accuracy and disease monitoring. Here we describe validation of NGS LymphoTrack (IGH, TCRG, Invivoscribe, Inc) with Ion Torrent S5 sequencing, which employs a different sequencing chemistry and has not been previously reported for NGS clonality to our knowledge. We also demonstrate the concordance of clonality by LymphoTrack with S5 sequencing with other molecular methodologies and with clinical measurements of disease. We show that LymphoTrack with S5 sequencing identifies previously detected IGH and TCRG clonal sequences across matched biopsy specimens and clinical timepoints, enabling more precise and sensitive disease monitoring for B- and T-cell cancers compared to PCR fragment or capillary sequencing. In sum, our study demonstrates that the LymphoTrack assays with Ion Torrent S5 sequencing 1) can be used successfully for IGH and TCR clonality with reproducible results; 2) generates and quantifies clonal sequences to enable highly precise comparison of samples; 3) are substantially more sensitive than PCR fragment and return clonality results in specimens that failed PCR fragment assays; and 4) the TCRG assays are highly concordant with clinical and histopathologic diagnoses. Taken together, the LymphoTrack with Ion S5 NGS clonality assays offer a sensitive and precise method for diagnostic testing and disease monitoring in B- and T-cell cancers.

摘要

B淋巴细胞和T淋巴细胞癌是美国最常见的血液系统恶性肿瘤。用于评估免疫球蛋白受体(IGH)和T细胞受体(TCR)克隆重排的分子检测,通常称为B细胞和T细胞克隆性,以及IGH体细胞突变状态的测定,能够提高诊断准确性和疾病监测水平。在此,我们描述了使用Ion Torrent S5测序对NGS LymphoTrack(IGH、TCRG,Invivoscribe公司)进行的验证,该测序采用了不同的测序化学方法,据我们所知,此前尚未有关于NGS克隆性的相关报道。我们还证明了LymphoTrack的克隆性与S5测序在其他分子方法以及疾病临床测量方面的一致性。我们表明,采用S5测序的LymphoTrack能够在匹配的活检标本和临床时间点识别先前检测到的IGH和TCRG克隆序列,与PCR片段或毛细管测序相比,能够对B细胞和T细胞癌症进行更精确、更灵敏的疾病监测。总之,我们的研究表明,采用Ion Torrent S5测序的LymphoTrack检测方法:1)可成功用于IGH和TCR克隆性检测,结果具有可重复性;2)生成并定量克隆序列,以便对样本进行高精度比较;3)比PCR片段检测灵敏得多,能在PCR片段检测失败的标本中得出克隆性结果;4)TCRG检测与临床和组织病理学诊断高度一致。综上所述,采用Ion S5 NGS克隆性检测的LymphoTrack为B细胞和T细胞癌症的诊断检测和疾病监测提供了一种灵敏且精确的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7347/7718169/5439b95bcaf3/gr1.jpg

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