Evolution of multiple cell clones over a 29-year period of a CLL patient

Zhikun Zhao; Lynn Goldin; Shiping Liu; Liang Wu; Weiyin Zhou; Hong Lou; Qichao Yu; Shirley X. Tsang; Miaomiao Jiang; Fuqiang Li; Mary Lou McMaster; Yang Li; Xinxin Lin; Zhifeng Wang; Liqin Xu; Gerald Marti; Guibo Li; Kui Wu; Meredith Yeager; Huanming Yang; Xun Xu; Stephen J. Chanock; Bo Li; Yong Hou; Neil Caporaso; Michael Dean

doi:10.1038/ncomms13765

Evolution of multiple cell clones over a 29-year period of a CLL patient

Zhikun Zhao
, Lynn Goldin
, Shiping Liu
, Liang Wu
, Weiyin Zhou
, Hong Lou
, Qichao Yu
, Shirley X. Tsang
, Miaomiao Jiang
, Fuqiang Li
, Mary Lou McMaster
, Yang Li
, Xinxin Lin
, Zhifeng Wang
, Liqin Xu
, Gerald Marti
, Guibo Li
, Kui Wu
, Meredith Yeager
, Huanming Yang

Xun Xu, Stephen J. Chanock, Bo Li, Yong Hou, Neil Caporaso, Michael Dean

Research output: Contribution to journal › Article › peer-review

27 Scopus citations

Abstract

Chronic lymphocytic leukaemia (CLL) is a frequent B-cell malignancy, characterized by recurrent somatic chromosome alterations and a low level of point mutations. Here we present single-nucleotide polymorphism microarray analyses of a single CLL patient over 29 years of observation and treatment, and transcriptome and whole-genome sequencing at selected time points. We identify chromosome alterations 13q14-, 6q- and 12q+ in early cell clones, elimination of clonal populations following therapy, and subsequent appearance of a clone containing trisomy 12 and chromosome 10 copy-neutral loss of heterogeneity that marks a major population dominant at death. Serial single-cell RNA sequencing reveals an expression pattern with high FOS, JUN and KLF4 at disease acceleration, which resolves following therapy, but reoccurs following relapse and death. Transcriptome evolution indicates complex changes in expression occur over time. In conclusion, CLL can evolve gradually during indolent phases, and undergo rapid changes following therapy.

Original language	English
Article number	13765
Pages (from-to)	13765
Number of pages	1
Journal	Nature Communications
Volume	7
DOIs	https://doi.org/10.1038/ncomms13765
State	Published - 16 Dec 2016
Externally published	Yes

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10.1038/ncomms13765

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@article{535537a4d2144dcfb8417633366a832b,

title = "Evolution of multiple cell clones over a 29-year period of a CLL patient",

abstract = "Chronic lymphocytic leukaemia (CLL) is a frequent B-cell malignancy, characterized by recurrent somatic chromosome alterations and a low level of point mutations. Here we present single-nucleotide polymorphism microarray analyses of a single CLL patient over 29 years of observation and treatment, and transcriptome and whole-genome sequencing at selected time points. We identify chromosome alterations 13q14-, 6q- and 12q+ in early cell clones, elimination of clonal populations following therapy, and subsequent appearance of a clone containing trisomy 12 and chromosome 10 copy-neutral loss of heterogeneity that marks a major population dominant at death. Serial single-cell RNA sequencing reveals an expression pattern with high FOS, JUN and KLF4 at disease acceleration, which resolves following therapy, but reoccurs following relapse and death. Transcriptome evolution indicates complex changes in expression occur over time. In conclusion, CLL can evolve gradually during indolent phases, and undergo rapid changes following therapy.",

author = "Zhikun Zhao and Lynn Goldin and Shiping Liu and Liang Wu and Weiyin Zhou and Hong Lou and Qichao Yu and Tsang, \{Shirley X.\} and Miaomiao Jiang and Fuqiang Li and McMaster, \{Mary Lou\} and Yang Li and Xinxin Lin and Zhifeng Wang and Liqin Xu and Gerald Marti and Guibo Li and Kui Wu and Meredith Yeager and Huanming Yang and Xun Xu and Chanock, \{Stephen J.\} and Bo Li and Yong Hou and Neil Caporaso and Michael Dean",

year = "2016",

month = dec,

day = "16",

doi = "10.1038/ncomms13765",

language = "英语",

volume = "7",

pages = "13765",

journal = "Nature Communications",

issn = "2041-1723",

publisher = "Nature Research",

}

Zhao, Z, Goldin, L, Liu, S, Wu, L, Zhou, W, Lou, H, Yu, Q, Tsang, SX, Jiang, M, Li, F, McMaster, ML, Li, Y, Lin, X, Wang, Z, Xu, L, Marti, G, Li, G, Wu, K, Yeager, M, Yang, H, Xu, X, Chanock, SJ, Li, B, Hou, Y, Caporaso, N & Dean, M 2016, 'Evolution of multiple cell clones over a 29-year period of a CLL patient', Nature Communications, vol. 7, 13765, pp. 13765. https://doi.org/10.1038/ncomms13765

TY - JOUR

T1 - Evolution of multiple cell clones over a 29-year period of a CLL patient

AU - Zhao, Zhikun

AU - Goldin, Lynn

AU - Liu, Shiping

AU - Wu, Liang

AU - Zhou, Weiyin

AU - Lou, Hong

AU - Yu, Qichao

AU - Tsang, Shirley X.

AU - Jiang, Miaomiao

AU - Li, Fuqiang

AU - McMaster, Mary Lou

AU - Li, Yang

AU - Lin, Xinxin

AU - Wang, Zhifeng

AU - Xu, Liqin

AU - Marti, Gerald

AU - Li, Guibo

AU - Wu, Kui

AU - Yeager, Meredith

AU - Yang, Huanming

AU - Xu, Xun

AU - Chanock, Stephen J.

AU - Li, Bo

AU - Hou, Yong

AU - Caporaso, Neil

AU - Dean, Michael

PY - 2016/12/16

Y1 - 2016/12/16

N2 - Chronic lymphocytic leukaemia (CLL) is a frequent B-cell malignancy, characterized by recurrent somatic chromosome alterations and a low level of point mutations. Here we present single-nucleotide polymorphism microarray analyses of a single CLL patient over 29 years of observation and treatment, and transcriptome and whole-genome sequencing at selected time points. We identify chromosome alterations 13q14-, 6q- and 12q+ in early cell clones, elimination of clonal populations following therapy, and subsequent appearance of a clone containing trisomy 12 and chromosome 10 copy-neutral loss of heterogeneity that marks a major population dominant at death. Serial single-cell RNA sequencing reveals an expression pattern with high FOS, JUN and KLF4 at disease acceleration, which resolves following therapy, but reoccurs following relapse and death. Transcriptome evolution indicates complex changes in expression occur over time. In conclusion, CLL can evolve gradually during indolent phases, and undergo rapid changes following therapy.

AB - Chronic lymphocytic leukaemia (CLL) is a frequent B-cell malignancy, characterized by recurrent somatic chromosome alterations and a low level of point mutations. Here we present single-nucleotide polymorphism microarray analyses of a single CLL patient over 29 years of observation and treatment, and transcriptome and whole-genome sequencing at selected time points. We identify chromosome alterations 13q14-, 6q- and 12q+ in early cell clones, elimination of clonal populations following therapy, and subsequent appearance of a clone containing trisomy 12 and chromosome 10 copy-neutral loss of heterogeneity that marks a major population dominant at death. Serial single-cell RNA sequencing reveals an expression pattern with high FOS, JUN and KLF4 at disease acceleration, which resolves following therapy, but reoccurs following relapse and death. Transcriptome evolution indicates complex changes in expression occur over time. In conclusion, CLL can evolve gradually during indolent phases, and undergo rapid changes following therapy.

UR - https://www.scopus.com/pages/publications/85030095823

U2 - 10.1038/ncomms13765

DO - 10.1038/ncomms13765

M3 - 文章

C2 - 27982015

AN - SCOPUS:85030095823

SN - 2041-1723

VL - 7

SP - 13765

JO - Nature Communications

JF - Nature Communications

M1 - 13765

ER -

Evolution of multiple cell clones over a 29-year period of a CLL patient

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