Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity

Chi Ling Chiang; Eileen Y. Hu; Lingqian Chang; Jadwiga Labanowska; Kevan Zapolnik; Xiaokui Mo; Junfeng Shi; Tzyy Jye Doong; Arletta Lozanski; Pearlly S. Yan; Ralf Bundschuh; Logan A. Walker; Daniel Gallego-Perez; Wu Lu; Meixiao Long; Sanggu Kim; Nyla A. Heerema; Gerard Lozanski; Jennifer A. Woyach; John C. Byrd; Ly James Lee; Natarajan Muthusamy

doi:10.1016/j.celrep.2022.111115

Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity

Chi Ling Chiang
, Eileen Y. Hu
, Lingqian Chang
, Jadwiga Labanowska
, Kevan Zapolnik
, Xiaokui Mo
, Junfeng Shi
, Tzyy Jye Doong
, Arletta Lozanski
, Pearlly S. Yan
, Ralf Bundschuh
, Logan A. Walker
, Daniel Gallego-Perez
, Wu Lu
, Meixiao Long
, Sanggu Kim
, Nyla A. Heerema
, Gerard Lozanski
, Jennifer A. Woyach
, John C. Byrd

Ly James Lee, Natarajan Muthusamy^*

^*此作品的通讯作者

Ohio State University

科研成果: 期刊稿件 › 文章 › 同行评审

4 引用（Scopus）

摘要

The existence of “leukemia-initiating cells” (LICs) in chronic lymphocytic leukemia (CLL) remains controversial due to the difficulty in isolating and identifying the tumor-initiating cells. Here, we demonstrate a microchannel electroporation (MEP) microarray that injects RNA-detecting probes into single live cells, allowing the imaging and characterization of heterogeneous LICs by intracellular RNA expression. Using limited-cell FACS sequencing (LC-FACSeq), we can detect and monitor rare live LICs during leukemogenesis and characterize their differential drug sensitivity. Disease-associated mutation accumulation in developing B lymphoid but not myeloid lineage in CLL patient hematopoietic stem cells (CLL-HSCs), and development of independent clonal CLL-like cells in murine patient-derived xenograft models, suggests the existence of CLL LICs. Furthermore, we identify differential protein ubiquitination and unfolding response signatures in GATA2^high CLL-HSCs that exhibit increased sensitivity to lenalidomide and resistance to fludarabine compared to GATA2^lowCLL-HSCs. These results highlight the existence of therapeutically targetable disease precursors in CLL.

源语言	英语
文章编号	111115
期刊	Cell Reports
卷	40
期	3
DOI	https://doi.org/10.1016/j.celrep.2022.111115
出版状态	已出版 - 19 7月 2022
已对外发布	是

联合国可持续发展目标

此成果有助于实现下列可持续发展目标：

可持续发展目标 3 良好健康与福祉

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10.1016/j.celrep.2022.111115

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Chiang, C. L., Hu, E. Y., Chang, L., Labanowska, J., Zapolnik, K., Mo, X., Shi, J., Doong, T. J., Lozanski, A., Yan, P. S., Bundschuh, R., Walker, L. A., Gallego-Perez, D., Lu, W., Long, M., Kim, S., Heerema, N. A., Lozanski, G., Woyach, J. A., ... Muthusamy, N. (2022). Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity. Cell Reports, 40(3), 文章 111115. https://doi.org/10.1016/j.celrep.2022.111115

@article{b7b14f45fc0c4a0ca4369f540469fcec,

title = "Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity",

abstract = "The existence of “leukemia-initiating cells” (LICs) in chronic lymphocytic leukemia (CLL) remains controversial due to the difficulty in isolating and identifying the tumor-initiating cells. Here, we demonstrate a microchannel electroporation (MEP) microarray that injects RNA-detecting probes into single live cells, allowing the imaging and characterization of heterogeneous LICs by intracellular RNA expression. Using limited-cell FACS sequencing (LC-FACSeq), we can detect and monitor rare live LICs during leukemogenesis and characterize their differential drug sensitivity. Disease-associated mutation accumulation in developing B lymphoid but not myeloid lineage in CLL patient hematopoietic stem cells (CLL-HSCs), and development of independent clonal CLL-like cells in murine patient-derived xenograft models, suggests the existence of CLL LICs. Furthermore, we identify differential protein ubiquitination and unfolding response signatures in GATA2high CLL-HSCs that exhibit increased sensitivity to lenalidomide and resistance to fludarabine compared to GATA2lowCLL-HSCs. These results highlight the existence of therapeutically targetable disease precursors in CLL.",

keywords = "CP: Cancer, GATA2, IKZF1, LC-FACSeq, chronic lymphocytic leukemia, fludarabine, lenalidomide, leukemia initiating cells, single-cell analysis, stem cells",

author = "Chiang, \{Chi Ling\} and Hu, \{Eileen Y.\} and Lingqian Chang and Jadwiga Labanowska and Kevan Zapolnik and Xiaokui Mo and Junfeng Shi and Doong, \{Tzyy Jye\} and Arletta Lozanski and Yan, \{Pearlly S.\} and Ralf Bundschuh and Walker, \{Logan A.\} and Daniel Gallego-Perez and Wu Lu and Meixiao Long and Sanggu Kim and Heerema, \{Nyla A.\} and Gerard Lozanski and Woyach, \{Jennifer A.\} and Byrd, \{John C.\} and Lee, \{Ly James\} and Natarajan Muthusamy",

note = "Publisher Copyright: {\textcopyright} 2022",

year = "2022",

month = jul,

day = "19",

doi = "10.1016/j.celrep.2022.111115",

language = "英语",

volume = "40",

journal = "Cell Reports",

issn = "2639-1856",

publisher = "Elsevier B.V.",

number = "3",

}

Chiang, CL, Hu, EY, Chang, L, Labanowska, J, Zapolnik, K, Mo, X, Shi, J, Doong, TJ, Lozanski, A, Yan, PS, Bundschuh, R, Walker, LA, Gallego-Perez, D, Lu, W, Long, M, Kim, S, Heerema, NA, Lozanski, G, Woyach, JA, Byrd, JC, Lee, LJ & Muthusamy, N 2022, 'Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity', Cell Reports, 卷 40, 号码 3, 111115. https://doi.org/10.1016/j.celrep.2022.111115

TY - JOUR

T1 - Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity

AU - Chiang, Chi Ling

AU - Hu, Eileen Y.

AU - Chang, Lingqian

AU - Labanowska, Jadwiga

AU - Zapolnik, Kevan

AU - Mo, Xiaokui

AU - Shi, Junfeng

AU - Doong, Tzyy Jye

AU - Lozanski, Arletta

AU - Yan, Pearlly S.

AU - Bundschuh, Ralf

AU - Walker, Logan A.

AU - Gallego-Perez, Daniel

AU - Lu, Wu

AU - Long, Meixiao

AU - Kim, Sanggu

AU - Heerema, Nyla A.

AU - Lozanski, Gerard

AU - Woyach, Jennifer A.

AU - Byrd, John C.

AU - Lee, Ly James

AU - Muthusamy, Natarajan

PY - 2022/7/19

Y1 - 2022/7/19

N2 - The existence of “leukemia-initiating cells” (LICs) in chronic lymphocytic leukemia (CLL) remains controversial due to the difficulty in isolating and identifying the tumor-initiating cells. Here, we demonstrate a microchannel electroporation (MEP) microarray that injects RNA-detecting probes into single live cells, allowing the imaging and characterization of heterogeneous LICs by intracellular RNA expression. Using limited-cell FACS sequencing (LC-FACSeq), we can detect and monitor rare live LICs during leukemogenesis and characterize their differential drug sensitivity. Disease-associated mutation accumulation in developing B lymphoid but not myeloid lineage in CLL patient hematopoietic stem cells (CLL-HSCs), and development of independent clonal CLL-like cells in murine patient-derived xenograft models, suggests the existence of CLL LICs. Furthermore, we identify differential protein ubiquitination and unfolding response signatures in GATA2high CLL-HSCs that exhibit increased sensitivity to lenalidomide and resistance to fludarabine compared to GATA2lowCLL-HSCs. These results highlight the existence of therapeutically targetable disease precursors in CLL.

AB - The existence of “leukemia-initiating cells” (LICs) in chronic lymphocytic leukemia (CLL) remains controversial due to the difficulty in isolating and identifying the tumor-initiating cells. Here, we demonstrate a microchannel electroporation (MEP) microarray that injects RNA-detecting probes into single live cells, allowing the imaging and characterization of heterogeneous LICs by intracellular RNA expression. Using limited-cell FACS sequencing (LC-FACSeq), we can detect and monitor rare live LICs during leukemogenesis and characterize their differential drug sensitivity. Disease-associated mutation accumulation in developing B lymphoid but not myeloid lineage in CLL patient hematopoietic stem cells (CLL-HSCs), and development of independent clonal CLL-like cells in murine patient-derived xenograft models, suggests the existence of CLL LICs. Furthermore, we identify differential protein ubiquitination and unfolding response signatures in GATA2high CLL-HSCs that exhibit increased sensitivity to lenalidomide and resistance to fludarabine compared to GATA2lowCLL-HSCs. These results highlight the existence of therapeutically targetable disease precursors in CLL.

KW - CP: Cancer

KW - GATA2

KW - IKZF1

KW - LC-FACSeq

KW - chronic lymphocytic leukemia

KW - fludarabine

KW - lenalidomide

KW - leukemia initiating cells

KW - single-cell analysis

KW - stem cells

UR - https://www.scopus.com/pages/publications/85134761023

U2 - 10.1016/j.celrep.2022.111115

DO - 10.1016/j.celrep.2022.111115

M3 - 文章

C2 - 35858552

AN - SCOPUS:85134761023

SN - 2639-1856

VL - 40

JO - Cell Reports

JF - Cell Reports

IS - 3

M1 - 111115

ER -

Leukemia-initiating HSCs in chronic lymphocytic leukemia reveal clonal leukemogenesis and differential drug sensitivity

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