4.2 Article

Single-cell cloning of human T-cell lines reveals clonal variation in cell death responses to chemotherapeutics

期刊

CANCER GENETICS
卷 237, 期 -, 页码 69-77

出版社

ELSEVIER SCIENCE INC
DOI: 10.1016/j.cancergen.2019.06.003

关键词

Cell death; Leukemia; Cloning; T-ALL; Chemotherapeutic resistance

资金

  1. V Foundation for Cancer Research
  2. Alex's Lemonade Stand Foundation
  3. Gabrielle's Angel Foundation for Cancer Research
  4. National Institute of Health [R56 AI103352]
  5. Howard Hughes Medical Institute Medical Student Research Fellowship
  6. Harvard Stem Cell Institute

向作者/读者索取更多资源

Genetic modification of human leukemic cell lines using CRISPR-Cas9 has become a staple of gene-function studies. Single-cell cloning of modified cells is frequently used to facilitate studies of gene function. Inherent in this approach is an assumption that the genetic drift, amplified in some cell lines by mutations in DNA replication and repair machinery, as well as non-genetic factors will not introduce significant levels of experimental cellular heterogeneity in clones derived from parental populations. In this study, we characterize the variation in cell death of fifty clonal cell lines generated from human Jurkat and MOLT-4 T-cells edited by CRISPR-Cas9. We demonstrate a wide distribution of sensitivity to chemotherapeutics between non-edited clonal human leukemia T-cell lines, and also following CRISPR-Cas9 editing at the NLRP1 locus, or following transfection with non-targeting sgRNA controls. The cell death sensitivity profile of clonal cell lines was consistent across experiments and failed to revert to the non-clonal parental phenotype. Whole genome sequencing of two clonal cell lines edited by CRISPR-Cas9 revealed unique and shared genetic variants, which had minimal read support in the non-clonal parental population and were not suspected CRISPR-Cas9 off-target effects. These variants included genes related to cell death and drug metabolism. The variation in cell death phenotype of clonal populations of human T-cell lines may be a consequence of T-cell line genetic instability, and to a lesser extent clonal heterogeneity in the parental population or CRISPR-Cas9 off-target effects not predicted by current models. This work highlights the importance of genetic variation between clonal T-cell lines in the design, conduct, and analysis of experiments to investigate gene function after single-cell cloning.

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