Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells

I. Wen Teng; Pei Chi Hou; Kuan Der Lee; Pei Yi Chu; Kun Tu Yeh; Victor X. Jin; Min Jen Tseng; Shaw Jenq Tsai; Yu Sun Chang; Chi Sheng Wu; H. Sunny Sun; Kuen Daw Tsai; Long Bin Jeng; Kenneth P. Nephew; Tim H.M. Huang; Shu Huei Hsiao; Yu Wei Leu

doi:10.1158/0008-5472.CAN-10-3418

Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells

I. Wen Teng
, Pei Chi Hou
, Kuan Der Lee
, Pei Yi Chu
, Kun Tu Yeh
, Victor X. Jin
, Min Jen Tseng
, Shaw Jenq Tsai
, Yu Sun Chang
, Chi Sheng Wu
, H. Sunny Sun
, Kuen Daw Tsai
, Long Bin Jeng
, Kenneth P. Nephew
, Tim H.M. Huang
, Shu Huei Hsiao^*
, Yu Wei Leu

^*Corresponding author for this work

National Chung Cheng University
Chang Gung Memorial Hospital
Changhua Christian Hospital
Ohio State University
National Cheng Kung University
Chang Gung University
China Medical University Taichung
Indiana University Bloomington

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

95 Scopus citations

Abstract

Although DNA hypermethylation within promoter CpG islands is highly correlated with tumorigenesis, it has not been established whether DNA hypermethylation within a specific tumor suppressor gene (TSG) is sufficient to fully transform a somatic stem cell. In this study, we addressed this question using a novel targeted DNA methylation technique to methylate the promoters of HIC1 and RassF1A, two well-established TSGs, along with a two-component reporter system to visualize successful targeting of human bone marrow-derived mesenchymal stem cells (MSC) as a model cell system. MSCs harboring targeted promoter methylations of HIC1/RassF1A displayed several features of cancer stem/initiating cells including loss of anchorage dependence, increased colony formation capability, drug resistance, and pluripotency. Notably, inoculation of immunodeficient mice with low numbers of targeted MSC resulted in tumor formation, and subsequent serial xenotransplantation and immunohistochemistry confirmed the presence of stem cell markers and MSC lineage in tumor xenografts. Consistent with the expected mechanism of TSG hypermethylation, treatment of the targeted MSC with a DNA methyltransferase inhibitor reversed their tumorigenic phenotype. To our knowledge, this is the first direct demonstration that aberrant TSG hypermethylation is sufficient to transform a somatic stem cell into a fully malignant cell with cancer stem/initiating properties.

Original language	English
Pages (from-to)	4653-4663
Number of pages	11
Journal	Cancer Research
Volume	71
Issue number	13
DOIs	https://doi.org/10.1158/0008-5472.CAN-10-3418
State	Published - 01 07 2011
Externally published	Yes

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

Access to Document

10.1158/0008-5472.CAN-10-3418

Cite this

Teng, I. W., Hou, P. C., Lee, K. D., Chu, P. Y., Yeh, K. T., Jin, V. X., Tseng, M. J., Tsai, S. J., Chang, Y. S., Wu, C. S., Sun, H. S., Tsai, K. D., Jeng, L. B., Nephew, K. P., Huang, T. H. M., Hsiao, S. H., & Leu, Y. W. (2011). Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells. Cancer Research, 71(13), 4653-4663. https://doi.org/10.1158/0008-5472.CAN-10-3418

@article{608c17ebfe75402fb008467c21ea5997,

title = "Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells",

abstract = "Although DNA hypermethylation within promoter CpG islands is highly correlated with tumorigenesis, it has not been established whether DNA hypermethylation within a specific tumor suppressor gene (TSG) is sufficient to fully transform a somatic stem cell. In this study, we addressed this question using a novel targeted DNA methylation technique to methylate the promoters of HIC1 and RassF1A, two well-established TSGs, along with a two-component reporter system to visualize successful targeting of human bone marrow-derived mesenchymal stem cells (MSC) as a model cell system. MSCs harboring targeted promoter methylations of HIC1/RassF1A displayed several features of cancer stem/initiating cells including loss of anchorage dependence, increased colony formation capability, drug resistance, and pluripotency. Notably, inoculation of immunodeficient mice with low numbers of targeted MSC resulted in tumor formation, and subsequent serial xenotransplantation and immunohistochemistry confirmed the presence of stem cell markers and MSC lineage in tumor xenografts. Consistent with the expected mechanism of TSG hypermethylation, treatment of the targeted MSC with a DNA methyltransferase inhibitor reversed their tumorigenic phenotype. To our knowledge, this is the first direct demonstration that aberrant TSG hypermethylation is sufficient to transform a somatic stem cell into a fully malignant cell with cancer stem/initiating properties.",

author = "Teng, \{I. Wen\} and Hou, \{Pei Chi\} and Lee, \{Kuan Der\} and Chu, \{Pei Yi\} and Yeh, \{Kun Tu\} and Jin, \{Victor X.\} and Tseng, \{Min Jen\} and Tsai, \{Shaw Jenq\} and Chang, \{Yu Sun\} and Wu, \{Chi Sheng\} and Sun, \{H. Sunny\} and Tsai, \{Kuen Daw\} and Jeng, \{Long Bin\} and Nephew, \{Kenneth P.\} and Huang, \{Tim H.M.\} and Hsiao, \{Shu Huei\} and Leu, \{Yu Wei\}",

year = "2011",

month = jul,

day = "1",

doi = "10.1158/0008-5472.CAN-10-3418",

language = "英语",

volume = "71",

pages = "4653--4663",

journal = "Cancer Research",

issn = "0008-5472",

publisher = "American Association for Cancer Research Inc.",

number = "13",

}

Teng, IW, Hou, PC, Lee, KD, Chu, PY, Yeh, KT, Jin, VX, Tseng, MJ, Tsai, SJ, Chang, YS, Wu, CS, Sun, HS, Tsai, KD, Jeng, LB, Nephew, KP, Huang, THM, Hsiao, SH & Leu, YW 2011, 'Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells', Cancer Research, vol. 71, no. 13, pp. 4653-4663. https://doi.org/10.1158/0008-5472.CAN-10-3418

TY - JOUR

T1 - Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells

AU - Teng, I. Wen

AU - Hou, Pei Chi

AU - Lee, Kuan Der

AU - Chu, Pei Yi

AU - Yeh, Kun Tu

AU - Jin, Victor X.

AU - Tseng, Min Jen

AU - Tsai, Shaw Jenq

AU - Chang, Yu Sun

AU - Wu, Chi Sheng

AU - Sun, H. Sunny

AU - Tsai, Kuen Daw

AU - Jeng, Long Bin

AU - Nephew, Kenneth P.

AU - Huang, Tim H.M.

AU - Hsiao, Shu Huei

AU - Leu, Yu Wei

PY - 2011/7/1

Y1 - 2011/7/1

N2 - Although DNA hypermethylation within promoter CpG islands is highly correlated with tumorigenesis, it has not been established whether DNA hypermethylation within a specific tumor suppressor gene (TSG) is sufficient to fully transform a somatic stem cell. In this study, we addressed this question using a novel targeted DNA methylation technique to methylate the promoters of HIC1 and RassF1A, two well-established TSGs, along with a two-component reporter system to visualize successful targeting of human bone marrow-derived mesenchymal stem cells (MSC) as a model cell system. MSCs harboring targeted promoter methylations of HIC1/RassF1A displayed several features of cancer stem/initiating cells including loss of anchorage dependence, increased colony formation capability, drug resistance, and pluripotency. Notably, inoculation of immunodeficient mice with low numbers of targeted MSC resulted in tumor formation, and subsequent serial xenotransplantation and immunohistochemistry confirmed the presence of stem cell markers and MSC lineage in tumor xenografts. Consistent with the expected mechanism of TSG hypermethylation, treatment of the targeted MSC with a DNA methyltransferase inhibitor reversed their tumorigenic phenotype. To our knowledge, this is the first direct demonstration that aberrant TSG hypermethylation is sufficient to transform a somatic stem cell into a fully malignant cell with cancer stem/initiating properties.

AB - Although DNA hypermethylation within promoter CpG islands is highly correlated with tumorigenesis, it has not been established whether DNA hypermethylation within a specific tumor suppressor gene (TSG) is sufficient to fully transform a somatic stem cell. In this study, we addressed this question using a novel targeted DNA methylation technique to methylate the promoters of HIC1 and RassF1A, two well-established TSGs, along with a two-component reporter system to visualize successful targeting of human bone marrow-derived mesenchymal stem cells (MSC) as a model cell system. MSCs harboring targeted promoter methylations of HIC1/RassF1A displayed several features of cancer stem/initiating cells including loss of anchorage dependence, increased colony formation capability, drug resistance, and pluripotency. Notably, inoculation of immunodeficient mice with low numbers of targeted MSC resulted in tumor formation, and subsequent serial xenotransplantation and immunohistochemistry confirmed the presence of stem cell markers and MSC lineage in tumor xenografts. Consistent with the expected mechanism of TSG hypermethylation, treatment of the targeted MSC with a DNA methyltransferase inhibitor reversed their tumorigenic phenotype. To our knowledge, this is the first direct demonstration that aberrant TSG hypermethylation is sufficient to transform a somatic stem cell into a fully malignant cell with cancer stem/initiating properties.

UR - https://www.scopus.com/pages/publications/79959868249

U2 - 10.1158/0008-5472.CAN-10-3418

DO - 10.1158/0008-5472.CAN-10-3418

M3 - 文章

C2 - 21518779

AN - SCOPUS:79959868249

SN - 0008-5472

VL - 71

SP - 4653

EP - 4663

JO - Cancer Research

JF - Cancer Research

IS - 13

ER -

Targeted methylation of two tumor suppressor genes is sufficient to transform mesenchymal stem cells into cancer stem/initiating cells

Abstract

UN SDGs

Access to Document

Other files and links

Fingerprint

Cite this