Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues

Gilad Landan; Netta Mendelson Cohen; Zohar Mukamel; Amir Bar; Alina Molchadsky; Ran Brosh; Shirley Horn-Saban; Daniela Amann Zalcenstein; Naomi Goldfinger; Adi Zundelevich; Einav Nil Gal-Yam; Varda Rotter; Amos Tanay

doi:10.1038/ng.2442

Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues

Gilad Landan, Netta Mendelson Cohen, Zohar Mukamel, Amir Bar, Alina Molchadsky, Ran Brosh, Shirley Horn-Saban, Daniela Amann Zalcenstein, Naomi Goldfinger, Adi Zundelevich, Einav Nil Gal-Yam, Varda Rotter, Amos Tanay

Weizmann Institute of Science

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

Abstract

DNA methylation has been comprehensively profiled in normal and cancer cells, but the dynamics that form, maintain and reprogram differentially methylated regions remain enigmatic. Here, we show that methylation patterns within populations of cells from individual somatic tissues are heterogeneous and polymorphic. Using in vitro evolution of immortalized fibroblasts for over 300 generations, we track the dynamics of polymorphic methylation at regions developing significant differential methylation on average. The data indicate that changes in population-averaged methylation occur through a stochastic process that generates a stream of local and uncorrelated methylation aberrations. Despite the stochastic nature of the process, nearly deterministic epigenetic remodeling emerges on average at loci that lose or gain resistance to methylation accumulation. Changes in the susceptibility to methylation accumulation are correlated with changes in histone modification and CTCF occupancy. Characterizing epigenomic polymorphism within cell populations is therefore critical to understanding methylation dynamics in normal and cancer cells.

Original language	English
Pages (from-to)	1207-1214
Number of pages	8
Journal	Nature Genetics
Volume	44
Issue number	11
DOIs	https://doi.org/10.1038/ng.2442
State	Published - Nov 2012

All Science Journal Classification (ASJC) codes

Genetics

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10.1038/ng.2442

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Landan, G., Cohen, N. M., Mukamel, Z., Bar, A., Molchadsky, A., Brosh, R., Horn-Saban, S., Zalcenstein, D. A., Goldfinger, N., Zundelevich, A., Gal-Yam, E. N., Rotter, V., & Tanay, A. (2012). Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues. Nature Genetics, 44(11), 1207-1214. https://doi.org/10.1038/ng.2442

@article{8404aad25a62453f86a2e7b2c227ab1c,

title = "Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues",

abstract = "DNA methylation has been comprehensively profiled in normal and cancer cells, but the dynamics that form, maintain and reprogram differentially methylated regions remain enigmatic. Here, we show that methylation patterns within populations of cells from individual somatic tissues are heterogeneous and polymorphic. Using in vitro evolution of immortalized fibroblasts for over 300 generations, we track the dynamics of polymorphic methylation at regions developing significant differential methylation on average. The data indicate that changes in population-averaged methylation occur through a stochastic process that generates a stream of local and uncorrelated methylation aberrations. Despite the stochastic nature of the process, nearly deterministic epigenetic remodeling emerges on average at loci that lose or gain resistance to methylation accumulation. Changes in the susceptibility to methylation accumulation are correlated with changes in histone modification and CTCF occupancy. Characterizing epigenomic polymorphism within cell populations is therefore critical to understanding methylation dynamics in normal and cancer cells.",

author = "Gilad Landan and Cohen, \{Netta Mendelson\} and Zohar Mukamel and Amir Bar and Alina Molchadsky and Ran Brosh and Shirley Horn-Saban and Zalcenstein, \{Daniela Amann\} and Naomi Goldfinger and Adi Zundelevich and Gal-Yam, \{Einav Nil\} and Varda Rotter and Amos Tanay",

note = "Israel Science Foundation [1372/08]; European Commission Framework Programme 7 Network of Excellence EPIGENESYS; BLUEPRINT European Union consortium; Center of Excellence grant from the Flight Attendant Medical Research Institute (FAMRI)We thank the members of the Tanay group for discussions. Research in the Tanay laboratory was supported by grants from the Israel Science Foundation (grant 1372/08), the European Commission Framework Programme 7 Network of Excellence EPIGENESYS and the BLUEPRINT European Union consortium. Research in the Rotter laboratory was supported by a Center of Excellence grant from the Flight Attendant Medical Research Institute (FAMRI). E.N.G.-Y. is a fellow of the Talpiot Medical Leadership Program at the Sheba Medical Center.",

year = "2012",

month = nov,

doi = "10.1038/ng.2442",

language = "الإنجليزيّة",

volume = "44",

pages = "1207--1214",

journal = "Nature Genetics",

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Landan, G, Cohen, NM, Mukamel, Z, Bar, A, Molchadsky, A, Brosh, R, Horn-Saban, S, Zalcenstein, DA, Goldfinger, N, Zundelevich, A, Gal-Yam, EN, Rotter, V & Tanay, A 2012, 'Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues', Nature Genetics, vol. 44, no. 11, pp. 1207-1214. https://doi.org/10.1038/ng.2442

TY - JOUR

T1 - Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues

AU - Landan, Gilad

AU - Cohen, Netta Mendelson

AU - Mukamel, Zohar

AU - Bar, Amir

AU - Molchadsky, Alina

AU - Brosh, Ran

AU - Horn-Saban, Shirley

AU - Zalcenstein, Daniela Amann

AU - Goldfinger, Naomi

AU - Zundelevich, Adi

AU - Gal-Yam, Einav Nil

AU - Rotter, Varda

AU - Tanay, Amos

N1 - Israel Science Foundation [1372/08]; European Commission Framework Programme 7 Network of Excellence EPIGENESYS; BLUEPRINT European Union consortium; Center of Excellence grant from the Flight Attendant Medical Research Institute (FAMRI)We thank the members of the Tanay group for discussions. Research in the Tanay laboratory was supported by grants from the Israel Science Foundation (grant 1372/08), the European Commission Framework Programme 7 Network of Excellence EPIGENESYS and the BLUEPRINT European Union consortium. Research in the Rotter laboratory was supported by a Center of Excellence grant from the Flight Attendant Medical Research Institute (FAMRI). E.N.G.-Y. is a fellow of the Talpiot Medical Leadership Program at the Sheba Medical Center.

PY - 2012/11

Y1 - 2012/11

N2 - DNA methylation has been comprehensively profiled in normal and cancer cells, but the dynamics that form, maintain and reprogram differentially methylated regions remain enigmatic. Here, we show that methylation patterns within populations of cells from individual somatic tissues are heterogeneous and polymorphic. Using in vitro evolution of immortalized fibroblasts for over 300 generations, we track the dynamics of polymorphic methylation at regions developing significant differential methylation on average. The data indicate that changes in population-averaged methylation occur through a stochastic process that generates a stream of local and uncorrelated methylation aberrations. Despite the stochastic nature of the process, nearly deterministic epigenetic remodeling emerges on average at loci that lose or gain resistance to methylation accumulation. Changes in the susceptibility to methylation accumulation are correlated with changes in histone modification and CTCF occupancy. Characterizing epigenomic polymorphism within cell populations is therefore critical to understanding methylation dynamics in normal and cancer cells.

AB - DNA methylation has been comprehensively profiled in normal and cancer cells, but the dynamics that form, maintain and reprogram differentially methylated regions remain enigmatic. Here, we show that methylation patterns within populations of cells from individual somatic tissues are heterogeneous and polymorphic. Using in vitro evolution of immortalized fibroblasts for over 300 generations, we track the dynamics of polymorphic methylation at regions developing significant differential methylation on average. The data indicate that changes in population-averaged methylation occur through a stochastic process that generates a stream of local and uncorrelated methylation aberrations. Despite the stochastic nature of the process, nearly deterministic epigenetic remodeling emerges on average at loci that lose or gain resistance to methylation accumulation. Changes in the susceptibility to methylation accumulation are correlated with changes in histone modification and CTCF occupancy. Characterizing epigenomic polymorphism within cell populations is therefore critical to understanding methylation dynamics in normal and cancer cells.

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U2 - 10.1038/ng.2442

DO - 10.1038/ng.2442

M3 - مقالة

SN - 1061-4036

VL - 44

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EP - 1214

JO - Nature Genetics

JF - Nature Genetics

IS - 11

ER -

Epigenetic polymorphism and the stochastic formation of differentially methylated regions in normal and cancerous tissues

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