Transcriptionally active HERV-H retrotransposons demarcate topologically associating domains in human pluripotent stem cells

Yanxiao Zhang; Ting Li; Sebastian Preissl; Maria Luisa Amaral; Jonathan D. Grinstein; Elie N. Farah; Eugin Destici; Yunjiang Qiu; Rong Hu; Ah Young Lee; Sora Chee; Kaiyue Ma; Zhen Ye; Quan Zhu; Hui Huang; Rongxin Fang; Leqian Yu; Juan Carlos Izpisua Belmonte; Jun Wu; Sylvia M. Evans; Neil C. Chi; Bing Ren

doi:10.1038/s41588-019-0479-7

Transcriptionally active HERV-H retrotransposons demarcate topologically associating domains in human pluripotent stem cells

Yanxiao Zhang, Ting Li, Sebastian Preissl, Maria Luisa Amaral, Jonathan D. Grinstein, Elie N. Farah, Eugin Destici, Yunjiang Qiu, Rong Hu, Ah Young Lee, Sora Chee, Kaiyue Ma, Zhen Ye, Quan Zhu, Hui Huang, Rongxin Fang, Leqian Yu, Juan Carlos Izpisua Belmonte, Jun Wu, Sylvia M. EvansNeil C. Chi, Bing Ren

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

174 Scopus citations

Abstract

Chromatin architecture has been implicated in cell type-specific gene regulatory programs, yet how chromatin remodels during development remains to be fully elucidated. Here, by interrogating chromatin reorganization during human pluripotent stem cell (hPSC) differentiation, we discover a role for the primate-specific endogenous retrotransposon human endogenous retrovirus subfamily H (HERV-H) in creating topologically associating domains (TADs) in hPSCs. Deleting these HERV-H elements eliminates their corresponding TAD boundaries and reduces the transcription of upstream genes, while de novo insertion of HERV-H elements can introduce new TAD boundaries. The ability of HERV-H to create TAD boundaries depends on high transcription, as transcriptional repression of HERV-H elements prevents the formation of boundaries. This ability is not limited to hPSCs, as these actively transcribed HERV-H elements and their corresponding TAD boundaries also appear in pluripotent stem cells from other hominids but not in more distantly related species lacking HERV-H elements. Overall, our results provide direct evidence for retrotransposons in actively shaping cell type- and species-specific chromatin architecture.

Original language	English (US)
Pages (from-to)	1380-1388
Number of pages	9
Journal	Nature genetics
Volume	51
Issue number	9
DOIs	https://doi.org/10.1038/s41588-019-0479-7
State	Published - Sep 1 2019

ASJC Scopus subject areas

Genetics

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Zhang, Y., Li, T., Preissl, S., Amaral, M. L., Grinstein, J. D., Farah, E. N., Destici, E., Qiu, Y., Hu, R., Lee, A. Y., Chee, S., Ma, K., Ye, Z., Zhu, Q., Huang, H., Fang, R., Yu, L., Izpisua Belmonte, J. C., Wu, J., ... Ren, B. (2019). Transcriptionally active HERV-H retrotransposons demarcate topologically associating domains in human pluripotent stem cells. Nature genetics, 51(9), 1380-1388. https://doi.org/10.1038/s41588-019-0479-7

Zhang, Y, Li, T, Preissl, S, Amaral, ML, Grinstein, JD, Farah, EN, Destici, E, Qiu, Y, Hu, R, Lee, AY, Chee, S, Ma, K, Ye, Z, Zhu, Q, Huang, H, Fang, R, Yu, L, Izpisua Belmonte, JC, Wu, J, Evans, SM, Chi, NC & Ren, B 2019, 'Transcriptionally active HERV-H retrotransposons demarcate topologically associating domains in human pluripotent stem cells', Nature genetics, vol. 51, no. 9, pp. 1380-1388. https://doi.org/10.1038/s41588-019-0479-7

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title = "Transcriptionally active HERV-H retrotransposons demarcate topologically associating domains in human pluripotent stem cells",

abstract = "Chromatin architecture has been implicated in cell type-specific gene regulatory programs, yet how chromatin remodels during development remains to be fully elucidated. Here, by interrogating chromatin reorganization during human pluripotent stem cell (hPSC) differentiation, we discover a role for the primate-specific endogenous retrotransposon human endogenous retrovirus subfamily H (HERV-H) in creating topologically associating domains (TADs) in hPSCs. Deleting these HERV-H elements eliminates their corresponding TAD boundaries and reduces the transcription of upstream genes, while de novo insertion of HERV-H elements can introduce new TAD boundaries. The ability of HERV-H to create TAD boundaries depends on high transcription, as transcriptional repression of HERV-H elements prevents the formation of boundaries. This ability is not limited to hPSCs, as these actively transcribed HERV-H elements and their corresponding TAD boundaries also appear in pluripotent stem cells from other hominids but not in more distantly related species lacking HERV-H elements. Overall, our results provide direct evidence for retrotransposons in actively shaping cell type- and species-specific chromatin architecture.",

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AU - Grinstein, Jonathan D.

AU - Farah, Elie N.

AU - Destici, Eugin

AU - Qiu, Yunjiang

AU - Hu, Rong

AU - Lee, Ah Young

AU - Chee, Sora

AU - Ma, Kaiyue

AU - Ye, Zhen

AU - Zhu, Quan

AU - Huang, Hui

AU - Fang, Rongxin

AU - Yu, Leqian

AU - Izpisua Belmonte, Juan Carlos

AU - Wu, Jun

AU - Evans, Sylvia M.

AU - Chi, Neil C.

AU - Ren, Bing

PY - 2019/9/1

Y1 - 2019/9/1

N2 - Chromatin architecture has been implicated in cell type-specific gene regulatory programs, yet how chromatin remodels during development remains to be fully elucidated. Here, by interrogating chromatin reorganization during human pluripotent stem cell (hPSC) differentiation, we discover a role for the primate-specific endogenous retrotransposon human endogenous retrovirus subfamily H (HERV-H) in creating topologically associating domains (TADs) in hPSCs. Deleting these HERV-H elements eliminates their corresponding TAD boundaries and reduces the transcription of upstream genes, while de novo insertion of HERV-H elements can introduce new TAD boundaries. The ability of HERV-H to create TAD boundaries depends on high transcription, as transcriptional repression of HERV-H elements prevents the formation of boundaries. This ability is not limited to hPSCs, as these actively transcribed HERV-H elements and their corresponding TAD boundaries also appear in pluripotent stem cells from other hominids but not in more distantly related species lacking HERV-H elements. Overall, our results provide direct evidence for retrotransposons in actively shaping cell type- and species-specific chromatin architecture.

AB - Chromatin architecture has been implicated in cell type-specific gene regulatory programs, yet how chromatin remodels during development remains to be fully elucidated. Here, by interrogating chromatin reorganization during human pluripotent stem cell (hPSC) differentiation, we discover a role for the primate-specific endogenous retrotransposon human endogenous retrovirus subfamily H (HERV-H) in creating topologically associating domains (TADs) in hPSCs. Deleting these HERV-H elements eliminates their corresponding TAD boundaries and reduces the transcription of upstream genes, while de novo insertion of HERV-H elements can introduce new TAD boundaries. The ability of HERV-H to create TAD boundaries depends on high transcription, as transcriptional repression of HERV-H elements prevents the formation of boundaries. This ability is not limited to hPSCs, as these actively transcribed HERV-H elements and their corresponding TAD boundaries also appear in pluripotent stem cells from other hominids but not in more distantly related species lacking HERV-H elements. Overall, our results provide direct evidence for retrotransposons in actively shaping cell type- and species-specific chromatin architecture.

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Transcriptionally active HERV-H retrotransposons demarcate topologically associating domains in human pluripotent stem cells

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