The bipartite TAD organization of the X-inactivation center ensures opposing developmental regulation of Tsix and Xist

Joke G. van Bemmel; Rafael Galupa; Chris Gard; Nicolas Servant; Christel Picard; James Davies; Anthony James Szempruch; Yinxiu Zhan; Jan J. Żylicz; Elphège P. Nora; Sonia Lameiras; Elzo de Wit; David Gentien; Sylvain Baulande; Luca Giorgetti; Mitchell Guttman; Jim R. Hughes; Douglas R. Higgs; Joost Gribnau; Edith Heard

doi:10.1038/s41588-019-0412-0

The bipartite TAD organization of the X-inactivation center ensures opposing developmental regulation of Tsix and Xist

Joke G. van Bemmel^*, Rafael Galupa, Chris Gard, Nicolas Servant, Christel Picard, James Davies, Anthony James Szempruch, Yinxiu Zhan, Jan J. Żylicz, Elphège P. Nora, Sonia Lameiras, Elzo de Wit, David Gentien, Sylvain Baulande, Luca Giorgetti, Mitchell Guttman, Jim R. Hughes, Douglas R. Higgs, Joost Gribnau, Edith Heard

^*Corresponding author af dette arbejde

Publikation: Bidrag til tidsskrift › Tidsskriftartikel › Forskning › peer review

56 Citationer (Scopus)

Abstract

The mouse X-inactivation center (Xic) locus represents a powerful model for understanding the links between genome architecture and gene regulation, with the non-coding genes Xist and Tsix showing opposite developmental expression patterns while being organized as an overlapping sense/antisense unit. The Xic is organized into two topologically associating domains (TADs) but the role of this architecture in orchestrating cis-regulatory information remains elusive. To explore this, we generated genomic inversions that swap the Xist/Tsix transcriptional unit and place their promoters in each other’s TAD. We found that this led to a switch in their expression dynamics: Xist became precociously and ectopically upregulated, both in male and female pluripotent cells, while Tsix expression aberrantly persisted during differentiation. The topological partitioning of the Xic is thus critical to ensure proper developmental timing of X inactivation. Our study illustrates how the genomic architecture of cis-regulatory landscapes can affect the regulation of mammalian developmental processes.

Originalsprog	Engelsk
Tidsskrift	Nature Genetics
Vol/bind	51
Udgave nummer	6
Sider (fra-til)	1024-1034
Antal sider	11
ISSN	1061-4036
DOI	https://doi.org/10.1038/s41588-019-0412-0
Status	Udgivet - 1 jun. 2019
Udgivet eksternt	Ja

Bibliografisk note

Publisher Copyright:
© 2019, The Author(s), under exclusive licence to Springer Nature America, Inc.

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10.1038/s41588-019-0412-0

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Citationsformater

van Bemmel, J. G., Galupa, R., Gard, C., Servant, N., Picard, C., Davies, J., Szempruch, A. J., Zhan, Y., Żylicz, J. J., Nora, E. P., Lameiras, S., de Wit, E., Gentien, D., Baulande, S., Giorgetti, L., Guttman, M., Hughes, J. R., Higgs, D. R., Gribnau, J., & Heard, E. (2019). The bipartite TAD organization of the X-inactivation center ensures opposing developmental regulation of Tsix and Xist. Nature Genetics, 51(6), 1024-1034. https://doi.org/10.1038/s41588-019-0412-0

van Bemmel, JG, Galupa, R, Gard, C, Servant, N, Picard, C, Davies, J, Szempruch, AJ, Zhan, Y, Żylicz, JJ, Nora, EP, Lameiras, S, de Wit, E, Gentien, D, Baulande, S, Giorgetti, L, Guttman, M, Hughes, JR, Higgs, DR, Gribnau, J & Heard, E 2019, 'The bipartite TAD organization of the X-inactivation center ensures opposing developmental regulation of Tsix and Xist', Nature Genetics, bind 51, nr. 6, s. 1024-1034. https://doi.org/10.1038/s41588-019-0412-0

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title = "The bipartite TAD organization of the X-inactivation center ensures opposing developmental regulation of Tsix and Xist",

abstract = "The mouse X-inactivation center (Xic) locus represents a powerful model for understanding the links between genome architecture and gene regulation, with the non-coding genes Xist and Tsix showing opposite developmental expression patterns while being organized as an overlapping sense/antisense unit. The Xic is organized into two topologically associating domains (TADs) but the role of this architecture in orchestrating cis-regulatory information remains elusive. To explore this, we generated genomic inversions that swap the Xist/Tsix transcriptional unit and place their promoters in each other{\textquoteright}s TAD. We found that this led to a switch in their expression dynamics: Xist became precociously and ectopically upregulated, both in male and female pluripotent cells, while Tsix expression aberrantly persisted during differentiation. The topological partitioning of the Xic is thus critical to ensure proper developmental timing of X inactivation. Our study illustrates how the genomic architecture of cis-regulatory landscapes can affect the regulation of mammalian developmental processes.",

author = "{van Bemmel}, {Joke G.} and Rafael Galupa and Chris Gard and Nicolas Servant and Christel Picard and James Davies and Szempruch, {Anthony James} and Yinxiu Zhan and {\.Z}ylicz, {Jan J.} and Nora, {Elph{\`e}ge P.} and Sonia Lameiras and {de Wit}, Elzo and David Gentien and Sylvain Baulande and Luca Giorgetti and Mitchell Guttman and Hughes, {Jim R.} and Higgs, {Douglas R.} and Joost Gribnau and Edith Heard",

note = "Funding Information: We would like to thank the Heard laboratory for their technical input and critical discussions; D. Noordermeer for critical discussion and advice on Capture-C data analysis and interpretation; A. Chow from the Guttman laboratory for RAP-DNA cell culture; members of the Bourc{\textquoteright}his laboratory; C. Reyes and A. Rapinat from the Nanostring platform and J. M. Telenius, M. Oudelaar and D. Downes from the Hughes and Higgs laboratories. This work was supported by an ERC Advanced Investigator award (ERC-2014-AdG no. 671027), Labelisation La Ligue, FRM (grant no. DEI20151234398), ANR DoseX 2017, Labex DEEP (no. ANR-11-LBX-0044), part of the IDEX Idex PSL (no. ANR-10-IDEX-0001-02 PSL) and ABS4NGS (no. ANR-11-BINF-0001) to E.H.; NWO-ALW Rubicon (no. 825.13.002) and Veni (no. 863.15.016) fellowships to J.G.v.B.; R{\'e}gion Ile-de-France (DIM Bioth{\'e}rapies) and Fondation pour la Recherche M{\'e}dicale (no. FDT20160435295) fellowships to R.G.; Sir Henry Wellcome Postdoctoral Fellowship (no. 201369/Z/16/Z) to J.J.Z.; MRC Clinician Scientist Fellowship (no. MR/R008108) to J.D.; Wellcome Trust Strategic Award (no. 106130/Z/14/Z) to J.R.H.; New York Stem Cell Foundation and California Institute of Technology funds to M.G. (M.G. is a New York Stem Cell Foundation—Robertson Investigator); Novartis Foundation and European Research Council (ERC) under the European Union{\textquoteright}s Horizon 2020 research and innovation programme (grant agreement no. 759366 {\textquoteleft}BioMeTre{\textquoteright}) to L.G.; LabEx and EquipEx (nos. ANR-10-IDEX-0001-02 PSL, ANR-11-LBX-0044 and {\textquoteleft}INCa-DGOS-4654{\textquoteright} SIRIC11-002) to the Nanostring platform of Institut Curie; Equipex (no. ANR-10-EQPX-03), France G{\'e}nomique Consortium from the Agence Nationale de la Recherche ({\textquoteleft}Investissements d{\textquoteright}Avenir{\textquoteright} program; no. ANR-10-INBS-09-08) and Canceropole Ile-de-France and by the SiRIC-Curie program—SiRIC grant (no. INCa-DGOS-4654) to the ICGex Next Generation Sequencing platform of the Institut Curie. Publisher Copyright: {\textcopyright} 2019, The Author(s), under exclusive licence to Springer Nature America, Inc.",

year = "2019",

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doi = "10.1038/s41588-019-0412-0",

language = "English",

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T1 - The bipartite TAD organization of the X-inactivation center ensures opposing developmental regulation of Tsix and Xist

AU - van Bemmel, Joke G.

AU - Galupa, Rafael

AU - Gard, Chris

AU - Servant, Nicolas

AU - Picard, Christel

AU - Davies, James

AU - Szempruch, Anthony James

AU - Zhan, Yinxiu

AU - Żylicz, Jan J.

AU - Nora, Elphège P.

AU - Lameiras, Sonia

AU - de Wit, Elzo

AU - Gentien, David

AU - Baulande, Sylvain

AU - Giorgetti, Luca

AU - Guttman, Mitchell

AU - Hughes, Jim R.

AU - Higgs, Douglas R.

AU - Gribnau, Joost

AU - Heard, Edith

N1 - Funding Information: We would like to thank the Heard laboratory for their technical input and critical discussions; D. Noordermeer for critical discussion and advice on Capture-C data analysis and interpretation; A. Chow from the Guttman laboratory for RAP-DNA cell culture; members of the Bourc’his laboratory; C. Reyes and A. Rapinat from the Nanostring platform and J. M. Telenius, M. Oudelaar and D. Downes from the Hughes and Higgs laboratories. This work was supported by an ERC Advanced Investigator award (ERC-2014-AdG no. 671027), Labelisation La Ligue, FRM (grant no. DEI20151234398), ANR DoseX 2017, Labex DEEP (no. ANR-11-LBX-0044), part of the IDEX Idex PSL (no. ANR-10-IDEX-0001-02 PSL) and ABS4NGS (no. ANR-11-BINF-0001) to E.H.; NWO-ALW Rubicon (no. 825.13.002) and Veni (no. 863.15.016) fellowships to J.G.v.B.; Région Ile-de-France (DIM Biothérapies) and Fondation pour la Recherche Médicale (no. FDT20160435295) fellowships to R.G.; Sir Henry Wellcome Postdoctoral Fellowship (no. 201369/Z/16/Z) to J.J.Z.; MRC Clinician Scientist Fellowship (no. MR/R008108) to J.D.; Wellcome Trust Strategic Award (no. 106130/Z/14/Z) to J.R.H.; New York Stem Cell Foundation and California Institute of Technology funds to M.G. (M.G. is a New York Stem Cell Foundation—Robertson Investigator); Novartis Foundation and European Research Council (ERC) under the European Union’s Horizon 2020 research and innovation programme (grant agreement no. 759366 ‘BioMeTre’) to L.G.; LabEx and EquipEx (nos. ANR-10-IDEX-0001-02 PSL, ANR-11-LBX-0044 and ‘INCa-DGOS-4654’ SIRIC11-002) to the Nanostring platform of Institut Curie; Equipex (no. ANR-10-EQPX-03), France Génomique Consortium from the Agence Nationale de la Recherche (‘Investissements d’Avenir’ program; no. ANR-10-INBS-09-08) and Canceropole Ile-de-France and by the SiRIC-Curie program—SiRIC grant (no. INCa-DGOS-4654) to the ICGex Next Generation Sequencing platform of the Institut Curie. Publisher Copyright: © 2019, The Author(s), under exclusive licence to Springer Nature America, Inc.

PY - 2019/6/1

Y1 - 2019/6/1

N2 - The mouse X-inactivation center (Xic) locus represents a powerful model for understanding the links between genome architecture and gene regulation, with the non-coding genes Xist and Tsix showing opposite developmental expression patterns while being organized as an overlapping sense/antisense unit. The Xic is organized into two topologically associating domains (TADs) but the role of this architecture in orchestrating cis-regulatory information remains elusive. To explore this, we generated genomic inversions that swap the Xist/Tsix transcriptional unit and place their promoters in each other’s TAD. We found that this led to a switch in their expression dynamics: Xist became precociously and ectopically upregulated, both in male and female pluripotent cells, while Tsix expression aberrantly persisted during differentiation. The topological partitioning of the Xic is thus critical to ensure proper developmental timing of X inactivation. Our study illustrates how the genomic architecture of cis-regulatory landscapes can affect the regulation of mammalian developmental processes.

AB - The mouse X-inactivation center (Xic) locus represents a powerful model for understanding the links between genome architecture and gene regulation, with the non-coding genes Xist and Tsix showing opposite developmental expression patterns while being organized as an overlapping sense/antisense unit. The Xic is organized into two topologically associating domains (TADs) but the role of this architecture in orchestrating cis-regulatory information remains elusive. To explore this, we generated genomic inversions that swap the Xist/Tsix transcriptional unit and place their promoters in each other’s TAD. We found that this led to a switch in their expression dynamics: Xist became precociously and ectopically upregulated, both in male and female pluripotent cells, while Tsix expression aberrantly persisted during differentiation. The topological partitioning of the Xic is thus critical to ensure proper developmental timing of X inactivation. Our study illustrates how the genomic architecture of cis-regulatory landscapes can affect the regulation of mammalian developmental processes.

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