Author Correction: Pan-cancer analysis of whole genomes

David Townend; ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium

doi:10.1038/s41586-022-05598-w

Author Correction: Pan-cancer analysis of whole genomes

David Townend, ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium

Research output: Contribution to journal › Erratum / corrigendum / retractions › Academic

Abstract

Cell adhesion molecules are ubiquitous in multicellular organisms, specifying precise cell-cell interactions in processes as diverse as tissue development, immune cell trafficking and the wiring of the nervous system(1-4). Here we show that a wide array of synthetic cell adhesion molecules can be generated by combining orthogonal extracellular interactions with intracellular domains from native adhesion molecules, such as cadherins and integrins. The resulting molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions. The identity of the intracellular domain of the synthetic cell adhesion molecules specifies interface morphology and mechanics, whereas diverse homotypic or heterotypic extracellular interaction domains independently specify the connectivity between cells. This toolkit of orthogonal adhesion molecules enables the rationally programmed assembly of multicellular architectures, as well as systematic remodelling of native tissues. The modularity of synthetic cell adhesion molecules provides fundamental insights into how distinct classes of cell-cell interfaces may have evolved. Overall, these tools offer powerful abilities for cell and tissue engineering and for systematically studying multicellular organization. Synthetic cell adhesion molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions, and offer abilities for cell and tissue engineering and for systematically studying multicellular organization.

Original language	English
Pages (from-to)	E39
Number of pages	1
Journal	Nature
Volume	614
Issue number	7948
DOIs	https://doi.org/10.1038/s41586-022-05598-w
Publication status	Published - 16 Feb 2023

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1 Article

Pan-cancer analysis of whole genomes
Campbell, P. J., Getz, G., Korbel, J. O., Stuart, J. M., Jennings, J. L., Stein, L. D., Perry, M. D., Nahal-Bose, H. K., Ouellette, B. F. F., Li, C. H., Rheinbay, E., Nielsen, G. P., Sgroi, D. C., Wu, C. L., Faquin, W. C., Deshpande, V., Boutros, P. C., Lazar, A. J., Hoadley, K. A. & Louis, D. N. & 31 others, Dursi, L. J., Yung, C. K., Bailey, M. H., Saksena, G., Raine, K. M., Buchhalter, I., Kleinheinz, K., Schlesner, M., Zhang, J., Wang, W., Wheeler, D. A., Ding, L., Simpson, J. T., O'Connor, B. D., Yakneen, S., Ellrott, K., Miyoshi, N., Butler, A. P., Royo, R., Shorser, S. I., Vazquez, M., Rausch, T., Tiao, G., Waszak, S. M., Rodriguez-Martin, B., Shringarpure, S., Wu, D. Y., Demidov, G. M., Delaneau, O., Hayashi, S. & Townend, D., 6 Feb 2020, In: Nature. 578, 7793, p. 82-93 50 p.
Research output: Contribution to journal › Article › Academic › peer-review

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@article{f15573991a8b446a8bbbb1299fa58aea,

title = "Author Correction: Pan-cancer analysis of whole genomes",

abstract = "Cell adhesion molecules are ubiquitous in multicellular organisms, specifying precise cell-cell interactions in processes as diverse as tissue development, immune cell trafficking and the wiring of the nervous system(1-4). Here we show that a wide array of synthetic cell adhesion molecules can be generated by combining orthogonal extracellular interactions with intracellular domains from native adhesion molecules, such as cadherins and integrins. The resulting molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions. The identity of the intracellular domain of the synthetic cell adhesion molecules specifies interface morphology and mechanics, whereas diverse homotypic or heterotypic extracellular interaction domains independently specify the connectivity between cells. This toolkit of orthogonal adhesion molecules enables the rationally programmed assembly of multicellular architectures, as well as systematic remodelling of native tissues. The modularity of synthetic cell adhesion molecules provides fundamental insights into how distinct classes of cell-cell interfaces may have evolved. Overall, these tools offer powerful abilities for cell and tissue engineering and for systematically studying multicellular organization. Synthetic cell adhesion molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions, and offer abilities for cell and tissue engineering and for systematically studying multicellular organization.",

author = "Aaltonen, \{Lauri A.\} and Federico Abascal and Adam Abeshouse and Hiroyuki Aburatani and Adams, \{David J.\} and Nishant Agrawal and Ahn, \{Keun Soo\} and Ahn, \{Sung Min\} and Hiroshi Aikata and Rehan Akbani and Akdemir, \{Kadir C.\} and Hikmat Al-Ahmadie and Al-Sedairy, \{Sultan T.\} and Fatima Al-Shahrour and Malik Alawi and Monique Albert and Kenneth Aldape and Alexandrov, \{Ludmil B.\} and Adrian Ally and Kathryn Alsop and Alvarez, \{Eva G.\} and Fernanda Amary and Amin, \{Samirkumar B.\} and Brice Aminou and Ole Ammerpohl and Anderson, \{Matthew J.\} and Yeng Ang and Davide Antonello and Pavana Anur and Samuel Aparicio and Appelbaum, \{Elizabeth L.\} and Yasuhito Arai and Axel Aretz and Koji Arihiro and Ariizumi, \{Shun ichi\} and Joshua Armenia and Laurent Arnould and Sylvia Asa and Yassen Assenov and Gurnit Atwal and Sietse Aukema and Auman, \{J. Todd\} and Aure, \{Miriam R.R.\} and Philip Awadalla and Marta Aymerich and Bader, \{Gary D.\} and Adrian Baez-Ortega and Bailey, \{Matthew H.\} and Bailey, \{Peter J.\} and Miruna Balasundaram and David Townend and \{ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2023.",

year = "2023",

month = feb,

day = "16",

doi = "10.1038/s41586-022-05598-w",

language = "English",

volume = "614",

pages = "E39",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Research",

number = "7948",

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TY - JOUR

T1 - Author Correction: Pan-cancer analysis of whole genomes

AU - Aaltonen, Lauri A.

AU - Abascal, Federico

AU - Abeshouse, Adam

AU - Aburatani, Hiroyuki

AU - Adams, David J.

AU - Agrawal, Nishant

AU - Ahn, Keun Soo

AU - Ahn, Sung Min

AU - Aikata, Hiroshi

AU - Akbani, Rehan

AU - Akdemir, Kadir C.

AU - Al-Ahmadie, Hikmat

AU - Al-Sedairy, Sultan T.

AU - Al-Shahrour, Fatima

AU - Alawi, Malik

AU - Albert, Monique

AU - Aldape, Kenneth

AU - Alexandrov, Ludmil B.

AU - Ally, Adrian

AU - Alsop, Kathryn

AU - Alvarez, Eva G.

AU - Amary, Fernanda

AU - Amin, Samirkumar B.

AU - Aminou, Brice

AU - Ammerpohl, Ole

AU - Anderson, Matthew J.

AU - Ang, Yeng

AU - Antonello, Davide

AU - Anur, Pavana

AU - Aparicio, Samuel

AU - Appelbaum, Elizabeth L.

AU - Arai, Yasuhito

AU - Aretz, Axel

AU - Arihiro, Koji

AU - Ariizumi, Shun ichi

AU - Armenia, Joshua

AU - Arnould, Laurent

AU - Asa, Sylvia

AU - Assenov, Yassen

AU - Atwal, Gurnit

AU - Aukema, Sietse

AU - Auman, J. Todd

AU - Aure, Miriam R.R.

AU - Awadalla, Philip

AU - Aymerich, Marta

AU - Bader, Gary D.

AU - Baez-Ortega, Adrian

AU - Bailey, Matthew H.

AU - Bailey, Peter J.

AU - Balasundaram, Miruna

AU - Townend, David

AU - ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium

PY - 2023/2/16

Y1 - 2023/2/16

N2 - Cell adhesion molecules are ubiquitous in multicellular organisms, specifying precise cell-cell interactions in processes as diverse as tissue development, immune cell trafficking and the wiring of the nervous system(1-4). Here we show that a wide array of synthetic cell adhesion molecules can be generated by combining orthogonal extracellular interactions with intracellular domains from native adhesion molecules, such as cadherins and integrins. The resulting molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions. The identity of the intracellular domain of the synthetic cell adhesion molecules specifies interface morphology and mechanics, whereas diverse homotypic or heterotypic extracellular interaction domains independently specify the connectivity between cells. This toolkit of orthogonal adhesion molecules enables the rationally programmed assembly of multicellular architectures, as well as systematic remodelling of native tissues. The modularity of synthetic cell adhesion molecules provides fundamental insights into how distinct classes of cell-cell interfaces may have evolved. Overall, these tools offer powerful abilities for cell and tissue engineering and for systematically studying multicellular organization. Synthetic cell adhesion molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions, and offer abilities for cell and tissue engineering and for systematically studying multicellular organization.

AB - Cell adhesion molecules are ubiquitous in multicellular organisms, specifying precise cell-cell interactions in processes as diverse as tissue development, immune cell trafficking and the wiring of the nervous system(1-4). Here we show that a wide array of synthetic cell adhesion molecules can be generated by combining orthogonal extracellular interactions with intracellular domains from native adhesion molecules, such as cadherins and integrins. The resulting molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions. The identity of the intracellular domain of the synthetic cell adhesion molecules specifies interface morphology and mechanics, whereas diverse homotypic or heterotypic extracellular interaction domains independently specify the connectivity between cells. This toolkit of orthogonal adhesion molecules enables the rationally programmed assembly of multicellular architectures, as well as systematic remodelling of native tissues. The modularity of synthetic cell adhesion molecules provides fundamental insights into how distinct classes of cell-cell interfaces may have evolved. Overall, these tools offer powerful abilities for cell and tissue engineering and for systematically studying multicellular organization. Synthetic cell adhesion molecules yield customized cell-cell interactions with adhesion properties that are similar to native interactions, and offer abilities for cell and tissue engineering and for systematically studying multicellular organization.

U2 - 10.1038/s41586-022-05598-w

DO - 10.1038/s41586-022-05598-w

M3 - Erratum / corrigendum / retractions

SN - 0028-0836

VL - 614

SP - E39

JO - Nature

JF - Nature

IS - 7948

ER -

Author Correction: Pan-cancer analysis of whole genomes

Abstract

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Pan-cancer analysis of whole genomes

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