Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures

Joo Sang Lee; Lital Adler; Hiren Karathia; Narin Carmel; Shiran Rabinovich; Noam Auslander; Rom Keshet; Noa Stettner; Alon Silberman; Lilach Agemy; Daniel Helbling; Raya Eilam; Qin Sun; Alexander Brandis; Sergey Malitsky; Maxim Itkin; Hila Weiss; Sivan Pinto; Shelly Kalaora; Ronen Levy; Eilon Barnea; Arie Admon; David Dimmock; Noam Stern-Ginossar; Avigdor Scherz; Sandesh C. S. Nagamani; Miguel Unda; David M. Wilson; Ronit Elhasid; Arkaitz Carracedo; Yardena Samuels; Sridhar Hannenhalli; Eytan Ruppin; Ayelet Erez

doi:10.1016/j.cell.2018.07.019

Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures

Joo Sang Lee, Lital Adler, Hiren Karathia, Narin Carmel, Shiran Rabinovich, Noam Auslander, Rom Keshet, Noa Stettner, Alon Silberman, Lilach Agemy, Daniel Helbling, Raya Eilam, Qin Sun, Alexander Brandis, Sergey Malitsky, Maxim Itkin, Hila Weiss, Sivan Pinto, Shelly Kalaora, Ronen LevyEilon Barnea, Arie Admon, David Dimmock, Noam Stern-Ginossar, Avigdor Scherz, Sandesh C. S. Nagamani, Miguel Unda, David M. Wilson, Ronit Elhasid, Arkaitz Carracedo, Yardena Samuels, Sridhar Hannenhalli, Eytan Ruppin, Ayelet Erez

Weizmann Institute of Science, Tel Aviv University

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

Abstract

The urea cycle (UC) is the main pathway by which mammals dispose of waste nitrogen. We find that specific alterations in the expression of most UC enzymes occur in many tumors, leading to a general metabolic hallmark termed “UC dysregulation” (UCD). UCD elicits nitrogen diversion toward carbamoyl-phosphate synthetase2, aspartate transcarbamylase, and dihydrooratase (CAD) activation and enhances pyrimidine synthesis, resulting in detectable changes in nitrogen metabolites in both patient tumors and their bio-fluids. The accompanying excess of pyrimidine versus purine nucleotides results in a genomic signature consisting of transversion mutations at the DNA, RNA, and protein levels. This mutational bias is associated with increased numbers of hydrophobic tumor antigens and a better response to immune checkpoint inhibitors independent of mutational load. Taken together, our findings demonstrate that UCD is a common feature of tumors that profoundly affects carcinogenesis, mutagenesis, and immunotherapy response. Urea cycle dysregulation (UCD) in cancer is a prevalent phenomenon in multiple cancers. UCD increases nitrogen utilization for pyrimidine synthesis, generating nucleotide imbalance that leads to detectable mutation patterns and biochemical signatures in cancer patients’ samples. UCD is associated with a worse prognosis but a better response to immunotherapy.

Original language	English
Pages (from-to)	1559-1570
Number of pages	12
Journal	Cell
Volume	174
Issue number	6
DOIs	https://doi.org/10.1016/j.cell.2018.07.019
State	Published - 6 Sep 2018

All Science Journal Classification (ASJC) codes

General Biochemistry,Genetics and Molecular Biology

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Lee, J. S., Adler, L., Karathia, H., Carmel, N., Rabinovich, S., Auslander, N., Keshet, R., Stettner, N., Silberman, A., Agemy, L., Helbling, D., Eilam, R., Sun, Q., Brandis, A., Malitsky, S., Itkin, M., Weiss, H., Pinto, S., Kalaora, S., ... Erez, A. (2018). Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures. Cell, 174(6), 1559-1570. https://doi.org/10.1016/j.cell.2018.07.019

@article{5e34ebd8e95c41e58e8b972221e69091,

title = "Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures",

abstract = "The urea cycle (UC) is the main pathway by which mammals dispose of waste nitrogen. We find that specific alterations in the expression of most UC enzymes occur in many tumors, leading to a general metabolic hallmark termed “UC dysregulation” (UCD). UCD elicits nitrogen diversion toward carbamoyl-phosphate synthetase2, aspartate transcarbamylase, and dihydrooratase (CAD) activation and enhances pyrimidine synthesis, resulting in detectable changes in nitrogen metabolites in both patient tumors and their bio-fluids. The accompanying excess of pyrimidine versus purine nucleotides results in a genomic signature consisting of transversion mutations at the DNA, RNA, and protein levels. This mutational bias is associated with increased numbers of hydrophobic tumor antigens and a better response to immune checkpoint inhibitors independent of mutational load. Taken together, our findings demonstrate that UCD is a common feature of tumors that profoundly affects carcinogenesis, mutagenesis, and immunotherapy response. Urea cycle dysregulation (UCD) in cancer is a prevalent phenomenon in multiple cancers. UCD increases nitrogen utilization for pyrimidine synthesis, generating nucleotide imbalance that leads to detectable mutation patterns and biochemical signatures in cancer patients{\textquoteright} samples. UCD is associated with a worse prognosis but a better response to immunotherapy.",

author = "Lee, {Joo Sang} and Lital Adler and Hiren Karathia and Narin Carmel and Shiran Rabinovich and Noam Auslander and Rom Keshet and Noa Stettner and Alon Silberman and Lilach Agemy and Daniel Helbling and Raya Eilam and Qin Sun and Alexander Brandis and Sergey Malitsky and Maxim Itkin and Hila Weiss and Sivan Pinto and Shelly Kalaora and Ronen Levy and Eilon Barnea and Arie Admon and David Dimmock and Noam Stern-Ginossar and Avigdor Scherz and Nagamani, {Sandesh C. S.} and Miguel Unda and Wilson, {David M.} and Ronit Elhasid and Arkaitz Carracedo and Yardena Samuels and Sridhar Hannenhalli and Eytan Ruppin and Ayelet Erez",

note = "We acknowledge and thank the Weizmann Institute for providing financial and infrastructural support. We are grateful to the Clalit-Weizmann joint analysis program (G. Barbash, R. Balicer, and A. Tanay) and, in particular, to Netta Mendelson Cohen for providing access to data on distributions of urea levels in healthy individuals. We thank Igor Ulitsky, Ron Rotkopf, Shifra Ben-Dor, Erez Persi, Edward M. Gertz, and Sivan Galai for the intellectual and technical assistance. We are thankful to the Basque Biobank for Research (BIOEF) for the support in the acquisition and management of human specimens. A.E. is an incumbent of the Leah Omenn Career Development Chair and is supported by research grants from the European Research Program (CIG618113, ERC614204), the Israel Science Foundation (1343/13; 1952/13), and from Minerva (711730). A.E. received additional support from the Adelis Foundation, the Henry S. and Anne S. Reich Research Fund, the Dukler Fund for Cancer Research, the Paul Sparr Foundation, the Saul and Theresa Esman Foundation, Joseph Piko Baruch, and the estate of Fannie Sherr. E.R. gratefully acknowledges support from I-CORE Center of Excellence in Gene Regulation in Complex Human Disease, the Israel Science Foundation (41/11), IPST, NIST, and NIH (R33 CA225291) to his lab. The work of A.C. was supported by the Basque Department of Industry, Tourism, and Trade (Etortek) and Education (IKERTALDE I.T.1106-16), the BBVA Foundation, MINECO (SAF2016-79381-R, FEDER/EU), MSCA-ITN-ETN (proposal number: 721532), a European Research Council Starting Grant (336343), and the European Research Council Proof-of-Concept Program (754627 – MetaboMARKER). The participation of A.C. and M.U. as part of CIBERONC was co-funded with FEDER funds. S.H. and H.K. were funded in part by an NSF award (1564785). D.M.W. was supported in part by the Intramural Research Program of the NIH and the National Institute on Aging. Y.S was supported by the Israel Science Foundation (696/17) and ERC-2016-PoC (754282).",

year = "2018",

month = sep,

day = "6",

doi = "10.1016/j.cell.2018.07.019",

language = "الإنجليزيّة",

volume = "174",

pages = "1559--1570",

journal = "Cell",

issn = "0092-8674",

publisher = "Elsevier B.V.",

number = "6",

}

Lee, JS, Adler, L, Karathia, H, Carmel, N, Rabinovich, S, Auslander, N, Keshet, R, Stettner, N, Silberman, A, Agemy, L, Helbling, D, Eilam, R, Sun, Q, Brandis, A, Malitsky, S, Itkin, M, Weiss, H, Pinto, S, Kalaora, S, Levy, R, Barnea, E, Admon, A, Dimmock, D, Stern-Ginossar, N, Scherz, A, Nagamani, SCS, Unda, M, Wilson, DM, Elhasid, R, Carracedo, A, Samuels, Y, Hannenhalli, S, Ruppin, E & Erez, A 2018, 'Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures', Cell, vol. 174, no. 6, pp. 1559-1570. https://doi.org/10.1016/j.cell.2018.07.019

TY - JOUR

T1 - Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures

AU - Lee, Joo Sang

AU - Adler, Lital

AU - Karathia, Hiren

AU - Carmel, Narin

AU - Rabinovich, Shiran

AU - Auslander, Noam

AU - Keshet, Rom

AU - Stettner, Noa

AU - Silberman, Alon

AU - Agemy, Lilach

AU - Helbling, Daniel

AU - Eilam, Raya

AU - Sun, Qin

AU - Brandis, Alexander

AU - Malitsky, Sergey

AU - Itkin, Maxim

AU - Weiss, Hila

AU - Pinto, Sivan

AU - Kalaora, Shelly

AU - Levy, Ronen

AU - Barnea, Eilon

AU - Admon, Arie

AU - Dimmock, David

AU - Stern-Ginossar, Noam

AU - Scherz, Avigdor

AU - Nagamani, Sandesh C. S.

AU - Unda, Miguel

AU - Wilson, David M.

AU - Elhasid, Ronit

AU - Carracedo, Arkaitz

AU - Samuels, Yardena

AU - Hannenhalli, Sridhar

AU - Ruppin, Eytan

AU - Erez, Ayelet

N1 - We acknowledge and thank the Weizmann Institute for providing financial and infrastructural support. We are grateful to the Clalit-Weizmann joint analysis program (G. Barbash, R. Balicer, and A. Tanay) and, in particular, to Netta Mendelson Cohen for providing access to data on distributions of urea levels in healthy individuals. We thank Igor Ulitsky, Ron Rotkopf, Shifra Ben-Dor, Erez Persi, Edward M. Gertz, and Sivan Galai for the intellectual and technical assistance. We are thankful to the Basque Biobank for Research (BIOEF) for the support in the acquisition and management of human specimens. A.E. is an incumbent of the Leah Omenn Career Development Chair and is supported by research grants from the European Research Program (CIG618113, ERC614204), the Israel Science Foundation (1343/13; 1952/13), and from Minerva (711730). A.E. received additional support from the Adelis Foundation, the Henry S. and Anne S. Reich Research Fund, the Dukler Fund for Cancer Research, the Paul Sparr Foundation, the Saul and Theresa Esman Foundation, Joseph Piko Baruch, and the estate of Fannie Sherr. E.R. gratefully acknowledges support from I-CORE Center of Excellence in Gene Regulation in Complex Human Disease, the Israel Science Foundation (41/11), IPST, NIST, and NIH (R33 CA225291) to his lab. The work of A.C. was supported by the Basque Department of Industry, Tourism, and Trade (Etortek) and Education (IKERTALDE I.T.1106-16), the BBVA Foundation, MINECO (SAF2016-79381-R, FEDER/EU), MSCA-ITN-ETN (proposal number: 721532), a European Research Council Starting Grant (336343), and the European Research Council Proof-of-Concept Program (754627 – MetaboMARKER). The participation of A.C. and M.U. as part of CIBERONC was co-funded with FEDER funds. S.H. and H.K. were funded in part by an NSF award (1564785). D.M.W. was supported in part by the Intramural Research Program of the NIH and the National Institute on Aging. Y.S was supported by the Israel Science Foundation (696/17) and ERC-2016-PoC (754282).

PY - 2018/9/6

Y1 - 2018/9/6

N2 - The urea cycle (UC) is the main pathway by which mammals dispose of waste nitrogen. We find that specific alterations in the expression of most UC enzymes occur in many tumors, leading to a general metabolic hallmark termed “UC dysregulation” (UCD). UCD elicits nitrogen diversion toward carbamoyl-phosphate synthetase2, aspartate transcarbamylase, and dihydrooratase (CAD) activation and enhances pyrimidine synthesis, resulting in detectable changes in nitrogen metabolites in both patient tumors and their bio-fluids. The accompanying excess of pyrimidine versus purine nucleotides results in a genomic signature consisting of transversion mutations at the DNA, RNA, and protein levels. This mutational bias is associated with increased numbers of hydrophobic tumor antigens and a better response to immune checkpoint inhibitors independent of mutational load. Taken together, our findings demonstrate that UCD is a common feature of tumors that profoundly affects carcinogenesis, mutagenesis, and immunotherapy response. Urea cycle dysregulation (UCD) in cancer is a prevalent phenomenon in multiple cancers. UCD increases nitrogen utilization for pyrimidine synthesis, generating nucleotide imbalance that leads to detectable mutation patterns and biochemical signatures in cancer patients’ samples. UCD is associated with a worse prognosis but a better response to immunotherapy.

AB - The urea cycle (UC) is the main pathway by which mammals dispose of waste nitrogen. We find that specific alterations in the expression of most UC enzymes occur in many tumors, leading to a general metabolic hallmark termed “UC dysregulation” (UCD). UCD elicits nitrogen diversion toward carbamoyl-phosphate synthetase2, aspartate transcarbamylase, and dihydrooratase (CAD) activation and enhances pyrimidine synthesis, resulting in detectable changes in nitrogen metabolites in both patient tumors and their bio-fluids. The accompanying excess of pyrimidine versus purine nucleotides results in a genomic signature consisting of transversion mutations at the DNA, RNA, and protein levels. This mutational bias is associated with increased numbers of hydrophobic tumor antigens and a better response to immune checkpoint inhibitors independent of mutational load. Taken together, our findings demonstrate that UCD is a common feature of tumors that profoundly affects carcinogenesis, mutagenesis, and immunotherapy response. Urea cycle dysregulation (UCD) in cancer is a prevalent phenomenon in multiple cancers. UCD increases nitrogen utilization for pyrimidine synthesis, generating nucleotide imbalance that leads to detectable mutation patterns and biochemical signatures in cancer patients’ samples. UCD is associated with a worse prognosis but a better response to immunotherapy.

UR - http://www.scopus.com/inward/record.url?scp=85052734974&partnerID=8YFLogxK

U2 - 10.1016/j.cell.2018.07.019

DO - 10.1016/j.cell.2018.07.019

M3 - مقالة

C2 - 30100185

SN - 0092-8674

VL - 174

SP - 1559

EP - 1570

JO - Cell

JF - Cell

IS - 6

ER -

Urea Cycle Dysregulation Generates Clinically Relevant Genomic and Biochemical Signatures

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