Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia

Nikos Kourtis; Charalampos Lazaris; Kathryn Hockemeyer; Juan Carlos Balandrán; Alejandra R. Jimenez; Jasper Mullenders; Yixiao Gong; Thomas Trimarchi; Kamala Bhatt; Hai Hu; Liza Shrestha; Alberto Ambesi-Impiombato; Michelle Kelliher; Elisabeth Paietta; Gabriela Chiosis; Monica L. Guzman; Adolfo A. Ferrando; Aristotelis Tsirigos; Iannis Aifantis

doi:10.1038/s41591-018-0105-8

Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia

Nikos Kourtis^*, Charalampos Lazaris, Kathryn Hockemeyer, Juan Carlos Balandrán, Alejandra R. Jimenez, Jasper Mullenders, Yixiao Gong, Thomas Trimarchi, Kamala Bhatt, Hai Hu, Liza Shrestha, Alberto Ambesi-Impiombato, Michelle Kelliher, Elisabeth Paietta, Gabriela Chiosis, Monica L. Guzman, Adolfo A. Ferrando, Aristotelis Tsirigos, Iannis Aifantis

^*Corresponding author for this work

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

Abstract

Cellular transformation is accompanied by extensive rewiring of many biological processes leading to augmented levels of distinct types of cellular stress, including proteotoxic stress. Cancer cells critically depend on stress-relief pathways for their survival. However, the mechanisms underlying the transcriptional initiation and maintenance of the oncogenic stress response remain elusive. Here, we show that the expression of heat shock transcription factor 1 (HSF1) and the downstream mediators of the heat shock response is transcriptionally upregulated in T cell acute lymphoblastic leukemia (T-ALL). Hsf1 ablation suppresses the growth of human T-ALL and eradicates leukemia in mouse models of T-ALL, while sparing normal hematopoiesis. HSF1 drives a compact transcriptional program and among the direct HSF1 targets, specific chaperones and co-chaperones mediate its critical role in T-ALL. Notably, we demonstrate that the central T-ALL oncogene NOTCH1 hijacks the cellular stress response machinery by inducing the expression of HSF1 and its downstream effectors. The NOTCH1 signaling status controls the levels of chaperone/co-chaperone complexes and predicts the response of T-ALL patient samples to HSP90 inhibition. Our data demonstrate an integral crosstalk between mediators of oncogene and non-oncogene addiction and reveal critical nodes of the heat shock response pathway that can be targeted therapeutically.

Original language	English
Pages (from-to)	1157-1166
Number of pages	10
Journal	Nature Medicine
Volume	24
Issue number	8
DOIs	https://doi.org/10.1038/s41591-018-0105-8
Publication status	Published - 1 Aug 2018

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10.1038/s41591-018-0105-8

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Kourtis, N., Lazaris, C., Hockemeyer, K., Balandrán, J. C., Jimenez, A. R., Mullenders, J., Gong, Y., Trimarchi, T., Bhatt, K., Hu, H., Shrestha, L., Ambesi-Impiombato, A., Kelliher, M., Paietta, E., Chiosis, G., Guzman, M. L., Ferrando, A. A., Tsirigos, A., & Aifantis, I. (2018). Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia. Nature Medicine, 24(8), 1157-1166. https://doi.org/10.1038/s41591-018-0105-8

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title = "Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia",

abstract = "Cellular transformation is accompanied by extensive rewiring of many biological processes leading to augmented levels of distinct types of cellular stress, including proteotoxic stress. Cancer cells critically depend on stress-relief pathways for their survival. However, the mechanisms underlying the transcriptional initiation and maintenance of the oncogenic stress response remain elusive. Here, we show that the expression of heat shock transcription factor 1 (HSF1) and the downstream mediators of the heat shock response is transcriptionally upregulated in T cell acute lymphoblastic leukemia (T-ALL). Hsf1 ablation suppresses the growth of human T-ALL and eradicates leukemia in mouse models of T-ALL, while sparing normal hematopoiesis. HSF1 drives a compact transcriptional program and among the direct HSF1 targets, specific chaperones and co-chaperones mediate its critical role in T-ALL. Notably, we demonstrate that the central T-ALL oncogene NOTCH1 hijacks the cellular stress response machinery by inducing the expression of HSF1 and its downstream effectors. The NOTCH1 signaling status controls the levels of chaperone/co-chaperone complexes and predicts the response of T-ALL patient samples to HSP90 inhibition. Our data demonstrate an integral crosstalk between mediators of oncogene and non-oncogene addiction and reveal critical nodes of the heat shock response pathway that can be targeted therapeutically.",

author = "Nikos Kourtis and Charalampos Lazaris and Kathryn Hockemeyer and Balandr{\'a}n, {Juan Carlos} and Jimenez, {Alejandra R.} and Jasper Mullenders and Yixiao Gong and Thomas Trimarchi and Kamala Bhatt and Hai Hu and Liza Shrestha and Alberto Ambesi-Impiombato and Michelle Kelliher and Elisabeth Paietta and Gabriela Chiosis and Guzman, {Monica L.} and Ferrando, {Adolfo A.} and Aristotelis Tsirigos and Iannis Aifantis",

note = "Funding Information: We thank all members of the Aifantis laboratory for discussions throughout the duration of this project; T. Papagiannakopoulos and P. Ntziachristos for critical assessment of this work; E. Christians (UPMC Univ. Paris 06, CNRS) for the Hsf1f/f mice; A. Heguy and the NYU Genome Technology Center (supported in part by National Institutes of Health (NIH)/National Cancer Institute (NCI) grant P30CA016087-30) for expertise with sequencing experiments; the NYU Histology Core (5P30CA16087-31) for assistance; C. Loomis and L. Chiriboga for immunohistochemistry experiments; C. Jamieson (UCSD) for human LICs; The ECOG-ACRIN Cancer Research Group for clinical specimens. This work has used computing resources at the High Performance Computing Facility at the NYU Medical Center. A.T. is supported by a Research Scholar Grant (RSG-15-189-01-RMC) from the American Cancer Society and a Leukemia & Lymphoma Society New Idea Award (8007-17). I.A. is supported by the NIH (R01CA133379, R01CA105129, R01CA149655, 5R01CA173636, 1R01CA194923), the NYSTEM program of the New York State Health Department (NYSTEM-N11G-255) and the Leukemia & Lymphoma Society (LLS) Translational Research Program (TRP). J.C.B. was supported by CONACyT (FOSISSS 2015-1-261848) and IMSS (FIS/IMSS/PROT/G14/1289). J.M. was supported by KWF BUIT2012-5358. N.K. is supported by a Human Frontiers Science Program (HFSP) Long Term Fellowship (LT000150/2013-L) and previously by a Charles H. Revson Senior Fellowship in Biomedical Science (15–31) and a European Molecular Biology Organization (EMBO) Long Term Fellowship (ALTF 850-2012). Publisher Copyright: {\textcopyright} 2018, The Author(s).",

year = "2018",

month = aug,

day = "1",

doi = "10.1038/s41591-018-0105-8",

language = "English",

volume = "24",

pages = "1157--1166",

journal = "Nature Medicine",

issn = "1078-8956",

publisher = "Nature Research",

number = "8",

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Kourtis, N, Lazaris, C, Hockemeyer, K, Balandrán, JC, Jimenez, AR, Mullenders, J, Gong, Y, Trimarchi, T, Bhatt, K, Hu, H, Shrestha, L, Ambesi-Impiombato, A, Kelliher, M, Paietta, E, Chiosis, G, Guzman, ML, Ferrando, AA, Tsirigos, A & Aifantis, I 2018, 'Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia', Nature Medicine, vol. 24, no. 8, pp. 1157-1166. https://doi.org/10.1038/s41591-018-0105-8

TY - JOUR

T1 - Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia

AU - Kourtis, Nikos

AU - Lazaris, Charalampos

AU - Hockemeyer, Kathryn

AU - Balandrán, Juan Carlos

AU - Jimenez, Alejandra R.

AU - Mullenders, Jasper

AU - Gong, Yixiao

AU - Trimarchi, Thomas

AU - Bhatt, Kamala

AU - Hu, Hai

AU - Shrestha, Liza

AU - Ambesi-Impiombato, Alberto

AU - Kelliher, Michelle

AU - Paietta, Elisabeth

AU - Chiosis, Gabriela

AU - Guzman, Monica L.

AU - Ferrando, Adolfo A.

AU - Tsirigos, Aristotelis

AU - Aifantis, Iannis

N1 - Funding Information: We thank all members of the Aifantis laboratory for discussions throughout the duration of this project; T. Papagiannakopoulos and P. Ntziachristos for critical assessment of this work; E. Christians (UPMC Univ. Paris 06, CNRS) for the Hsf1f/f mice; A. Heguy and the NYU Genome Technology Center (supported in part by National Institutes of Health (NIH)/National Cancer Institute (NCI) grant P30CA016087-30) for expertise with sequencing experiments; the NYU Histology Core (5P30CA16087-31) for assistance; C. Loomis and L. Chiriboga for immunohistochemistry experiments; C. Jamieson (UCSD) for human LICs; The ECOG-ACRIN Cancer Research Group for clinical specimens. This work has used computing resources at the High Performance Computing Facility at the NYU Medical Center. A.T. is supported by a Research Scholar Grant (RSG-15-189-01-RMC) from the American Cancer Society and a Leukemia & Lymphoma Society New Idea Award (8007-17). I.A. is supported by the NIH (R01CA133379, R01CA105129, R01CA149655, 5R01CA173636, 1R01CA194923), the NYSTEM program of the New York State Health Department (NYSTEM-N11G-255) and the Leukemia & Lymphoma Society (LLS) Translational Research Program (TRP). J.C.B. was supported by CONACyT (FOSISSS 2015-1-261848) and IMSS (FIS/IMSS/PROT/G14/1289). J.M. was supported by KWF BUIT2012-5358. N.K. is supported by a Human Frontiers Science Program (HFSP) Long Term Fellowship (LT000150/2013-L) and previously by a Charles H. Revson Senior Fellowship in Biomedical Science (15–31) and a European Molecular Biology Organization (EMBO) Long Term Fellowship (ALTF 850-2012). Publisher Copyright: © 2018, The Author(s).

PY - 2018/8/1

Y1 - 2018/8/1

N2 - Cellular transformation is accompanied by extensive rewiring of many biological processes leading to augmented levels of distinct types of cellular stress, including proteotoxic stress. Cancer cells critically depend on stress-relief pathways for their survival. However, the mechanisms underlying the transcriptional initiation and maintenance of the oncogenic stress response remain elusive. Here, we show that the expression of heat shock transcription factor 1 (HSF1) and the downstream mediators of the heat shock response is transcriptionally upregulated in T cell acute lymphoblastic leukemia (T-ALL). Hsf1 ablation suppresses the growth of human T-ALL and eradicates leukemia in mouse models of T-ALL, while sparing normal hematopoiesis. HSF1 drives a compact transcriptional program and among the direct HSF1 targets, specific chaperones and co-chaperones mediate its critical role in T-ALL. Notably, we demonstrate that the central T-ALL oncogene NOTCH1 hijacks the cellular stress response machinery by inducing the expression of HSF1 and its downstream effectors. The NOTCH1 signaling status controls the levels of chaperone/co-chaperone complexes and predicts the response of T-ALL patient samples to HSP90 inhibition. Our data demonstrate an integral crosstalk between mediators of oncogene and non-oncogene addiction and reveal critical nodes of the heat shock response pathway that can be targeted therapeutically.

AB - Cellular transformation is accompanied by extensive rewiring of many biological processes leading to augmented levels of distinct types of cellular stress, including proteotoxic stress. Cancer cells critically depend on stress-relief pathways for their survival. However, the mechanisms underlying the transcriptional initiation and maintenance of the oncogenic stress response remain elusive. Here, we show that the expression of heat shock transcription factor 1 (HSF1) and the downstream mediators of the heat shock response is transcriptionally upregulated in T cell acute lymphoblastic leukemia (T-ALL). Hsf1 ablation suppresses the growth of human T-ALL and eradicates leukemia in mouse models of T-ALL, while sparing normal hematopoiesis. HSF1 drives a compact transcriptional program and among the direct HSF1 targets, specific chaperones and co-chaperones mediate its critical role in T-ALL. Notably, we demonstrate that the central T-ALL oncogene NOTCH1 hijacks the cellular stress response machinery by inducing the expression of HSF1 and its downstream effectors. The NOTCH1 signaling status controls the levels of chaperone/co-chaperone complexes and predicts the response of T-ALL patient samples to HSP90 inhibition. Our data demonstrate an integral crosstalk between mediators of oncogene and non-oncogene addiction and reveal critical nodes of the heat shock response pathway that can be targeted therapeutically.

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U2 - 10.1038/s41591-018-0105-8

DO - 10.1038/s41591-018-0105-8

M3 - Article

C2 - 30038221

AN - SCOPUS:85050530624

SN - 1078-8956

VL - 24

SP - 1157

EP - 1166

JO - Nature Medicine

JF - Nature Medicine

IS - 8

ER -

Oncogenic hijacking of the stress response machinery in T cell acute lymphoblastic leukemia

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