Elevated NSD3 histone methylation activity drives squamous cell lung cancer

Gang Yuan; Natasha M. Flores; Simone Hausmann; Shane M. Lofgren; Vladlena Kharchenko; Maria Angulo-Ibanez; Deepanwita Sengupta; Xiaoyin Lu; Iwona Czaban; Dulat Azhibek; Silvestre Vicent; Wolfgang Fischle; Mariusz Jaremko; Bingliang Fang; Ignacio I. Wistuba; Katrin F. Chua; Jack A. Roth; John D. Minna; Ning Yi Shao; Łukasz Jaremko; Pawel K. Mazur; Or Gozani

doi:10.1038/s41586-020-03170-y

Elevated NSD3 histone methylation activity drives squamous cell lung cancer

Gang Yuan, Natasha M. Flores, Simone Hausmann, Shane M. Lofgren, Vladlena Kharchenko, Maria Angulo-Ibanez, Deepanwita Sengupta, Xiaoyin Lu, Iwona Czaban, Dulat Azhibek, Silvestre Vicent, Wolfgang Fischle, Mariusz Jaremko, Bingliang Fang, Ignacio I. Wistuba, Katrin F. Chua, Jack A. Roth, John D. Minna, Ning Yi Shao, Łukasz JaremkoPawel K. Mazur, Or Gozani

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

70 Scopus citations

Abstract

Amplification of chromosomal region 8p11–12 is a common genetic alteration that has been implicated in the aetiology of lung squamous cell carcinoma (LUSC)^1–3. The FGFR1 gene is the main candidate driver of tumorigenesis within this region⁴. However, clinical trials evaluating FGFR1 inhibition as a targeted therapy have been unsuccessful⁵. Here we identify the histone H3 lysine 36 (H3K36) methyltransferase NSD3, the gene for which is located in the 8p11–12 amplicon, as a key regulator of LUSC tumorigenesis. In contrast to other 8p11–12 candidate LUSC drivers, increased expression of NSD3 correlated strongly with its gene amplification. Ablation of NSD3, but not of FGFR1, attenuated tumour growth and extended survival in a mouse model of LUSC. We identify an LUSC-associated variant NSD3(T1232A) that shows increased catalytic activity for dimethylation of H3K36 (H3K36me2) in vitro and in vivo. Structural dynamic analyses revealed that the T1232A substitution elicited localized mobility changes throughout the catalytic domain of NSD3 to relieve auto-inhibition and to increase accessibility of the H3 substrate. Expression of NSD3(T1232A) in vivo accelerated tumorigenesis and decreased overall survival in mouse models of LUSC. Pathological generation of H3K36me2 by NSD3(T1232A) reprograms the chromatin landscape to promote oncogenic gene expression signatures. Furthermore, NSD3, in a manner dependent on its catalytic activity, promoted transformation in human tracheobronchial cells and growth of xenografted human LUSC cell lines with amplification of 8p11–12. Depletion of NSD3 in patient-derived xenografts from primary LUSCs containing NSD3 amplification or the NSD3(T1232A)-encoding variant attenuated neoplastic growth in mice. Finally, NSD3-regulated LUSC-derived xenografts were hypersensitive to bromodomain inhibition. Thus, our work identifies NSD3 as a principal 8p11–12 amplicon-associated oncogenic driver in LUSC, and suggests that NSD3-dependency renders LUSC therapeutically vulnerable to bromodomain inhibition.

Original language	English (US)
Pages (from-to)	504-508
Number of pages	5
Journal	Nature
Volume	590
Issue number	7846
DOIs	https://doi.org/10.1038/s41586-020-03170-y
State	Published - Feb 18 2021

ASJC Scopus subject areas

General

Access to Document

10.1038/s41586-020-03170-y

Cite this

Yuan, G., Flores, N. M., Hausmann, S., Lofgren, S. M., Kharchenko, V., Angulo-Ibanez, M., Sengupta, D., Lu, X., Czaban, I., Azhibek, D., Vicent, S., Fischle, W., Jaremko, M., Fang, B., Wistuba, I. I., Chua, K. F., Roth, J. A., Minna, J. D., Shao, N. Y., ... Gozani, O. (2021). Elevated NSD3 histone methylation activity drives squamous cell lung cancer. Nature, 590(7846), 504-508. https://doi.org/10.1038/s41586-020-03170-y

Yuan, G, Flores, NM, Hausmann, S, Lofgren, SM, Kharchenko, V, Angulo-Ibanez, M, Sengupta, D, Lu, X, Czaban, I, Azhibek, D, Vicent, S, Fischle, W, Jaremko, M, Fang, B, Wistuba, II, Chua, KF, Roth, JA, Minna, JD, Shao, NY, Jaremko, Ł, Mazur, PK & Gozani, O 2021, 'Elevated NSD3 histone methylation activity drives squamous cell lung cancer', Nature, vol. 590, no. 7846, pp. 504-508. https://doi.org/10.1038/s41586-020-03170-y

@article{083e277649ff41e4aff13bd5393ede9f,

title = "Elevated NSD3 histone methylation activity drives squamous cell lung cancer",

abstract = "Amplification of chromosomal region 8p11–12 is a common genetic alteration that has been implicated in the aetiology of lung squamous cell carcinoma (LUSC)1–3. The FGFR1 gene is the main candidate driver of tumorigenesis within this region4. However, clinical trials evaluating FGFR1 inhibition as a targeted therapy have been unsuccessful5. Here we identify the histone H3 lysine 36 (H3K36) methyltransferase NSD3, the gene for which is located in the 8p11–12 amplicon, as a key regulator of LUSC tumorigenesis. In contrast to other 8p11–12 candidate LUSC drivers, increased expression of NSD3 correlated strongly with its gene amplification. Ablation of NSD3, but not of FGFR1, attenuated tumour growth and extended survival in a mouse model of LUSC. We identify an LUSC-associated variant NSD3(T1232A) that shows increased catalytic activity for dimethylation of H3K36 (H3K36me2) in vitro and in vivo. Structural dynamic analyses revealed that the T1232A substitution elicited localized mobility changes throughout the catalytic domain of NSD3 to relieve auto-inhibition and to increase accessibility of the H3 substrate. Expression of NSD3(T1232A) in vivo accelerated tumorigenesis and decreased overall survival in mouse models of LUSC. Pathological generation of H3K36me2 by NSD3(T1232A) reprograms the chromatin landscape to promote oncogenic gene expression signatures. Furthermore, NSD3, in a manner dependent on its catalytic activity, promoted transformation in human tracheobronchial cells and growth of xenografted human LUSC cell lines with amplification of 8p11–12. Depletion of NSD3 in patient-derived xenografts from primary LUSCs containing NSD3 amplification or the NSD3(T1232A)-encoding variant attenuated neoplastic growth in mice. Finally, NSD3-regulated LUSC-derived xenografts were hypersensitive to bromodomain inhibition. Thus, our work identifies NSD3 as a principal 8p11–12 amplicon-associated oncogenic driver in LUSC, and suggests that NSD3-dependency renders LUSC therapeutically vulnerable to bromodomain inhibition.",

author = "Gang Yuan and Flores, {Natasha M.} and Simone Hausmann and Lofgren, {Shane M.} and Vladlena Kharchenko and Maria Angulo-Ibanez and Deepanwita Sengupta and Xiaoyin Lu and Iwona Czaban and Dulat Azhibek and Silvestre Vicent and Wolfgang Fischle and Mariusz Jaremko and Bingliang Fang and Wistuba, {Ignacio I.} and Chua, {Katrin F.} and Roth, {Jack A.} and Minna, {John D.} and Shao, {Ning Yi} and {\L}ukasz Jaremko and Mazur, {Pawel K.} and Or Gozani",

note = "Funding Information: Acknowledgements We thank members of the Gozani and Mazur laboratories for critical reading of the manuscript, and M. Lin for the AkaLuc vector. This work was supported in part by grants from the NIH to O.G. (R01 GM079641 and R35 GM139569), K.F.C. (R01AG050997) and P.K.M. (R00 CA197816), 1U54CA224065 to B.F. and J.A.R., VA Merit Award to K.F.C., intramural funds from KAUST to W.F., {\L}.J. and M.J., the P. Neuroendocrine Tumor Research Foundation, AACR, DOD PRCRP Career Development Award (CA181486), Career Enhancement Grant – The University of Texas NIH SPORE in Lung Cancer (P50CA070907), and the Andrew Sabin Family Foundation Scientist and CPRIT Scholar in Cancer Research (RR160078) to P.K.M. N.-Y.S. was supported by SRG2019-00177-FHS and FDCT0038/2020/AFJ, N.M.F. by the American Cancer Society – Joe & Jessie Crump Foundation Fellowship (PF-20-108-01-DMC), X.L. by a CPRIT Research Training Grant (RP170067) and S.H. by a Deutsche Forschungsgemeinschaft Fellowship (HA8434/1-1). Publisher Copyright: {\textcopyright} 2021, The Author(s), under exclusive licence to Springer Nature Limited.",

year = "2021",

month = feb,

day = "18",

doi = "10.1038/s41586-020-03170-y",

language = "English (US)",

volume = "590",

pages = "504--508",

journal = "Nature",

issn = "0028-0836",

publisher = "Nature Publishing Group",

number = "7846",

}

TY - JOUR

T1 - Elevated NSD3 histone methylation activity drives squamous cell lung cancer

AU - Yuan, Gang

AU - Flores, Natasha M.

AU - Hausmann, Simone

AU - Lofgren, Shane M.

AU - Kharchenko, Vladlena

AU - Angulo-Ibanez, Maria

AU - Sengupta, Deepanwita

AU - Lu, Xiaoyin

AU - Czaban, Iwona

AU - Azhibek, Dulat

AU - Vicent, Silvestre

AU - Fischle, Wolfgang

AU - Jaremko, Mariusz

AU - Fang, Bingliang

AU - Wistuba, Ignacio I.

AU - Chua, Katrin F.

AU - Roth, Jack A.

AU - Minna, John D.

AU - Shao, Ning Yi

AU - Jaremko, Łukasz

AU - Mazur, Pawel K.

AU - Gozani, Or

N1 - Funding Information: Acknowledgements We thank members of the Gozani and Mazur laboratories for critical reading of the manuscript, and M. Lin for the AkaLuc vector. This work was supported in part by grants from the NIH to O.G. (R01 GM079641 and R35 GM139569), K.F.C. (R01AG050997) and P.K.M. (R00 CA197816), 1U54CA224065 to B.F. and J.A.R., VA Merit Award to K.F.C., intramural funds from KAUST to W.F., Ł.J. and M.J., the P. Neuroendocrine Tumor Research Foundation, AACR, DOD PRCRP Career Development Award (CA181486), Career Enhancement Grant – The University of Texas NIH SPORE in Lung Cancer (P50CA070907), and the Andrew Sabin Family Foundation Scientist and CPRIT Scholar in Cancer Research (RR160078) to P.K.M. N.-Y.S. was supported by SRG2019-00177-FHS and FDCT0038/2020/AFJ, N.M.F. by the American Cancer Society – Joe & Jessie Crump Foundation Fellowship (PF-20-108-01-DMC), X.L. by a CPRIT Research Training Grant (RP170067) and S.H. by a Deutsche Forschungsgemeinschaft Fellowship (HA8434/1-1). Publisher Copyright: © 2021, The Author(s), under exclusive licence to Springer Nature Limited.

PY - 2021/2/18

Y1 - 2021/2/18

N2 - Amplification of chromosomal region 8p11–12 is a common genetic alteration that has been implicated in the aetiology of lung squamous cell carcinoma (LUSC)1–3. The FGFR1 gene is the main candidate driver of tumorigenesis within this region4. However, clinical trials evaluating FGFR1 inhibition as a targeted therapy have been unsuccessful5. Here we identify the histone H3 lysine 36 (H3K36) methyltransferase NSD3, the gene for which is located in the 8p11–12 amplicon, as a key regulator of LUSC tumorigenesis. In contrast to other 8p11–12 candidate LUSC drivers, increased expression of NSD3 correlated strongly with its gene amplification. Ablation of NSD3, but not of FGFR1, attenuated tumour growth and extended survival in a mouse model of LUSC. We identify an LUSC-associated variant NSD3(T1232A) that shows increased catalytic activity for dimethylation of H3K36 (H3K36me2) in vitro and in vivo. Structural dynamic analyses revealed that the T1232A substitution elicited localized mobility changes throughout the catalytic domain of NSD3 to relieve auto-inhibition and to increase accessibility of the H3 substrate. Expression of NSD3(T1232A) in vivo accelerated tumorigenesis and decreased overall survival in mouse models of LUSC. Pathological generation of H3K36me2 by NSD3(T1232A) reprograms the chromatin landscape to promote oncogenic gene expression signatures. Furthermore, NSD3, in a manner dependent on its catalytic activity, promoted transformation in human tracheobronchial cells and growth of xenografted human LUSC cell lines with amplification of 8p11–12. Depletion of NSD3 in patient-derived xenografts from primary LUSCs containing NSD3 amplification or the NSD3(T1232A)-encoding variant attenuated neoplastic growth in mice. Finally, NSD3-regulated LUSC-derived xenografts were hypersensitive to bromodomain inhibition. Thus, our work identifies NSD3 as a principal 8p11–12 amplicon-associated oncogenic driver in LUSC, and suggests that NSD3-dependency renders LUSC therapeutically vulnerable to bromodomain inhibition.

AB - Amplification of chromosomal region 8p11–12 is a common genetic alteration that has been implicated in the aetiology of lung squamous cell carcinoma (LUSC)1–3. The FGFR1 gene is the main candidate driver of tumorigenesis within this region4. However, clinical trials evaluating FGFR1 inhibition as a targeted therapy have been unsuccessful5. Here we identify the histone H3 lysine 36 (H3K36) methyltransferase NSD3, the gene for which is located in the 8p11–12 amplicon, as a key regulator of LUSC tumorigenesis. In contrast to other 8p11–12 candidate LUSC drivers, increased expression of NSD3 correlated strongly with its gene amplification. Ablation of NSD3, but not of FGFR1, attenuated tumour growth and extended survival in a mouse model of LUSC. We identify an LUSC-associated variant NSD3(T1232A) that shows increased catalytic activity for dimethylation of H3K36 (H3K36me2) in vitro and in vivo. Structural dynamic analyses revealed that the T1232A substitution elicited localized mobility changes throughout the catalytic domain of NSD3 to relieve auto-inhibition and to increase accessibility of the H3 substrate. Expression of NSD3(T1232A) in vivo accelerated tumorigenesis and decreased overall survival in mouse models of LUSC. Pathological generation of H3K36me2 by NSD3(T1232A) reprograms the chromatin landscape to promote oncogenic gene expression signatures. Furthermore, NSD3, in a manner dependent on its catalytic activity, promoted transformation in human tracheobronchial cells and growth of xenografted human LUSC cell lines with amplification of 8p11–12. Depletion of NSD3 in patient-derived xenografts from primary LUSCs containing NSD3 amplification or the NSD3(T1232A)-encoding variant attenuated neoplastic growth in mice. Finally, NSD3-regulated LUSC-derived xenografts were hypersensitive to bromodomain inhibition. Thus, our work identifies NSD3 as a principal 8p11–12 amplicon-associated oncogenic driver in LUSC, and suggests that NSD3-dependency renders LUSC therapeutically vulnerable to bromodomain inhibition.

UR - http://www.scopus.com/inward/record.url?scp=85100414615&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85100414615&partnerID=8YFLogxK

U2 - 10.1038/s41586-020-03170-y

DO - 10.1038/s41586-020-03170-y

M3 - Article

C2 - 33536620

AN - SCOPUS:85100414615

SN - 0028-0836

VL - 590

SP - 504

EP - 508

JO - Nature

JF - Nature

IS - 7846

ER -

Elevated NSD3 histone methylation activity drives squamous cell lung cancer

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this