EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC

Gnana P. Krishnamoorthy; Natalie R. Davidson; Steven D. Leach; Zhen Zhao; Scott W. Lowe; Gina Lee; Iňigo Landa; James Nagarajah; Mahesh Saqcena; Kamini Singh; Hans Guido Wendel; Snjezana Dogan; Prasanna P. Tamarapu; John Blenis; Ronald A. Ghossein; Jeffrey A. Knauf; Gunnar Rätsch; James A. Fagin

doi:10.1158/2159-8290.CD-18-0606

EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC

Gnana P. Krishnamoorthy, Natalie R. Davidson, Steven D. Leach, Zhen Zhao, Scott W. Lowe, Gina Lee, Iňigo Landa, James Nagarajah, Mahesh Saqcena, Kamini Singh, Hans Guido Wendel, Snjezana Dogan, Prasanna P. Tamarapu, John Blenis, Ronald A. Ghossein, Jeffrey A. Knauf, Gunnar Rätsch, James A. Fagin

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

56 Scopus citations

Abstract

Translation initiation is orchestrated by the cap binding and 43S preinitiation complexes (PIC). Eukaryotic initiation factor 1A (EIF1A) is essential for recruitment of the ternary complex and for assembling the 43S PIC. Recurrent EIF1AX mutations in papillary thyroid cancers are mutually exclusive with other drivers, including RAS. EIF1AX mutations are enriched in advanced thyroid cancers, where they display a striking co-occurrence with RAS, which cooperates to induce tumorigenesis in mice and isogenic cell lines. The C-terminal EIF1AX-A113splice mutation is the most prevalent in advanced thyroid cancer. EIF1AX-A113splice variants stabilize the PIC and induce ATF4, a sensor of cellular stress, which is co-opted to suppress EIF2α phosphorylation, enabling a general increase in protein synthesis. RAS stabilizes c-MYC, an effect augmented by EIF1AX-A113splice. ATF4 and c-MYC induce expression of amino acid transporters and enhance sensitivity of mTOR to amino acid supply. These mutually reinforcing events generate therapeutic vulnerabilities to MEK, BRD4, and mTOR kinase inhibitors. Significance: Mutations of EIF1AX, a component of the translation PIC, co-occur with RAS in advanced thyroid cancers and promote tumorigenesis. EIF1AX-A113splice drives an ATF4-induced dephosphorylation of EIF2α, resulting in increased protein synthesis. ATF4 also cooperates with c-MYC to sensitize mTOR to amino acid supply, thus generating vulnerability to mTOR kinase inhibitors.

Original language	English (US)
Pages (from-to)	264-281
Number of pages	18
Journal	Cancer discovery
Volume	9
Issue number	2
DOIs	https://doi.org/10.1158/2159-8290.CD-18-0606
State	Published - 2019
Externally published	Yes

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Oncology

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10.1158/2159-8290.CD-18-0606

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Krishnamoorthy, G. P., Davidson, N. R., Leach, S. D., Zhao, Z., Lowe, S. W., Lee, G., Landa, I., Nagarajah, J., Saqcena, M., Singh, K., Wendel, H. G., Dogan, S., Tamarapu, P. P., Blenis, J., Ghossein, R. A., Knauf, J. A., Rätsch, G., & Fagin, J. A. (2019). EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC. Cancer discovery, 9(2), 264-281. https://doi.org/10.1158/2159-8290.CD-18-0606

Krishnamoorthy, GP, Davidson, NR, Leach, SD, Zhao, Z, Lowe, SW, Lee, G, Landa, I, Nagarajah, J, Saqcena, M, Singh, K, Wendel, HG, Dogan, S, Tamarapu, PP, Blenis, J, Ghossein, RA, Knauf, JA, Rätsch, G & Fagin, JA 2019, 'EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC', Cancer discovery, vol. 9, no. 2, pp. 264-281. https://doi.org/10.1158/2159-8290.CD-18-0606

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title = "EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC",

abstract = "Translation initiation is orchestrated by the cap binding and 43S preinitiation complexes (PIC). Eukaryotic initiation factor 1A (EIF1A) is essential for recruitment of the ternary complex and for assembling the 43S PIC. Recurrent EIF1AX mutations in papillary thyroid cancers are mutually exclusive with other drivers, including RAS. EIF1AX mutations are enriched in advanced thyroid cancers, where they display a striking co-occurrence with RAS, which cooperates to induce tumorigenesis in mice and isogenic cell lines. The C-terminal EIF1AX-A113splice mutation is the most prevalent in advanced thyroid cancer. EIF1AX-A113splice variants stabilize the PIC and induce ATF4, a sensor of cellular stress, which is co-opted to suppress EIF2α phosphorylation, enabling a general increase in protein synthesis. RAS stabilizes c-MYC, an effect augmented by EIF1AX-A113splice. ATF4 and c-MYC induce expression of amino acid transporters and enhance sensitivity of mTOR to amino acid supply. These mutually reinforcing events generate therapeutic vulnerabilities to MEK, BRD4, and mTOR kinase inhibitors. Significance: Mutations of EIF1AX, a component of the translation PIC, co-occur with RAS in advanced thyroid cancers and promote tumorigenesis. EIF1AX-A113splice drives an ATF4-induced dephosphorylation of EIF2α, resulting in increased protein synthesis. ATF4 also cooperates with c-MYC to sensitize mTOR to amino acid supply, thus generating vulnerability to mTOR kinase inhibitors.",

author = "Krishnamoorthy, {Gnana P.} and Davidson, {Natalie R.} and Leach, {Steven D.} and Zhen Zhao and Lowe, {Scott W.} and Gina Lee and I{\v n}igo Landa and James Nagarajah and Mahesh Saqcena and Kamini Singh and Wendel, {Hans Guido} and Snjezana Dogan and Tamarapu, {Prasanna P.} and John Blenis and Ghossein, {Ronald A.} and Knauf, {Jeffrey A.} and Gunnar R{\"a}tsch and Fagin, {James A.}",

note = "Publisher Copyright: {\textcopyright} 2019 American Association for Cancer Research.",

year = "2019",

doi = "10.1158/2159-8290.CD-18-0606",

language = "English (US)",

volume = "9",

pages = "264--281",

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T1 - EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC

AU - Krishnamoorthy, Gnana P.

AU - Davidson, Natalie R.

AU - Leach, Steven D.

AU - Zhao, Zhen

AU - Lowe, Scott W.

AU - Lee, Gina

AU - Landa, Iňigo

AU - Nagarajah, James

AU - Saqcena, Mahesh

AU - Singh, Kamini

AU - Wendel, Hans Guido

AU - Dogan, Snjezana

AU - Tamarapu, Prasanna P.

AU - Blenis, John

AU - Ghossein, Ronald A.

AU - Knauf, Jeffrey A.

AU - Rätsch, Gunnar

AU - Fagin, James A.

PY - 2019

Y1 - 2019

N2 - Translation initiation is orchestrated by the cap binding and 43S preinitiation complexes (PIC). Eukaryotic initiation factor 1A (EIF1A) is essential for recruitment of the ternary complex and for assembling the 43S PIC. Recurrent EIF1AX mutations in papillary thyroid cancers are mutually exclusive with other drivers, including RAS. EIF1AX mutations are enriched in advanced thyroid cancers, where they display a striking co-occurrence with RAS, which cooperates to induce tumorigenesis in mice and isogenic cell lines. The C-terminal EIF1AX-A113splice mutation is the most prevalent in advanced thyroid cancer. EIF1AX-A113splice variants stabilize the PIC and induce ATF4, a sensor of cellular stress, which is co-opted to suppress EIF2α phosphorylation, enabling a general increase in protein synthesis. RAS stabilizes c-MYC, an effect augmented by EIF1AX-A113splice. ATF4 and c-MYC induce expression of amino acid transporters and enhance sensitivity of mTOR to amino acid supply. These mutually reinforcing events generate therapeutic vulnerabilities to MEK, BRD4, and mTOR kinase inhibitors. Significance: Mutations of EIF1AX, a component of the translation PIC, co-occur with RAS in advanced thyroid cancers and promote tumorigenesis. EIF1AX-A113splice drives an ATF4-induced dephosphorylation of EIF2α, resulting in increased protein synthesis. ATF4 also cooperates with c-MYC to sensitize mTOR to amino acid supply, thus generating vulnerability to mTOR kinase inhibitors.

AB - Translation initiation is orchestrated by the cap binding and 43S preinitiation complexes (PIC). Eukaryotic initiation factor 1A (EIF1A) is essential for recruitment of the ternary complex and for assembling the 43S PIC. Recurrent EIF1AX mutations in papillary thyroid cancers are mutually exclusive with other drivers, including RAS. EIF1AX mutations are enriched in advanced thyroid cancers, where they display a striking co-occurrence with RAS, which cooperates to induce tumorigenesis in mice and isogenic cell lines. The C-terminal EIF1AX-A113splice mutation is the most prevalent in advanced thyroid cancer. EIF1AX-A113splice variants stabilize the PIC and induce ATF4, a sensor of cellular stress, which is co-opted to suppress EIF2α phosphorylation, enabling a general increase in protein synthesis. RAS stabilizes c-MYC, an effect augmented by EIF1AX-A113splice. ATF4 and c-MYC induce expression of amino acid transporters and enhance sensitivity of mTOR to amino acid supply. These mutually reinforcing events generate therapeutic vulnerabilities to MEK, BRD4, and mTOR kinase inhibitors. Significance: Mutations of EIF1AX, a component of the translation PIC, co-occur with RAS in advanced thyroid cancers and promote tumorigenesis. EIF1AX-A113splice drives an ATF4-induced dephosphorylation of EIF2α, resulting in increased protein synthesis. ATF4 also cooperates with c-MYC to sensitize mTOR to amino acid supply, thus generating vulnerability to mTOR kinase inhibitors.

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JO - Cancer discovery

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ER -

EIF1AX and RAS mutations cooperate to drive thyroid tumorigenesis through ATF4 and C-MYC

Abstract

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