Selective inhibitors of mTORC1 activate 4EBP1 and suppress tumor growth

被引：47

作者：

Lee, Bianca J. ^{[1
]}

Boyer, Jacob A. ^{[2
,3
]}

Burnett, G. Leslie ^{[4
]}

Thottumkara, Arun P. ^{[4
]}

Tibrewal, Nidhi ^{[5
]}

Wilson, Stacy L. ^{[1
]}

Hsieh, Tientien ^{[5
]}

Marquez, Abby ^{[5
]}

Lorenzana, Edward G. ^{[1
]}

Evans, James W. ^{[1
]}

Hulea, Laura ^{[6
,7
,8
,9
,10
,11
]}

Kiss, Gert

Liu, Hui

Lee, Dong ^{[13
]}

Larsson, Ola ^{[12
]}

McLaughlan, Shannon ^{[6
,7
,8
]}

Topisirovic, Ivan ^{[6
,7
,8
]}

Wang, Zhengping ^{[13
]}

Wang, Zhican ^{[13
]}

Zhao, Yongyuan ^{[13
]}

Wildes, David ^{[1
]}

Aggen, James B. ^{[4
]}

Singh, Mallika ^{[1
]}

Gill, Adrian L. ^{[4
]}

Smith, Jacqueline A. M. ^{[1
]}

Rosen, Neal ^{[3
]}

机构：

[1] Revolut Med Inc, Dept Biol, Redwood City, CA 94063 USA

[2] Mem Sloan Kettering Canc Ctr, Grad Sch Biomed Sci, New York, NY 10065 USA

[3] Mem Sloan Kettering Canc Ctr, Dept Med, Program Mol Pharmacol, New York, NY 10065 USA

[4] Revolut Med Inc, Dept Chem, Redwood City, CA 94063 USA

[5] Revolut Med Inc, Dept Discovery Technol, Redwood City, CA 94063 USA

[6] McGill Univ, Gerald Bronfman Dept Oncol, Montreal, PQ, Canada

[7] McGill Univ, Lady Davis Inst, Dept Biochem, Montreal, PQ, Canada

[8] McGill Univ, Lady Davis Inst, Dept Expt Med, Montreal, PQ, Canada

[9] Univ Montreal, Dept Med, Montreal, PQ, Canada

[10] Univ Montreal, Dept Biochim & Med Mol, Montreal, PQ, Canada

[11] Maisonneuve Rosemont Hosp, Res Ctr, Montreal, PQ, Canada

[12] Karolinska Inst, Dept Oncol Pathol, Sci Life Lab, Solna, Sweden

[13] Revolut Med Inc, Dept Non clin Dev & Clin Pharmacol, Redwood City, CA 94063 USA

来源：

NATURE CHEMICAL BIOLOGY | 2021年 / 17卷 / 10期

关键词：

MAMMALIAN TARGET; TRANSLATIONAL CONTROL; RAPAMYCIN ANALOGS; CELL-GROWTH; PATHWAY; COMPLEX; KINASE; RNA; AKT; DOMAIN;

D O I：

10.1038/s41589-021-00813-7

中图分类号：

Q5 [生物化学]; Q7 [分子生物学];

学科分类号：

071010 ; 081704 ;

摘要：

The clinical benefits of pan-mTOR active-site inhibitors are limited by toxicity and relief of feedback inhibition of receptor expression. To address these limitations, we designed a series of compounds that selectively inhibit mTORC1 and not mTORC2. These 'bi-steric inhibitors' comprise a rapamycin-like core moiety covalently linked to an mTOR active-site inhibitor. Structural modification of these components modulated their affinities for their binding sites on mTOR and the selectivity of the bi-steric compound. mTORC1-selective compounds potently inhibited 4EBP1 phosphorylation and caused regressions of breast cancer xenografts. Inhibition of 4EBP1 phosphorylation was sufficient to block cancer cell growth and was necessary for maximal antitumor activity. At mTORC1-selective doses, these compounds do not alter glucose tolerance, nor do they relieve AKT-dependent feedback inhibition of HER3. Thus, in preclinical models, selective inhibitors of mTORC1 potently inhibit tumor growth while causing less toxicity and receptor reactivation as compared to pan-mTOR inhibitors.

引用

页码：1065 / 1074

页数：10

共 50 条

[1] Selective inhibitors of mTORC1 activate 4EBP1 and suppress tumor growth
Bianca J. Lee
Jacob A. Boyer
G. Leslie Burnett
Arun P. Thottumkara
Nidhi Tibrewal
Stacy L. Wilson
Tientien Hsieh
Abby Marquez
Edward G. Lorenzana
James W. Evans
Laura Hulea
Gert Kiss
Hui Liu
Dong Lee
Ola Larsson
Shannon McLaughlan
Ivan Topisirovic
Zhengping Wang
Zhican Wang
Yongyuan Zhao
David Wildes
James B. Aggen
Mallika Singh
Adrian L. Gill
Jacqueline A. M. Smith
Neal Rosen
Nature Chemical Biology, 2021, 17 : 1065 - 1074
[2] Author Correction: Selective inhibitors of mTORC1 activate 4EBP1 and suppress tumor growth
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Jacob A. Boyer
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