De novo GTP synthesis is a metabolic vulnerability for the interception of brain metastases

被引：0

作者：

Kieliszek, Agata M. ^{[1
,2
,4
]}

Mobilio, Daniel ^{[1
,2
,4
]}

Bassey-Archibong, Blessing I. ^{[1
,3
,4
]}

Johnson, Jarrod W. ^{[2
,4
]}

Piotrowski, Mathew L. ^{[2
,4
]}

de Araujo, Elvin D. ^{[4
]}

Sedighi, Abootaleb ^{[4
]}

Aghaei, Nikoo ^{[1
,2
,4
]}

Escudero, Laura ^{[1
,3
,4
]}

Ang, Patrick ^{[1
,4
]}

Gwynne, William D. ^{[1
,3
,4
]}

Zhang, Cunjie ^{[4
,5
,6
]}

Quaile, Andrew ^{[4
,5
,6
]}

McKenna, Dillon ^{[1
,3
,4
]}

Subapanditha, Minomi ^{[3
,4
]}

Tokar, Tomas ^{[4
,7
]}

Shaikh, Muhammad Vaseem ^{[1
,3
,4
]}

Zhai, Kui ^{[1
,3
,4
]}

Chafe, Shawn C. ^{[1
,3
,4
]}

Gunning, Patrick T. ^{[4
]}

Montenegro-Burke, J. Rafael ^{[4
,5
,6
]}

Venugopal, Chitra

Magolan, Jakob ^{[2
,4
]}

Singh, Sheila K. ^{[1
,2
,3
,4
]}

机构：

[1] McMaster Univ, Ctr Discovery Canc Res, Hamilton, ON, Canada

[2] McMaster Univ, Dept Biochem & Biomed Sci, Hamilton, ON, Canada

[3] McMaster Univ, Dept Surg, Hamilton, ON, Canada

[4] Univ Toronto Mississauga, Ctr Med Chem, Mississauga, ON, Canada

[5] Univ Toronto, Terrence Donnelly Ctr Cellular & Biomol Res, Toronto, ON, Canada

[6] Univ Toronto, Dept Mol Genet, Toronto, ON, Canada

[7] Univ Hlth Network, Krembil Res Inst, Toronto, ON, Canada

来源：

CELL REPORTS MEDICINE | 2024年 / 5卷 / 10期

基金：

加拿大自然科学与工程研究理事会; 加拿大创新基金会;

关键词：

TUMOR-INITIATING CELLS; MYCOPHENOLIC-ACID; SMALL MOLECULES; STEM-CELL; CANCER; EXPRESSION; INHIBITORS; TARGET; SURVIVAL; DESIGN;

D O I：

10.1016/j.xcrm.2024.101755

中图分类号：

Q2 [细胞生物学];

学科分类号：

071009 ; 090102 ;

摘要：

Patients with brain metastases (BM) face a 90% mortality rate within one year of diagnosis and the current standard of care is palliative. Targeting BM-initiating cells (BMICs) is a feasible strategy to treat BM, but druggable targets are limited. Here, we apply Connectivity Map analysis to lung-, breast-, and melanoma- pre-metastatic BMIC gene expression signatures and identify inosine monophosphate dehydrogenase (IMPDH), the rate-limiting enzyme in the de novo GTP synthesis pathway, as a target for BM. We show that pharmacological and genetic perturbation of IMPDH attenuates BMIC proliferation in vitro and the formation of BM in vivo. Metabolomic analyses and CRISPR knockout studies confirm that de novo GTP synthesis is a potent metabolic vulnerability in BM. Overall, our work employs a phenotype-guided therapeutic strategy to uncover IMPDH as a relevant target for attenuating BM outgrowth, which may provide an alternative treatment strategy for patients who are otherwise limited to palliation.

引用

页数：21

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