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Literature DB >> 31123088

Differential Activity of ATR and WEE1 Inhibitors in a Highly Sensitive Subpopulation of DLBCL Linked to Replication Stress.

Lucy A Young¹, Lenka Oplustil O'Connor¹, Christelle de Renty¹, Margaret H Veldman-Jones², Thierry Dorval³, Zena Wilson², David R Jones², Deborah Lawson⁴, Rajesh Odedra², Apolinar Maya-Mendoza⁵, Corinne Reimer⁴, Jiri Bartek^5,6, Alan Lau¹, Mark J O'Connor⁷.

Abstract

DNA damage checkpoint kinases ATR and WEE1 are among key regulators of DNA damage response pathways protecting cells from replication stress, a hallmark of cancer that has potential to be exploited for therapeutic use. ATR and WEE1 inhibitors are in early clinical trials and success will require greater understanding of both their mechanism of action and biomarkers for patient selection. Here, we report selective antitumor activity of ATR and WEE1 inhibitors in a subset of non-germinal center B-cell (GCB) diffuse large B-cell lymphoma (DLBCL) cell lines, characterized by high MYC protein expression and CDKN2A/B deletion. Activity correlated with the induction of replication stress, indicated by increased origin firing and retardation of replication fork progression. However, ATR and WEE1 inhibitors caused different amounts of DNA damage and cell death in distinct phases of the cell cycle, underlying the increased potency observed with WEE1 inhibition. ATR inhibition caused DNA damage to manifest as 53BP1 nuclear bodies in daughter G1 cells leading to G1 arrest, whereas WEE1 inhibition caused DNA damage and arrest in S phase, leading to earlier onset apoptosis. In vivo xenograft DLBCL models confirmed differences in single-agent antitumor activity, but also showed potential for effective ATR inhibitor combinations. Importantly, insights into the different inhibitor mechanisms may guide differentiated clinical development strategies aimed at exploiting specific vulnerabilities of tumor cells while maximizing therapeutic index. Our data therefore highlight clinical development opportunities for both ATR and WEE1 inhibitors in non-GCB DLBCL subtypes that represent an area of unmet clinical need. SIGNIFICANCE: ATR and WEE1 inhibitors demonstrate effective antitumor activity in preclinical models of DLBCL associated with replication stress, but new mechanistic insights and biomarkers of response support a differentiated clinical development strategy. ©2019 American Association for Cancer Research.

Entities: Disease Gene Species

Year: 2019 PMID： 31123088 DOI： 10.1158/0008-5472.CAN-18-2480

Source DB: PubMed Journal: Cancer Res ISSN： 0008-5472 Impact factor: 12.701

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Cited

22 in total

1. PTEN and DNA-PK determine sensitivity and recovery in response to WEE1 inhibition in human breast cancer.

Authors: Andrä Brunner; Aldwin Suryo Rahmanto; Henrik Johansson; Marcela Franco; Johanna Viiliäinen; Mohiuddin Gazi; Oliver Frings; Erik Fredlund; Charles Spruck; Janne Lehtiö; Juha K Rantala; Lars-Gunnar Larsson; Olle Sangfelt
Journal: Elife Date: 2020-07-06 Impact factor: 8.140

Review 2. Biomarker-Guided Development of DNA Repair Inhibitors.

Authors: James M Cleary; Andrew J Aguirre; Geoffrey I Shapiro; Alan D D'Andrea
Journal: Mol Cell Date: 2020-05-26 Impact factor: 17.970

Review 3. Targeting replication stress in cancer therapy.

Authors: Alexandre André B A da Costa; Dipanjan Chowdhury; Geoffrey I Shapiro; Alan D D'Andrea; Panagiotis A Konstantinopoulos
Journal: Nat Rev Drug Discov Date: 2022-10-06 Impact factor: 112.288

4. The Influence of PARP, ATR, CHK1 Inhibitors on Premature Mitotic Entry and Genomic Instability in High-Grade Serous BRCA^MUT and BRCA^WT Ovarian Cancer Cells.

Authors: Patrycja Gralewska; Arkadiusz Gajek; Dorota Rybaczek; Agnieszka Marczak; Aneta Rogalska
Journal: Cells Date: 2022-06-10 Impact factor: 7.666

5. CDK2-Mediated Upregulation of TNFα as a Mechanism of Selective Cytotoxicity in Acute Leukemia.

Authors: Husheng Ding; Nicole D Vincelette; Cordelia D McGehee; Mira A Kohorst; Brian D Koh; Annapoorna Venkatachalam; X Wei Meng; Paula A Schneider; Karen S Flatten; Kevin L Peterson; Cristina Correia; Sun-Hee Lee; Mrinal Patnaik; Jonathan A Webster; Gabriel Ghiaur; B Douglas Smith; Judith E Karp; Keith W Pratz; Hu Li; Larry M Karnitz; Scott H Kaufmann
Journal: Cancer Res Date: 2021-01-07 Impact factor: 13.312

6. Combined PARP and ATR inhibition potentiates genome instability and cell death in ATM-deficient cancer cells.

Authors: Rebecca L Lloyd; Paul W G Wijnhoven; Antonio Ramos-Montoya; Zena Wilson; Giuditta Illuzzi; Katarzyna Falenta; Gemma N Jones; Neil James; Christophe D Chabbert; Jonathan Stott; Emma Dean; Alan Lau; Lucy A Young
Journal: Oncogene Date: 2020-05-23 Impact factor: 9.867

7. Enhanced Efficacy of Aurora Kinase Inhibitors in G2/M Checkpoint Deficient TP53 Mutant Uterine Carcinomas Is Linked to the Summation of LKB1-AKT-p53 Interactions.

Authors: Katherine N Lynch; Joyce F Liu; Nikolas Kesten; Kin-Hoe Chow; Aniket Shetty; Ruiyang He; Mosammat Faria Afreen; Liping Yuan; Ursula A Matulonis; Whitfield B Growdon; Michael G Muto; Neil S Horowitz; Colleen M Feltmate; Michael J Worley; Ross S Berkowitz; Christopher P Crum; Bo R Rueda; Sarah J Hill
Journal: Cancers (Basel) Date: 2021-05-03 Impact factor: 6.639

Differential Activity of ATR and WEE1 Inhibitors in a Highly Sensitive Subpopulation of DLBCL Linked to Replication Stress.

1. PTEN and DNA-PK determine sensitivity and recovery in response to WEE1 inhibition in human breast cancer.

Review 2. Biomarker-Guided Development of DNA Repair Inhibitors.

Review 3. Targeting replication stress in cancer therapy.

4. The Influence of PARP, ATR, CHK1 Inhibitors on Premature Mitotic Entry and Genomic Instability in High-Grade Serous BRCA^MUT and BRCA^WT Ovarian Cancer Cells.

5. CDK2-Mediated Upregulation of TNFα as a Mechanism of Selective Cytotoxicity in Acute Leukemia.

6. Combined PARP and ATR inhibition potentiates genome instability and cell death in ATM-deficient cancer cells.

7. Enhanced Efficacy of Aurora Kinase Inhibitors in G2/M Checkpoint Deficient TP53 Mutant Uterine Carcinomas Is Linked to the Summation of LKB1-AKT-p53 Interactions.

Review 8. Exploiting Replication Stress as a Novel Therapeutic Intervention.

Review 9. WEE1 Inhibitor: Clinical Development.

10. Efficacy and Biomarker Analysis of Adavosertib in Differentiated Thyroid Cancer.

Differential Activity of ATR and WEE1 Inhibitors in a Highly Sensitive Subpopulation of DLBCL Linked to Replication Stress.

1. PTEN and DNA-PK determine sensitivity and recovery in response to WEE1 inhibition in human breast cancer.

Review 2. Biomarker-Guided Development of DNA Repair Inhibitors.

Review 3. Targeting replication stress in cancer therapy.

4. The Influence of PARP, ATR, CHK1 Inhibitors on Premature Mitotic Entry and Genomic Instability in High-Grade Serous BRCAMUT and BRCAWT Ovarian Cancer Cells.

5. CDK2-Mediated Upregulation of TNFα as a Mechanism of Selective Cytotoxicity in Acute Leukemia.

6. Combined PARP and ATR inhibition potentiates genome instability and cell death in ATM-deficient cancer cells.

7. Enhanced Efficacy of Aurora Kinase Inhibitors in G2/M Checkpoint Deficient TP53 Mutant Uterine Carcinomas Is Linked to the Summation of LKB1-AKT-p53 Interactions.

Review 8. Exploiting Replication Stress as a Novel Therapeutic Intervention.

Review 9. WEE1 Inhibitor: Clinical Development.

10. Efficacy and Biomarker Analysis of Adavosertib in Differentiated Thyroid Cancer.

4. The Influence of PARP, ATR, CHK1 Inhibitors on Premature Mitotic Entry and Genomic Instability in High-Grade Serous BRCA^MUT and BRCA^WT Ovarian Cancer Cells.