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

SIMPLE SUMMARY: Cancers arising from the lining of the uterus, endometrial cancers, are the most common gynecologic malignancy in the United States. Once endometrial cancer escapes the uterus and grows in distant locations, there are limited therapeutic options. The most aggressive and lethal endome...

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Autores principales: Lynch, Katherine N., Liu, Joyce F., Kesten, Nikolas, Chow, Kin-Hoe, Shetty, Aniket, He, Ruiyang, Afreen, Mosammat Faria, Yuan, Liping, Matulonis, Ursula A., Growdon, Whitfield B., Muto, Michael G., Horowitz, Neil S., Feltmate, Colleen M., Worley, Michael J., Berkowitz, Ross S., Crum, Christopher P., Rueda, Bo R., Hill, Sarah J.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8125555/
https://www.ncbi.nlm.nih.gov/pubmed/34063609
http://dx.doi.org/10.3390/cancers13092195
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author Lynch, Katherine N.
Liu, Joyce F.
Kesten, Nikolas
Chow, Kin-Hoe
Shetty, Aniket
He, Ruiyang
Afreen, Mosammat Faria
Yuan, Liping
Matulonis, Ursula A.
Growdon, Whitfield B.
Muto, Michael G.
Horowitz, Neil S.
Feltmate, Colleen M.
Worley, Michael J.
Berkowitz, Ross S.
Crum, Christopher P.
Rueda, Bo R.
Hill, Sarah J.
author_facet Lynch, Katherine N.
Liu, Joyce F.
Kesten, Nikolas
Chow, Kin-Hoe
Shetty, Aniket
He, Ruiyang
Afreen, Mosammat Faria
Yuan, Liping
Matulonis, Ursula A.
Growdon, Whitfield B.
Muto, Michael G.
Horowitz, Neil S.
Feltmate, Colleen M.
Worley, Michael J.
Berkowitz, Ross S.
Crum, Christopher P.
Rueda, Bo R.
Hill, Sarah J.
author_sort Lynch, Katherine N.
collection PubMed
description SIMPLE SUMMARY: Cancers arising from the lining of the uterus, endometrial cancers, are the most common gynecologic malignancy in the United States. Once endometrial cancer escapes the uterus and grows in distant locations, there are limited therapeutic options. The most aggressive and lethal endometrial cancers carry alterations in the protein p53, which is a critical guardian of many cellular functions. The role of these p53 alterations in endometrial cancer is not well understood. The goal of this work was to use p53 altered models of endometrial cancer to understand which, if any, therapeutically targetable vulnerabilities these p53 alterations may confer in endometrial cancer. Here we show that many of these p53 altered cells have problems with cell division which can be targeted with novel single and combination therapies. These discoveries may lead to relevant new therapies for difficult to treat advanced stage endometrial cancers. ABSTRACT: Uterine carcinoma (UC) is the most common gynecologic malignancy in the United States. TP53 mutant UCs cause a disproportionate number of deaths due to limited therapies for these tumors and the lack of mechanistic understanding of their fundamental vulnerabilities. Here we sought to understand the functional and therapeutic relevance of TP53 mutations in UC. We functionally profiled targetable TP53 dependent DNA damage repair and cell cycle control pathways in a panel of TP53 mutant UC cell lines and patient-derived organoids. There were no consistent defects in DNA damage repair pathways. Rather, most models demonstrated dependence on defective G2/M cell cycle checkpoints and subsequent upregulation of Aurora kinase-LKB1-p53-AKT signaling in the setting of baseline mitotic defects. This combination makes them sensitive to Aurora kinase inhibition. Resistant lines demonstrated an intact G2/M checkpoint, and combining Aurora kinase and WEE1 inhibitors, which then push these cells through mitosis with Aurora kinase inhibitor-induced spindle defects, led to apoptosis in these cases. Overall, this work presents Aurora kinase inhibitors alone or in combination with WEE1 inhibitors as relevant mechanism driven therapies for TP53 mutant UCs. Context specific functional assessment of the G2/M checkpoint may serve as a biomarker in identifying Aurora kinase inhibitor sensitive tumors.
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spelling pubmed-81255552021-05-17 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 Lynch, Katherine N. Liu, Joyce F. Kesten, Nikolas Chow, Kin-Hoe Shetty, Aniket He, Ruiyang Afreen, Mosammat Faria Yuan, Liping Matulonis, Ursula A. Growdon, Whitfield B. Muto, Michael G. Horowitz, Neil S. Feltmate, Colleen M. Worley, Michael J. Berkowitz, Ross S. Crum, Christopher P. Rueda, Bo R. Hill, Sarah J. Cancers (Basel) Article SIMPLE SUMMARY: Cancers arising from the lining of the uterus, endometrial cancers, are the most common gynecologic malignancy in the United States. Once endometrial cancer escapes the uterus and grows in distant locations, there are limited therapeutic options. The most aggressive and lethal endometrial cancers carry alterations in the protein p53, which is a critical guardian of many cellular functions. The role of these p53 alterations in endometrial cancer is not well understood. The goal of this work was to use p53 altered models of endometrial cancer to understand which, if any, therapeutically targetable vulnerabilities these p53 alterations may confer in endometrial cancer. Here we show that many of these p53 altered cells have problems with cell division which can be targeted with novel single and combination therapies. These discoveries may lead to relevant new therapies for difficult to treat advanced stage endometrial cancers. ABSTRACT: Uterine carcinoma (UC) is the most common gynecologic malignancy in the United States. TP53 mutant UCs cause a disproportionate number of deaths due to limited therapies for these tumors and the lack of mechanistic understanding of their fundamental vulnerabilities. Here we sought to understand the functional and therapeutic relevance of TP53 mutations in UC. We functionally profiled targetable TP53 dependent DNA damage repair and cell cycle control pathways in a panel of TP53 mutant UC cell lines and patient-derived organoids. There were no consistent defects in DNA damage repair pathways. Rather, most models demonstrated dependence on defective G2/M cell cycle checkpoints and subsequent upregulation of Aurora kinase-LKB1-p53-AKT signaling in the setting of baseline mitotic defects. This combination makes them sensitive to Aurora kinase inhibition. Resistant lines demonstrated an intact G2/M checkpoint, and combining Aurora kinase and WEE1 inhibitors, which then push these cells through mitosis with Aurora kinase inhibitor-induced spindle defects, led to apoptosis in these cases. Overall, this work presents Aurora kinase inhibitors alone or in combination with WEE1 inhibitors as relevant mechanism driven therapies for TP53 mutant UCs. Context specific functional assessment of the G2/M checkpoint may serve as a biomarker in identifying Aurora kinase inhibitor sensitive tumors. MDPI 2021-05-03 /pmc/articles/PMC8125555/ /pubmed/34063609 http://dx.doi.org/10.3390/cancers13092195 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Lynch, Katherine N.
Liu, Joyce F.
Kesten, Nikolas
Chow, Kin-Hoe
Shetty, Aniket
He, Ruiyang
Afreen, Mosammat Faria
Yuan, Liping
Matulonis, Ursula A.
Growdon, Whitfield B.
Muto, Michael G.
Horowitz, Neil S.
Feltmate, Colleen M.
Worley, Michael J.
Berkowitz, Ross S.
Crum, Christopher P.
Rueda, Bo R.
Hill, Sarah J.
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
title 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
title_full 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
title_fullStr 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
title_full_unstemmed 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
title_short 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
title_sort 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
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8125555/
https://www.ncbi.nlm.nih.gov/pubmed/34063609
http://dx.doi.org/10.3390/cancers13092195
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