Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer

P. Jake Slavish; Liying Chi; Mi Kyung Yun; Lyudmila Tsurkan; Nancy E. Martinez; Barbara Jonchere; Sergio C. Chai; Michele Connelly; M. Brett Waddell; Sourav Das; Geoffrey Neale; Zhenmei Li; William R. Shadrick; Rachelle R. Olsen; Kevin W. Freeman; Jonathan A. Low; Jeanine E. Price; Brandon M. Young; Nagakumar Bharatham; Vincent A. Boyd; Jun Yang; Richard E. Lee; Marie Morfouace; Martine F. Roussel; Taosheng Chen; Daniel Savic; R. Kiplin Guy; Stephen W. White; Anang A. Shelat; Philip M. Potter

doi:10.1158/0008-5472.CAN-19-3934

Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer

P. Jake Slavish
, Liying Chi
, Mi Kyung Yun
, Lyudmila Tsurkan
, Nancy E. Martinez
, Barbara Jonchere
, Sergio C. Chai
, Michele Connelly
, M. Brett Waddell
, Sourav Das
, Geoffrey Neale
, Zhenmei Li
, William R. Shadrick
, Rachelle R. Olsen
, Kevin W. Freeman
, Jonathan A. Low
, Jeanine E. Price
, Brandon M. Young
, Nagakumar Bharatham
, Vincent A. Boyd

Jun Yang, Richard E. Lee, Marie Morfouace, Martine F. Roussel, Taosheng Chen, Daniel Savic, R. Kiplin Guy, Stephen W. White, Anang A. Shelat, Philip M. Potter

Producción científica: Article › revisión exhaustiva

37 Citas (Scopus)

Resumen

Inhibition of members of the bromodomain and extraterminal (BET) family of proteins has proven a valid strategy for cancer chemotherapy. All BET identified to date contain two bromodomains (BD; BD1 and BD2) that are necessary for recognition of acetylated lysine residues in the N-terminal regions of histones. Chemical matter that targets BET (BETi) also interact via these domains. Molecular and cellular data indicate that BD1 and BD2 have different biological roles depending upon their cellular context, with BD2 particularly associated with cancer. We have therefore pursued the development of BD2-selective molecules both as chemical probes and as potential leads for drug development. Here we report the structure-based generation of a novel series of tetrahydroquinoline analogs that exhibit >50-fold selectivity for BD2 versus BD1. This selective targeting resulted in engagement with BD-containing proteins in cells, resulting in modulation of MYC proteins and downstream targets. These compounds were potent cytotoxins toward numerous pediatric cancer cell lines and were minimally toxic to nontumorigenic cells. In addition, unlike the pan BETi (þ)-JQ1, these BD2-selective inhibitors demonstrated no rebound expression effects. Finally, we report a pharmacokinetic-optimized, metabolically stable derivative that induced growth delay in a neuroblastoma xenograft model with minimal toxicity. We conclude that BD2-selective agents are valid candidates for antitumor drug design for pediatric malignancies driven by the MYC oncogene.

Idioma original	English
Páginas (desde-hasta)	3507-3518
Número de páginas	12
Publicación	Cancer Research
Volumen	80
N.º	17
DOI	https://doi.org/10.1158/0008-5472.CAN-19-3934
Estado	Published - sept 1 2020

Nota bibliográfica

Publisher Copyright:
© 2020 American Association for Cancer Research.

Financiación

We would like to acknowledge Dr. Aaron Pitre from the Cellular Imaging Shared Resource at St. Jude Children's Research Hospital for his assistance with the FRAP experiments. High-resolution microscopy images were acquired in the Cell & Tissue Imaging Center at St. Jude. This work was supported, in part, by NIH grants (P01 CA096832 to M.F. Roussel; R01 CA225945 to A.A. Shelat and P.M. Potter), a Cancer Center Core grant (NCI, P30 CA021765), and by the American Lebanese Syrian Associated Charities (ALSAC). We would like to acknowledge Dr. Aaron Pitre from the Cellular Imaging Shared Resource at St. Jude Children’s Research Hospital for his assistance with the FRAP experiments. High-resolution microscopy images were acquired in the Cell & Tissue Imaging Center at St. Jude. This work was supported, in part, by NIH grants (P01 CA096832 to M.F. Roussel; R01 CA225945 to A.A. Shelat and P.M. Potter), a Cancer Center Core grant (NCI, P30 CA021765), and by the American Lebanese Syrian Associated Charities (ALSAC).

Financiadores	Número del financiador
Cancer Center Core
National Institutes of Health (NIH)	R01 CA225945
National Institutes of Health (NIH)
National Childhood Cancer Registry – National Cancer Institute	P30 CA021765, P01CA096832
National Childhood Cancer Registry – National Cancer Institute
St. Jude Medical Center
American Lebanese Syrian Associated Charities

ODS de las Naciones Unidas

Este resultado contribuye a los siguientes Objetivos de Desarrollo Sostenible

Good health and well being

ASJC Scopus subject areas

Oncology
Cancer Research

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10.1158/0008-5472.CAN-19-3934

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Jake Slavish, P., Chi, L., Yun, M. K., Tsurkan, L., Martinez, N. E., Jonchere, B., Chai, S. C., Connelly, M., Brett Waddell, M., Das, S., Neale, G., Li, Z., Shadrick, W. R., Olsen, R. R., Freeman, K. W., Low, J. A., Price, J. E., Young, B. M., Bharatham, N., ... Potter, P. M. (2020). Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer. Cancer Research, 80(17), 3507-3518. https://doi.org/10.1158/0008-5472.CAN-19-3934

@article{137dc2aaeb5f4a19977c270261b3d883,

title = "Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer",

abstract = "Inhibition of members of the bromodomain and extraterminal (BET) family of proteins has proven a valid strategy for cancer chemotherapy. All BET identified to date contain two bromodomains (BD; BD1 and BD2) that are necessary for recognition of acetylated lysine residues in the N-terminal regions of histones. Chemical matter that targets BET (BETi) also interact via these domains. Molecular and cellular data indicate that BD1 and BD2 have different biological roles depending upon their cellular context, with BD2 particularly associated with cancer. We have therefore pursued the development of BD2-selective molecules both as chemical probes and as potential leads for drug development. Here we report the structure-based generation of a novel series of tetrahydroquinoline analogs that exhibit >50-fold selectivity for BD2 versus BD1. This selective targeting resulted in engagement with BD-containing proteins in cells, resulting in modulation of MYC proteins and downstream targets. These compounds were potent cytotoxins toward numerous pediatric cancer cell lines and were minimally toxic to nontumorigenic cells. In addition, unlike the pan BETi ({\th})-JQ1, these BD2-selective inhibitors demonstrated no rebound expression effects. Finally, we report a pharmacokinetic-optimized, metabolically stable derivative that induced growth delay in a neuroblastoma xenograft model with minimal toxicity. We conclude that BD2-selective agents are valid candidates for antitumor drug design for pediatric malignancies driven by the MYC oncogene.",

author = "\{Jake Slavish\}, P. and Liying Chi and Yun, \{Mi Kyung\} and Lyudmila Tsurkan and Martinez, \{Nancy E.\} and Barbara Jonchere and Chai, \{Sergio C.\} and Michele Connelly and \{Brett Waddell\}, M. and Sourav Das and Geoffrey Neale and Zhenmei Li and Shadrick, \{William R.\} and Olsen, \{Rachelle R.\} and Freeman, \{Kevin W.\} and Low, \{Jonathan A.\} and Price, \{Jeanine E.\} and Young, \{Brandon M.\} and Nagakumar Bharatham and Boyd, \{Vincent A.\} and Jun Yang and Lee, \{Richard E.\} and Marie Morfouace and Roussel, \{Martine F.\} and Taosheng Chen and Daniel Savic and \{Kiplin Guy\}, R. and White, \{Stephen W.\} and Shelat, \{Anang A.\} and Potter, \{Philip M.\}",

note = "Publisher Copyright: {\textcopyright} 2020 American Association for Cancer Research.",

year = "2020",

month = sep,

day = "1",

doi = "10.1158/0008-5472.CAN-19-3934",

language = "English",

volume = "80",

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Jake Slavish, P, Chi, L, Yun, MK, Tsurkan, L, Martinez, NE, Jonchere, B, Chai, SC, Connelly, M, Brett Waddell, M, Das, S, Neale, G, Li, Z, Shadrick, WR, Olsen, RR, Freeman, KW, Low, JA, Price, JE, Young, BM, Bharatham, N, Boyd, VA, Yang, J, Lee, RE, Morfouace, M, Roussel, MF, Chen, T, Savic, D, Kiplin Guy, R, White, SW, Shelat, AA & Potter, PM 2020, 'Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer', Cancer Research, vol. 80, n.º 17, pp. 3507-3518. https://doi.org/10.1158/0008-5472.CAN-19-3934

TY - JOUR

T1 - Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer

AU - Jake Slavish, P.

AU - Chi, Liying

AU - Yun, Mi Kyung

AU - Tsurkan, Lyudmila

AU - Martinez, Nancy E.

AU - Jonchere, Barbara

AU - Chai, Sergio C.

AU - Connelly, Michele

AU - Brett Waddell, M.

AU - Das, Sourav

AU - Neale, Geoffrey

AU - Li, Zhenmei

AU - Shadrick, William R.

AU - Olsen, Rachelle R.

AU - Freeman, Kevin W.

AU - Low, Jonathan A.

AU - Price, Jeanine E.

AU - Young, Brandon M.

AU - Bharatham, Nagakumar

AU - Boyd, Vincent A.

AU - Yang, Jun

AU - Lee, Richard E.

AU - Morfouace, Marie

AU - Roussel, Martine F.

AU - Chen, Taosheng

AU - Savic, Daniel

AU - Kiplin Guy, R.

AU - White, Stephen W.

AU - Shelat, Anang A.

AU - Potter, Philip M.

PY - 2020/9/1

Y1 - 2020/9/1

N2 - Inhibition of members of the bromodomain and extraterminal (BET) family of proteins has proven a valid strategy for cancer chemotherapy. All BET identified to date contain two bromodomains (BD; BD1 and BD2) that are necessary for recognition of acetylated lysine residues in the N-terminal regions of histones. Chemical matter that targets BET (BETi) also interact via these domains. Molecular and cellular data indicate that BD1 and BD2 have different biological roles depending upon their cellular context, with BD2 particularly associated with cancer. We have therefore pursued the development of BD2-selective molecules both as chemical probes and as potential leads for drug development. Here we report the structure-based generation of a novel series of tetrahydroquinoline analogs that exhibit >50-fold selectivity for BD2 versus BD1. This selective targeting resulted in engagement with BD-containing proteins in cells, resulting in modulation of MYC proteins and downstream targets. These compounds were potent cytotoxins toward numerous pediatric cancer cell lines and were minimally toxic to nontumorigenic cells. In addition, unlike the pan BETi (þ)-JQ1, these BD2-selective inhibitors demonstrated no rebound expression effects. Finally, we report a pharmacokinetic-optimized, metabolically stable derivative that induced growth delay in a neuroblastoma xenograft model with minimal toxicity. We conclude that BD2-selective agents are valid candidates for antitumor drug design for pediatric malignancies driven by the MYC oncogene.

AB - Inhibition of members of the bromodomain and extraterminal (BET) family of proteins has proven a valid strategy for cancer chemotherapy. All BET identified to date contain two bromodomains (BD; BD1 and BD2) that are necessary for recognition of acetylated lysine residues in the N-terminal regions of histones. Chemical matter that targets BET (BETi) also interact via these domains. Molecular and cellular data indicate that BD1 and BD2 have different biological roles depending upon their cellular context, with BD2 particularly associated with cancer. We have therefore pursued the development of BD2-selective molecules both as chemical probes and as potential leads for drug development. Here we report the structure-based generation of a novel series of tetrahydroquinoline analogs that exhibit >50-fold selectivity for BD2 versus BD1. This selective targeting resulted in engagement with BD-containing proteins in cells, resulting in modulation of MYC proteins and downstream targets. These compounds were potent cytotoxins toward numerous pediatric cancer cell lines and were minimally toxic to nontumorigenic cells. In addition, unlike the pan BETi (þ)-JQ1, these BD2-selective inhibitors demonstrated no rebound expression effects. Finally, we report a pharmacokinetic-optimized, metabolically stable derivative that induced growth delay in a neuroblastoma xenograft model with minimal toxicity. We conclude that BD2-selective agents are valid candidates for antitumor drug design for pediatric malignancies driven by the MYC oncogene.

UR - https://www.scopus.com/pages/publications/85100330759

UR - https://www.scopus.com/pages/publications/85100330759#tab=citedBy

U2 - 10.1158/0008-5472.CAN-19-3934

DO - 10.1158/0008-5472.CAN-19-3934

M3 - Article

C2 - 32651255

AN - SCOPUS:85100330759

SN - 0008-5472

VL - 80

SP - 3507

EP - 3518

JO - Cancer Research

JF - Cancer Research

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ER -

Bromodomain-selective BET inhibitors are potent antitumor agents against MYC-driven pediatric cancer

Resumen

Nota bibliográfica

Financiación

ODS de las Naciones Unidas

ASJC Scopus subject areas

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