Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues

Yizhou Dong; Qian Shi; Huei Chen Pai; Chieh Yu Peng; Shiow Lin Pan; Che Ming Teng; Kyoko Nakagawa-Goto; Donglei Yu; Yi Nan Liu; Pei Chi Wu; Kenneth F. Bastow; Susan L. Morris-Natschke; Arnold Brossi; Jing Yu Lang; Jennifer L. Hsu; Mien Chie Hung; Eva Y.H.P. Lee; Kuo Hsiung Lee

doi:10.1021/jm1000858

Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues

Yizhou Dong
, Qian Shi
, Huei Chen Pai
, Chieh Yu Peng
, Shiow Lin Pan
, Che Ming Teng
, Kyoko Nakagawa-Goto
, Donglei Yu
, Yi Nan Liu
, Pei Chi Wu
, Kenneth F. Bastow
, Susan L. Morris-Natschke
, Arnold Brossi
, Jing Yu Lang
, Jennifer L. Hsu
, Mien Chie Hung
, Eva Y.H.P. Lee
, Kuo Hsiung Lee

Research output: Contribution to journal › Article › peer-review

70 Citations (Scopus)

Abstract

Neo-tanshinlactone (1) and its previously reported analogues, such as 2, are potent and selective in vitro antibreast cancer agents. The synthetic pathway to 2 was optimized from seven to five steps, with a better overall yield. Structure-activity relationships studies on these compounds revealed some key molecular determinants for this family of antibreast agents. Several derivatives (19-21 and 24) exerted potent and selective antibreast cancer activity with IC₅₀ values of 0.3,0.2,0.1, and 0.1 μg/mL, respectively, against the ZR-75-1 cell lines. Compound 24 was 2- to 3-fold more potent than 1 against SK-BR-3 and ZR-75-1. Importantly, 21 exhibited high selectivity; it was 23 times more active against ZR-75-1 than MCF-7. Compound 20 had an approximately 12-fold ratio of SK-BR-3/MCF-7 selectivity. In addition, analogue 2 showed potent activity against a ZR-75-1 xenograft model, but not PC-3 and MDA-MB-231 xenografts, as well as high selectivity against breast cancer cell line compared with normal breast tissue-derived cell lines. Further development of lead compounds 19-21 and 24 as clinical trial candidates is warranted.

Original language	English
Pages (from-to)	2299-2308
Number of pages	10
Journal	Journal of Medicinal Chemistry
Volume	53
Issue number	5
DOIs	https://doi.org/10.1021/jm1000858
Publication status	Published - Mar 11 2010

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

SDG 3 Good Health and Well-being

ASJC Scopus subject areas

Molecular Medicine
Drug Discovery

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10.1021/jm1000858

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Dong, Y., Shi, Q., Pai, H. C., Peng, C. Y., Pan, S. L., Teng, C. M., Nakagawa-Goto, K., Yu, D., Liu, Y. N., Wu, P. C., Bastow, K. F., Morris-Natschke, S. L., Brossi, A., Lang, J. Y., Hsu, J. L., Hung, M. C., Lee, E. Y. H. P., & Lee, K. H. (2010). Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues. Journal of Medicinal Chemistry, 53(5), 2299-2308. https://doi.org/10.1021/jm1000858

Dong, Y, Shi, Q, Pai, HC, Peng, CY, Pan, SL, Teng, CM, Nakagawa-Goto, K, Yu, D, Liu, YN, Wu, PC, Bastow, KF, Morris-Natschke, SL, Brossi, A, Lang, JY, Hsu, JL, Hung, MC, Lee, EYHP & Lee, KH 2010, 'Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues', Journal of Medicinal Chemistry, vol. 53, no. 5, pp. 2299-2308. https://doi.org/10.1021/jm1000858

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title = "Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues",

abstract = "Neo-tanshinlactone (1) and its previously reported analogues, such as 2, are potent and selective in vitro antibreast cancer agents. The synthetic pathway to 2 was optimized from seven to five steps, with a better overall yield. Structure-activity relationships studies on these compounds revealed some key molecular determinants for this family of antibreast agents. Several derivatives (19-21 and 24) exerted potent and selective antibreast cancer activity with IC50 values of 0.3,0.2,0.1, and 0.1 μg/mL, respectively, against the ZR-75-1 cell lines. Compound 24 was 2- to 3-fold more potent than 1 against SK-BR-3 and ZR-75-1. Importantly, 21 exhibited high selectivity; it was 23 times more active against ZR-75-1 than MCF-7. Compound 20 had an approximately 12-fold ratio of SK-BR-3/MCF-7 selectivity. In addition, analogue 2 showed potent activity against a ZR-75-1 xenograft model, but not PC-3 and MDA-MB-231 xenografts, as well as high selectivity against breast cancer cell line compared with normal breast tissue-derived cell lines. Further development of lead compounds 19-21 and 24 as clinical trial candidates is warranted.",

author = "Yizhou Dong and Qian Shi and Pai, \{Huei Chen\} and Peng, \{Chieh Yu\} and Pan, \{Shiow Lin\} and Teng, \{Che Ming\} and Kyoko Nakagawa-Goto and Donglei Yu and Liu, \{Yi Nan\} and Wu, \{Pei Chi\} and Bastow, \{Kenneth F.\} and Morris-Natschke, \{Susan L.\} and Arnold Brossi and Lang, \{Jing Yu\} and Hsu, \{Jennifer L.\} and Hung, \{Mien Chie\} and Lee, \{Eva Y.H.P.\} and Lee, \{Kuo Hsiung\}",

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doi = "10.1021/jm1000858",

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AU - Dong, Yizhou

AU - Shi, Qian

AU - Pai, Huei Chen

AU - Peng, Chieh Yu

AU - Pan, Shiow Lin

AU - Teng, Che Ming

AU - Nakagawa-Goto, Kyoko

AU - Yu, Donglei

AU - Liu, Yi Nan

AU - Wu, Pei Chi

AU - Bastow, Kenneth F.

AU - Morris-Natschke, Susan L.

AU - Brossi, Arnold

AU - Lang, Jing Yu

AU - Hsu, Jennifer L.

AU - Hung, Mien Chie

AU - Lee, Eva Y.H.P.

AU - Lee, Kuo Hsiung

PY - 2010/3/11

Y1 - 2010/3/11

N2 - Neo-tanshinlactone (1) and its previously reported analogues, such as 2, are potent and selective in vitro antibreast cancer agents. The synthetic pathway to 2 was optimized from seven to five steps, with a better overall yield. Structure-activity relationships studies on these compounds revealed some key molecular determinants for this family of antibreast agents. Several derivatives (19-21 and 24) exerted potent and selective antibreast cancer activity with IC50 values of 0.3,0.2,0.1, and 0.1 μg/mL, respectively, against the ZR-75-1 cell lines. Compound 24 was 2- to 3-fold more potent than 1 against SK-BR-3 and ZR-75-1. Importantly, 21 exhibited high selectivity; it was 23 times more active against ZR-75-1 than MCF-7. Compound 20 had an approximately 12-fold ratio of SK-BR-3/MCF-7 selectivity. In addition, analogue 2 showed potent activity against a ZR-75-1 xenograft model, but not PC-3 and MDA-MB-231 xenografts, as well as high selectivity against breast cancer cell line compared with normal breast tissue-derived cell lines. Further development of lead compounds 19-21 and 24 as clinical trial candidates is warranted.

AB - Neo-tanshinlactone (1) and its previously reported analogues, such as 2, are potent and selective in vitro antibreast cancer agents. The synthetic pathway to 2 was optimized from seven to five steps, with a better overall yield. Structure-activity relationships studies on these compounds revealed some key molecular determinants for this family of antibreast agents. Several derivatives (19-21 and 24) exerted potent and selective antibreast cancer activity with IC50 values of 0.3,0.2,0.1, and 0.1 μg/mL, respectively, against the ZR-75-1 cell lines. Compound 24 was 2- to 3-fold more potent than 1 against SK-BR-3 and ZR-75-1. Importantly, 21 exhibited high selectivity; it was 23 times more active against ZR-75-1 than MCF-7. Compound 20 had an approximately 12-fold ratio of SK-BR-3/MCF-7 selectivity. In addition, analogue 2 showed potent activity against a ZR-75-1 xenograft model, but not PC-3 and MDA-MB-231 xenografts, as well as high selectivity against breast cancer cell line compared with normal breast tissue-derived cell lines. Further development of lead compounds 19-21 and 24 as clinical trial candidates is warranted.

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Antitumor agents. 272. Structure-activity relationships and in vivo selective anti-breast cancer activity of novel neo-tanshinlactone analogues

Abstract

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