Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response

Jason C. Wong; Guozhi Tang; Xihan Wu; Chungen Liang; Zhenshan Zhang; Lei Guo; Zhenghong Peng; Weixing Zhang; Xianfeng Lin; Zhanguo Wang; Jianghua Mei; Junli Chen; Song Pan; Nan Zhang; Yongfu Liu; Mingwei Zhou; Lichun Feng; Weili Zhao; Shijie Li; Chao Zhang; Meifang Zhang; Yiping Rong; Tai Guang Jin; Xiongwen Zhang; Shuang Ren; Ying Ji; Rong Zhao; Jin She; Yi Ren; Chunping Xu; Dawei Chen; Jie Cai; Song Shan; Desi Pan; Zhiqiang Ning; Xianping Lu; Taiping Chen; Yun He; Li Chen

doi:10.1021/jm3011838

Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response

Jason C. Wong^*
, Guozhi Tang
, Xihan Wu
, Chungen Liang
, Zhenshan Zhang
, Lei Guo
, Zhenghong Peng
, Weixing Zhang
, Xianfeng Lin
, Zhanguo Wang
, Jianghua Mei
, Junli Chen
, Song Pan
, Nan Zhang
, Yongfu Liu
, Mingwei Zhou
, Lichun Feng
, Weili Zhao
, Shijie Li
, Chao Zhang

Meifang Zhang, Yiping Rong, Tai Guang Jin, Xiongwen Zhang, Shuang Ren, Ying Ji, Rong Zhao, Jin She, Yi Ren, Chunping Xu, Dawei Chen, Jie Cai, Song Shan, Desi Pan, Zhiqiang Ning, Xianping Lu, Taiping Chen, Yun He, Li Chen

^*Corresponding author for this work

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

28 Scopus citations

Abstract

Herein, we describe the pharmacokinetic optimization of a series of class-selective histone deacetylase (HDAC) inhibitors and the subsequent identification of candidate predictive biomarkers of hepatocellular carcinoma (HCC) tumor response for our clinical lead using patient-derived HCC tumor xenograft models. Through a combination of conformational constraint and scaffold hopping, we lowered the in vivo clearance (CL) and significantly improved the bioavailability (F) and exposure (AUC) of our HDAC inhibitors while maintaining selectivity toward the class I HDAC family with particular potency against HDAC1, resulting in clinical lead 5 (HDAC1 IC₅₀ = 60 nM, mouse CL = 39 mL/min/kg, mouse F = 100%, mouse AUC after single oral dose at 10 mg/kg = 6316 h·ng/mL). We then evaluated 5 in a biomarker discovery pilot study using patient-derived tumor xenograft models, wherein two out of the three models responded to treatment. By comparing tumor response status to compound tumor exposure, induction of acetylated histone H3, candidate gene expression changes, and promoter DNA methylation status from all three models at various time points, we identified preliminary candidate response prediction biomarkers that warrant further validation in a larger cohort of patient-derived tumor models and through confirmatory functional studies.

Original language	English
Pages (from-to)	8903-8925
Number of pages	23
Journal	Journal of Medicinal Chemistry
Volume	55
Issue number	20
DOIs	https://doi.org/10.1021/jm3011838
State	Published - 25 Oct 2012
Externally published	Yes

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10.1021/jm3011838

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Wong, J. C., Tang, G., Wu, X., Liang, C., Zhang, Z., Guo, L., Peng, Z., Zhang, W., Lin, X., Wang, Z., Mei, J., Chen, J., Pan, S., Zhang, N., Liu, Y., Zhou, M., Feng, L., Zhao, W., Li, S., ... Chen, L. (2012). Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response. Journal of Medicinal Chemistry, 55(20), 8903-8925. https://doi.org/10.1021/jm3011838

@article{6f63661929ca4148b2f53ad3c034b7ac,

title = "Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response",

abstract = "Herein, we describe the pharmacokinetic optimization of a series of class-selective histone deacetylase (HDAC) inhibitors and the subsequent identification of candidate predictive biomarkers of hepatocellular carcinoma (HCC) tumor response for our clinical lead using patient-derived HCC tumor xenograft models. Through a combination of conformational constraint and scaffold hopping, we lowered the in vivo clearance (CL) and significantly improved the bioavailability (F) and exposure (AUC) of our HDAC inhibitors while maintaining selectivity toward the class I HDAC family with particular potency against HDAC1, resulting in clinical lead 5 (HDAC1 IC50 = 60 nM, mouse CL = 39 mL/min/kg, mouse F = 100\%, mouse AUC after single oral dose at 10 mg/kg = 6316 h·ng/mL). We then evaluated 5 in a biomarker discovery pilot study using patient-derived tumor xenograft models, wherein two out of the three models responded to treatment. By comparing tumor response status to compound tumor exposure, induction of acetylated histone H3, candidate gene expression changes, and promoter DNA methylation status from all three models at various time points, we identified preliminary candidate response prediction biomarkers that warrant further validation in a larger cohort of patient-derived tumor models and through confirmatory functional studies.",

author = "Wong, \{Jason C.\} and Guozhi Tang and Xihan Wu and Chungen Liang and Zhenshan Zhang and Lei Guo and Zhenghong Peng and Weixing Zhang and Xianfeng Lin and Zhanguo Wang and Jianghua Mei and Junli Chen and Song Pan and Nan Zhang and Yongfu Liu and Mingwei Zhou and Lichun Feng and Weili Zhao and Shijie Li and Chao Zhang and Meifang Zhang and Yiping Rong and Jin, \{Tai Guang\} and Xiongwen Zhang and Shuang Ren and Ying Ji and Rong Zhao and Jin She and Yi Ren and Chunping Xu and Dawei Chen and Jie Cai and Song Shan and Desi Pan and Zhiqiang Ning and Xianping Lu and Taiping Chen and Yun He and Li Chen",

year = "2012",

month = oct,

day = "25",

doi = "10.1021/jm3011838",

language = "英语",

volume = "55",

pages = "8903--8925",

journal = "Journal of Medicinal Chemistry",

issn = "0022-2623",

publisher = "American Chemical Society",

number = "20",

}

Wong, JC, Tang, G, Wu, X, Liang, C, Zhang, Z, Guo, L, Peng, Z, Zhang, W, Lin, X, Wang, Z, Mei, J, Chen, J, Pan, S, Zhang, N, Liu, Y, Zhou, M, Feng, L, Zhao, W, Li, S, Zhang, C, Zhang, M, Rong, Y, Jin, TG, Zhang, X, Ren, S, Ji, Y, Zhao, R, She, J, Ren, Y, Xu, C, Chen, D, Cai, J, Shan, S, Pan, D, Ning, Z, Lu, X, Chen, T, He, Y & Chen, L 2012, 'Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response', Journal of Medicinal Chemistry, vol. 55, no. 20, pp. 8903-8925. https://doi.org/10.1021/jm3011838

Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response. / Wong, Jason C.; Tang, Guozhi; Wu, Xihan et al.
In: Journal of Medicinal Chemistry, Vol. 55, No. 20, 25.10.2012, p. 8903-8925.

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

TY - JOUR

T1 - Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response

AU - Wong, Jason C.

AU - Tang, Guozhi

AU - Wu, Xihan

AU - Liang, Chungen

AU - Zhang, Zhenshan

AU - Guo, Lei

AU - Peng, Zhenghong

AU - Zhang, Weixing

AU - Lin, Xianfeng

AU - Wang, Zhanguo

AU - Mei, Jianghua

AU - Chen, Junli

AU - Pan, Song

AU - Zhang, Nan

AU - Liu, Yongfu

AU - Zhou, Mingwei

AU - Feng, Lichun

AU - Zhao, Weili

AU - Li, Shijie

AU - Zhang, Chao

AU - Zhang, Meifang

AU - Rong, Yiping

AU - Jin, Tai Guang

AU - Zhang, Xiongwen

AU - Ren, Shuang

AU - Ji, Ying

AU - Zhao, Rong

AU - She, Jin

AU - Ren, Yi

AU - Xu, Chunping

AU - Chen, Dawei

AU - Cai, Jie

AU - Shan, Song

AU - Pan, Desi

AU - Ning, Zhiqiang

AU - Lu, Xianping

AU - Chen, Taiping

AU - He, Yun

AU - Chen, Li

PY - 2012/10/25

Y1 - 2012/10/25

N2 - Herein, we describe the pharmacokinetic optimization of a series of class-selective histone deacetylase (HDAC) inhibitors and the subsequent identification of candidate predictive biomarkers of hepatocellular carcinoma (HCC) tumor response for our clinical lead using patient-derived HCC tumor xenograft models. Through a combination of conformational constraint and scaffold hopping, we lowered the in vivo clearance (CL) and significantly improved the bioavailability (F) and exposure (AUC) of our HDAC inhibitors while maintaining selectivity toward the class I HDAC family with particular potency against HDAC1, resulting in clinical lead 5 (HDAC1 IC50 = 60 nM, mouse CL = 39 mL/min/kg, mouse F = 100%, mouse AUC after single oral dose at 10 mg/kg = 6316 h·ng/mL). We then evaluated 5 in a biomarker discovery pilot study using patient-derived tumor xenograft models, wherein two out of the three models responded to treatment. By comparing tumor response status to compound tumor exposure, induction of acetylated histone H3, candidate gene expression changes, and promoter DNA methylation status from all three models at various time points, we identified preliminary candidate response prediction biomarkers that warrant further validation in a larger cohort of patient-derived tumor models and through confirmatory functional studies.

AB - Herein, we describe the pharmacokinetic optimization of a series of class-selective histone deacetylase (HDAC) inhibitors and the subsequent identification of candidate predictive biomarkers of hepatocellular carcinoma (HCC) tumor response for our clinical lead using patient-derived HCC tumor xenograft models. Through a combination of conformational constraint and scaffold hopping, we lowered the in vivo clearance (CL) and significantly improved the bioavailability (F) and exposure (AUC) of our HDAC inhibitors while maintaining selectivity toward the class I HDAC family with particular potency against HDAC1, resulting in clinical lead 5 (HDAC1 IC50 = 60 nM, mouse CL = 39 mL/min/kg, mouse F = 100%, mouse AUC after single oral dose at 10 mg/kg = 6316 h·ng/mL). We then evaluated 5 in a biomarker discovery pilot study using patient-derived tumor xenograft models, wherein two out of the three models responded to treatment. By comparing tumor response status to compound tumor exposure, induction of acetylated histone H3, candidate gene expression changes, and promoter DNA methylation status from all three models at various time points, we identified preliminary candidate response prediction biomarkers that warrant further validation in a larger cohort of patient-derived tumor models and through confirmatory functional studies.

UR - https://www.scopus.com/pages/publications/84867790360

U2 - 10.1021/jm3011838

DO - 10.1021/jm3011838

M3 - 文章

C2 - 23061376

AN - SCOPUS:84867790360

SN - 0022-2623

VL - 55

SP - 8903

EP - 8925

JO - Journal of Medicinal Chemistry

JF - Journal of Medicinal Chemistry

IS - 20

ER -

Pharmacokinetic optimization of class-selective histone deacetylase inhibitors and identification of associated candidate predictive biomarkers of hepatocellular carcinoma tumor response

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