. 2017 Jan 6;355(6320):84-88.

doi: 10.1126/science.aah4307.

SOX2 promotes lineage plasticity and antiandrogen resistance in TP53- and RB1-deficient prostate cancer

Ping Mu¹, Zeda Zhang^{1

2}, Matteo Benelli³, Wouter R Karthaus¹, Elizabeth Hoover¹, Chi-Chao Chen^{4

5}, John Wongvipat¹, Sheng-Yu Ku⁶, Dong Gao¹, Zhen Cao^{1

5}, Neel Shah^{1

2}, Elizabeth J Adams¹, Wassim Abida¹, Philip A Watson¹, Davide Prandi³, Chun-Hao Huang^{4

5}, Elisa de Stanchina⁷, Scott W Lowe^{4

5

8}, Leigh Ellis⁶, Himisha Beltran^{9

10}, Mark A Rubin^{9

10}, David W Goodrich⁶, Francesca Demichelis^{3

9}, Charles L Sawyers^{11

8}

Affiliations

¹ Human Oncology and Pathology Program, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA.
² Louis V. Gerstner, Jr. Graduate School of Biomedical Sciences, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
³ Centre for Integrative Biology, University of Trento, Trento, Italy.
⁴ Cancer Biology and Genetics Program, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA.
⁵ Weill Cornell Graduate School of Medical Sciences of Cornell University, New York, NY 10021, USA.
⁶ Department of Pharmacology and Therapeutics, Roswell Park Cancer Institute, New York, NY 14263, USA.
⁷ Department of Molecular Pharmacology, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA.
⁸ Howard Hughes Medical Institute, Chevy Chase, MD 20815, USA.
⁹ Englander Institute for Precision Medicine, Weill Cornell Medicine and New York Presbyterian Hospital, New York, NY 10065, USA.
¹⁰ Sandra and Edward Meyer Cancer Center at Weill Cornell Medicine, New York, NY 10021, USA.
¹¹ Human Oncology and Pathology Program, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA. sawyersc@www.qiuluzeuv.cn.

PMID: 28059768
PMCID: PMC5247742
DOI: 10.1126/science.aah4307

SOX2 promotes lineage plasticity and antiandrogen resistance in TP53- and RB1-deficient prostate cancer

"VSports在线直播" Ping Mu et al. Science. 2017.

. 2017 Jan 6;355(6320):84-88.

doi: 10.1126/science.aah4307.

"VSports" Authors

Affiliations (V体育ios版)

¹ Human Oncology and Pathology Program, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA.
² Louis V. Gerstner, Jr. Graduate School of Biomedical Sciences, Memorial Sloan Kettering Cancer Center, New York, NY 10065, USA.
³ Centre for Integrative Biology, University of Trento, Trento, Italy.
⁴ Cancer Biology and Genetics Program, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA.
⁵ Weill Cornell Graduate School of Medical Sciences of Cornell University, New York, NY 10021, USA.
⁶ Department of Pharmacology and Therapeutics, Roswell Park Cancer Institute, New York, NY 14263, USA.
⁷ Department of Molecular Pharmacology, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA.
⁸ Howard Hughes Medical Institute, Chevy Chase, MD 20815, USA.
⁹ Englander Institute for Precision Medicine, Weill Cornell Medicine and New York Presbyterian Hospital, New York, NY 10065, USA.
¹⁰ Sandra and Edward Meyer Cancer Center at Weill Cornell Medicine, New York, NY 10021, USA.
¹¹ Human Oncology and Pathology Program, Memorial Sloan Kettering Cancer Center, 1275 York Avenue, New York, NY 10065, USA. sawyersc@www.qiuluzeuv.cn.

PMID: 28059768
PMCID: PMC5247742
DOI: 10.1126/science.aah4307

Abstract

Some cancers evade targeted therapies through a mechanism known as lineage plasticity, whereby tumor cells acquire phenotypic characteristics of a cell lineage whose survival no longer depends on the drug target VSports手机版. We use in vitro and in vivo human prostate cancer models to show that these tumors can develop resistance to the antiandrogen drug enzalutamide by a phenotypic shift from androgen receptor (AR)-dependent luminal epithelial cells to AR-independent basal-like cells. This lineage plasticity is enabled by the loss of TP53 and RB1 function, is mediated by increased expression of the reprogramming transcription factor SOX2, and can be reversed by restoring TP53 and RB1 function or by inhibiting SOX2 expression. Thus, mutations in tumor suppressor genes can create a state of increased cellular plasticity that, when challenged with antiandrogen therapy, promotes resistance through lineage switching. .

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Figures

**Fig. 1. Combined *TP53* and *RB1* loss of function confers enzalutamide resistance**
(A) Western blot showing TP53 and RB1 protein levels in LNCaP/AR cells transduced with annotated hairpins. Glyceraldehyde-3-phosphate dehydrogenase (GAPDH) served as a loading control. (B) Growth curve of LNCaP/AR cells transduced with annotated hairpins in charcoal-stripped serum (CSS) medium, following LNCaP/AR protocol B (see materials and methods). Enz denotes 10-µg/ml enzalutamide treatment. Mock denotes the equivalent volume of dimethyl sulfoxide (DMSO) treatment. (C) Tumor growth curve of xenografted LNCaP/AR cells transduced with annotated hairpins. +Enz denotes enzalutamide treatment at 10 mg/kg orally 1 day after grafting. +Mock denotes DMSO treatment at the same dosage. (D) Number of cases of co-occurrence of *TP53* and *RB1* alterations in primary prostate cancer (PCa), CRPC with adenocarcinoma histology (CRPC-Adeno), and CRPC with neuroendocrine-like histology (CRPC-NE) (n = 559). The genomic status of the two genes was assessed from whole-exome sequencing data, as in (12). P values were calculated using Fisher’s exact test. The percentage of cases with alterations in both *TP53* and *RB1* in primary PCa, CRPC-Adeno, and CRPC-NE is shown. (E) Number of cases with *TP53^Alt, RB1^Alt*, based on whether the patient had already received therapy with enzalutamide or abiraterone (Abi/Enz) (n = 44 cases: 14 cases in the *TP53^WT, RB1^WT* group and 30 cases in the *TP53^Alt, RB1^Alt* group). P values were calculated using Fisher’s exact test. (F) Relative gene expression of AR and AR target genes in tumors collected from the LNCaP/AR xenograft model. Enz denotes enzalutamide treatment at 10 mg/kg from day 1 of grafting. Minus signs denote DMSO treatment at the same dosage. For all panels unless otherwise noted, mean ± SEM (error bars) is represented, and P values were calculated using multiple t tests. NS, not significant.

**Fig. 2. Combined *TP53* and *RB1* loss of function leads to increased lineage plasticity**
(A) Western blot of selected cellular lineage markers in LNCaP/AR cells transduced with annotated hairpins in a stable vector system. GAPDH served as a loading control. (B) Relative gene expression of lineage markers in LNCaP/AR cells transduced with annotated hairpins in a stable vector system. (C) Expression of luminal- and basal-signature genes [as defined in table S1 and (30)] was compared in LNCaP/AR cells transduced with annotated hairpins (shTP53/RB1 versus shNT) by gene set enrichment analysis. (D) Western blot showing protein levels of selected lineage markers in LNCaP/AR cells transduced with hairpins against *TP53* and *RB1* in an inducible vector system at various time points. GAPDH served as a loading control. (E) Relative gene expression of lineage markers in LNCaP/AR cells transduced with hairpins against *TP53* and *RB1* in an inducible vector system at various time points. (F) Cell number of LNCaP/AR cells transduced with annotated hairpins in an inducible vector system, normalized to the −Enz group. Cells were treated with doxycycline for 48 hours and then treated with 7 days of enzalutamide in CSS medium, following LNCaP/AR protocol A. +Enz denotes 10-µg/ml enzalutamide treatment; −Enz denotes DMSO treatment with same volume as enzalutamide. For all panels unless otherwise noted, mean ± SEM (error bars) is represented, and P values were calculated using multiple t tests. NS, not significant. Cell types that express each set of lineage markers are indicated with different colors.

Fig. 3. Elevation of *SOX2* gene expression is highly correlated with the inactivation of *TP53* and *RB1*
(A) Area under the curve (AUC)–based analysis indicating transcription factors (TFs) overexpressed in the *TP53*- and *RB1*-altered phenotype in both the CRPC patients from IPM-Cornell (12) and the SU2C–Prostate Cancer Foundation (PCF) 2015 cohorts (6) (AUC ≥ 0.65). (B) (Left) Fold change (FC) of transcript levels of the identified TFs in *TP53*- and *RB1*-altered versus *TP53* and *RB1* WT samples. Median values are shown. (Right) FC of identified TFs versus normalized expression in *TP53* and *RB1* WT samples, expressed as log₂(FPKM+1). FPKM, fragments per kilobase of transcript per million mapped reads. The y axis serves both the left and right panels. (C) Relative expression of *SOX2* in *TP53*- and *RB1*-altered and *TP53* and *RB1* WT samples for the IPM-Cornell (n = 35) (12) and SU2C-PCF 2015 (n = 77) data sets (6). For each cohort, data are scaled to the median of the *TP53* and *RB1* WT status. P value is Wilcoxon-Mann-Whitney, with lower and upper whiskers corresponding to the minimum and maximum nonoutlier values of the data distribution, respectively. (D) Relative gene expression of *TP53, RB1*, and *SOX2* in LNCaP/AR cells transduced with annotated hairpins in a stable vector system. (E) Relative gene expression of *TP53, RB1*, and *SOX2* in CWR22Pc-EP cells transduced with annotated hairpins in a stable vector system. (F) Relative gene expression of *Trp53, Rb1*, and *Sox2* in *Trp53^loxP/loxP, Rb1^loxP/loxP* mouse organoids transduced with annotated Cre or empty vector. (G) Relative gene expression of *TP53, RB1*, and *SOX2* in LNCaP/AR cells transduced with annotated hairpins in an inducible vector system at various time points. For all panels unless otherwise noted, mean ± SEM (error bars) is represented, and P values were calculated using multiple t tests.

Fig. 4. *SOX2* is required for lineage plasticity and enzalutamide resistance induced by inactivation of *TP53* and *RB1*
(A) Relative gene expression of *SOX2* and lineage marker genes in LNCaP/AR cells transduced with annotated hairpins in a stable vector system. (B) Cell numbers of LNCaP/AR transduced with annotated hairpins (shTP53 and *RB1* versus shTP53 and *RB1*+shSOX2), normalized to the parental −Enz group. Cells were treated for 7 days with enzalutamide or DMSO in CSS medium, following LNCaP/AR protocol A. (C) Tumor growth curve of xenografted LNCaP/AR cells transduced with annotated hairpins. +Enz denotes enzalutamide treatment at 10 mg/kg orally 1 day after grafting. For panels (A) to (C) unless otherwise noted, mean ± SEM (error bars) is represented and P values were calculated using multiple t tests. (D) Model depicting the lineage plasticity change and antiandrogen resistance in CRPC-Adeno due to *TP53* and *RB1* alterations (*TP53^Alt, RB1^Alt*) compared to CRPC-Adeno with WT *TP53* and *RB1* (*TP53^WT, RB1^WT*).

See this image and copyright information in PMC

Comment in

Reprogramming to resist.
Kelly K, Balk SP. Kelly K, et al. Science. 2017 Jan 6;355(6320):29-30. doi: 10.1126/science.aam5355. Science. 2017. PMID: 28059730 No abstract available.
Re: SOX2 Promotes Lineage Plasticity and Antiandrogen Resistance in TP53- and RB1-Deficient Prostate Cancer.
Atala A. Atala A. J Urol. 2017 Aug;198(2):259. doi: 10.1016/j.juro.2017.05.011. Epub 2017 May 11. J Urol. 2017. PMID: 29370655 No abstract available.

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SOX2 promotes lineage plasticity and antiandrogen resistance in TP53- and RB1-deficient prostate cancer

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SOX2 promotes lineage plasticity and antiandrogen resistance in TP53- and RB1-deficient prostate cancer

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