Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer

Rasmi R. Mishra; Nevin Belder; Suhail A. Ansari; Merve Kayhan; Hilal Bal; Umar Raza; Pelin G. Ersan; Unal M. Tokat; Erol Eyupoglu; Ozge Saatci; Pouria Jandaghi; Stefan Wiemann; Ayşegul Uner; Caglar Cekic; Yasser Riazalhosseini; Ozgur Şahin

doi:10.1158/1078-0432.CCR-17-2776

Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer

Rasmi R. Mishra, Nevin Belder, Suhail A. Ansari, Merve Kayhan, Hilal Bal, Umar Raza, Pelin G. Ersan, Unal M. Tokat, Erol Eyupoglu, Ozge Saatci, Pouria Jandaghi, Stefan Wiemann, Ayşegul Uner, Caglar Cekic, Yasser Riazalhosseini, Ozgur Şahin

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

37 Scopus citations

Abstract

Purpose: Tamoxifen remains an important hormonal therapy for ER-positive breast cancer; however, development of resistance is a major obstacle in clinics. Here, we aimed to identify novel mechanisms of tamoxifen resistance and provide actionable drug targets overcoming resistance. Experimental Design: Whole-transcriptome sequencing, downstream pathway analysis, and drug repositioning approaches were used to identify novel modulators [here: phosphodiesterase 4D (PDE4D)] of tamoxifen resistance. Clinical data involving tamoxifen-treated patients with ER-positive breast cancer were used to assess the impact of PDE4D in tamoxifen resistance. Tamoxifen sensitization role of PDE4D was tested in vitro and in vivo. Cytobiology, biochemistry, and functional genomics tools were used to elucidate the mechanisms of PDE4D-mediated tamoxifen resistance. Results: PDE4D, which hydrolyzes cyclic AMP (cAMP), was significantly overexpressed in both MCF-7 and T47D tamoxifen-resistant (TamR) cells. Higher PDE4D expression predicted worse survival in tamoxifen-treated patients with breast cancer (n ¼ 469, P ¼ 0.0036 for DMFS; n ¼ 561, P ¼ 0.0229 for RFS) and remained an independent prognostic factor for RFS in multivariate analysis (n ¼ 132, P ¼ 0.049). Inhibition of PDE4D by either siRNAs or pharmacologic inhibitors (dipyridamole and Gebr-7b) restored tamoxifen sensitivity. Sensitization to tamoxifen is achieved via cAMP-mediated induction of unfolded protein response/ER stress pathway leading to activation of p38/JNK signaling and apoptosis. Remarkably, acetylsalicylic acid (aspirin) was predicted to be a tamoxifen sensitizer using a drug repositioning approach and was shown to reverse resistance by targeting PDE4D/ cAMP/ER stress axis. Finally, combining PDE4D inhibitors and tamoxifen suppressed tumor growth better than individual groups in vivo. Conclusions: PDE4D plays a pivotal role in acquired tamoxifen resistance via blocking cAMP/ER stress/p38-JNK signaling and apoptosis.

Original language	English (US)
Pages (from-to)	1987-2001
Number of pages	15
Journal	Clinical Cancer Research
Volume	24
Issue number	8
DOIs	https://doi.org/10.1158/1078-0432.CCR-17-2776
State	Published - Apr 2018

ASJC Scopus subject areas

Oncology
Cancer Research

Access to Document

10.1158/1078-0432.CCR-17-2776

Cite this

Mishra, R. R., Belder, N., Ansari, S. A., Kayhan, M., Bal, H., Raza, U., Ersan, P. G., Tokat, U. M., Eyupoglu, E., Saatci, O., Jandaghi, P., Wiemann, S., Uner, A., Cekic, C., Riazalhosseini, Y., & Şahin, O. (2018). Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer. Clinical Cancer Research, 24(8), 1987-2001. https://doi.org/10.1158/1078-0432.CCR-17-2776

Mishra, RR, Belder, N, Ansari, SA, Kayhan, M, Bal, H, Raza, U, Ersan, PG, Tokat, UM, Eyupoglu, E, Saatci, O, Jandaghi, P, Wiemann, S, Uner, A, Cekic, C, Riazalhosseini, Y & Şahin, O 2018, 'Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer', Clinical Cancer Research, vol. 24, no. 8, pp. 1987-2001. https://doi.org/10.1158/1078-0432.CCR-17-2776

@article{3ce351cd6de4469e933d61885dd88ab9,

title = "Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer",

abstract = "Purpose: Tamoxifen remains an important hormonal therapy for ER-positive breast cancer; however, development of resistance is a major obstacle in clinics. Here, we aimed to identify novel mechanisms of tamoxifen resistance and provide actionable drug targets overcoming resistance. Experimental Design: Whole-transcriptome sequencing, downstream pathway analysis, and drug repositioning approaches were used to identify novel modulators [here: phosphodiesterase 4D (PDE4D)] of tamoxifen resistance. Clinical data involving tamoxifen-treated patients with ER-positive breast cancer were used to assess the impact of PDE4D in tamoxifen resistance. Tamoxifen sensitization role of PDE4D was tested in vitro and in vivo. Cytobiology, biochemistry, and functional genomics tools were used to elucidate the mechanisms of PDE4D-mediated tamoxifen resistance. Results: PDE4D, which hydrolyzes cyclic AMP (cAMP), was significantly overexpressed in both MCF-7 and T47D tamoxifen-resistant (TamR) cells. Higher PDE4D expression predicted worse survival in tamoxifen-treated patients with breast cancer (n ¼ 469, P ¼ 0.0036 for DMFS; n ¼ 561, P ¼ 0.0229 for RFS) and remained an independent prognostic factor for RFS in multivariate analysis (n ¼ 132, P ¼ 0.049). Inhibition of PDE4D by either siRNAs or pharmacologic inhibitors (dipyridamole and Gebr-7b) restored tamoxifen sensitivity. Sensitization to tamoxifen is achieved via cAMP-mediated induction of unfolded protein response/ER stress pathway leading to activation of p38/JNK signaling and apoptosis. Remarkably, acetylsalicylic acid (aspirin) was predicted to be a tamoxifen sensitizer using a drug repositioning approach and was shown to reverse resistance by targeting PDE4D/ cAMP/ER stress axis. Finally, combining PDE4D inhibitors and tamoxifen suppressed tumor growth better than individual groups in vivo. Conclusions: PDE4D plays a pivotal role in acquired tamoxifen resistance via blocking cAMP/ER stress/p38-JNK signaling and apoptosis.",

author = "Mishra, {Rasmi R.} and Nevin Belder and Ansari, {Suhail A.} and Merve Kayhan and Hilal Bal and Umar Raza and Ersan, {Pelin G.} and Tokat, {Unal M.} and Erol Eyupoglu and Ozge Saatci and Pouria Jandaghi and Stefan Wiemann and Ay{\c s}egul Uner and Caglar Cekic and Yasser Riazalhosseini and Ozgur {\c S}ahin",

note = "Publisher Copyright: {\textcopyright} 2018 American Association for Cancer Research.",

year = "2018",

month = apr,

doi = "10.1158/1078-0432.CCR-17-2776",

language = "English (US)",

volume = "24",

pages = "1987--2001",

journal = "Clinical Cancer Research",

issn = "1078-0432",

publisher = "American Association for Cancer Research Inc.",

number = "8",

}

TY - JOUR

T1 - Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer

AU - Mishra, Rasmi R.

AU - Belder, Nevin

AU - Ansari, Suhail A.

AU - Kayhan, Merve

AU - Bal, Hilal

AU - Raza, Umar

AU - Ersan, Pelin G.

AU - Tokat, Unal M.

AU - Eyupoglu, Erol

AU - Saatci, Ozge

AU - Jandaghi, Pouria

AU - Wiemann, Stefan

AU - Uner, Ayşegul

AU - Cekic, Caglar

AU - Riazalhosseini, Yasser

AU - Şahin, Ozgur

PY - 2018/4

Y1 - 2018/4

N2 - Purpose: Tamoxifen remains an important hormonal therapy for ER-positive breast cancer; however, development of resistance is a major obstacle in clinics. Here, we aimed to identify novel mechanisms of tamoxifen resistance and provide actionable drug targets overcoming resistance. Experimental Design: Whole-transcriptome sequencing, downstream pathway analysis, and drug repositioning approaches were used to identify novel modulators [here: phosphodiesterase 4D (PDE4D)] of tamoxifen resistance. Clinical data involving tamoxifen-treated patients with ER-positive breast cancer were used to assess the impact of PDE4D in tamoxifen resistance. Tamoxifen sensitization role of PDE4D was tested in vitro and in vivo. Cytobiology, biochemistry, and functional genomics tools were used to elucidate the mechanisms of PDE4D-mediated tamoxifen resistance. Results: PDE4D, which hydrolyzes cyclic AMP (cAMP), was significantly overexpressed in both MCF-7 and T47D tamoxifen-resistant (TamR) cells. Higher PDE4D expression predicted worse survival in tamoxifen-treated patients with breast cancer (n ¼ 469, P ¼ 0.0036 for DMFS; n ¼ 561, P ¼ 0.0229 for RFS) and remained an independent prognostic factor for RFS in multivariate analysis (n ¼ 132, P ¼ 0.049). Inhibition of PDE4D by either siRNAs or pharmacologic inhibitors (dipyridamole and Gebr-7b) restored tamoxifen sensitivity. Sensitization to tamoxifen is achieved via cAMP-mediated induction of unfolded protein response/ER stress pathway leading to activation of p38/JNK signaling and apoptosis. Remarkably, acetylsalicylic acid (aspirin) was predicted to be a tamoxifen sensitizer using a drug repositioning approach and was shown to reverse resistance by targeting PDE4D/ cAMP/ER stress axis. Finally, combining PDE4D inhibitors and tamoxifen suppressed tumor growth better than individual groups in vivo. Conclusions: PDE4D plays a pivotal role in acquired tamoxifen resistance via blocking cAMP/ER stress/p38-JNK signaling and apoptosis.

AB - Purpose: Tamoxifen remains an important hormonal therapy for ER-positive breast cancer; however, development of resistance is a major obstacle in clinics. Here, we aimed to identify novel mechanisms of tamoxifen resistance and provide actionable drug targets overcoming resistance. Experimental Design: Whole-transcriptome sequencing, downstream pathway analysis, and drug repositioning approaches were used to identify novel modulators [here: phosphodiesterase 4D (PDE4D)] of tamoxifen resistance. Clinical data involving tamoxifen-treated patients with ER-positive breast cancer were used to assess the impact of PDE4D in tamoxifen resistance. Tamoxifen sensitization role of PDE4D was tested in vitro and in vivo. Cytobiology, biochemistry, and functional genomics tools were used to elucidate the mechanisms of PDE4D-mediated tamoxifen resistance. Results: PDE4D, which hydrolyzes cyclic AMP (cAMP), was significantly overexpressed in both MCF-7 and T47D tamoxifen-resistant (TamR) cells. Higher PDE4D expression predicted worse survival in tamoxifen-treated patients with breast cancer (n ¼ 469, P ¼ 0.0036 for DMFS; n ¼ 561, P ¼ 0.0229 for RFS) and remained an independent prognostic factor for RFS in multivariate analysis (n ¼ 132, P ¼ 0.049). Inhibition of PDE4D by either siRNAs or pharmacologic inhibitors (dipyridamole and Gebr-7b) restored tamoxifen sensitivity. Sensitization to tamoxifen is achieved via cAMP-mediated induction of unfolded protein response/ER stress pathway leading to activation of p38/JNK signaling and apoptosis. Remarkably, acetylsalicylic acid (aspirin) was predicted to be a tamoxifen sensitizer using a drug repositioning approach and was shown to reverse resistance by targeting PDE4D/ cAMP/ER stress axis. Finally, combining PDE4D inhibitors and tamoxifen suppressed tumor growth better than individual groups in vivo. Conclusions: PDE4D plays a pivotal role in acquired tamoxifen resistance via blocking cAMP/ER stress/p38-JNK signaling and apoptosis.

UR - http://www.scopus.com/inward/record.url?scp=85047635452&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85047635452&partnerID=8YFLogxK

U2 - 10.1158/1078-0432.CCR-17-2776

DO - 10.1158/1078-0432.CCR-17-2776

M3 - Article

C2 - 29386221

AN - SCOPUS:85047635452

SN - 1078-0432

VL - 24

SP - 1987

EP - 2001

JO - Clinical Cancer Research

JF - Clinical Cancer Research

IS - 8

ER -

Reactivation of cAMP Pathway by PDE4D Inhibition Represents a Novel Druggable Axis for Overcoming Tamoxifen Resistance in ER-positive Breast Cancer

Abstract

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this