Direct Co-Targeting of Bcl-xL and Mcl-1 Exhibits Synergistic Effects in AR-V7–Expressing CRPC Models

Benjamin C. Brim; Andres F. Leon; Erica L. Beatson; Jessica D. Kindrick; Kinjal Bhadresha; Xiaohu Zhang; Giulia C. Napoli; Emily N. Risdon; Keith T. Schmidt; Kelli M. Wilson; Crystal McKnight; Erin Beck; Carleen Klumpp-Thomas; Michele Ceribelli; Juan Juan Yin; Adam G. Sowalsky; Douglas K. Price; Cindy H. Chau; Craig J. Thomas; William D. Figg

doi:10.1158/2767-9764.CRC-25-0096

Direct Co-Targeting of Bcl-xL and Mcl-1 Exhibits Synergistic Effects in AR-V7–Expressing CRPC Models

Benjamin C. Brim, Andres F. Leon, Erica L. Beatson, Jessica D. Kindrick, Kinjal Bhadresha, Xiaohu Zhang, Giulia C. Napoli, Emily N. Risdon, Keith T. Schmidt, Kelli M. Wilson, Crystal McKnight, Erin Beck, Carleen Klumpp-Thomas, Michele Ceribelli, Juan Juan Yin, Adam G. Sowalsky, Douglas K. Price, Cindy H. Chau, Craig J. Thomas, William D. Figg^*

^*Corresponding author for this work

Surgery

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

2 Scopus citations

Abstract

There is an unmet need to develop novel treatment options for patients with metastatic castration-resistant prostate cancer (mCRPC). Patients often develop resistance to next-generation hormonal therapies that target the androgen receptor (AR) axis (e.g., abiraterone and enzalutamide). A splice variant of AR, AR-V7, is associated with resistance to these inhibitors as well as mCRPC progression and poor prognoses. We embarked upon a high-throughput screen to identify synergistic combinations of targeted therapies using two CRPC cell lines, LNCaP95 and VCaP-CR. Combinations targeting BCL2L1 (Bcl-xL) (A-1331852 and navitoclax) and MCL1 (S63845) synergistically decreased cell viability and induced apoptotic activity via cleavage of PARP, caspase 3, and caspase 7 across AR-V7–expressing CRPC cell lines (LNCaP95, VCaPCR, and 22Rv1) and a patient-derived organoid model (LuCaP 167CR). We also explored the use of a Bcl-xL–specific proteolysis-targeting chimera degrader (PROTAC) to minimize platelet toxicity associated with Bcl-xL inhibitors. We showed similar synergistic efficacy with the Bcl-xL–targeting PROTAC in combination with S63845 in the threedimensional spheroid models. Our findings support further preclinical development of Bcl-xL and Mcl-1 inhibitors for mCRPC.

Original language	English
Pages (from-to)	1396-1408
Number of pages	13
Journal	Cancer research communications
Volume	5
Issue number	8
DOIs	https://doi.org/10.1158/2767-9764.CRC-25-0096
State	Published - 2025

Access to Document

10.1158/2767-9764.CRC-25-0096

Cite this

Brim, B. C., Leon, A. F., Beatson, E. L., Kindrick, J. D., Bhadresha, K., Zhang, X., Napoli, G. C., Risdon, E. N., Schmidt, K. T., Wilson, K. M., McKnight, C., Beck, E., Klumpp-Thomas, C., Ceribelli, M., Yin, J. J., Sowalsky, A. G., Price, D. K., Chau, C. H., Thomas, C. J., & Figg, W. D. (2025). Direct Co-Targeting of Bcl-xL and Mcl-1 Exhibits Synergistic Effects in AR-V7–Expressing CRPC Models. Cancer research communications, 5(8), 1396-1408. https://doi.org/10.1158/2767-9764.CRC-25-0096

@article{f0dfdf0d70d24be58c4730ff739765af,

title = "Direct Co-Targeting of Bcl-xL and Mcl-1 Exhibits Synergistic Effects in AR-V7–Expressing CRPC Models",

abstract = "There is an unmet need to develop novel treatment options for patients with metastatic castration-resistant prostate cancer (mCRPC). Patients often develop resistance to next-generation hormonal therapies that target the androgen receptor (AR) axis (e.g., abiraterone and enzalutamide). A splice variant of AR, AR-V7, is associated with resistance to these inhibitors as well as mCRPC progression and poor prognoses. We embarked upon a high-throughput screen to identify synergistic combinations of targeted therapies using two CRPC cell lines, LNCaP95 and VCaP-CR. Combinations targeting BCL2L1 (Bcl-xL) (A-1331852 and navitoclax) and MCL1 (S63845) synergistically decreased cell viability and induced apoptotic activity via cleavage of PARP, caspase 3, and caspase 7 across AR-V7–expressing CRPC cell lines (LNCaP95, VCaPCR, and 22Rv1) and a patient-derived organoid model (LuCaP 167CR). We also explored the use of a Bcl-xL–specific proteolysis-targeting chimera degrader (PROTAC) to minimize platelet toxicity associated with Bcl-xL inhibitors. We showed similar synergistic efficacy with the Bcl-xL–targeting PROTAC in combination with S63845 in the threedimensional spheroid models. Our findings support further preclinical development of Bcl-xL and Mcl-1 inhibitors for mCRPC.",

author = "Brim, {Benjamin C.} and Leon, {Andres F.} and Beatson, {Erica L.} and Kindrick, {Jessica D.} and Kinjal Bhadresha and Xiaohu Zhang and Napoli, {Giulia C.} and Risdon, {Emily N.} and Schmidt, {Keith T.} and Wilson, {Kelli M.} and Crystal McKnight and Erin Beck and Carleen Klumpp-Thomas and Michele Ceribelli and Yin, {Juan Juan} and Sowalsky, {Adam G.} and Price, {Douglas K.} and Chau, {Cindy H.} and Thomas, {Craig J.} and Figg, {William D.}",

note = "Publisher Copyright: {\textcopyright}2025 The Authors; Published by the American Association for Cancer Research",

year = "2025",

doi = "10.1158/2767-9764.CRC-25-0096",

language = "English",

volume = "5",

pages = "1396--1408",

journal = "Cancer research communications",

issn = "2767-9764",

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

number = "8",

}

Brim, BC, Leon, AF, Beatson, EL, Kindrick, JD, Bhadresha, K, Zhang, X, Napoli, GC, Risdon, EN, Schmidt, KT, Wilson, KM, McKnight, C, Beck, E, Klumpp-Thomas, C, Ceribelli, M, Yin, JJ, Sowalsky, AG, Price, DK, Chau, CH, Thomas, CJ & Figg, WD 2025, 'Direct Co-Targeting of Bcl-xL and Mcl-1 Exhibits Synergistic Effects in AR-V7–Expressing CRPC Models', Cancer research communications, vol. 5, no. 8, pp. 1396-1408. https://doi.org/10.1158/2767-9764.CRC-25-0096

TY - JOUR

T1 - Direct Co-Targeting of Bcl-xL and Mcl-1 Exhibits Synergistic Effects in AR-V7–Expressing CRPC Models

AU - Brim, Benjamin C.

AU - Leon, Andres F.

AU - Beatson, Erica L.

AU - Kindrick, Jessica D.

AU - Bhadresha, Kinjal

AU - Zhang, Xiaohu

AU - Napoli, Giulia C.

AU - Risdon, Emily N.

AU - Schmidt, Keith T.

AU - Wilson, Kelli M.

AU - McKnight, Crystal

AU - Beck, Erin

AU - Klumpp-Thomas, Carleen

AU - Ceribelli, Michele

AU - Yin, Juan Juan

AU - Sowalsky, Adam G.

AU - Price, Douglas K.

AU - Chau, Cindy H.

AU - Thomas, Craig J.

AU - Figg, William D.

PY - 2025

Y1 - 2025

N2 - There is an unmet need to develop novel treatment options for patients with metastatic castration-resistant prostate cancer (mCRPC). Patients often develop resistance to next-generation hormonal therapies that target the androgen receptor (AR) axis (e.g., abiraterone and enzalutamide). A splice variant of AR, AR-V7, is associated with resistance to these inhibitors as well as mCRPC progression and poor prognoses. We embarked upon a high-throughput screen to identify synergistic combinations of targeted therapies using two CRPC cell lines, LNCaP95 and VCaP-CR. Combinations targeting BCL2L1 (Bcl-xL) (A-1331852 and navitoclax) and MCL1 (S63845) synergistically decreased cell viability and induced apoptotic activity via cleavage of PARP, caspase 3, and caspase 7 across AR-V7–expressing CRPC cell lines (LNCaP95, VCaPCR, and 22Rv1) and a patient-derived organoid model (LuCaP 167CR). We also explored the use of a Bcl-xL–specific proteolysis-targeting chimera degrader (PROTAC) to minimize platelet toxicity associated with Bcl-xL inhibitors. We showed similar synergistic efficacy with the Bcl-xL–targeting PROTAC in combination with S63845 in the threedimensional spheroid models. Our findings support further preclinical development of Bcl-xL and Mcl-1 inhibitors for mCRPC.

AB - There is an unmet need to develop novel treatment options for patients with metastatic castration-resistant prostate cancer (mCRPC). Patients often develop resistance to next-generation hormonal therapies that target the androgen receptor (AR) axis (e.g., abiraterone and enzalutamide). A splice variant of AR, AR-V7, is associated with resistance to these inhibitors as well as mCRPC progression and poor prognoses. We embarked upon a high-throughput screen to identify synergistic combinations of targeted therapies using two CRPC cell lines, LNCaP95 and VCaP-CR. Combinations targeting BCL2L1 (Bcl-xL) (A-1331852 and navitoclax) and MCL1 (S63845) synergistically decreased cell viability and induced apoptotic activity via cleavage of PARP, caspase 3, and caspase 7 across AR-V7–expressing CRPC cell lines (LNCaP95, VCaPCR, and 22Rv1) and a patient-derived organoid model (LuCaP 167CR). We also explored the use of a Bcl-xL–specific proteolysis-targeting chimera degrader (PROTAC) to minimize platelet toxicity associated with Bcl-xL inhibitors. We showed similar synergistic efficacy with the Bcl-xL–targeting PROTAC in combination with S63845 in the threedimensional spheroid models. Our findings support further preclinical development of Bcl-xL and Mcl-1 inhibitors for mCRPC.

UR - http://www.scopus.com/inward/record.url?scp=105013875855&partnerID=8YFLogxK

U2 - 10.1158/2767-9764.CRC-25-0096

DO - 10.1158/2767-9764.CRC-25-0096

M3 - Article

C2 - 40704654

AN - SCOPUS:105013875855

SN - 2767-9764

VL - 5

SP - 1396

EP - 1408

JO - Cancer research communications

JF - Cancer research communications

IS - 8

ER -