Your search keyword '"Borzilleri, Robert"' showing total 3 results

1. Long-Acting Tumor-Activated Prodrug of a TGFβR Inhibitor

Author

Zhang, Yong, Parrish, Karen E., Tortolani, David R., Poss, Michael A., Huang, Audris, Wan, Honghe, Purandare, Ashok V., Donnell, Andrew F., Kempson, James, Hou, Xiaoping, Pawluczyk, Joseph, Yip, Shiuhang, Luk, Emily, Raghavan, Nimmi, Swanson, Jesse, Smalley, James, Murtaza, Anwar, Yang, Zheng, Augustine-Rauch, Karen, Lombardo, Louis J., and Borzilleri, Robert

Abstract

Inhibition of TGFβ signaling in concert with a checkpoint blockade has been shown to provide improved and durable antitumor immune response in mouse models. However, on-target adverse cardiovascular effects have limited the clinical use of TGFβ receptor (TGFβR) inhibitors in cancer therapy. To restrict the activity of TGFβR inhibitors to tumor tissues and thereby widen the therapeutic index, a series of tumor-activated prodrugs of a selective small molecule TGFβR1 inhibitor 1were prepared by appending 1to a serine protease substrate and a half-life extension fatty acid carbon chain. The prodrugs were shown to be selectively metabolized in tumor tissues relative to the heart and blood and demonstrated a prolonged favorable increase in the tumor-to-heart ratio of the active drug in tissue distribution studies. Once-weekly administration of the most tissue-selective compound 10provided anti-tumor efficacy comparable to the parent compound and reduced systemic exposure of the active drug.

Published

2021

2. Discovery and Synthesis of Heterobifunctional Degraders of Rearranged during Transfection (RET) Kinase

Author

Qiao, Jennifer X., Williams, David, Gill, Patrice, Li, Ling, Norris, Derek, Tokarski, John S., Wong, Jessica, Qi, Huilin, Hafeji, Yamnah, Downes, Daniel P., Degnen, Bill, Wang, Ying-Kai, Locke, Gregory, Fang, Hua, Yu, Fei, Xu, Songmei, Naglich, Joseph, Zhang, Jun, Nanjappa, Purushothama, Dai, Chao, Chourb, Lisa, Napoline, Jonathan, Tester, Richland, Jorge, Christine, Li, Yi-Xin, Mathur, Arvind, Barbieri, Christopher, Soars, Matthew G., Venkatanarayan, Avinashnarayan, Lees, Emma, Borzilleri, Robert M., Gavai, Ashvinikumar V., Wichroski, Michael, and Dhar, T. G. Murali

Abstract

We describe the design, synthesis, and structure–activity relationship (SAR) of heterobifunctional RET ligand-directed degraders (LDDs) derived from three different second-generation RET inhibitors. These LDDs are composed of a target binding motif (TBM) that binds to the RET protein, a linker, and a cereblon binding motif (CBM) as the E3 ligase recognition unit. This led to the identification of a series of pyrazolopyridine-based heterobifunctional LDDs, as exemplified by compound 39. LDD 39demonstrated high in vitro inhibitory and degradation potency against both RET wild-type and the two representative mutants, V804M and G810R. Importantly, in PK/PD studies, 39exhibited a differentiated and favorable in vivo profile compared to the corresponding tyrosine kinase inhibitor (TKI), compound 3. Robust and sustained degradation of total-RET (tRET) protein and inhibition of phospho-RET (pRET) signaling were observed in TPC-1 xenograft tumors driven by RET and the RET/G810R mutant following a single dose of LDD 39at 15 and 75 mg/kg, respectively.

Published

2024

3. DGKα/ζ inhibitors combine with PD-1 checkpoint therapy to promote T cell–mediated antitumor immunity

Author

Wichroski, Michael, Benci, Joseph, Liu, Si-Qi, Chupak, Louis, Fang, Jie, Cao, Carolyn, Wang, Cindy, Onorato, Joelle, Qiu, Hongchen, Shan, Yongli, Banas, Dana, Powles, Ryan, Locke, Gregory, Witt, Abigail, Stromko, Caitlyn, Qi, Huilin, Zheng, Xiaofan, Martin, Scott, Ding, Min, Gentles, Robert, Meanwell, Nicholas, Velaparthi, Upender, Olson, Richard, Wee, Susan, Tenney, Daniel, Parker, Christopher G., Cravatt, Benjamin F., Lawrence, Michael, Borzilleri, Robert, and Lees, Emma

Published

2023