Dual-Hit Strategy for Therapeutic Targeting of Pancreatic Cancer in Patient-Derived Xenograft Tumors

Tista Roy Chaudhuri; Qingxiang Lin; Ewa K Stachowiak; Spencer R Rosario; Joseph A Spernyak; Wen Wee Ma; Michal K Stachowiak; Michelle K Greene; Gerard P Quinn; Simon S McDade; Martin Clynes; Christopher J Scott; Robert M Straubinger

doi:10.1158/1078-0432.CCR-23-0131

Dual-Hit Strategy for Therapeutic Targeting of Pancreatic Cancer in Patient-Derived Xenograft Tumors

Clin Cancer Res. 2024 Apr 1;30(7):1367-1381. doi: 10.1158/1078-0432.CCR-23-0131.

Authors

Affiliations

¹ Department of Pharmaceutical Sciences, University at Buffalo, State University of New York, Buffalo, New York.
² Department of Cell Stress Biology, Roswell Park Comprehensive Cancer Center, Buffalo, New York.
³ Department of Pathology and Anatomical Sciences, University at Buffalo, State University of New York, Buffalo, New York.
⁴ Department of Bioinformatics and Biostatistics, Roswell Park Comprehensive Cancer Center, Buffalo, New York.
⁵ Department of Hematology and Oncology, Taussig Cancer Institute, Cleveland Clinic, Cleveland, Ohio.
⁶ The Patrick G Johnston Centre for Cancer Research, School of Medicine, Dentistry and Biomedical Sciences, Queen's University Belfast, Belfast, United Kingdom.
⁷ The National Institute for Cellular Biotechnology, Dublin City University, Dublin, Ireland.

PMID: 38270582
PMCID: PMC11019863 (available on 2024-10-01)
DOI: 10.1158/1078-0432.CCR-23-0131

Abstract

Purpose: Paracrine activation of pro-fibrotic hedgehog (HH) signaling in pancreatic ductal adenocarcinoma (PDAC) results in stromal amplification that compromises tumor drug delivery, efficacy, and patient survival. Interdiction of HH-mediated tumor-stroma crosstalk with smoothened (SMO) inhibitors (SHHi) "primes" PDAC patient-derived xenograft (PDX) tumors for increased drug delivery by transiently increasing vascular patency/permeability, and thereby macromolecule delivery. However, patient tumor isolates vary in their responsiveness, and responders show co-induction of epithelial-mesenchymal transition (EMT). We aimed to identify the signal derangements responsible for EMT induction and reverse them and devise approaches to stratify SHHi-responsive tumors noninvasively based on clinically-quantifiable parameters.

Experimental design: Animals underwent diffusion-weighted magnetic resonance (DW-MR) imaging for measurement of intratumor diffusivity. In parallel, tissue-level deposition of nanoparticle probes was quantified as a marker of vascular permeability/perfusion. Transcriptomic and bioinformatic analysis was employed to investigate SHHi-induced gene reprogramming and identify key "nodes" responsible for EMT induction.

Results: Multiple patient tumor isolates responded to short-term SHH inhibitor exposure with increased vascular patency and permeability, with proportionate increases in tumor diffusivity. Nonresponding PDXs did not. SHHi-treated tumors showed elevated FGF drive and distinctly higher nuclear localization of fibroblast growth factor receptor (FGFR1) in EMT-polarized tumor cells. Pan-FGFR inhibitor NVP-BGJ398 (Infigratinib) reversed the SHHi-induced EMT marker expression and nuclear FGFR1 accumulation without compromising the enhanced permeability effect.

Conclusions: This dual-hit strategy of SMO and FGFR inhibition provides a clinically-translatable approach to compromise the profound impermeability of PDAC tumors. Furthermore, clinical deployment of DW-MR imaging could fulfill the essential clinical-translational requirement for patient stratification.

MeSH terms

Animals
Carcinoma, Pancreatic Ductal* / drug therapy
Carcinoma, Pancreatic Ductal* / genetics
Carcinoma, Pancreatic Ductal* / metabolism
Cell Line, Tumor
Disease Models, Animal
Hedgehog Proteins / genetics
Hedgehog Proteins / metabolism
Heterografts
Humans
Pancreatic Neoplasms* / drug therapy
Pancreatic Neoplasms* / genetics
Pancreatic Neoplasms* / metabolism
Signal Transduction

Substances

Hedgehog Proteins

Abstract

MeSH terms

Substances

Grants and funding