Integrating Pharmacogenomics Data-Driven Computational Drug Prediction with Single-Cell RNAseq to Demonstrate the Efficacy of a NAMPT Inhibitor against Aggressive, Taxane-Resistant, and Stem-like Cells in Lethal Prostate Cancer

Suman Mazumder; Taraswi Mitra Ghosh; Ujjal K Mukherjee; Sayak Chakravarti; Farshad Amiri; Razan S Waliagha; Farnaz Hemmati; Panagiotis Mistriotis; Salsabil Ahmed; Isra Elhussin; Ahmad-Bin Salam; Windy Dean-Colomb; Clayton Yates; Robert D Arnold; Amit K Mitra

doi:10.3390/cancers14236009

Integrating Pharmacogenomics Data-Driven Computational Drug Prediction with Single-Cell RNAseq to Demonstrate the Efficacy of a NAMPT Inhibitor against Aggressive, Taxane-Resistant, and Stem-like Cells in Lethal Prostate Cancer

Cancers (Basel). 2022 Dec 6;14(23):6009. doi: 10.3390/cancers14236009.

Authors

Suman Mazumder^{1

2}, Taraswi Mitra Ghosh^{1

3}, Ujjal K Mukherjee^{4

5}, Sayak Chakravarti¹, Farshad Amiri⁶, Razan S Waliagha¹, Farnaz Hemmati⁶, Panagiotis Mistriotis⁶, Salsabil Ahmed^{1

2}, Isra Elhussin⁷, Ahmad-Bin Salam⁷, Windy Dean-Colomb^{7

8}, Clayton Yates^{7

9

10

11

12}, Robert D Arnold^{1

12}, Amit K Mitra^{1

2

12}

Affiliations

¹ Department of Drug Discovery and Development, Harrison College of Pharmacy, Auburn University, Auburn, AL 36849, USA.
² Center for Pharmacogenomics and Single-Cell Omics (AUPharmGx), Harrison College of Pharmacy, Auburn University, Auburn, AL 36849, USA.
³ Department of Urology Research, Brigham and Women's Hospital, Harvard Medical School, Boston, MA 02215, USA.
⁴ Department of Business Administration, University of Illinois at Urbana-Champaign, Champaign, IL 61820, USA.
⁵ Biomedical and Translational Sciences, Carle Illinois College of Medicine, University of Illinois Urbana-Champaign, Champaign, IL 61820, USA.
⁶ Department of Chemical Engineering, Samuel Ginn College of Engineering, Auburn University, Auburn, AL 36849, USA.
⁷ Department of Biology and Canter for Cancer Research, Tuskegee University, Tuskegee, AL 36088, USA.
⁸ Piedmont Hospital, Newnan, GA 30309, USA.
⁹ Department of Pathology, Johns Hopkins University School of Medicine, Baltimore, MD 21218, USA.
¹⁰ Sidney Kimmel Comprehensive Cancer Center, Johns Hopkins University School of Medicine, Baltimore, MD 21218, USA.
¹¹ Department of Urology, Johns Hopkins University School of Medicine, Baltimore, MD 21218, USA.
¹² UAB O'Neal Comprehensive Cancer, University of Alabama at Birmingham School of Medicine, Birmingham, AL 35233, USA.

Abstract

Metastatic prostate cancer/PCa is the second leading cause of cancer deaths in US men. Most early-stage PCa are dependent on overexpression of the androgen receptor (AR) and, therefore, androgen deprivation therapies/ADT-sensitive. However, eventual resistance to standard medical castration (AR-inhibitors) and secondary chemotherapies (taxanes) is nearly universal. Further, the presence of cancer stem-like cells (EMT/epithelial-to-mesenchymal transdifferentiation) and neuroendocrine PCa (NEPC) subtypes significantly contribute to aggressive/lethal/advanced variants of PCa (AVPC). In this study, we introduced a pharmacogenomics data-driven optimization-regularization-based computational prediction algorithm ("secDrugs") to predict novel drugs against lethal PCa. Integrating secDrug with single-cell RNA-sequencing/scRNAseq as a 'Double-Hit' drug screening tool, we demonstrated that single-cells representing drug-resistant and stem-cell-like cells showed high expression of the NAMPT pathway genes, indicating potential efficacy of the secDrug FK866 which targets NAMPT. Next, using several cell-based assays, we showed substantial impact of FK866 on clinically advanced PCa as a single agent and in combination with taxanes or AR-inhibitors. Bulk-RNAseq and scRNAseq revealed that, in addition to NAMPT inhibition, FK866 regulates tumor metastasis, cell migration, invasion, DNA repair machinery, redox homeostasis, autophagy, as well as cancer stemness-related genes, HES1 and CD44. Further, we combined a microfluidic chip-based cell migration assay with a traditional cell migration/'scratch' assay and demonstrated that FK866 reduces cancer cell invasion and motility, indicating abrogation of metastasis. Finally, using PCa patient datasets, we showed that FK866 is potentially capable of reversing the expression of several genes associated with biochemical recurrence, including IFITM3 and LTB4R. Thus, using FK866 as a proof-of-concept candidate for drug repurposing, we introduced a novel, universally applicable preclinical drug development pipeline to circumvent subclonal aggressiveness, drug resistance, and stemness in lethal PCa.

Keywords: DEGs; FK866; IPA; RNAseq; prostate cancer; scRNAseq; secDrug; synergism; taxane.

Grants and funding

This research received no external funding.