Journal of Experimental & Clinical Cancer Research (Jan 2025)

PRMT5 inhibition has a potent anti-tumor activity against adenoid cystic carcinoma of salivary glands

  • Vasudha Mishra,
  • Alka Singh,
  • Michael Korzinkin,
  • Xiangying Cheng,
  • Claudia Wing,
  • Viktoria Sarkisova,
  • Ashwin L. Koppayi,
  • Alexandra Pogorelskaya,
  • Oksana Glushchenko,
  • Manu Sundaresan,
  • Venkat Thodima,
  • Jack Carter,
  • Koichi Ito,
  • Peggy Scherle,
  • Anna Trzcinska,
  • Ivan Ozerov,
  • Everett E. Vokes,
  • Grayson Cole,
  • Frank W. Pun,
  • Le Shen,
  • Yuxuan Miao,
  • Alexander T. Pearson,
  • Mark W. Lingen,
  • Bruce Ruggeri,
  • Ari J. Rosenberg,
  • Alex Zhavoronkov,
  • Nishant Agrawal,
  • Evgeny Izumchenko

DOI
https://doi.org/10.1186/s13046-024-03270-x
Journal volume & issue
Vol. 44, no. 1
pp. 1 – 20

Abstract

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Abstract Background Adenoid cystic carcinoma (ACC) is a rare glandular malignancy, commonly originating in salivary glands of the head and neck. Given its protracted growth, ACC is usually diagnosed in advanced stage. Treatment of ACC is limited to surgery and/or adjuvant radiotherapy, which often fails to prevent disease recurrence, and no FDA-approved targeted therapies are currently available. As such, identification of new therapeutic targets specific to ACC is crucial for improved patients’ outcomes. Methods After thoroughly evaluating the gene expression and signaling patterns characterizing ACC, we applied PandaOmics (an AI-driven software platform for novel therapeutic target discovery) on the unique transcriptomic dataset of 87 primary ACCs. Identifying protein arginine methyl transferase 5 (PRMT5) as a putative candidate with the top-scored druggability, we next determined the applicability of PRMT5 inhibitors (PRT543 and PRT811) using ACC cell lines, organoids, and patient derived xenograft (PDX) models. Molecular changes associated with response to PRMT5 inhibition and anti-proliferative effect of the combination therapy with lenvatinib was then analyzed. Results Using a comprehensive AI-powered engine for target identification, PRMT5 was predicted among potential therapeutic target candidates for ACC. Here we show that monotherapy with selective PRMT5 inhibitors induced a potent anti-tumor activity across several cellular and animal models of ACC, which was paralleled by downregulation of genes associated with ACC tumorigenesis, including MYB and MYC (the recognized drivers of ACC progression). Furthermore, as a subset of genes targeted by lenvatinib is upregulated in ACC, we demonstrate that addition of lenvatinib enhanced the growth inhibitory effect of PRMT5 blockade in vitro, suggesting a potential clinical benefit for patients expressing lenvatinib favorable molecular profile. Conclusion Taken together, our study underscores the role of PRMT5 in ACC oncogenesis and provides a strong rationale for the clinical development of PRMT5 inhibitors as a targeted monotherapy or combination therapy for treatment of patients with this rare disease, based on the analysis of their underlying molecular profile.

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