High-throughput Screening Identifies Aurora Kinase B As a Critical Therapeutic Target for Merkel Cell Carcinoma

Overview

Journal Nat Commun

Specialty Biology

Date 2025 Feb 12

PMID 39939315

Authors

Tara Gelb

Khalid A Garman

Daniel Urban

Amy Coxon

Berkley Gryder

Natasha T Hill

Lingling Miao

Tobie Lee

Olivia Lee

Sirisha Chakka

John Braisted

Jordan E Jarvis

Rachael Glavin

Trisha S Raj

Ying Xiao

Simone Difilippantonio

Amy Q Wang

Min Shen

Ken Chih-Chien Cheng

Madhu Lal-Nag

Matthew D Hall

Isaac Brownell

Affiliations

Soon will be listed here.

Abstract

Merkel cell carcinoma (MCC) is a rare, aggressive skin cancer. Most MCCs contain Merkel cell polyomavirus (virus-positive MCC; VP-MCC), and the remaining are virus-negative (VN-MCC). Immune checkpoint inhibitors are the first-line treatment for metastatic MCC, but durable responses are achieved in less than 50% of patients. To identify new treatments, we screen ~4,000 compounds for their ability to reduce MCC viability and demonstrate that VP-MCC and VN-MCC exhibit distinct response profiles. Aurora kinase inhibitors selectively reduce VP-MCC viability, with RNAi screening independently identifying AURKB as an essential gene for MCC survival, especially in VP-MCC. AZD2811, a selective AURKB inhibitor, induces mitotic dysregulation and apoptosis in MCC cells, with greater efficacy in VP-MCC. In mice, AZD2811 nanoparticles inhibit tumor growth and increase survival in both VP-MCC and VN-MCC xenograft models. Overall, our unbiased screens identify AURKB as a promising therapeutic target and AZD2811NP as a potential treatment for MCC.

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