Chromosomal 3q Amplicon Encodes Essential Regulators of Secretory Vesicles That Drive Secretory Addiction in Cancer

Authors

Xiaochao Tan
Shike Wang
Guan-Yu Xiao
Chao Wu
Xin Liu
Biyao Zhou
Jiang Yu
Dzifa Yawa Duose
Yuanxin Xi
Jing Wang
Kunika Gupta
Apar Pataer
Jack A Roth
Michael P Kim
Fengju Chen
Chad J Creighton
William K Russell
Jonathan M Kurie

Publication Date

4-25-2024

Journal

The Journal of Clinical Investigation

DOI

10.1172/JCI176355

PMID

38662435

PMCID

PMC11178546

PubMedCentral® Posted Date

April 2024

PubMedCentral® Full Text Version

Post-print

Abstract

Cancer cells exhibit heightened secretory states that drive tumor progression. Here, we identify a chromosome 3q amplicon that serves as a platform for secretory regulation in cancer. The 3q amplicon encodes multiple Golgi-resident proteins, including the scaffold Golgi integral membrane protein 4 (GOLIM4) and the ion channel ATPase Secretory Pathway Ca2+ Transporting 1 (ATP2C1). We show that GOLIM4 recruits ATP2C1 and Golgi phosphoprotein 3 (GOLPH3) to coordinate calcium-dependent cargo loading and Golgi membrane bending and vesicle scission. GOLIM4 depletion disrupts the protein complex, resulting in a secretory blockade that inhibits the progression of 3q-amplified malignancies. In addition to its role as a scaffold, GOLIM4 maintains intracellular manganese (Mn) homeostasis by binding excess Mn in the Golgi lumen, which initiates the routing of Mn-bound GOLIM4 to lysosomes for degradation. We show that Mn treatment inhibits the progression of multiple types of 3q-amplified malignancies by degrading GOLIM4, resulting in a secretory blockade that interrupts pro-survival autocrine loops and attenuates pro-metastatic processes in the tumor microenvironment. Potentially underlying the selective activity of Mn against 3q-amplified malignancies, ATP2C1 co-amplification increases Mn influx into the Golgi lumen, resulting in a more rapid degradation of GOLIM4. These findings show that functional cooperativity between co-amplified genes underlies heightened secretion and a targetable secretory addiction in 3q-amplified malignancies.

Keywords

Cancer gene therapy, Lung cancer, Protein traffic, Cell biology, Oncology

Published Open-Access

yes

Recommended Citation

Tan, Xiaochao; Wang, Shike; Xiao, Guan-Yu; et al., "Chromosomal 3q Amplicon Encodes Essential Regulators of Secretory Vesicles That Drive Secretory Addiction in Cancer" (2024). Faculty, Staff and Student Publications. 1307.
https://digitalcommons.library.tmc.edu/uthgsbs_docs/1307