Characterization of Proteome-size Scaling by Integrative Omics Reveals Mechanisms of Proliferation Control in Cancer

Overview

Journal Sci Adv

Specialties Biology
Science

Date 2023 Jan 25

PMID 36696495

Authors

Ian Jones

Lucas Dent

Tomoaki Higo

Theodoros Roumeliotis

Maria Arias Garcia

Hansa Shree

Jyoti Choudhary

Malin Pedersen

Chris Bakal

Affiliations

Soon will be listed here.

Abstract

Almost all living cells maintain size uniformity through successive divisions. Proteins that over and underscale with size can act as rheostats, which regulate cell cycle progression. Using a multiomic strategy, we leveraged the heterogeneity of melanoma cell lines to identify peptides, transcripts, and phosphorylation events that differentially scale with cell size. Subscaling proteins are enriched in regulators of the DNA damage response and cell cycle progression, whereas super-scaling proteins included regulators of the cytoskeleton, extracellular matrix, and inflammatory response. Mathematical modeling suggested that decoupling growth and proliferative signaling may facilitate cell cycle entry over senescence in large cells when mitogenic signaling is decreased. Regression analysis reveals that up-regulation of TP53 or CDKN1A/p21CIP1 is characteristic of proliferative cancer cells with senescent-like sizes/proteomes. This study provides one of the first demonstrations of size-scaling phenomena in cancer and how morphology influences the chemistry of the cell.

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