Adipocytes and Metabolism: Contributions to Multiple Myeloma

Overview

Journal J Bone Oncol

Publisher Elsevier

Date 2024 Jun 14

PMID 38872708

Authors

Heather Fairfield

Michelle Karam

Allyson Schimelman

Ya-Wei Qiang

Michaela R Reagan

Affiliations

Soon will be listed here.

Abstract

Obesity contributes to many cancers, including breast cancer and multiple myeloma, two cancers that often colonize the bone marrow (BM). Obesity often causes metabolic disease, but at the cellular level, there is uncertainty regarding how these shifts affect cellular phenotypes. Evidence is building that different types of fuel affect tumor cell metabolism, mitochondrial function, and signaling pathways differently, but tumor cells are also flexible and adapt to less-than ideal metabolic conditions, suggesting that single-pronged attacks on tumor metabolism may not be efficacious enough to be effective clinically. In this review, we describe the newest research at the pre-clinical level on how tumor metabolic pathways and energy sources affect cancer cells, with a special focus on multiple myeloma (MM). We also describe the known forward-feedback loops between bone marrow adipocytes (BMAds) and local tumor cells that support tumor growth. We describe how metabolic targets and transcription factors related to fatty acid (FA) oxidation, FA biosynthesis, glycolysis, oxidative phosphorylation (OXPHOS), and other pathways hold great promise as new vulnerabilities in myeloma cells. Specifically, we describe the importance of the acetyl-CoA synthetase (ACSS) and the acyl-CoA synthetase long chain (ACSL) families, which are both involved in FA metabolism. We also describe new data on the importance of lactate metabolism and lactate transporters in supporting the growth of tumor cells in a hypoxic BM microenvironment. We highlight new data showing the dependency of myeloma cells on the mitochondrial pyruvate carrier (MPC), which transports pyruvate to the mitochondria to fuel the tricarboxylic acid (TCA) cycle and electron transport chain (ETC), boosting OXPHOS. Inhibiting the MPC affects myeloma cell mitochondrial metabolism and growth, and synergizes with proteosome inhibitors in killing myeloma cells. We also describe how metabolic signaling pathways intersect established survival and proliferation pathways; for example, the fatty acid binding proteins (FABPs) affect MYC signaling and support growth, survival, and metabolism of myeloma cells. Our goal is to review the current the field so that novel, metabolic-focused therapeutic interventions and treatments can be imagined, developed and tested to decrease the burden of MM and related cancers.

Citing Articles

Monoclonal anti-CD38 therapy in human myeloma: retrospects and prospects.

Horenstein A, Faini A, Morandi F, Ortolan E, Storti P, Giuliani N Front Immunol. 2025; 16:1519300.

PMID: 40013150 PMC: 11860881. DOI: 10.3389/fimmu.2025.1519300.

Editors' introduction: The microenvironment in bone metastasis - New dimensions.

Holen I, Edwards C J Bone Oncol. 2025; 48:100633.

PMID: 39886736 PMC: 11780373. DOI: 10.1016/j.jbo.2024.100633.

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