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25-04-2022 | COMMENTARY

The paradoxical role of inositol in cancer: a consequence of the metabolic state of a tumor

Authors: Kendall C. Case, Michael W. Schmidtke, Miriam L. Greenberg

Published in: Cancer and Metastasis Reviews | Issue 2/2022

Abstract

Inositol is an essential nutrient, obtained either by uptake from the environment or by de novo synthesis from glucose. Inositol and its derivatives exhibit tumor-suppressive effects, potentially mediated by inhibition of the ERK-MAPK or PI3K-Akt pathways. Accordingly, many cancers have been documented to silence expression of the ISYNA1 gene, which encodes the rate-limiting enzyme of inositol synthesis. Paradoxically, recent studies have also reported upregulation of ISYNA1 in some cancers. Upregulation may reflect a compensatory response brought about by defective inositol uptake or oncogenic mutations that preclude its tumor-suppressive effects. In these scenarios, de novo synthesis of inositol may be upregulated to promote cell proliferation. The role of inositol in cancer is further complicated by its ability to inhibit the master metabolic regulator AMPK, which upon activation can either decrease cell proliferation and metastasis or promote cell survival. Due to its potential dual role in cancer, inositol homeostasis must be tightly regulated in tumor cells. Thus, whether inositol acts to suppress or promote tumor progression is determined by the metabolic profile and oncogenic background of the cancer.

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Title: The paradoxical role of inositol in cancer: a consequence of the metabolic state of a tumor
Authors: Kendall C. Case
Michael W. Schmidtke
Miriam L. Greenberg
Publication date: 25-04-2022
Publisher: Springer US
Published in: Cancer and Metastasis Reviews / Issue 2/2022
Print ISSN: 0167-7659
Electronic ISSN: 1573-7233
DOI: https://doi.org/10.1007/s10555-022-10032-8

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