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. 2024 Nov;27(6):1258-1272.
doi: 10.1007/s10120-024-01552-z. Epub 2024 Sep 19.

Lipolysis-stimulated lipoprotein receptor promote lipid uptake and fatty acid oxidation in gastric cancer

Kota Kawabata  1 Tsuyoshi Takahashi  2 Koji Tanaka  1 Yukinori Kurokawa  1 Kazuyoshi Yamamoto  1 Takuro Saito  1 Kota Momose  1 Kotaro Yamashita  1 Tomoki Makino  1 Takashi Yokouchi  1 Kunihiko Kawai  1 Satoshi Serada  3 Minoru Fujimoto  4 Kiyokazu Nakajima  1 Tetsuji Naka  3   4 Hidetoshi Eguchi  1 Yuichiro Doki  1
Affiliations

Lipolysis-stimulated lipoprotein receptor promote lipid uptake and fatty acid oxidation in gastric cancer

Kota Kawabata et al. Gastric Cancer. 2024 Nov.

Abstract

Background: Lipolysis-stimulated lipoprotein receptor (LSR), a lipid receptor, is associated with cancer progression. However, detailed effects on intracellular metabolism are unclear. We aimed to elucidate the mechanism of LSR-mediated lipid metabolism in gastric cancer.

Methods: We investigated lipid metabolic changes induced by lipoprotein administration in gastric cancer cells and evaluated the significance of LSR expression and lipid droplets formation in gastric cancer patients. The efficacy of inhibiting β-oxidation in gastric cancer cells was also examined in vitro and vivo.

Results: In gastric cancer cells, LSR promoted cellular uptake of lipoprotein and cell proliferation. Furthermore, the inhibition of LSR in gastric cancer cells expressing high levels of LSR counteracted both effects. Immunohistochemical analysis of human gastric cancer tissues showed that the increase in lipid droplets via LSR is a factor that influences prognosis. Lipidomics analysis of LSR-high-expressing gastric cancer cells revealed an increase in β-oxidation. Based on these results, we used etomoxir, a β-oxidation inhibitor, and found that it inhibited cell proliferation as well as the suppression of LSR. Similarly, in a mouse xenograft model of LSR-highly expressing gastric cancer cells, the tumor growth effect of high-fat diet feeding was counteracted by etomoxir, consistent with the Ki-67 labeling index.

Conclusions: We demonstrated that lipids are taken up into gastric cancer cells via LSR and cause an increase in β-oxidation, resulting in the promotion of cancer progression. Controlling LSR-mediated lipid metabolism may be a novel therapeutic strategy for gastric cancer.

Keywords: Fatty acid oxidation; Gastric cancer; Lipid uptake; Lipolysis-stimulated lipoprotein receptor.

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