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A promising magnesium-related alloy with metabolic reprogramming and antitumor effects in hepatocellular and pancreatic cancer.

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Bioactive materials 2026 Vol.59() p. 186-204 cited 1 OA Aluminum toxicity and tolerance in p
TL;DR These findings position Al-Mg as a promising antitumor material and provide a mechanistic framework supporting the development of magnesium-related alloys for local oncologic intervention.
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PubMed DOI PMC OpenAlex Semantic 마지막 보강 2026-04-29
OpenAlex 토픽 · Aluminum toxicity and tolerance in plants and animals Magnesium Alloys: Properties and Applications Magnesium in Health and Disease

Zhang J, Gu J, Xia R, Yin J, Wang X, Yang J, Wang Y, Yi Z, Wang S, Zhang Q, Wang H, She J, Guo S

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These findings position Al-Mg as a promising antitumor material and provide a mechanistic framework supporting the development of magnesium-related alloys for local oncologic intervention.

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APA J.S. Zhang, Jianyou Gu, et al. (2026). A promising magnesium-related alloy with metabolic reprogramming and antitumor effects in hepatocellular and pancreatic cancer.. Bioactive materials, 59, 186-204. https://doi.org/10.1016/j.bioactmat.2025.12.039
MLA J.S. Zhang, et al.. "A promising magnesium-related alloy with metabolic reprogramming and antitumor effects in hepatocellular and pancreatic cancer.." Bioactive materials, vol. 59, 2026, pp. 186-204.
PMID 41536919

Abstract

Hepatocellular and pancreatic cancers are highly aggressive malignancies with dismal clinical outcomes, highlighting an urgent need for new therapeutic strategies. Magnesium-related alloys, widely explored for their biocompatibility and bioactivity, are attractive candidates for biliary and pancreatic duct stents. However, their antitumor potential and underlying mechanisms remain incompletely defined. Here, we systematically characterized the physicochemical properties and anticancer activities of a panel of magnesium-related alloy powders and identified an aluminum-magnesium (Al-Mg) alloy as the most potent candidate. Compared with pure Mg, Al-Mg rods exhibited stronger antitumor efficacy together with more controllable degradation. and assays confirmed that Al-Mg significantly inhibited hepatocellular carcinoma and pancreatic cancer progression. Integrated metabolomic and transcriptomic analyses indicated that Al-Mg activates AMPK signaling and suppresses purine and pyrimidine metabolism, consistent with metabolic reprogramming that limits tumor cell proliferation. Furthermore, single-cell and spatial transcriptomic analyses delineated Al-Mg-sensitive tumor cell subpopulations and mapped their spatial distribution within pancreatic cancer tissues. Collectively, these findings position Al-Mg as a promising antitumor material and provide a mechanistic framework supporting the development of magnesium-related alloys for local oncologic intervention.

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