What question did this study set out to answer?

To synthesize the mechanistic and clinical evidence supporting the use of metformin in cancer treatment, particularly in breast cancer and non-small cell lung cancer.

March 23, 2026Open Access

Old Drug, New Uses: A Comprehensive Review of the Evolving Role of Metformin in Oncology

Key Points

To synthesize the mechanistic and clinical evidence supporting the use of metformin in cancer treatment, particularly in breast cancer and non-small cell lung cancer.
Conducted a targeted narrative review of existing literature
Prioritized randomized controlled trials and presurgical biomarker studies
Analyzed preclinical, translational, and clinical studies
Metformin may improve insulin sensitivity and reduce markers of inflammation in breast cancer
The MA.32 trial found no overall benefit of metformin in non-diabetic patients for disease-free or overall survival
In NSCLC, the evidence varies, with mixed results from combination therapies and challenges in patient adherence due to gastrointestinal side effects.

Abstract

Background: Metformin is a first-line therapy for type 2 diabetes mellitus and a prominent candidate for oncology drug repurposing following observational associations with lower cancer incidence and mortality in diabetic cohorts. Objective: To synthesise mechanistic rationale and clinical evidence for metformin in oncology, focusing on breast cancer and non-small cell lung cancer (NSCLC), and to identify major sources of heterogeneity and priorities for future research. Methods: Targeted narrative review of peer-reviewed preclinical, translational, and clinical studies, prioritising randomised controlled trials, presurgical biomarker studies, and higher-quality observational analyses with clinically interpretable endpoints. Results: Metformin is proposed to act through host-mediated mechanisms, including improved insulin sensitivity and reduced hyperinsulinaemia and inflammatory signalling, and tumour-cell effects, including mitochondrial complex I inhibition, energetic stress, and AMPK to mTOR modulation. In breast cancer, metformin consistently improves metabolic and inflammatory biomarkers. However, the large MA.32 adjuvant trial in non-diabetic patients showed no overall benefit in invasive disease-free survival or overall survival. Presurgical studies suggest antiproliferative effects such as Ki-67 reduction may be limited to insulin-resistant or otherwise biologically defined subgroups. In NSCLC, evidence is heterogeneous. Combination trials with EGFR tyrosine kinase inhibitors or chemotherapy report mixed efficacy, and gastrointestinal toxicity can limit adherence. Emerging supportive-care studies indicate possible reductions in selected chemotherapy-related toxicities. Conclusions: Current evidence supports context-dependent, rather than universal, oncologic utility of metformin. Future trials should prospectively stratify by metabolic status and tumour biology, optimise dose and timing, and test biomarker-guided combinations and patient-centred supportive endpoints.

Bookmark

View Full Paper

Cite This Study

Myszewski et al. (Thu,) studied this question.

synapsesocial.com/papers/69c0de74fddb9876e79c13e8 https://doi.org/https://doi.org/10.31435/ijitss.1(49).2026.5067

Bookmark

View Full Paper