# The Effect of Metformin on Atezolizumab/Bevacizumab Treatment in Patients with Hepatocellular Carcinoma and Diabetes

**Authors:** Andrea Dalbeni, Marco Vicardi, Leonardo A. Natola, Alessandra Auriemma, Bernardo Stefanini, Caterina Vivaldi, Piera Federico, Andrea Polloni, Caterina Soldà, Lorenzo Lani, Ingrid Garajová, Stefano Tamberi, Stefania De Lorenzo, Fabio Piscaglia, Vincenzo Di Maria, Gianluca Masi, Sara Lonardi, Giovanni Brandi, Bruno Daniele, Franco Trevisani, Gianluca Svegliati-Baroni, Laura Schiada, Fabio Marra, Claudia Campani, Ciro Celsa, Giuseppe Cabibbo, Mariangela Bruccoleri, Massimo Iavarone, Leonardo Stella, Francesca R. Ponziani, Tiziana Pressiani, Lorenza Rimassa, Francesco Tovoli, David Sacerdoti

PMC · DOI: 10.32604/or.2026.073063 · Oncology Research · 2026-03-23

## TL;DR

This study found that metformin does not improve treatment outcomes for liver cancer patients with diabetes who are receiving atezolizumab and bevacizumab.

## Contribution

This is the first study to evaluate metformin's impact on A+B therapy outcomes in HCC patients with diabetes using a large multicenter dataset.

## Key findings

- Metformin use showed no significant improvement in progression-free survival or overall survival in the overall population.
- In patients with type 2 diabetes, metformin did not significantly affect progression-free survival, overall survival, or time to progression.
- IPTW analysis confirmed the lack of benefit from metformin in this treatment context.

## Abstract

The combination of atezolizumab plus bevacizumab (A+B) represents one of the standards first-line treatments for unresectable hepatocellular carcinoma (HCC). Metformin has garnered attention for its potential antitumour and immunomodulatory properties beyond glycaemic control. This study aimed to assess metformin’s impact in patients with type 2 diabetes mellitus (T2DM) receiving A+B therapy.

This retrospective analysis of a prospectively-maintained multicentre database included 523 patients with HCC treated with A+B from the ARTE (Atezolizumab-bevacizumab Real-life Experience for Treatment of Hepatocellular Carcinoma) dataset across 18 Italian centres (May 2020–January 2024). We evaluated objective response rate (ORR), disease control rate (DCR), progression-free survival (PFS), overall survival (OS), and time to progression (TTP) using Cox regression analysis and Inverse Probability of Treatment Weighting (IPTW) to address confounding.

Among 523 patients, 341 (65.2%) did not have diabetes and 182 (34.8%) had T2DM. In the overall population, metformin showed no significant benefit for PFS (HR = 1.15, 95% CI [0.88–1.50], p = 0.316) or OS (HR = 1.28, 95% CI [0.94–1.74], p = 0.124). In the subgroup with T2DM (N = 180), metformin showed no significant benefit for PFS (HR = 1.41, 95% CI [0.97–2.05], p = 0.069), OS (HR = 1.23, 95% CI [0.81–1.86], p = 0.333), or TTP (HR = 0.82, 95% CI [0.53–1.26], p = 0.363). IPTW analysis confirmed these negative findings.

This study found no evidence of improved outcomes with metformin use in patients with HCC in particular with T2DM receiving A+B therapy. Routine metformin use should not be expected to enhance A+B efficacy based on current evidence.

## Linked entities

- **Chemicals:** metformin (PubChem CID 4091)
- **Diseases:** hepatocellular carcinoma (MONDO:0007256), type 2 diabetes mellitus (MONDO:0005148)

## Full-text entities

- **Genes:** INS (insulin) [NCBI Gene 3630] {aka IDDM, IDDM1, IDDM2, ILPR, IRDN, MODY10}, PRKAA1 (protein kinase AMP-activated catalytic subunit alpha 1) [NCBI Gene 5562] {aka AMPK, AMPK alpha 1, AMPKa1}, CD274 (CD274 molecule) [NCBI Gene 29126] {aka ADMIO5, B7-H, B7H1, PD-L1, PDCD1L1, PDCD1LG1}, GLP1R (glucagon like peptide 1 receptor) [NCBI Gene 2740] {aka GLP-1, GLP-1-R, GLP-1R}, VEGFA (vascular endothelial growth factor A) [NCBI Gene 7422] {aka L-VEGF, MVCD1, VEGF, VPF}, CTLA4 (cytotoxic T-lymphocyte associated protein 4) [NCBI Gene 1493] {aka ALPS5, CD, CD152, CELIAC3, CTLA-4, GRD4}, MTOR (mechanistic target of rapamycin kinase) [NCBI Gene 2475] {aka FRAP, FRAP1, FRAP2, RAFT1, RAPT1, SKS}, CD8A (CD8 subunit alpha) [NCBI Gene 925] {aka CD8, CD8alpha, IMD116, Leu2, p32}, PDCD1 (programmed cell death 1) [NCBI Gene 5133] {aka ADMIO4, AIMTBS, CD279, PD-1, PD1, SLEB2}, AFP (alpha fetoprotein) [NCBI Gene 174] {aka AFPD, FETA, HPAFP}
- **Diseases:** tumorigenic (MESH:D002471), BCLC (MESH:D006528), liver dysfunction (MESH:D017093), ALD (MESH:D000326), metabolic complications (MESH:D020739), non-small-cell lung cancer (MESH:D002289), Metabolic dysfunction-associated steatotic liver disease (MESH:D008107), Toxicity (MESH:D064420), OS (MESH:D011475), hepatic steatosis (MESH:D005234), Diabetes (MESH:D003920), insulin resistance (MESH:D007333), Metabolic dysfunction (MESH:D008659), melanoma (MESH:D008545), hepatitis (MESH:D056486), MetALD (MESH:D008108), portal vein thrombosis (MESH:D012170), par-ticipation (MESH:D015868), viral (MESH:D014777), TTP (MESH:D000377), cancer (MESH:D009369), obese (MESH:D009765), T2DM (MESH:D003924), lung cancer (MESH:D008175), death (MESH:D003643), hypoxia (MESH:D000860), -Stage Liver Disease (MESH:D058625)
- **Chemicals:** Metformin (MESH:D008687), durvalumab (MESH:C000613593), alcohol (MESH:D000438), lipid (MESH:D008055), glucose (MESH:D005947), nivolumab (MESH:D000077594), Triglycerides (MESH:D014280), ipilimumab (MESH:D000074324), cholesterol (MESH:D002784), HgbA1c (-), biguanide (MESH:D001645), blood glucose (MESH:D001786), Bevacizumab (MESH:D000068258), Atezolizumab (MESH:C000594389), tremelimumab (MESH:C520704)
- **Species:** Hepatitis B virus (no rank) [taxon 10407], hepatitis C virus [taxon 11103], Homo sapiens (human, species) [taxon 9606]

## Full text

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## Figures

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## References

33 references — full list in the complete paper: https://tomesphere.com/paper/PMC13040334/full.md

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Source: https://tomesphere.com/paper/PMC13040334