# Reproducible safety and efficacy of durvalumab with or without tremelimumab for hepatocellular carcinoma in clinical practice: Results of the DT-real study

**Authors:** Ciro Celsa, Tiziana Pressiani, Naoshi Nishida, Shadi Mohamad Chamseddine, Ashwini Arvind, Michael Li, Marta Fortuny, Najib Ben Khaled, Massimo Iavarone, Hidenori Toyoda, Ilario Giovanni Rapposelli, Andrea Casadei-Gardini, Caterina Vivaldi, Susanna Ulahannan, Haripriya Andanamala, Bernhard Scheiner, Matthias Pinter, Elena Orlandi, Claudia A.M. Fulgenzi, Giulia F. Manfredi, Pasquale Lombardi, Antonio D’Alessio, Bernardo Stefanini, Rosanna Villani, Francesca Romana Ponziani, Leonardo Stella, Ornella Carminati, Angela Dalia Ricci, Melina Gonzalez, Alba Sparacino, Gabriele Di Maria, Marco Vaccaro, Giuseppe Cabibbo, Calogero Cammà, Maria Reig, Robin K. Kelley, Amit G. Singal, Ahmed O. Kaseb, Masatoshi Kudo, Lorenza Rimassa, David James Pinato

PMC · DOI: 10.1016/j.jhepr.2025.101685 · JHEP Reports · 2025-11-20

## TL;DR

This study confirms that STRIDE (durvalumab plus tremelimumab) is effective and safe for treating advanced liver cancer in real-world settings, especially for patients who meet key trial criteria.

## Contribution

The study validates the reproducibility of STRIDE's efficacy and safety in routine clinical practice beyond the controlled trial setting.

## Key findings

- HIMALAYA-eligible patients had significantly longer survival (23 months) compared to ineligible patients (12 months).
- Macrovascular invasion and hepatic decompensation were identified as negative prognostic factors.
- Nearly half of patients received STRIDE despite not meeting trial eligibility criteria, highlighting its clinical need.

## Abstract

Durvalumab plus tremelimumab (STRIDE) has emerged as a first-line systemic treatment option for unresectable hepatocellular carcinoma (HCC). This international multicentre study aimed to evaluate the efficacy and tolerability of STRIDE or durvalumab monotherapy in routine clinical practice, comparing outcomes between patients within and outside key eligibility criteria for the HIMALAYA trial.

From a database of 1,423 patients with advanced/unresectable HCC treated with immunotherapy across 35 centres, we analysed 233 patients receiving STRIDE or durvalumab monotherapy. Patients were categorized as HIMALAYA-IN or HIMALAYA-OUT based on key trial eligibility criteria (no prior systemic therapy, ECOG-PS 0–1, Child-Pugh class A, no Vp4 thrombosis). Baseline characteristics were assessed for overall survival (OS) and hepatic decompensation using a multivariable Cox model and competing-risk analysis, respectively. Objective response rates and treatment-related adverse events were recorded.

Of the 233 patients, 123 (53%) were HIMALAYA-IN and 110 (47%) were HIMALAYA-OUT. STRIDE was given in 95% of HIMALAYA-IN patients. After median follow-up of 6.0 months, median OS was 20.4 months (95% CI 11.7-NR) in the overall population. HIMALAYA-IN patients achieved significantly longer OS than HIMALAYA-OUT patients (23.0 vs. 12.2 months; hazard ratio 0.61; 95% CI 0.39-0.96; p = 0.03). Macrovascular invasion and hepatic decompensation were independent negative prognostic factors in the whole cohort. Hepatic decompensation occurred in 10.5% of patients within 12 months from treatment start. Objective response rate was 23.7% and 17.8% of HIMALAYA-IN and -OUT patients, respectively. Patients achieving disease control (whole cohort: 59.4%) demonstrated 24-month OS of 58.2% in HIMALAYA-IN and 44.8% in HIMALAYA-OUT groups. Grade 3-4 treatment-related adverse events occurred in 16.3% of patients.

STRIDE shows reproducible effectiveness and an acceptable safety profile in real-world practice. Achieving disease control and maintaining liver function emerged as key determinants of long-term survival benefit.

The DT-real study validates the efficacy and safety of STRIDE (durvalumab plus tremelimumab) in routine clinical practice, with HIMALAYA trial-eligible patients achieving 23-month median survival, and showing a safety profile comparable to that observed in the pivotal trial. Nearly half of real-world patients received treatment despite not meeting original trial criteria, reflecting urgent clinical need in this population with limited therapeutic options. As for other immunotherapy-based combinations, hepatic decompensation is a critical determinant of survival. Patients achieving disease control demonstrated substantially improved 24-month overall survival rates compared to those with progressive disease, confirming the findings of the exploratory analyses of the HIMALAYA trial.

Image 1

•STRIDE shows reproducible efficacy in real-world practice for patients with HCC.•HIMALAYA-eligible patients achieved 23-month survival compared with 12-month survival in ineligible patients.•Nearly half of patients received treatment despite not meeting trial eligibility criteria.•Macrovascular invasion and hepatic decompensation predict worse outcomes.

STRIDE shows reproducible efficacy in real-world practice for patients with HCC.

HIMALAYA-eligible patients achieved 23-month survival compared with 12-month survival in ineligible patients.

Nearly half of patients received treatment despite not meeting trial eligibility criteria.

Macrovascular invasion and hepatic decompensation predict worse outcomes.

## Linked entities

- **Diseases:** hepatocellular carcinoma (MONDO:0007256)

## Full-text entities

- **Diseases:** Hepatic decompensation (MESH:D006333), thrombosis (MESH:D013927), HCC (MESH:D006528)
- **Chemicals:** tremelimumab (MESH:C520704), Durvalumab (MESH:C000613593), STRIDE (-)
- **Species:** 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/PMC12886069/full.md

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Source: https://tomesphere.com/paper/PMC12886069