In the evolving landscape of cancer therapeutics, a recent retrospective study from Beijing You’an Hospital provides an insightful comparison of immune checkpoint inhibitors (ICIs) combined with antiangiogenic agents (AAs) in treating unresectable hepatocellular carcinoma (uHCC) among patients with varying degrees of liver cirrhosis. Recognized as a pivotal treatment approach, ICIs plus AAs have reshaped the first-line systemic therapy for uHCC, yet their efficacy and safety in patients with compromised liver function, particularly Child-Pugh B (CP B) cirrhosis, remain underexplored.
Clinical trials investigating systemic therapies for uHCC have traditionally excluded patients with CP B cirrhosis, reflecting concerns regarding safety and diminished liver reserve. This study addresses this crucial gap by performing a single-center, retrospective analysis of 94 uHCC patients treated with ICIs plus AAs between 2020 and 2024. Among them, 63 had Child-Pugh A (CP A) cirrhosis, while 31 presented with CP B cirrhosis, allowing for a comparative evaluation of treatment outcomes and tolerability.
The study’s findings reveal an encouraging overall objective response rate (ORR) of 44.7% across the whole cohort, with a disease control rate (DCR) of 72.3%. These clinical endpoints offer a promising perspective on the tumor response to combination therapy in a population with traditionally poor prognoses. Median progression-free survival (mPFS) was reported at 6.3 months, and notably, the median overall survival (mOS) reached 28.3 months, underscoring sustained benefits in systemic therapy for uHCC patients.
When stratified by liver function status, patients with CP A cirrhosis exhibited higher ORR (50.8%) compared to those with CP B cirrhosis (32.3%), though this difference approached but did not reach statistical significance (P = 0.089). Similarly, DCR and mPFS were numerically superior in the CP A group but lacked statistical significance. Intriguingly, mOS demonstrated a marked and statistically significant disparity, favoring the CP A group (39.2 months) over CP B patients (15.9 months, P = 0.035). This dichotomy highlights the profound impact of hepatic functional reserve on long-term survival despite comparable response rates to therapy.
Several prognostic factors independent of cirrhosis status emerged from the analysis. Poor performance status, denoted by an Eastern Cooperative Oncology Group (ECOG) score of 2, prior treatments, and absence of concurrent locoregional therapies were associated with diminished objective responses. Additionally, CP B cirrhosis and advanced Barcelona Clinic Liver Cancer (BCLC) stages C or D independently predicted worse overall survival, underscoring the nuanced interactions between tumor burden, liver function, and systemic therapy efficacy.
The safety profile of ICIs combined with AAs was carefully assessed, revealing that an overwhelming majority (93.6%) of patients experienced at least one treatment-related adverse event (TRAE), with 27.7% encountering grade 3 or higher toxicities. Crucially, the incidence and severity of TRAEs did not differ significantly between CP A and CP B subgroups, suggesting that the addition of ICIs and AAs does not disproportionately increase treatment-related risks even in patients with moderately impaired liver function.
Remarkably, 32.3% of patients with CP B cirrhosis demonstrated improvement in their Child-Pugh score following systemic therapy, indicating a potential for therapeutic intervention to not only control tumor progression but also enhance hepatic functional reserve. This finding challenges conventional therapeutic nihilism associated with CP B patients and advocates for a more inclusive approach in clinical practice.
Understanding the mechanistic underpinnings of ICIs combined with AAs in uHCC is essential. Immune checkpoint inhibitors function by unleashing the immune system’s cytotoxic T cells against tumor cells, a mechanism often suppressed in the tumor microenvironment. Antiangiogenic agents complement this by inhibiting vascular endothelial growth factor (VEGF) pathways, effectively starving the tumor of its blood supply and promoting an immunologically active milieu. Their synergy is thought to enhance antitumor immunity and counteract resistance pathways frequently encountered in hepatocellular carcinoma.
The study’s retrospective design, although inherently limited by potential selection biases and confounding variables, offers valuable real-world insights. Incorporating patients with CP B cirrhosis, typically excluded from randomized trials, enhances the generalizability of findings and contributes toward personalized treatment paradigms. However, larger, prospective studies are essential to validate these observations and elucidate optimal treatment sequencing and combination strategies.
Previous research on systemic therapies in uHCC mainly focused on patients with preserved liver function, limiting evidence for CP B populations. This study significantly advances the field by demonstrating that systemic immunotherapy combined with antiangiogenic treatment can be both efficacious and tolerable in these patients, opening new therapeutic avenues. The observed survival benefit and Child-Pugh score improvements further emphasize the need to reconsider exclusion criteria in future clinical trials.
Translating these findings into clinical practice necessitates careful patient selection and monitoring. While ICIs plus AAs show robust efficacy, attention to adverse events remains paramount, particularly in patients with compromised liver function. The comparable safety profiles between Child-Pugh groups provide reassurance but warrant vigilant management to optimize outcomes.
The integration of locoregional therapies alongside systemic treatments appeared to improve objective response rates, underscoring the potential benefit of multimodal approaches in managing uHCC. Combining transarterial chemoembolization, radiofrequency ablation, or other localized interventions with ICIs and AAs may potentiate antitumor effects and prolong survival, as suggested by the independent predictive value of simultaneous locoregional therapy.
Moreover, patient performance status remained a critical determinant of treatment success, emphasizing the importance of pre-treatment evaluation and supportive care to maintain functional capacity. Incorporating comprehensive assessments and potential interventions to improve performance status might broaden eligibility and enhance clinical benefit.
This study’s implications extend beyond clinical outcomes, prompting a paradigm shift in conceptualizing systemic therapy candidacy for uHCC patients with advanced liver disease. By demonstrating safety and efficacy in CP B patients, it challenges existing treatment algorithms and supports a more nuanced, inclusive therapeutic approach balancing risk and benefit.
In conclusion, the retrospective analysis conducted at Beijing You’an Hospital highlights the promise of combining immune checkpoint inhibitors with antiangiogenic agents in the management of unresectable hepatocellular carcinoma among patients with varied liver function statuses. While significant survival differences remain linked to hepatic reserve, the overall favorable safety profile and some improvements in liver function underscore the potential to expand treatment access and improve outcomes for historically underserved patient groups in oncology.
Further well-structured prospective trials with larger cohorts and longer follow-up are imperative to refine patient stratification, optimize dosing regimens, and elucidate combinatory strategies involving ICIs, AAs, and locoregional therapies. Such investigations will be foundational to establishing new standards of care in hepatocellular carcinoma treatment, ultimately aiming to enhance survival and quality of life for patients within this challenging clinical context.
Subject of Research: Evaluation of the efficacy and safety of immune checkpoint inhibitors combined with antiangiogenic agents in unresectable hepatocellular carcinoma patients with Child-Pugh A versus B cirrhosis.
Article Title: Comparative efficacy and safety of immune checkpoint inhibitors combined with antiangiogenic agents for unresectable hepatocellular carcinoma in patients with Child-Pugh A versus B cirrhosis: a single-center, retrospective study.
Article References:
Liu, D., Yang, Z., Wang, L. et al. Comparative efficacy and safety of immune checkpoint inhibitors combined with antiangiogenic agents for unresectable hepatocellular carcinoma in patients with Child-Pugh A versus B cirrhosis: a single-center, retrospective study. BMC Cancer 25, 1651 (2025). https://doi.org/10.1186/s12885-025-15126-4
Image Credits: Scienmag.com
DOI: https://doi.org/10.1186/s12885-025-15126-4
