# Neoadjuvant immunochemotherapy plus thymalfasin in locally advanced gastric cancer: a prospective clinical trial

**Authors:** Hao Xu, Fengyuan Li, Bowen Li, Dinghua Yang, Tianyu Liu, Yiwen Xia, Hongjin Hua, Qiong Li, Jian Wang, Hongda Liu, Zekuan Xu

PMC · DOI: 10.1186/s12916-026-04740-z · 2026-02-26

## TL;DR

This clinical trial tested a new treatment combining immunotherapy, chemotherapy, and thymalfasin for advanced stomach cancer, showing promising results in tumor response and safety.

## Contribution

The study introduces thymalfasin as a potential enhancer of immunochemotherapy in gastric cancer, with novel immune and transcriptomic insights.

## Key findings

- 30% of patients achieved a pathological complete response, and 56.7% had a major pathological response.
- Thymalfasin was associated with immune cell changes and gene activity linked to improved antitumor immunity.
- The treatment showed substantial nodal clearance and an acceptable safety profile.

## Abstract

Neoadjuvant immunochemotherapy has emerged as a promising strategy for locally advanced gastric and gastroesophageal junction (G/EGJ) adenocarcinoma, but a substantial proportion of patients derive limited benefit. Thymalfasin is an immunomodulatory peptide that may amplify antitumor immunity while attenuating toxicity. We conducted a phase II trial to evaluate anti-PD-1 plus SOX (S-1 and oxaliplatin) immunochemotherapy combined with thymalfasin as neoadjuvant treatment for G/EGJ adenocarcinoma.

The prospective trial enrolled patients aged 18–75 with cStage III G/EGJ adenocarcinoma, ECOG 0–1, and adequate organ function. Treatment included three 21-day cycles of serplulimab (anti-PD-1) plus SOX (S-1 and oxaliplatin) and 9 weeks of thymalfasin, followed by curative gastrectomy. The primary endpoint was pathological complete response (pCR). Secondary endpoints included major pathological response (MPR), safety, survival, and other efficacy measures. Peripheral immune remodeling was assessed by flow cytometry, and bulk RNA sequencing of peripheral blood mononuclear cells (PBMCs) interrogated thymalfasin-associated transcriptional programs.

Thirty patients were enrolled and all underwent curative-intent minimally invasive gastrectomy. pCR was achieved in 30.0% (9/30), and MPR in 56.7% (17/30). ypN0 status was observed in 63.3% (19/30), with N-stage downstaging in 80.0% (24/30). At a median follow-up of 14.0 months (range 10.0–17.2), only one retroperitoneal nodal relapse had occurred at 14.4 months after diagnosis; no deaths were documented. Any-grade adverse events (AEs) occurred in 93.3% of patients, grade ≥ 3 AEs in 26.7%, and immune-related AEs in 23.3%. Flow cytometry showed expansion of CD8⁺ T cells with increased CD69 expression and a concurrent reduction in HLA-DR-positive T cells, suggesting dynamic remodeling from broad systemic activation toward a more focused effector or memory response. RNA-seq revealed thymalfasin-associated upregulation of genes involved in antigen processing and presentation, type I interferon signaling, and identified immune co-expression modules linked to treatment and response.

Neoadjuvant serplulimab, SOX, and thymalfasin produced encouraging pathological response, substantial nodal clearance, and an acceptable safety profile in stage III G/EGJ adenocarcinoma. Peripheral immune and transcriptomic profiling are consistent with a hypothesis in which thymalfasin may help preserve and coordinate systemic antitumor immunity without excessive toxicity. These findings warrant further larger randomized trials.

ClinicalTrials.gov, NCT06461910, 2024–06-14.

The online version contains supplementary material available at 10.1186/s12916-026-04740-z.

## Linked entities

- **Chemicals:** thymalfasin (PubChem CID 16130571), S-1 (PubChem CID 1497102), oxaliplatin (PubChem CID 9887053)
- **Diseases:** gastric cancer (MONDO:0001056), gastroesophageal junction adenocarcinoma (MONDO:0003219)

## Full-text entities

- **Genes:** ISG20 (interferon stimulated exonuclease gene 20) [NCBI Gene 3669] {aka CD25, HEM45}, CD4 (CD4 molecule) [NCBI Gene 920] {aka CD4mut, IMD79, Leu-3, OKT4D, T4}, CD19 (CD19 molecule) [NCBI Gene 930] {aka B4, CVID3}, ERBB2 (erb-b2 receptor tyrosine kinase 2) [NCBI Gene 2064] {aka CD340, HER-2, HER-2/neu, HER2, MLN 19, MLN-19}, TRG (T cell receptor gamma locus) [NCBI Gene 6965] {aka TCRG, TRG@}, CD274 (CD274 molecule) [NCBI Gene 29126] {aka ADMIO5, B7-H, B7H1, PD-L1, PDCD1L1, PDCD1LG1}, 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}, NCAM1 (neural cell adhesion molecule 1) [NCBI Gene 4684] {aka CD56, MSK39, NCAM}, PGR (progesterone receptor) [NCBI Gene 5241] {aka NR3C3, PR}, CD69 (CD69 molecule) [NCBI Gene 969] {aka AIM, BL-AC/P26, CLEC2C, EA1, GP32/28, MLR-3}, ME1 (malic enzyme 1) [NCBI Gene 4199] {aka HUMNDME, MES}, PTPRC (protein tyrosine phosphatase receptor type C) [NCBI Gene 5788] {aka B220, CD45, CD45R, GP180, IMD105, L-CA}
- **Diseases:** damage (MESH:D020263), pleural effusion (MESH:D010996), autoimmune diseases (MESH:D001327), lymph node metastasis (MESH:D008207), Gastric and gastroesophageal junction (G/EGJ) adenocarcinomas (MESH:D013274), diarrhea (MESH:D003967), infections (MESH:D007239), irAEs (MESH:D002318), EGJ adenocarcinoma (MESH:D000230), Stable disease (MESH:D060050), Cancer (MESH:D009369), gastrointestinal fistula (MESH:D005767), thrombocytopenia (MESH:D013921), G (MESH:D004314), cytotoxic (MESH:D064420), dMMR (MESH:C536928), nodal (MESH:D013611), ulcerated lesion (MESH:D014456), anorexia (MESH:D000855), decreased (MESH:D009123), gastrointestinal symptoms (MESH:D012817), anemia (MESH:D000740), pulmonary infection (MESH:D012141), metastases (MESH:D009362), fibrosis (MESH:D005355), deaths (MESH:D003643), cStage III (MESH:C537189), H. pylori infection (MESH:D016481), blood (MESH:D006402)
- **Chemicals:** nivolumab (MESH:D000077594), apatinib (MESH:C553458), oxaliplatin (MESH:D000077150), docetaxel (MESH:D000077143), CapeOx (MESH:C519688), sintilimab (MESH:C000632826), camrelizumab (MESH:C000631724), capecitabine (MESH:D000069287), pembrolizumab (MESH:C582435), DCR (-)
- **Species:** Homo sapiens (human, species) [taxon 9606]

## Figures

5 figures with captions in the complete paper: https://tomesphere.com/paper/PMC12964648/full.md

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Source: https://tomesphere.com/paper/PMC12964648