What question did this study set out to answer?

The aim is to understand how targeting TGF-beta signaling affects tumor progression in small cell lung cancer.

April 19, 2026

Abstract LB426: Blockade of tumor-intrinsic TGF-beta signaling drives hyperprogression in small cell lung cancer

Key Points

The aim is to understand how targeting TGF-beta signaling affects tumor progression in small cell lung cancer.
Evaluated bintrafusp alfa, a fusion protein targeting PD-L1 and TGF-beta in a clinical trial.
Included 37 patients with small cell lung cancer, 34 of whom were evaluable for response.
Analyzed blood samples and tumor biopsies before treatment.
18% of patients achieved partial responses, 20% had stable disease, and 62% experienced disease progression.
38% of patients with progression met criteria for hyperprogressive disease.
Hyperprogression linked to immune suppression and tumor-intrinsic TGF-beta activation.

Abstract

Abstract Therapeutic strategies targeting TGF-beta signaling are increasingly combined with immune checkpoint blockade to overcome stromal immunosuppression, yet the tumor-intrinsic consequences of this approach remain poorly defined. We evaluated bintrafusp alfa, a bifunctional fusion protein targeting PD-L1 and TGF-beta, in a clinical trial of patients with small cell lung cancer (SCLC). Among 37 treated patients, 34 were evaluable for response: six (18 percent) achieved partial responses, seven (20 percent) had stable disease, and 21 (62 percent) experienced progressive disease. Notably, 13 of 21 patients with progression (38 percent) met criteria for hyperprogressive disease. Integrated analyses of peripheral blood, circulating tumor DNA, and pretreatment tumor biopsies revealed that clinical responses were associated with an inflamed tumor microenvironment, whereas hyperprogression was characterized by systemic immune suppression, impaired cytotoxic immune function, and unexpectedly, tumor-intrinsic activation of TGF-beta signaling and stem-like transcriptional programs. Functional studies demonstrated that intact TGF-beta receptor 2 signaling constrains tumor proliferation, indicating a context-dependent tumor-suppressive role for TGF-beta in SCLC. These findings highlight a previously underappreciated risk of tumor acceleration with TGF-beta-targeted immunotherapies and support the need for biomarker-driven patient selection as TGF-beta-directed agents continue to advance in oncology. Citation Format: Anish Thomas, Brett Schroeder, Chirayu Mohindroo, Anna-Lena Meinhardt, Nobuyuki Takahashi, Rajesh Kumar, Yang Zhang, Ajit Kumar Sharma. Blockade of tumor-intrinsic TGF-beta signaling drives hyperprogression in small cell lung cancer abstract. In: Proceedings of the American Association for Cancer Research Annual Meeting 2026; Part 2 (Late-Breaking, Clinical Trial, and Invited Abstracts) ; 2026 Apr 17-22; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2026;86 (8Suppl): Abstract nr LB426.

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Abstract LB426: Blockade of tumor-intrinsic TGF-beta signaling drives hyperprogression in small cell lung cancer

Key Points

Abstract

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