What is the clinical evidence from this study?

Study design: Other. Population: Viral myocarditis. Intervention: Gelated cells with high-affinity CAR mutant (GC-PMs) vs. Control. Primary outcome: Viral load and myocardial injury.

What question did this study set out to answer?

To develop a novel biomimetic antiviral strategy targeting coxsackievirus B3 via receptor engineering.

May 19, 2026Open Access

Combining receptor engineering and intracellular gelation for cell-based antiviral therapy against coxsackievirus B3

Key Result

Gelated cells engineered with a high-affinity Coxsackievirus and adenovirus receptor mutant effectively lowered viral load and mitigated myocardial injury in a murine model of viral myocarditis.

Key Points

To develop a novel biomimetic antiviral strategy targeting coxsackievirus B3 via receptor engineering.
Generated Mut-1_CAR receptor to enhance cardiomyocyte binding to CVB3.
Used photochemical crosslinking for intracellular gelation, creating gelated cells (PMs).
Evaluated PMs for viral load reduction and myocardial injury mitigation in murine model.
PMs reduced CVB3 plaque formation significantly in vitro.
In vivo, PMs lowered viral load and improved myocardial health, demonstrating excellent safety and biocompatibility.

Structured PICO

Does treatment with engineered gelated cells expressing a high-affinity receptor mutant reduce viral load and mitigate myocardial injury in a murine model of viral myocarditis?

Population

In vitro host cardiomyocytes and a murine model of viral myocarditis caused by coxsackievirus B3 (CVB3)

Intervention

Engineered gelated cells (PMs) expressing a high-affinity Coxsackievirus and adenovirus receptor mutant (Mut-1_CAR)

Outcome

Reduction of viral load and mitigation of myocardial injurysurrogate

A novel biomimetic antiviral strategy using engineered gelated cells effectively neutralizes coxsackievirus B3 and reduces myocardial injury in a preclinical model, offering a potential new therapeutic approach for viral myocarditis.

Abstract

Viral myocarditis (VMC), caused by pathogens such as coxsackievirus B3 (CVB3), leads to severe cardiac injury and currently lacks specific therapeutic options. Here, we report a biomimetic antiviral strategy based on receptor engineering and intracellular gelation. By combining genetic and protein engineering, we generated a high-affinity Coxsackievirus and adenovirus receptor mutant (Mut-1CAR) that markedly enhances the binding of host cardiomyocytes to CVB3. Using photochemical crosslinking, these engineered cells were converted into structurally stable, function-retaining gelated cells (PMs). PMs efficiently adsorb and neutralize virus particles, significantly reducing CVB3 plaque formation in vitro. In a murine model of viral myocarditis, PMs demonstrated excellent in vivo safety and biocompatibility while effectively lowering viral load and mitigating myocardial injury. This study establishes a “receptor enhancement + function fixation” approach for non-immune-dependent viral neutralization, providing a conceptual and technical foundation for the development of novel cell-based biomimetic antiviral therapies.

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