Thrombomodulin facilitates melanoma progression via FAK- and ezrin-mediated phenotypic plasticity

Key Points

Tumor progression is facilitated by thrombomodulin, enhancing melanoma cell plasticity through specific pathways.
Key findings indicate that targeting thrombomodulin could potentially suppress melanoma growth effectively.
Analysis focused on FAK and ezrin-mediated mechanisms within melanoma cells, establishing their role in tumor dynamics.
Highlights the need for further exploration into therapeutics that can disrupt cancer cell plasticity effectively.

Abstract

TM promotes melanoma cell plasticity and VM through FAK- and ezrin-dependent pathways. These findings position TM as a key regulator of tumor progression and suggest that targeting TM may offer a novel therapeutic strategy to disrupt cancer cell plasticity and suppress melanoma growth.

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Thrombomodulin facilitates melanoma progression via FAK- and ezrin-mediated phenotypic plasticity

Key Points

Abstract

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