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Cancer-associated mutations in VAV1 trigger variegated signaling outputs and T-cell lymphomagenesis.

The EMBO journal (2021-10-08)
Javier Robles-Valero, Lucía Fernández-Nevado, L Francisco Lorenzo-Martín, Myriam Cuadrado, Isabel Fernández-Pisonero, Sonia Rodríguez-Fdez, Elsa N Astorga-Simón, Antonio Abad, Rubén Caloto, Xosé R Bustelo
ABSTRACT

Mutations in VAV1, a gene that encodes a multifunctional protein important for lymphocytes, are found at different frequencies in peripheral T-cell lymphoma (PTCL), non-small cell lung cancer, and other tumors. However, their pathobiological significance remains unsettled. After cataloguing 51 cancer-associated VAV1 mutations, we show here that they can be classified in five subtypes according to functional impact on the three main VAV1 signaling branches, GEF-dependent activation of RAC1, GEF-independent adaptor-like, and tumor suppressor functions. These mutations target new and previously established regulatory layers of the protein, leading to quantitative and qualitative changes in VAV1 signaling output. We also demonstrate that the most frequent VAV1 mutant subtype drives PTCL formation in mice. This process requires the concurrent engagement of two downstream signaling branches that promote the chronic activation and transformation of follicular helper T cells. Collectively, these data reveal the genetic constraints associated with the lymphomagenic potential of VAV1 mutant subsets, similarities with other PTCL driver genes, and potential therapeutic vulnerabilities.

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Sigma-Aldrich
Sieroalbumina, cold ethanol fraction, pH 5.2, ≥96%
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Sodium orthovanadate, ≥90% (titration)
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Isopropil β-D-1-tiogalattopiranoside, ≥99% (TLC)
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Anti-CD3 Mouse mAb (UCHT1), liquid, >95% (immunoglobulin, SDS-PAGE), clone UCHT1