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Recurrent mTORC1-activating RRAGC mutations in follicular lymphoma.

Jessica OkosunRachel L WolfsonJun WangShamzah ArafLucy WilkinsBrian M CastellanoLeire Escudero-IbarzAhad Fahad Al SeraihiJulia RichterStephan H BernhartAlejo EfeyanSameena IqbalJanet MatthewsAndrew ClearJosé Afonso Guerra-AssunçãoCsaba BödörHilmar QuentmeierChristopher MansbridgePeter JohnsonAndrew DaviesJonathan C StreffordGraham PackhamSharon BarransAndrew JackMing-Qing DuMaria CalaminiciT Andrew ListerRebecca AuerSilvia MontotoJohn G GribbenReiner SiebertClaude ChelalaRoberto ZoncuDavid M SabatiniJude Fitzgibbon
Published in: Nature genetics (2015)
Follicular lymphoma is an incurable B cell malignancy characterized by the t(14;18) translocation and mutations affecting the epigenome. Although frequent gene mutations in key signaling pathways, including JAK-STAT, NOTCH and NF-κB, have also been defined, the spectrum of these mutations typically overlaps with that in the closely related diffuse large B cell lymphoma (DLBCL). Using a combination of discovery exome and extended targeted sequencing, we identified recurrent somatic mutations in RRAGC uniquely enriched in patients with follicular lymphoma (17%). More than half of the mutations preferentially co-occurred with mutations in ATP6V1B2 and ATP6AP1, which encode components of the vacuolar H(+)-ATP ATPase (V-ATPase) known to be necessary for amino acid-induced activation of mTORC1. The RagC variants increased raptor binding while rendering mTORC1 signaling resistant to amino acid deprivation. The activating nature of the RRAGC mutations, their existence in the dominant clone and their stability during disease progression support their potential as an excellent candidate for therapeutic targeting.
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