2019
DOI: 10.1038/s42255-019-0098-8
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Oncogenic Rag GTPase signalling enhances B cell activation and drives follicular lymphoma sensitive to pharmacological inhibition of mTOR

Abstract: The humoral immune response demands that B cells undergo a sudden anabolic shift and high cellular nutrient levels which are required to sustain the subsequent proliferative burst. Follicular lymphoma (FL) originates from B cells that have participated in the humoral response, and 15% of FL samples harbor point, activating mutations in RRAGC, an essential activator of mTORC1 *

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Cited by 48 publications
(70 citation statements)
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References 75 publications
(107 reference statements)
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“…67 Constitutively active RagA renders mTORC1 signaling independent of the presence of amino acids and has been shown to reduce B cell competitiveness in the GC 56 (Figure 2). In contrast, expression of mutant alleles of the gene RagC that drive partial but not complete uncoupling of mTORC1 activity from amino acid dependence has been shown to boost GC expansion 68 (Figure 2). Nutrient and energy levels are also sensed by the LKB1/AMPK pathway, which impinges on mTORC1 activity.…”
Section: Me Taboli C Bal An Ce In Ac Tivated and G Erminal Center Bmentioning
confidence: 99%
“…67 Constitutively active RagA renders mTORC1 signaling independent of the presence of amino acids and has been shown to reduce B cell competitiveness in the GC 56 (Figure 2). In contrast, expression of mutant alleles of the gene RagC that drive partial but not complete uncoupling of mTORC1 activity from amino acid dependence has been shown to boost GC expansion 68 (Figure 2). Nutrient and energy levels are also sensed by the LKB1/AMPK pathway, which impinges on mTORC1 activity.…”
Section: Me Taboli C Bal An Ce In Ac Tivated and G Erminal Center Bmentioning
confidence: 99%
“…The same was observed on a Bcl2-transgenic background using VavP-Bcl2 transgenic mice, 10 which also revealed accelerated FL development in vivo. 9 Transcriptional profiling analysis showed enrichment of the mTORC1 signature in RagC- what has previously been observed for mTORC1 hyperactivation. 11 Specifically, strong mTORC1 activation negatively impacted the generation of high-affinity antibodies against the immunizing antigen, which in a competitive setting led to the disappearance of mTORC1-hyperactive versus wild-type GC B-cells over time.…”
Section: Takedownmentioning
confidence: 55%
“…Experiments performed by Ortega-Molina et al with the mTOR inhibitor rapamycin indicate that such mice, in contrast to mice with Bcl2-translocations only, showed a lower incidence and grade of lymphomas. 9 The observed higher selective sensitivity to mTORC1 inhibition in this mouse model suggests that patients with mutations in the nutrient-signaling pathway may benefit from treatment with mTOR inhibitors.…”
Section: Takedownmentioning
confidence: 85%
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