P38 Mediates Tumor Suppression through Reduced Autophagy and Actin Cytoskeleton Changes in NRAS-Mutant Melanoma

P38 Mediates Tumor Suppression through Reduced Autophagy and Actin Cytoskeleton Changes in NRAS-Mutant Melanoma

Hotspot mutations in the NRAS gene are causative genetic events associated with the development of melanoma. Currently, there are no FDA-approved drugs directly targeting NRAS mutations. Previously, we showed that p38 acts as a tumor suppressor in vitro and in vivo with respect to NRAS-mutant melano...

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Veröffentlicht in:Cancers 2023-02, Vol.15 (3), p.877
Hauptverfasser: Banik, Ishani, Ghosh, Adhideb, Beebe, Erin, Burja, Blaž, Frank Bertoncelj, Mojca, Dooley, Christopher M, Markkanen, Enni, Dummer, Reinhard, Busch-Nentwich, Elisabeth M, Levesque, Mitchell P
Format: Artikel
Sprache:eng
Schlagworte:
Actin
Anisomycin
Apoptosis
Autophagy
Cancer
Cancer therapies
Care and treatment
Cell adhesion & migration
Chloroquine
Collagen
Cytoskeleton
Drug approval
Drug delivery
Drug development
Extracellular matrix
Hydroxychloroquine
Invasiveness
Investigations
Kinases
Localization
MAP kinase
MEK inhibitors
Melanoma
Motility
Mutants
Mutation
Mutation hot spots
Phosphorylation
Physiology
Polymerization
Protein biosynthesis
Proteins
Rapamycin
TOR protein
Transcription factors
Tumor suppressor genes
Tumorigenesis
Tumors
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Zusammenfassung:Hotspot mutations in the NRAS gene are causative genetic events associated with the development of melanoma. Currently, there are no FDA-approved drugs directly targeting NRAS mutations. Previously, we showed that p38 acts as a tumor suppressor in vitro and in vivo with respect to NRAS-mutant melanoma. We observed that because of p38 activation through treatment with the protein synthesis inhibitor, anisomycin leads to a transient upregulation of several targets of the cAMP pathway, representing a stressed cancer cell state that is often observed by therapeutic doses of MAPK inhibitors in melanoma patients. Meanwhile, genetically induced p38 or its stable transduction leads to a distinct cellular transcriptional state. Contrary to previous work showing an association of invasiveness with high p38 levels in BRAF-mutated melanoma, there was no correlation of p38 expression with NRAS-mutant melanoma invasion, highlighting the difference in BRAF and NRAS-driven melanomas. Although the role of p38 has been reported to be that of both tumor suppressor and oncogene, we show here that p38 specifically plays the role of a tumor suppressor in NRAS-mutant melanoma. Both the transient and stable activation of p38 elicits phosphorylation of mTOR, reported to be a master switch in regulating autophagy. Indeed, we observed a correlation between elevated levels of phosphorylated mTOR and a reduction in LC3 conversion (LCII/LCI), indicative of suppressed autophagy. Furthermore, a reduction in actin intensity in p38-high cells strongly suggests a role of mTOR in regulating actin and a remodeling in the NRAS-mutant melanoma cells. Therefore, p38 plays a tumor suppressive role in NRAS-mutant melanomas at least partially through the mechanism of mTOR upregulation, suppressed autophagy, and reduced actin polymerization. One or more combinations of MEK inhibitors with either anisomycin, rapamycin, chloroquine/bafilomycin, and cytochalasin modulate p38 activation, mTOR phosphorylation, autophagy, and actin polymerization, respectively, and they may provide an alternate route to targeting NRAS-mutant melanoma.
ISSN:2072-6694
2072-6694
DOI:10.3390/cancers15030877