2017
DOI: 10.1016/j.jid.2016.12.012
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Do the Side Effects of BRAF Inhibitors Mimic RASopathies?

Abstract: Recent advances in targeted anticancer therapies have substantially improved the prognosis of several cancers. Such targeted therapies are not, however, free of side effects, and these side effects are clearly distinct from those induced by classical cytotoxic chemotherapies. This is likely so because targeted therapies are designed to interfere with specific oncogenic signaling pathways rather than to inhibit cell proliferation in general. In fact, interference with specific signaling pathways may lead to eff… Show more

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Cited by 8 publications
(4 citation statements)
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“…Consistent with this mechanism, there is evidence for paradoxical hyperactivation of the MAPK pathway in cells with wild-type BRAF but mutated RAS through allosteric and catalytic mechanisms that relieve the auto-inhibition of wild-type RAF kinase ( Hatzivassiliou et al, 2010 ; Heidorn et al, 2010 ; Poulikakos et al, 2010 ). Indeed, many of these BRAFi features overlap with the cutaneous manifestations of RASopathies – genetic diseases such as cardiofaciocutaneous and Costello syndromes characterized by activating germ line mutations in RAS ( Rinderknecht et al, 2013 ; Sfecci et al, 2017 ). Also consistent with this, 18–60% of BRAFi-cSCC have somatic mutations in HRAS or KRAS, which is significantly higher than in sporadic cSCC ( Oberholzer et al, 2012 ; Su et al, 2012 ; South et al, 2014 ).…”
Section: Introductionmentioning
confidence: 99%
“…Consistent with this mechanism, there is evidence for paradoxical hyperactivation of the MAPK pathway in cells with wild-type BRAF but mutated RAS through allosteric and catalytic mechanisms that relieve the auto-inhibition of wild-type RAF kinase ( Hatzivassiliou et al, 2010 ; Heidorn et al, 2010 ; Poulikakos et al, 2010 ). Indeed, many of these BRAFi features overlap with the cutaneous manifestations of RASopathies – genetic diseases such as cardiofaciocutaneous and Costello syndromes characterized by activating germ line mutations in RAS ( Rinderknecht et al, 2013 ; Sfecci et al, 2017 ). Also consistent with this, 18–60% of BRAFi-cSCC have somatic mutations in HRAS or KRAS, which is significantly higher than in sporadic cSCC ( Oberholzer et al, 2012 ; Su et al, 2012 ; South et al, 2014 ).…”
Section: Introductionmentioning
confidence: 99%
“…This could be explained either by a synergistic effect of the combination therapy or by an inhibition of the paradoxical activation of MAPK pathway observed under BRAF inhibitors alone (Holderfield, Nagel, & Stuart, ). In fact a paradoxical activation of MAPK pathway has been described with single inhibition of BRAF in the BRAF ‐wild‐type nonmelanoma cells, explaining most of side effects of the monotherapy such as cutaneous squamous‐cell carcinomas under BRAF inhibitors (Lacouture, O'Reilly, Rosen, & Solit, ; Su et al, ) or skin effects of single inhibition mimicking RASopathies (Sfecci et al, ). However, this paradoxical activation could prevent the dilutional hyponatremia observed under BRAF inhibitors alone.…”
Section: Pathophysiological Aspectsmentioning
confidence: 99%
“…RASopathies (Sfecci et al, 2017). However, this paradoxical activation could prevent the dilutional hyponatremia observed under BRAF inhibitors alone.…”
Section: Pathophys Iolog Ic Al a S Pec Tsmentioning
confidence: 99%
“…Cutaneous adverse event profiles of BRAF and MEK inhibitors are very distinct, and unlike many other combinations some specific cutaneous adverse events occur less frequently when BRAF and MEK inhibitors are used concomitantly. A paradoxical activation of the MAPK pathway induced by BRAF inhibitors in BRAF wild‐type cells is thought to be counteracted by MEK inhibitors that block a kinase downstream of RAF and vice versa.…”
mentioning
confidence: 99%