Biochemical Pharmacology 2015-02-01

Concurrent MEK and autophagy inhibition is required to restore cell death associated danger-signalling in Vemurafenib-resistant melanoma cells.

S Martin, A M Dudek-Perić, H Maes, A D Garg, M Gabrysiak, S Demirsoy, J V Swinnen, P Agostinis

文献索引:Biochem. Pharmacol. 93(3) , 290-304, (2015)

全文:HTML全文

摘要

Vemurafenib (PLX4032), an inhibitor of BRAF(V600E), has demonstrated significant clinical anti-melanoma effects. However, the majority of treated patients develop resistance, due to a variety of molecular mechanisms including MAPK reactivation through MEK. The induction of a cancer cell death modality associated with danger-signalling resulting in surface mobilization of crucial damage-associated-molecular-patterns (DAMPs), e.g. calreticulin (CRT) and heat shock protein-90 (HSP90), from dying cells, is emerging to be crucial for therapeutic success. Both cell death and danger-signalling are modulated by autophagy, a key adaptation mechanism stimulated during melanoma progression. However, whether melanoma cell death induced by MAPK inhibition is associated with danger-signalling, and the reliance of these mechanisms on autophagy, has not yet been scrutinized. Using a panel of isogenic PLX4032-sensitive and resistant melanoma cell lines we show that PLX4032-induced caspase-dependent cell death and DAMPs exposure in the drug-sensitive cells, but failed to do so in the drug-resistant cells, displaying heightened MEK activation. MEK inhibitor, U0126, treatment sensitized PLX4032-resistant cells to death and re-established their danger-signalling capacity. Only melanoma cells exposing death-induced danger-signals were phagocytosed and induced DC maturation. Although the PLX4032-resistant melanoma cells displayed higher basal and drug-induced autophagy, compromising autophagy, pharmacologically or by ATG5 knockdown, was insufficient to re-establish their PLX4032 sensitivity. Interestingly, autophagy abrogation was particularly efficacious in boosting cell death and ecto-CRT/ecto-HSP90 in PLX4032-resistant cells upon blockage of MEK hyper-activation by U0126. Thus combination of MEK inhibitors with autophagy blockers may represent a novel treatment regime to increase both cell death and danger-signalling in Vemurafenib-resistant metastatic melanoma. Copyright © 2015 Elsevier Inc. All rights reserved.


相关化合物

  • 丙酮酸钠
  • 二甲基亚砜
  • 苄磺酰氟
  • 巴佛洛霉素A1
  • 巯基乙醇
  • 11-巯基十一烷基氢...
  • 7-氨基放线菌素D
  • 8-辛酰氧基芘-1,3,6...
  • 4-甲基伞形酮庚酯

相关文献:

Driving cartilage formation in high-density human adipose-derived stem cell aggregate and sheet constructs without exogenous growth factor delivery.

2014-12-01

[Tissue Eng. Part A 20(23-24) , 3163-75, (2014)]

A short splice form of Xin-actin binding repeat containing 2 (XIRP2) lacking the Xin repeats is required for maintenance of stereocilia morphology and hearing function.

2015-02-04

[J. Neurosci. 35(5) , 1999-2014, (2015)]

Oversulfated heparins with low anticoagulant activity are strong and fast inhibitors of hepcidin expression in vitro and in vivo.

2014-12-01

[Biochem. Pharmacol. 92(3) , 467-75, (2014)]

Establishment and characterization of an air-liquid canine corneal organ culture model to study acute herpes keratitis.

2014-12-01

[J. Virol. 88(23) , 13669-77, (2014)]

Hypoxia reduces MAX expression in endothelial cells by unproductive splicing.

2014-12-20

[FEBS Lett. 588(24) , 4784-90, (2014)]

更多文献...