Resistance to ERK1/2 pathway inhibitors; sweet spots, fitness deficits and drug addiction

Matthew J Sale; Kathryn Balmanno; Simon J Cook

doi:10.20517/cdr.2019.14

Resistance to ERK1/2 pathway inhibitors; sweet spots, fitness deficits and drug addiction

Cancer Drug Resist. 2019 Jun 19;2(2):365-380. doi: 10.20517/cdr.2019.14. eCollection 2019.

Authors

Matthew J Sale¹, Kathryn Balmanno¹, Simon J Cook¹

Affiliation

¹ Signalling Programme, The Babraham Institute, Babraham Research Campus, Cambridge CB22 3AT, UK.

Abstract

MEK1/2 inhibitors are clinically approved for the treatment of BRAF-mutant melanoma, where they are used in combination with BRAF inhibitors, and are undergoing evaluation in other malignancies. Acquired resistance to MEK1/2 inhibitors, including selumetinib (AZD6244/ARRY-142866), can arise through amplification of BRAF^V600E or KRAS^G13D to reinstate ERK1/2 signalling. We have found that BRAF^V600E amplification and selumetinib resistance are fully reversible following drug withdrawal. This is because resistant cells with BRAF^V600E amplification become addicted to selumetinib to maintain a precise level of ERK1/2 signalling (2%-3% of total ERK1/2 active), that is optimal for cell proliferation and survival. Selumetinib withdrawal drives ERK1/2 activation outside of this critical "sweet spot" (~20%-30% of ERK1/2 active) resulting in a p57^KIP2-dependent G1 cell cycle arrest and senescence or expression of NOXA and cell death with features of autophagy; these terminal responses select against cells with amplified BRAF^V600E. ERK1/2-dependent p57^KIP2 expression is required for loss of BRAF^V600E amplification and determines the rate of reversal of selumetinib resistance. Growth of selumetinib-resistant cells with BRAF^V600E amplification as tumour xenografts also requires the presence of selumetinib to "clamp" ERK1/2 activity within the sweet spot. Thus, BRAF^V600E amplification confers a selective disadvantage or "fitness deficit" during drug withdrawal, providing a rationale for intermittent dosing to forestall resistance. Remarkably, selumetinib resistance driven by KRAS^G13D amplification/upregulation is not reversible. In these cells ERK1/2 reactivation does not inhibit proliferation but drives a ZEB1-dependent epithelial-to-mesenchymal transition that increases cell motility and promotes resistance to traditional chemotherapy agents. Our results reveal that the emergence of drug-addicted, MEKi-resistant cells, and the opportunity this may afford for intermittent dosing schedules ("drug holidays"), may be determined by the nature of the amplified driving oncogene (BRAF^V600E vs. KRAS^G13D), further exemplifying the difficulties of targeting KRAS mutant tumour cells.

Keywords: BRAF; CDKN1C/p57KIP2; EMT; ERK; KRAS; MEK; MEK inhibitor; resistance; selumetinib.

Abstract

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