Scholars@Duke

Data from Metastatic Melanoma Patient–Derived Xenografts Respond to MDM2 Inhibition as a Single Agent or in Combination with BRAF/MEK Inhibition

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Shattuck-Brandt, RL; Chen, S-C; Murray, E; Johnson, CA; Crandall, H; O'Neal, JF; Al-Rohil, RN; Nebhan, CA; Bharti, V; Dahlman, KB; Ayers, GD ...
March 31, 2023
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<div>AbstractPurpose:<p>Over 60% of patients with melanoma respond to immune checkpoint inhibitor (ICI) therapy, but many subsequently progress on these therapies. Second-line targeted therapy is based on <i>BRAF</i> mutation status, but no available agents are available for <i>NRAS, NF1, CDKN2A, PTEN</i>, and <i>TP53</i> mutations. Over 70% of melanoma tumors have activation of the MAPK pathway due to <i>BRAF</i> or <i>NRAS</i> mutations, while loss or mutation of <i>CDKN2A</i> occurs in approximately 40% of melanomas, resulting in unregulated MDM2-mediated ubiquitination and degradation of p53. Here, we investigated the therapeutic efficacy of over-riding MDM2-mediated degradation of p53 in melanoma with an MDM2 inhibitor that interrupts MDM2 ubiquitination of p53, treating tumor-bearing mice with the MDM2 inhibitor alone or combined with MAPK-targeted therapy.</p>Experimental Design:<p>To characterize the ability of the MDM2 antagonist, KRT-232, to inhibit tumor growth, we established patient-derived xenografts (PDX) from 15 patients with melanoma. Mice were treated with KRT-232 or a combination with BRAF and/or MEK inhibitors. Tumor growth, gene mutation status, as well as protein and protein–phosphoprotein changes, were analyzed.</p>Results:<p>One-hundred percent of the 15 PDX tumors exhibited significant growth inhibition either in response to KRT-232 alone or in combination with BRAF and/or MEK inhibitors. Only <i>BRAF<sup>V600WT</sup></i> tumors responded to KRT-232 treatment alone while <i>BRAF<sup>V600E/M</sup></i> PDXs exhibited a synergistic response to the combination of KRT-232 and BRAF/MEK inhibitors.</p>Conclusions:<p>KRT-232 is an effective therapy for the treatment of either <i>BRAF<sup>WT</sup></i> or PAN<sup><i>WT</i></sup> <i>(BRAF<sup>WT</sup>, NRAS<sup>WT</sup>) TP53<sup>WT</sup></i> melanomas. In combination with BRAF and/or MEK inhibitors, KRT-232 may be an effective treatment strategy for BRAF<sup>V600</sup>-mutant tumors.</p></div>

Duke Scholars

Rami Nayef Al-Rohil
Author Rami Nayef Al-Rohil Pathology

DOI

10.1158/1078-0432.c.6526829.v1

Publication Date

March 31, 2023
 

Citation

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Shattuck-Brandt, R. L., Chen, S.-C., Murray, E., Johnson, C. A., Crandall, H., O’Neal, J. F., … Richmond, A. (2023). Data from Metastatic Melanoma Patient–Derived Xenografts Respond to MDM2 Inhibition as a Single Agent or in Combination with BRAF/MEK Inhibition. https://doi.org/10.1158/1078-0432.c.6526829.v1
Shattuck-Brandt, Rebecca L., Sheau-Chiann Chen, Emily Murray, Christopher Andrew Johnson, Holly Crandall, Jamye F. O’Neal, Rami Nayef Al-Rohil, et al. “Data from Metastatic Melanoma Patient–Derived Xenografts Respond to MDM2 Inhibition as a Single Agent or in Combination with BRAF/MEK Inhibition,” March 31, 2023. https://doi.org/10.1158/1078-0432.c.6526829.v1.
Shattuck-Brandt RL, Chen S-C, Murray E, Johnson CA, Crandall H, O’Neal JF, Al-Rohil RN, Nebhan CA, Bharti V, Dahlman KB, Ayers GD, Yan C, Kelley MC, Kauffmann RM, Hooks M, Grau A, Johnson DB, Vilgelm AE, Richmond A. Data from Metastatic Melanoma Patient–Derived Xenografts Respond to MDM2 Inhibition as a Single Agent or in Combination with BRAF/MEK Inhibition. 2023.

DOI

10.1158/1078-0432.c.6526829.v1

Publication Date

March 31, 2023