Inhibition of the GAS6/AXL pathway augments the efficacy of chemotherapies
Mihalis S. Kariolis, … , Jennifer R. Cochran, Amato J. Giaccia
Mihalis S. Kariolis, … , Jennifer R. Cochran, Amato J. Giaccia
Published November 28, 2016
Citation Information: J Clin Invest. 2017;127(1):183-198. https://doi.org/10.1172/JCI85610.
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Research Article Oncology Therapeutics

Inhibition of the GAS6/AXL pathway augments the efficacy of chemotherapies

Abstract

The AXL receptor and its activating ligand, growth arrest–specific 6 (GAS6), are important drivers of metastasis and therapeutic resistance in human cancers. Given the critical roles that GAS6 and AXL play in refractory disease, this signaling axis represents an attractive target for therapeutic intervention. However, the strong picomolar binding affinity between GAS6 and AXL and the promiscuity of small molecule inhibitors represent important challenges faced by current anti-AXL therapeutics. Here, we have addressed these obstacles by engineering a second-generation, high-affinity AXL decoy receptor with an apparent affinity of 93 femtomolar to GAS6. Our decoy receptor, MYD1-72, profoundly inhibited disease progression in aggressive preclinical models of human cancers and induced cell killing in leukemia cells. When directly compared with the most advanced anti-AXL small molecules in the clinic, MYD1-72 achieved superior antitumor efficacy while displaying no toxicity. Moreover, we uncovered a relationship between AXL and the cellular response to DNA damage whereby abrogation of AXL signaling leads to accumulation of the DNA-damage markers γH2AX, 53BP1, and RAD51. MYD1-72 exploited this relationship, leading to improvements upon the therapeutic index of current standard-of-care chemotherapies in preclinical models of advanced pancreatic and ovarian cancer.

Authors

Mihalis S. Kariolis, Yu Rebecca Miao, Anh Diep, Shannon E. Nash, Monica M. Olcina, Dadi Jiang, Douglas S. Jones II, Shiven Kapur, Irimpan I. Mathews, Albert C. Koong, Erinn B. Rankin, Jennifer R. Cochran, Amato J. Giaccia

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Figure 1

Engineering and characterization of a second-generation AXL decoy receptor.

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Engineering and characterization of a second-generation AXL decoy recept...
(A) The first immunoglobulin domain of the AXL receptor was engineered for improved affinity to GAS6. When administered, the engineered soluble AXL sequesters GAS6, preventing it from binding to and activating endogenous cell surface–expressed AXL. (B) GAS6/MYD1-72 1:1 cocomplex. GAS6 is shown in gray and MYD1-72 in blue. V72 is highlighted in red, and its location on the structure is indicated (arrows). (C) Cutaway showing A72 on the MYD1 and V72 on the MYD1-72. The sidechains of both are shown as dotted spheres, illustrating the space occupied by the larger valine mutation. The new interaction gained in the MYD1-72 structure is shown in the middle.