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Abstract
Mixed Lineage Kinase 3 (MLK3) is a viable target for neoplastic diseases; however, it is unclear whether its activators or inhibitors can act as anti-neoplastic agents. We reported that the MLK3 kinase activity was higher in triple-negative (TNBC) than in hormone receptor-positive human breast tumors, where estrogen inhibited MLK3 kinase activity and provided a survival advantage to ER+ breast cancer cells. Herein, we show that in TNBC, the higher MLK3 kinase activity paradoxically promotes cancer cell survival. Knockdown of MLK3 or MLK3 inhibitors, CEP-1347 and URMC-099, attenuated tumorigenesis of TNBC cell line and Patient-Derived (PDX) xenografts. The MLK3 kinase inhibitors decreased both the expression and activation of MLK3, PAK1, and NF-kB protein and caused cell death in TNBC breast xenografts. RNA-seq analysis identified several genes downregulated by MLK3 inhibition, and the NGF/TrkA MAPK pathway was significantly enriched in tumors sensitive to growth inhibition by MLK3 inhibitors. The TNBC cell line unresponsive to kinase inhibitor had substantially lower TrkA, and overexpression of TrkA restored the sensitivity to MLK3 inhibition. These results suggest that the functions of MLK3 in breast cancer cells depend on downstream targets in TNBC tumors expressing TrkA, and MLK3 kinase inhibition may provide a novel targeted therapy.
Details
; Das, Subhasis 2
; Singh, Sunil Kumar 1
; Srivastava, Piush 1
; Sondarva, Gautam 1
; Rao, Arundhati 3 ; Sinha, Subhash C. 4
; Xiong, Rui 5 ; Bloem, Laura 5
; Hoskins, Kent 6 ; Thatcher, Gregory R. J. 7 ; Rana, Basabi 8
; Rana, Ajay 8
1 The University of Illinois at Chicago, Department of Surgery, Division of Surgical Oncology, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319)
2 The University of Illinois at Chicago, Department of Surgery, Division of Surgical Oncology, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319); The University of Illinois at Chicago, University of Illinois Hospital & Health Sciences System Cancer Center, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319)
3 Baylor Scott & White Medical Center, Department of Pathology and Laboratory Medicine, Temple, USA (GRID:grid.508013.f)
4 Weill Cornell Medicine, New York, USA (GRID:grid.5386.8) (ISNI:000000041936877X)
5 University of Illinois at Chicago, UICentre for Drug Discovery, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319)
6 The University of Illinois at Chicago, Department of Medicine, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319)
7 University of Arizona, Department of Pharmacology and Toxicology, Coit College of Pharmacy, Tucson, USA (GRID:grid.134563.6) (ISNI:0000 0001 2168 186X)
8 The University of Illinois at Chicago, Department of Surgery, Division of Surgical Oncology, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319); The University of Illinois at Chicago, University of Illinois Hospital & Health Sciences System Cancer Center, Chicago, USA (GRID:grid.185648.6) (ISNI:0000 0001 2175 0319); Jesse Brown VA Medical Center, Chicago, USA (GRID:grid.280892.9) (ISNI:0000 0004 0419 4711)