Designing Dual Inhibitors of Autotaxin-LPAR GPCR Axis

Banerjee, Souvik; Lee, Sue-Chin; Norman, Dean C.; Tigyi, Gábor

doi:10.3390/molecules27175487

Cited by 8 publications

(9 citation statements)

References 92 publications

(174 reference statements)

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“…Pre-clinical investigations in both cell cultures and murine tumor models have provided considerable support for inhibitors against the ATX-LPAR-LPP pathway, some of which, especially against ATX and the LPARs, are currently in clinical trials [ 4 , 27 , 28 , 29 , 30 , 31 ]. However, there are no therapies under clinical investigation to restore LPP1/3 levels or suppress LPP2 levels in cancers.…”

Section: Introductionmentioning

confidence: 99%

Decreased Lipid Phosphate Phosphatase 1/3 and Increased Lipid Phosphate Phosphatase 2 Expression in the Human Breast Cancer Tumor Microenvironment Promotes Tumor Progression and Immune System Evasion

Benesch

Tang

et al. 2023

Cancers

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The LPP family is comprised of three enzymes that dephosphorylate bioactive lipid phosphates both intracellularly and extracellularly. Pre-clinical breast cancer models have demonstrated that decreased LPP1/3 with increased LPP2 expression correlates to tumorigenesis. This though has not been well verified in human specimens. In this study, we correlate LPP expression data to clinical outcomes in over 5000 breast cancers from three independent cohorts (TCGA, METABRIC, and GSE96058), investigate biological function using gene set enrichment analysis (GSEA) and the xCell cell-type enrichment analysis, and confirm sources of LPP production in the tumor microenvironment (TME) using single-cell RNA-sequencing (scRNAseq) data. Decreased LPP1/3 and increased LPP2 expression correlated to increased tumor grade, proliferation, and tumor mutational burden (all p < 0.001), as well as worse overall survival (hazard ratios 1.3–1.5). Further, cytolytic activity was decreased, consistent with immune system invasion. GSEA data demonstrated multiple increased inflammatory signaling, survival, stemness, and cell signaling pathways with this phenotype across all three cohorts. scRNAseq and the xCell algorithm demonstrated that most tumor LPP1/3 was expressed by endothelial cells and tumor-associated fibroblasts and LPP2 by cancer cells (all p < 0.01). Restoring the balance in LPP expression levels, particularly through LPP2 inhibition, could represent novel adjuvant therapeutic options in breast cancer treatment.

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Section: Introductionmentioning

confidence: 99%

Decreased Lipid Phosphate Phosphatase 1/3 and Increased Lipid Phosphate Phosphatase 2 Expression in the Human Breast Cancer Tumor Microenvironment Promotes Tumor Progression and Immune System Evasion

Benesch

Tang

et al. 2023

Cancers

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“…In the last years, several small molecules have been developed to act as ATX inhibitors. These molecules can act by competing with LPC for the hydrophobic pocket and by binding to the active site of the enzyme [ 15 ]. IOA-289 is an orally available ATX inhibitor in clinical development by iOnctura for the treatment of solid tumors with a high degree of fibrosis [ 16 ].…”

Section: Introductionmentioning

confidence: 99%

Autotaxin inhibitor IOA-289 reduces gastrointestinal cancer progression in preclinical models

Centonze,

Di Conza,

Lahn

et al. 2023

J Exp Clin Cancer Res

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Background Autotaxin (ATX) is a secreted enzyme that converts lysophosphatidylcholine to lysophosphatidic acid (LPA). LPA stimulates cell proliferation and migration and promotes wound repair following tissue damage. ATX levels are directly correlated with stage and grade in several human cancers. Several small molecule ATX inhibitors have been developed in recent years. IOA-289 is a potent ATX inhibitor, developed to treat cancers containing fibrosis. In this study, we tested IOA-289 treatment on different gastrointestinal tract tumor cell lines, in order to evaluate its effects on viability and motility. Methods To determine the effects on cell viability and proliferation of treatment with increasing concentrations of IOA-289, we used the crystal violet assay, a clonogenic assay in matrigel, and we evaluated the inhibitor’s effect on formation of 3D spheroids in an in vitro model. The effect of IOA-289 on cell cycle phases was analysed with a redox dye reagent. Cell migration capacity was evaluated by wound healing assay and transwell migration assay. To evaluate the pro-apoptotic effect of the inhibitor, cells were stained with Annexin V and immunofluorescence and flow cytometry analysis were performed. An antibody array was also used, to discriminate, in various samples, the differential expression of 43 proteins involved in the apoptosis pathway. Results We found that IOA-289 is able to inhibit both growth and migration of gastrointestinal tract tumor cell lines, both in 2D (crystal violet assay) and 3D in vitro models (spheroid formation and clonogenic assay in matrigel). This effect is dose-dependent, and the drug is most effective when administered in FBS-free culture medium. The inhibitory effect on cell growth is due to a pro-apoptotic effect of IOA-289. Staining with FITC-conjugated Annexin V showed that IOA-289 induced a dose-dependent increase in fluorescence following incubation for 24 h, and apoptotic cells were also distinguished in flow cytometry using Annexin/PI staining. The antibody array shows that treatment with IOA-289 causes the increased expression of several pro-apoptotic proteins in all tested cell lines. Conclusions These results indicate that IOA-289 may be an effective drug for the treatment of tumors of the gastrointestinal tract, particularly those characterized by a high degree of fibrosis.

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“…Class I are lipid-like or orthosteric inhibitors, with the early inhibitor PF-8380 being the prototypical inhibitor of this class [ 84 , 85 ]. None of these compounds have entered advanced clinical trials, secondary to their off-target effects related to their high partition coefficient [ 86 ]. More modern inhibitors are non-carboxylic and non-lipid in design [ 86 ].…”

Section: Summary Of the Current State Of Lpa Pathway Pharmacological ...mentioning

confidence: 99%

“…None of these compounds have entered advanced clinical trials, secondary to their off-target effects related to their high partition coefficient [ 86 ]. More modern inhibitors are non-carboxylic and non-lipid in design [ 86 ]. Class II inhibitors target the hydrophobic pocket (including GRI-918013, none of which are in trials), obstructing binding of LPC to ATX [ 83 ].…”

Section: Summary Of the Current State Of Lpa Pathway Pharmacological ...mentioning

confidence: 99%

“…Such inhibitors, however, may not have the intended therapeutic potency if the other LPARs can adequately compensate following their blockage, but further investigation in animal models will be required to determine this. If this were to be the case, a combination compound in the form of a dual ATX-inhibitor and selective LPAR inhibitor might be able to provide robust adjuvant therapy, as has been demonstrated with dual ATX-LPAR1 inhibition in metastatic melanoma models [ 86 , 106 ]. Finally, pharmacological targeting of the LPPs remains an essentially untapped area of investigation.…”

Section: Future Perspective On Modern Atx and Lpa Signaling Translati...mentioning

confidence: 99%

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Autotaxin and Lysophosphatidate Signaling: Prime Targets for Mitigating Therapy Resistance in Breast Cancer

Benesch,

Tang,

Brindley

et al. 2024

World J Oncol

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Overcoming and preventing cancer therapy resistance is the most pressing challenge in modern breast cancer management. Consequently, most modern breast cancer research is aimed at understanding and blocking these therapy resistance mechanisms. One increasingly promising therapeutic target is the autotaxin (ATX)-lysophosphatidate (LPA)-lipid phosphate phosphatase (LPP) axis. Extracellular LPA, produced from albumin-bound lysophosphatidylcholine by ATX and degraded by the ecto-activity of the LPPs, is a potent cell-signaling mediator of tumor growth, invasion, angiogenesis, immune evasion, and resistance to cancer treatment modalities. LPA signaling in the post-natal organism has central roles in physiological wound healing, but these mechanisms are subverted to fuel pathogenesis in diseases that arise from chronic inflammatory processes, including cancer. Over the last 10 years, our understanding of the role of LPA signaling in the breast tumor microenvironment has begun to mature. Tumor-promoting inflammation in breast cancer leads to increased ATX production within the tumor microenvironment. This results in increased local concentrations of LPA that are maintained in part by decreased overall cancer cell LPP expression that would otherwise more rapidly break it down. LPA signaling through six G-protein-coupled LPA receptors expressed by cancer cells can then activate virtually every known tumorigenic pathway. Consequently, to target therapy resistance and tumor growth mediated by LPA signaling, multiple inhibitors against the LPA signaling axis are entering clinical trials. In this review, we summarize recent developments in LPA breast cancer biology, and illustrate how these novel therapeutics against the LPA signaling pathway may be excellent adjuncts to extend the efficacy of evolving breast cancer treatments.

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Designing Dual Inhibitors of Autotaxin-LPAR GPCR Axis

Cited by 8 publications

References 92 publications

Decreased Lipid Phosphate Phosphatase 1/3 and Increased Lipid Phosphate Phosphatase 2 Expression in the Human Breast Cancer Tumor Microenvironment Promotes Tumor Progression and Immune System Evasion

Decreased Lipid Phosphate Phosphatase 1/3 and Increased Lipid Phosphate Phosphatase 2 Expression in the Human Breast Cancer Tumor Microenvironment Promotes Tumor Progression and Immune System Evasion

Autotaxin inhibitor IOA-289 reduces gastrointestinal cancer progression in preclinical models

Autotaxin and Lysophosphatidate Signaling: Prime Targets for Mitigating Therapy Resistance in Breast Cancer

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