Your search keyword '"Poh AR"' showing total 42 results

1. Combination of bazedoxifene with chemotherapy and SMAC-mimetics for the treatment of colorectal cancer

Author

Dmello, RS, Palmieri, M, Thilakasiri, PS, Doughty, L, Nero, TL, Poh, AR, To, SQ, Lee, EF, Fairlie, WD, Mielke, L, Parker, MW, Poon, IKH, Batlle, E, Ernst, M, Chand, AL, Dmello, RS, Palmieri, M, Thilakasiri, PS, Doughty, L, Nero, TL, Poh, AR, To, SQ, Lee, EF, Fairlie, WD, Mielke, L, Parker, MW, Poon, IKH, Batlle, E, Ernst, M, and Chand, AL

Abstract

Excessive STAT3 signalling via gp130, the shared receptor subunit for IL-6 and IL-11, contributes to disease progression and poor survival outcomes in patients with colorectal cancer. Here, we provide evidence that bazedoxifene inhibits tumour growth via direct interaction with the gp130 receptor to suppress IL-6 and IL-11-mediated STAT3 signalling. Additionally, bazedoxifene combined with chemotherapy synergistically reduced cell proliferation and induced apoptosis in patient-derived colon cancer organoids. We elucidated that the primary mechanism of anti-tumour activity conferred by bazedoxifene treatment occurs via pro-apoptotic responses in tumour cells. Co-treatment with bazedoxifene and the SMAC-mimetics, LCL161 or Birinapant, that target the IAP family of proteins, demonstrated increased apoptosis and reduced proliferation in colorectal cancer cells. Our findings provide evidence that bazedoxifene treatment could be combined with SMAC-mimetics and chemotherapy to enhance tumour cell apoptosis in colorectal cancer, where gp130 receptor signalling promotes tumour growth and progression.

Published

2024

2. Therapeutic inhibition of the SRC-kinase HCK facilitates T cell tumor infiltration and improves response to immunotherapy

Author

Poh, AR, Love, CG, Chisanga, D, Steer, JH, Baloyan, D, Chopin, M, Nutt, S, Rautela, J, Huntington, ND, Etemadi, N, O'Brien, M, O'Keefe, R, Ellies, LG, Macri, C, Mintern, JD, Whitehead, L, Gangadhara, G, Boon, L, Chand, AL, Lowell, CA, Shi, W, Pixley, FJ, Ernst, M, Poh, AR, Love, CG, Chisanga, D, Steer, JH, Baloyan, D, Chopin, M, Nutt, S, Rautela, J, Huntington, ND, Etemadi, N, O'Brien, M, O'Keefe, R, Ellies, LG, Macri, C, Mintern, JD, Whitehead, L, Gangadhara, G, Boon, L, Chand, AL, Lowell, CA, Shi, W, Pixley, FJ, and Ernst, M

Abstract

Although immunotherapy has revolutionized cancer treatment, many immunogenic tumors remain refractory to treatment. This can be largely attributed to an immunologically "cold" tumor microenvironment characterized by an accumulation of immunosuppressive myeloid cells and exclusion of activated T cells. Here, we demonstrate that genetic ablation or therapeutic inhibition of the myeloid-specific hematopoietic cell kinase (HCK) enables activity of antagonistic anti-programmed cell death protein 1 (anti-PD1), anti-CTLA4, or agonistic anti-CD40 immunotherapies in otherwise refractory tumors and augments response in treatment-susceptible tumors. Mechanistically, HCK ablation reprograms tumor-associated macrophages and dendritic cells toward an inflammatory endotype and enhances CD8+ T cell recruitment and activation when combined with immunotherapy in mice. Meanwhile, therapeutic inhibition of HCK in humanized mice engrafted with patient-derived xenografts counteracts tumor immunosuppression, improves T cell recruitment, and impairs tumor growth. Collectively, our results suggest that therapeutic targeting of HCK activity enhances response to immunotherapy by simultaneously stimulating immune cell activation and inhibiting the immunosuppressive tumor microenvironment.

Published

2022

3. Tumor Growth Remains Refractory to Myc Ablation in Host Macrophages.

Author

Morrow, RJ, Allam, AH, Konecnik, J, Baloyan, D, Dijkstra, C, Eissmann, MF, Jacob, SP, O'Brien, M, Poh, AR, Ernst, M, Morrow, RJ, Allam, AH, Konecnik, J, Baloyan, D, Dijkstra, C, Eissmann, MF, Jacob, SP, O'Brien, M, Poh, AR, and Ernst, M

Abstract

Aberrant expression of the oncoprotein c-Myc (Myc) is frequently observed in solid tumors and is associated with reduced overall survival. In addition to well-recognized cancer cell-intrinsic roles of Myc, studies have also suggested tumor-promoting roles for Myc in cells of the tumor microenvironment, including macrophages and other myeloid cells. Here, we benchmark Myc inactivation in tumor cells against the contribution of its expression in myeloid cells of murine hosts that harbor endogenous or allograft tumors. Surprisingly, we observe that LysMCre-mediated Myc ablation in host macrophages does not attenuate tumor growth regardless of immunogenicity, the cellular origin of the tumor, the site it develops, or the stage along the tumor progression cascade. Likewise, we find no evidence for Myc ablation to revert or antagonize the polarization of alternatively activated immunosuppressive macrophages. Thus, we surmise that systemic targeting of Myc activity may confer therapeutic benefits primarily through limiting Myc activity in tumor cells rather than reinvigorating the anti-tumor activity of macrophages.

Published

2022

4. Multicellular Effects of STAT3 in Non-small Cell Lung Cancer: Mechanistic Insights and Therapeutic Opportunities.

Author

Parakh, S, Ernst, M, Poh, AR, Parakh, S, Ernst, M, and Poh, AR

Abstract

Non-small cell lung cancer (NSCLC) is the most common type of lung cancer and accounts for 85% of lung cancer cases. Aberrant activation of the Signal Transducer and Activator of Transcription 3 (STAT3) is frequently observed in NSCLC and is associated with a poor prognosis. Pre-clinical studies have revealed an unequivocal role for tumor cell-intrinsic and extrinsic STAT3 signaling in NSCLC by promoting angiogenesis, cell survival, cancer cell stemness, drug resistance, and evasion of anti-tumor immunity. Several STAT3-targeting strategies have also been investigated in pre-clinical models, and include preventing upstream receptor/ligand interactions, promoting the degradation of STAT3 mRNA, and interfering with STAT3 DNA binding. In this review, we discuss the molecular and immunological mechanisms by which persistent STAT3 activation promotes NSCLC development, and the utility of STAT3 as a prognostic and predictive biomarker in NSCLC. We also provide a comprehensive update of STAT3-targeting therapies that are currently undergoing clinical evaluation, and discuss the challenges associated with these treatment modalities in human patients.

Published

2021

5. Tumor-Associated Macrophages in Pancreatic Ductal Adenocarcinoma: Therapeutic Opportunities and Clinical Challenges

Author

Poh, AR, Ernst, M, Poh, AR, and Ernst, M

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an aggressive malignant disease with a 5-year survival rate of less than 10%. Macrophages are one of the earliest infiltrating cells in the pancreatic tumor microenvironment, and are associated with an increased risk of disease progression, recurrence, metastasis, and shorter overall survival. Pre-clinical studies have demonstrated an unequivocal role of macrophages in PDAC by contributing to chronic inflammation, cancer cell stemness, desmoplasia, immune suppression, angiogenesis, invasion, metastasis, and drug resistance. Several macrophage-targeting therapies have also been investigated in pre-clinical models, and include macrophage depletion, inhibiting macrophage recruitment, and macrophage reprogramming. However, the effectiveness of these drugs in pre-clinical models has not always translated into clinical trials. In this review, we discuss the molecular mechanisms that underpin macrophage heterogeneity within the pancreatic tumor microenvironment, and examine the contribution of macrophages at various stages of PDAC progression. We also provide a comprehensive update of macrophage-targeting therapies that are currently undergoing clinical evaluation, and discuss clinical challenges associated with these treatment modalities in human PDAC patients.

Published

2021

6. BCL-XL is an actionable target for treatment of malignant pleural mesothelioma (vol 6, 114, 2020)

Author

Arulananda, S, O'Brien, M, Evangelista, M, Harris, TJ, Steinohrt, NS, Jenkins, LJ, Walkiewicz, M, O'Donoghue, RJJ, Poh, AR, Thapa, B, Williams, DS, Leong, T, Mariadason, JM, Li, X, Cebon, J, Lee, EF, John, T, Fairlie, WD, Arulananda, S, O'Brien, M, Evangelista, M, Harris, TJ, Steinohrt, NS, Jenkins, LJ, Walkiewicz, M, O'Donoghue, RJJ, Poh, AR, Thapa, B, Williams, DS, Leong, T, Mariadason, JM, Li, X, Cebon, J, Lee, EF, John, T, and Fairlie, WD

Published

2021

7. A novel BH3-mimetic, AZD0466, targeting BCL-XL and BCL-2 is effective in pre-clinical models of malignant pleural mesothelioma

Author

Arulananda, S, O'Brien, M, Evangelista, M, Jenkins, LJ, Poh, AR, Walkiewicz, M, Leong, T, Mariadason, JM, Cebon, J, Balachander, SB, Cidado, JR, Lee, EF, John, T, Fairlie, WD, Arulananda, S, O'Brien, M, Evangelista, M, Jenkins, LJ, Poh, AR, Walkiewicz, M, Leong, T, Mariadason, JM, Cebon, J, Balachander, SB, Cidado, JR, Lee, EF, John, T, and Fairlie, WD

Abstract

Malignant pleural mesothelioma (MPM) is an aggressive cancer with treatment limited to Cisplatin and Pemetrexed chemotherapy. Recently, we showed that drugs targeting the BCL-2-regulated apoptosis pathway could kill MPM cell lines in vitro, and control tumor growth in vivo. These studies showed BCL-XL was the dominant pro-survival BCL-2 family member correlating with its high-level expression in cells and patient tumor samples. In this study we show another inhibitor, AZD4320 that targets BCL-XL (and BCL-2), can also potently kill MPM tumor cells in vitro (EC50 values in the 200 nM range) and this effect is enhanced by co-inhibition of MCL-1 using AZD5991. Moreover, we show that a novel nanoparticle, AZD0466, where AZD4320 is chemically conjugated to a PEGylated poly-lysine dendrimer, was as effective as standard-of-care chemotherapy, Cisplatin, at inhibiting tumor growth in mouse xenograft studies, and this effect was enhanced when both drugs were combined. Critically, the degree of thrombocytopenia, an on-target toxicity associated with BCL-XL inhibition, was significantly reduced throughout the treatment period compared to other BCL-XL-targeting BH3-mimetics. These pre-clinical findings provide a rationale for the future clinical evaluation for novel BH3-mimetic formulations in MPM, and indeed, other solid tumor types dependent on BCL-XL.

Published

2021

8. Loss of Bcl-G, a Bcl-2 family member, augments the development of inflammation-associated colorectal cancer

Author

Nguyen, PM, Dagley, LF, Preaudet, A, Lam, N, Giam, M, Fung, KY, Aizel, K, van Duijneveldt, G, Tan, CW, Hirokawa, Y, Yip, HYK, Love, CG, Poh, AR, D' Cruz, A, Burstroem, C, Feltham, R, Abdirahman, SM, Meiselbach, K, Low, RRJ, Palmieri, M, Ernst, M, Webb, AI, Burgess, T, Sieber, OM, Bouillet, P, Putoczki, TL, Nguyen, PM, Dagley, LF, Preaudet, A, Lam, N, Giam, M, Fung, KY, Aizel, K, van Duijneveldt, G, Tan, CW, Hirokawa, Y, Yip, HYK, Love, CG, Poh, AR, D' Cruz, A, Burstroem, C, Feltham, R, Abdirahman, SM, Meiselbach, K, Low, RRJ, Palmieri, M, Ernst, M, Webb, AI, Burgess, T, Sieber, OM, Bouillet, P, and Putoczki, TL

Abstract

Gastrointestinal epithelial cells provide a selective barrier that segregates the host immune system from luminal microorganisms, thereby contributing directly to the regulation of homeostasis. We have shown that from early embryonic development Bcl-G, a Bcl-2 protein family member with unknown function, was highly expressed in gastrointestinal epithelial cells. While Bcl-G was dispensable for normal growth and development in mice, the loss of Bcl-G resulted in accelerated progression of colitis-associated cancer. A label-free quantitative proteomics approach revealed that Bcl-G may contribute to the stability of a mucin network, which when disrupted, is linked to colon tumorigenesis. Consistent with this, we observed a significant reduction in Bcl-G expression in human colorectal tumors. Our study identifies an unappreciated role for Bcl-G in colon cancer.

Published

2020

9. BCL-XL is an actionable target for treatment of malignant pleural mesothelioma

Author

Arulananda, S, O'Brien, M, Evangelista, M, Harris, TJ, Steinohrt, NS, Jenkins, LJ, Walkiewicz, M, O'Donoghue, RJJ, Poh, AR, Thapa, B, Williams, DS, Leong, T, Mariadason, JM, Li, X, Cebon, J, Lee, EF, John, T, Douglas Fairlie, W, Arulananda, S, O'Brien, M, Evangelista, M, Harris, TJ, Steinohrt, NS, Jenkins, LJ, Walkiewicz, M, O'Donoghue, RJJ, Poh, AR, Thapa, B, Williams, DS, Leong, T, Mariadason, JM, Li, X, Cebon, J, Lee, EF, John, T, and Douglas Fairlie, W

Abstract

Despite having one of the lowest survival rates of all cancers, there have been no new approved treatments for malignant pleural mesothelioma (MPM) in over a decade. Standard-of-care treatment relies on Cisplatin plus Pemetrexed chemotherapy. Here, we tested a suite of BH3-mimetic drugs targeting BCL-2 pro-survival proteins of the intrinsic apoptotic pathway. We found BCL-XL is the dominant pro-survival protein in a panel of cell lines in vitro, though potent, synergistic cell killing occurred with MCL-1 co-targeting. This correlates with high-level expression of BCL-XL and MCL-1 in cell lines and a large cohort of patient tumour samples. BCL-XL inhibition combined with Cisplatin also enhanced cell killing. In vivo BCL-XL inhibition was as effective as Cisplatin, and the combination enhanced tumour growth control and survival. Genetic ablation of MCL-1 also enhanced the effects of BCL-XL inhibitors, in vivo. Combined, these data provide a compelling rationale for the clinical investigation of BH3-mimetics targeting BCL-XL in MPM.

Published

2020

10. IL-33-mediated mast cell activation promotes gastric cancer through macrophage mobilization

Author

Eissmann, MF, Dijkstra, C, Jarnicki, A, Phesse, T, Brunnberg, J, Poh, AR, Etemadi, N, Tsantikos, E, Thiem, S, Huntington, ND, Hibbs, ML, Boussioutas, A, Grimbaldeston, MA, Buchert, M, O'Donoghue, RJJ, Masson, F, Ernst, M, Eissmann, MF, Dijkstra, C, Jarnicki, A, Phesse, T, Brunnberg, J, Poh, AR, Etemadi, N, Tsantikos, E, Thiem, S, Huntington, ND, Hibbs, ML, Boussioutas, A, Grimbaldeston, MA, Buchert, M, O'Donoghue, RJJ, Masson, F, and Ernst, M

Abstract

The contribution of mast cells in the microenvironment of solid malignancies remains controversial. Here we functionally assess the impact of tumor-adjacent, submucosal mast cell accumulation in murine and human intestinal-type gastric cancer. We find that genetic ablation or therapeutic inactivation of mast cells suppresses accumulation of tumor-associated macrophages, reduces tumor cell proliferation and angiogenesis, and diminishes tumor burden. Mast cells are activated by interleukin (IL)-33, an alarmin produced by the tumor epithelium in response to the inflammatory cytokine IL-11, which is required for the growth of gastric cancers in mice. Accordingly, ablation of the cognate IL-33 receptor St2 limits tumor growth, and reduces mast cell-dependent production and release of the macrophage-attracting factors Csf2, Ccl3, and Il6. Conversely, genetic or therapeutic macrophage depletion reduces tumor burden without affecting mast cell abundance. Therefore, tumor-derived IL-33 sustains a mast cell and macrophage-dependent signaling cascade that is amenable for the treatment of gastric cancer.

Published

2019

11. Targeting Macrophages in Cancer: From Bench to Bedside

Author

Poh, AR, Ernst, M, Poh, AR, and Ernst, M

Abstract

Macrophages are a major component of the tumor microenvironment and orchestrate various aspects of immunity. Within tumors, macrophages can reversibly alter their endotype in response to environmental cues, including hypoxia and stimuli derived from other immune cells, as well as the extracellular matrix. Depending on their activation status, macrophages can exert dual influences on tumorigenesis by either antagonizing the cytotoxic activity immune cells or by enhancing antitumor responses. In most solid cancers, increased infiltration with tumor-associated macrophages (TAMs) has long been associated with poor patient prognosis, highlighting their value as potential diagnostic and prognostic biomarkers in cancer. A number of macrophage-centered approaches to anticancer therapy have been investigated, and include strategies to block their tumor-promoting activities or exploit their antitumor effector functions. Integrating therapeutic strategies to target TAMs to complement conventional therapies has yielded promising results in preclinical trials and warrants further investigation to determine its translational benefit in human cancer patients. In this review, we discuss the molecular mechanisms underlying the pro-tumorigenic programming of macrophages and provide a comprehensive update of macrophage-targeted therapies for the treatment of solid cancers.

Published

2018

12. Targeting H(i)ck education for cancer therapy?

Author

Ernst, M, O'Donoghue, RJJ, Poh, AR, Ernst, M, O'Donoghue, RJJ, and Poh, AR

Published

2017

13. Mouse models for gastric cancer: Matching models to biological questions

Author

Poh, AR, O'Donoghue, RJJ, Ernst, M, Putoczki, TL, Poh, AR, O'Donoghue, RJJ, Ernst, M, and Putoczki, TL

Abstract

Gastric cancer is the third leading cause of cancer-related mortality worldwide. This is in part due to the asymptomatic nature of the disease, which often results in late-stage diagnosis, at which point there are limited treatment options. Even when treated successfully, gastric cancer patients have a high risk of tumor recurrence and acquired drug resistance. It is vital to gain a better understanding of the molecular mechanisms underlying gastric cancer pathogenesis to facilitate the design of new-targeted therapies that may improve patient survival. A number of chemically and genetically engineered mouse models of gastric cancer have provided significant insight into the contribution of genetic and environmental factors to disease onset and progression. This review outlines the strengths and limitations of current mouse models of gastric cancer and their relevance to the pre-clinical development of new therapeutics.

Published

2016

14. Hematopoietic cell kinase (HCK) as a therapeutic target in immune and cancer cells

Author

Poh, AR, O'Donoghue, RJJ, Ernst, M, Poh, AR, O'Donoghue, RJJ, and Ernst, M

Abstract

The hematopoietic cell kinase (HCK) is a member of the SRC family of cytoplasmic tyrosine kinases (SFKs), and is expressed in cells of the myeloid and B-lymphocyte cell lineages. Excessive HCK activation is associated with several types of leukemia and enhances cell proliferation and survival by physical association with oncogenic fusion proteins, and with functional interactions with receptor tyrosine kinases. Elevated HCK activity is also observed in many solid malignancies, including breast and colon cancer, and correlates with decreased patient survival rates. HCK enhances the secretion of growth factors and pro-inflammatory cytokines from myeloid cells, and promotes macrophage polarization towards a wound healing and tumor-promoting alternatively activated phenotype. Within tumor associated macrophages, HCK stimulates the formation of podosomes that facilitate extracellular matrix degradation, which enhance immune and epithelial cell invasion. By virtue of functional cooperation between HCK and bona fide oncogenic tyrosine kinases, excessive HCK activation can also reduce drug efficacy and contribute to chemo-resistance, while genetic ablation of HCK results in minimal physiological consequences in healthy mice. Given its known crystal structure, HCK therefore provides an attractive therapeutic target to both, directly inhibit the growth of cancer cells, and indirectly curb the source of tumor-promoting changes in the tumor microenvironment.

Published

2015

15. Mutant TP53 switches therapeutic vulnerability during gastric cancer progression within interleukin-6 family cytokines.

Author

Huber A, Allam AH, Dijkstra C, Thiem S, Huynh J, Poh AR, Konecnik J, Jacob SP, Busuttil R, Liao Y, Chisanga D, Shi W, Alorro MG, Forrow S, Tauriello DVF, Batlle E, Boussioutas A, Williams DS, Buchert M, Ernst M, and Eissmann MF

Subjects

Animals, Mice, Signal Transduction, Mutation genetics, PTEN Phosphohydrolase metabolism, PTEN Phosphohydrolase genetics, Humans, Proto-Oncogene Proteins p21(ras) genetics, Proto-Oncogene Proteins p21(ras) metabolism, Interleukin-11 metabolism, Interleukin-11 genetics, Stomach Neoplasms genetics, Stomach Neoplasms pathology, Stomach Neoplasms metabolism, Tumor Suppressor Protein p53 metabolism, Tumor Suppressor Protein p53 genetics, Interleukin-6 metabolism, Interleukin-6 genetics, STAT3 Transcription Factor metabolism, Disease Progression

Abstract

Although aberrant activation of the KRAS and PI3K pathway alongside TP53 mutations account for frequent aberrations in human gastric cancers, neither the sequence nor the individual contributions of these mutations have been clarified. Here, we establish an allelic series of mice to afford conditional expression in the glandular epithelium of Kras G12D ;Pik3ca H1047R or Trp53 R172H and/or ablation of Pten or Trp53. We find that Kras G12D ;Pik3ca H1047R is sufficient to induce adenomas and that lesions progress to carcinoma when also harboring Pten deletions. An additional challenge with either Trp53 loss- or gain-of-function alleles further accelerated tumor progression and triggered metastatic disease. While tumor-intrinsic STAT3 signaling in response to gp130 family cytokines remained as a gatekeeper for all stages of tumor development, metastatic progression required a mutant Trp53-induced interleukin (IL)-11 to IL-6 dependency switch. Consistent with the poorer survival of patients with high IL-6 expression, we identify IL-6/STAT3 signaling as a therapeutic vulnerability for TP53-mutant gastric cancer., Competing Interests: Declaration of interests M.E. serves on the scientific advisory board of Lassen Therapeutics, which develops anti-IL-11 therapeutics., (Copyright © 2024 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2024

16. Combination of bazedoxifene with chemotherapy and SMAC-mimetics for the treatment of colorectal cancer.

Author

Dmello RS, Palmieri M, Thilakasiri PS, Doughty L, Nero TL, Poh AR, To SQ, Lee EF, Douglas Fairlie W, Mielke L, Parker MW, Poon IKH, Batlle E, Ernst M, and Chand AL

Subjects

Humans, Cell Line, Tumor, Interleukin-6 metabolism, Cytokine Receptor gp130 metabolism, Apoptosis, Interleukin-11 therapeutic use, Colonic Neoplasms drug therapy, Indoles

Abstract

Excessive STAT3 signalling via gp130, the shared receptor subunit for IL-6 and IL-11, contributes to disease progression and poor survival outcomes in patients with colorectal cancer. Here, we provide evidence that bazedoxifene inhibits tumour growth via direct interaction with the gp130 receptor to suppress IL-6 and IL-11-mediated STAT3 signalling. Additionally, bazedoxifene combined with chemotherapy synergistically reduced cell proliferation and induced apoptosis in patient-derived colon cancer organoids. We elucidated that the primary mechanism of anti-tumour activity conferred by bazedoxifene treatment occurs via pro-apoptotic responses in tumour cells. Co-treatment with bazedoxifene and the SMAC-mimetics, LCL161 or Birinapant, that target the IAP family of proteins, demonstrated increased apoptosis and reduced proliferation in colorectal cancer cells. Our findings provide evidence that bazedoxifene treatment could be combined with SMAC-mimetics and chemotherapy to enhance tumour cell apoptosis in colorectal cancer, where gp130 receptor signalling promotes tumour growth and progression., (© 2024. The Author(s).)

Published

2024

17. Tumor macrophage functional heterogeneity can inform the development of novel cancer therapies.

Author

Nasir I, McGuinness C, Poh AR, Ernst M, Darcy PK, and Britt KL

Subjects

Humans, Macrophages pathology, Phenotype, Tumor Microenvironment, Neoplasms therapy, Neoplasms pathology

Abstract

Macrophages represent a key component of the tumor microenvironment (TME) and are largely associated with poor prognosis. Therapeutic targeting of macrophages has historically focused on inhibiting their recruitment or reprogramming their phenotype from a protumor (M2-like) to an antitumor (M1-like) one. Unfortunately, this approach has not provided clinical breakthroughs that have changed practice. Emerging studies utilizing single-cell RNA-sequencing (scRNA-seq) and spatial transcriptomics have improved our understanding of the ontogeny, phenotype, and functional plasticity of macrophages. Overlaying the wealth of current information regarding macrophage molecular subtypes and functions has also identified novel therapeutic vulnerabilities that might drive better control of tumor-associated macrophages (TAMs). Here, we discuss the functional profiling of macrophages and provide an update of novel macrophage-targeted therapies in development., Competing Interests: Declaration of interests No interests are declared., (Copyright © 2023 The Authors. Published by Elsevier Ltd.. All rights reserved.)

Published

2023

18. Mechanisms of cellular crosstalk in the gastric tumor microenvironment are mediated by YAP1 and STAT3.

Author

Thilakasiri P, O'Keefe RN, To SQ, Chisanga D, Eissmann MF, Carli AL, Duscio B, Baloyan D, Dmello RS, Williams D, Mariadason J, Poh AR, Pal B, Kile BT, Vissers JH, Harvey KF, Buchert M, Shi W, Ernst M, and Chand AL

Subjects

Humans, Tumor Microenvironment, Adaptor Proteins, Signal Transducing genetics, Adaptor Proteins, Signal Transducing metabolism, Transcription Factors genetics, Transcription Factors metabolism, Hippo Signaling Pathway, STAT3 Transcription Factor metabolism, Stomach Neoplasms genetics, Stomach Neoplasms metabolism, Stomach Neoplasms pathology

Abstract

Deregulation of the Hippo pathway is a driver for cancer progression and treatment resistance. In the context of gastric cancer, YAP1 is a biomarker for poor patient prognosis. Although genomic tumor profiling provides information of Hippo pathway activation, the present study demonstrates that inhibition of Yap1 activity has anti-tumor effects in gastric tumors driven by oncogenic mutations and inflammatory cytokines. We show that Yap1 is a key regulator of cell metabolism, proliferation, and immune responses in normal and neoplastic gastric epithelium. We propose that the Hippo pathway is targetable across gastric cancer subtypes and its therapeutic benefits are likely to be mediated by both cancer cell-intrinsic and -extrinsic mechanisms., (© 2023 Thilakasiri et al.)

Published

2023

19. A tuft cell - ILC2 signaling circuit provides therapeutic targets to inhibit gastric metaplasia and tumor development.

Author

O'Keefe RN, Carli ALE, Baloyan D, Chisanga D, Shi W, Afshar-Sterle S, Eissmann MF, Poh AR, Pal B, Seillet C, Locksley RM, Ernst M, and Buchert M

Subjects

Humans, Mice, Animals, Interleukin-13 metabolism, Lymphocytes metabolism, Hyperplasia metabolism, Metaplasia metabolism, Immunity, Innate, Stomach Neoplasms pathology

Abstract

Although gastric cancer is a leading cause of cancer-related deaths, systemic treatment strategies remain scarce. Here, we report the pro-tumorigenic properties of the crosstalk between intestinal tuft cells and type 2 innate lymphoid cells (ILC2) that is evolutionarily optimized for epithelial remodeling in response to helminth infection. We demonstrate that tuft cell-derived interleukin 25 (IL25) drives ILC2 activation, inducing the release of IL13 and promoting epithelial tuft cell hyperplasia. While the resulting tuft cell - ILC2 feed-forward circuit promotes gastric metaplasia and tumor formation, genetic depletion of tuft cells or ILC2s, or therapeutic targeting of IL13 or IL25 alleviates these pathologies in mice. In gastric cancer patients, tuft cell and ILC2 gene signatures predict worsening survival in intestinal-type gastric cancer where ~40% of the corresponding cancers show enriched co-existence of tuft cells and ILC2s. Our findings suggest a role for ILC2 and tuft cells, along with their associated cytokine IL13 and IL25 as gatekeepers and enablers of metaplastic transformation and gastric tumorigenesis, thereby providing an opportunity to therapeutically inhibit early-stage gastric cancer through repurposing antibody-mediated therapies., (© 2023. The Author(s).)

Published

2023

20. Editorial: Overcoming drug relapse and therapy resistance in NSCLC.

Author

Parakh S, Leong TL, Best SA, and Poh AR

Abstract

Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published

2023

21. Functional roles of SRC signaling in pancreatic cancer: Recent insights provide novel therapeutic opportunities.

Author

Poh AR and Ernst M

Subjects

Humans, Cell Line, Tumor, Signal Transduction, Cell Proliferation, Cell Movement, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, Pancreatic Neoplasms drug therapy, Pancreatic Neoplasms genetics, Pancreatic Neoplasms metabolism, Carcinoma, Pancreatic Ductal genetics

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an aggressive malignant disease with a 5-year survival rate of <10%. Aberrant activation or elevated expression of the tyrosine kinase c-SRC (SRC) is frequently observed in PDAC and is associated with a poor prognosis. Preclinical studies have revealed a multifaceted role for SRC activation in PDAC, including promoting chronic inflammation, tumor cell proliferation and survival, cancer cell stemness, desmoplasia, hypoxia, angiogenesis, invasion, metastasis, and drug resistance. Strategies to inhibit SRC signaling include suppressing its catalytic activity, inhibiting protein stability, or by interfering with signaling components of the SRC signaling pathway including suppressing protein interactions of SRC. In this review, we discuss the molecular and immunological mechanisms by which aberrant SRC activity promotes PDAC tumorigenesis. We also provide a comprehensive update of SRC inhibitors in the clinic, and discuss the clinical challenges associated with targeting SRC in pancreatic cancer., (© 2023. The Author(s).)

Published

2023

22. Longitudinal quantification of mouse gastric tumor organoid viability and growth using luminescence and microscopy.

Author

Morrow RJ, Ernst M, and Poh AR

Subjects

Animals, Mice, Microscopy, Luminescence, Organoids pathology, Stomach Neoplasms, Antineoplastic Agents pharmacology

Abstract

Tumor-derived organoids are valuable for testing anti-cancer drugs in vitro, but existing lysis-based protocols for viability measurement are laborious and restricted at a single time point. Here, we provide a lysis-free protocol for longitudinal and rapid assessment of mouse gastric tumor organoid viability and growth. We describe organoid plating, viability assessment via luminescence measurement, quantification of organoid growth by microscopy imaging, and treatment of organoids with test compounds to evaluate the effects on viability and growth at various time points., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2023 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2023

23. An intrasplenic injection model of pancreatic cancer metastasis to the liver in mice.

Author

O'Brien M, Ernst M, and Poh AR

Subjects

Mice, Animals, Neoplasm Transplantation, Pancreatic Neoplasms, Pancreatic Neoplasms pathology, Liver Neoplasms pathology

Abstract

Here, we provide a protocol for an intrasplenic injection model to establish pancreatic tumors in the mouse liver. We describe the steps to inject tumor cells into mouse spleen and to perform a splenectomy, followed by animal recovery and end point analysis of tumors in the liver. This model allows rapid and reproducible tumor growth in a clinically relevant metastatic site, providing a platform to evaluate the efficacy of anti-cancer drugs. This technique can be expanded to other cancer cell lines. For complete details on the use and execution of this protocol, please refer to Poh et al. (2022). 1 ., Competing Interests: Declaration of interests The authors declare no competing interests., (Copyright © 2022 The Author(s). Published by Elsevier Inc. All rights reserved.)

Published

2023

24. Tumor Growth Remains Refractory to Myc Ablation in Host Macrophages.

Author

Morrow RJ, Allam AH, Konecnik J, Baloyan D, Dijkstra C, Eissmann MF, Jacob SP, O'Brien M, Poh AR, and Ernst M

Subjects

Mice, Animals, Myeloid Cells metabolism, Tumor Microenvironment, Macrophages metabolism, Neoplasms metabolism

Abstract

Aberrant expression of the oncoprotein c-Myc (Myc) is frequently observed in solid tumors and is associated with reduced overall survival. In addition to well-recognized cancer cell-intrinsic roles of Myc, studies have also suggested tumor-promoting roles for Myc in cells of the tumor microenvironment, including macrophages and other myeloid cells. Here, we benchmark Myc inactivation in tumor cells against the contribution of its expression in myeloid cells of murine hosts that harbor endogenous or allograft tumors. Surprisingly, we observe that LysM Cre -mediated Myc ablation in host macrophages does not attenuate tumor growth regardless of immunogenicity, the cellular origin of the tumor, the site it develops, or the stage along the tumor progression cascade. Likewise, we find no evidence for Myc ablation to revert or antagonize the polarization of alternatively activated immunosuppressive macrophages. Thus, we surmise that systemic targeting of Myc activity may confer therapeutic benefits primarily through limiting Myc activity in tumor cells rather than reinvigorating the anti-tumor activity of macrophages.

Published

2022

25. Inhibition of HCK in myeloid cells restricts pancreatic tumor growth and metastasis.

Author

Poh AR, O'Brien M, Chisanga D, He H, Baloyan D, Traichel J, Dijkstra C, Chopin M, Nutt S, Whitehead L, Boon L, Parkin A, Lowell C, Pajic M, Shi W, Nikfarjam M, and Ernst M

Subjects

Animals, Mice, Myeloid Cells metabolism, Tumor Microenvironment, Carcinoma, Pancreatic Ductal genetics, Pancreatic Neoplasms pathology, Proto-Oncogene Proteins c-hck genetics

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an aggressive disease with a low 5-year survival rate and is associated with poor response to therapy. Elevated expression of the myeloid-specific hematopoietic cell kinase (HCK) is observed in PDAC and correlates with reduced patient survival. To determine whether aberrant HCK signaling in myeloid cells is involved in PDAC growth and metastasis, we established orthotopic and intrasplenic PDAC tumors in wild-type and HCK knockout mice. Genetic ablation of HCK impaired PDAC growth and metastasis by inducing an immune-stimulatory endotype in myeloid cells, which in turn reduced the desmoplastic microenvironment and enhanced cytotoxic effector cell infiltration. Consequently, genetic ablation or therapeutic inhibition of HCK minimized metastatic spread, enhanced the efficacy of chemotherapy, and overcame resistance to anti-PD1, anti-CTLA4, or stimulatory anti-CD40 immunotherapy. Our results provide strong rationale for HCK to be developed as a therapeutic target to improve the response of PDAC to chemo- and immunotherapy., Competing Interests: Declaration of interests A.R.P. and M.E. are inventors on a patent application related to this work filed by The Olivia Newton-John Cancer Research Institute (PCT/AU2021/051073) on the 16(th) of September 2021., (Copyright © 2022 The Authors. Published by Elsevier Inc. All rights reserved.)

Published

2022

26. Therapeutic inhibition of the SRC-kinase HCK facilitates T cell tumor infiltration and improves response to immunotherapy.

Author

Poh AR, Love CG, Chisanga D, Steer JH, Baloyan D, Chopin M, Nutt S, Rautela J, Huntington ND, Etemadi N, O'Brien M, O'Keefe R, Ellies LG, Macri C, Mintern JD, Whitehead L, Gangadhara G, Boon L, Chand AL, Lowell CA, Shi W, Pixley FJ, and Ernst M

Abstract

Although immunotherapy has revolutionized cancer treatment, many immunogenic tumors remain refractory to treatment. This can be largely attributed to an immunologically "cold" tumor microenvironment characterized by an accumulation of immunosuppressive myeloid cells and exclusion of activated T cells. Here, we demonstrate that genetic ablation or therapeutic inhibition of the myeloid-specific hematopoietic cell kinase (HCK) enables activity of antagonistic anti-programmed cell death protein 1 (anti-PD1), anti-CTLA4, or agonistic anti-CD40 immunotherapies in otherwise refractory tumors and augments response in treatment-susceptible tumors. Mechanistically, HCK ablation reprograms tumor-associated macrophages and dendritic cells toward an inflammatory endotype and enhances CD8 + T cell recruitment and activation when combined with immunotherapy in mice. Meanwhile, therapeutic inhibition of HCK in humanized mice engrafted with patient-derived xenografts counteracts tumor immunosuppression, improves T cell recruitment, and impairs tumor growth. Collectively, our results suggest that therapeutic targeting of HCK activity enhances response to immunotherapy by simultaneously stimulating immune cell activation and inhibiting the immunosuppressive tumor microenvironment.

Published

2022

27. Multicellular Effects of STAT3 in Non-small Cell Lung Cancer: Mechanistic Insights and Therapeutic Opportunities.

Author

Parakh S, Ernst M, and Poh AR

Abstract

Non-small cell lung cancer (NSCLC) is the most common type of lung cancer and accounts for 85% of lung cancer cases. Aberrant activation of the Signal Transducer and Activator of Transcription 3 (STAT3) is frequently observed in NSCLC and is associated with a poor prognosis. Pre-clinical studies have revealed an unequivocal role for tumor cell-intrinsic and extrinsic STAT3 signaling in NSCLC by promoting angiogenesis, cell survival, cancer cell stemness, drug resistance, and evasion of anti-tumor immunity. Several STAT3-targeting strategies have also been investigated in pre-clinical models, and include preventing upstream receptor/ligand interactions, promoting the degradation of STAT3 mRNA, and interfering with STAT3 DNA binding. In this review, we discuss the molecular and immunological mechanisms by which persistent STAT3 activation promotes NSCLC development, and the utility of STAT3 as a prognostic and predictive biomarker in NSCLC. We also provide a comprehensive update of STAT3-targeting therapies that are currently undergoing clinical evaluation, and discuss the challenges associated with these treatment modalities in human patients.

Published

2021

28. Correction: BCL-XL is an actionable target for treatment of malignant pleural mesothelioma.

Author

Arulananda S, O'Brien M, Evangelista M, Harris TJ, Steinohrt NS, Jenkins LJ, Walkiewicz M, O'Donoghue RJJ, Poh AR, Thapa B, Williams DS, Leong T, Mariadason JM, Li X, Cebon J, Lee EF, John T, and Fairlie WD

Published

2021

29. Tumor-Associated Macrophages in Pancreatic Ductal Adenocarcinoma: Therapeutic Opportunities and Clinical Challenges.

Author

Poh AR and Ernst M

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is an aggressive malignant disease with a 5-year survival rate of less than 10%. Macrophages are one of the earliest infiltrating cells in the pancreatic tumor microenvironment, and are associated with an increased risk of disease progression, recurrence, metastasis, and shorter overall survival. Pre-clinical studies have demonstrated an unequivocal role of macrophages in PDAC by contributing to chronic inflammation, cancer cell stemness, desmoplasia, immune suppression, angiogenesis, invasion, metastasis, and drug resistance. Several macrophage-targeting therapies have also been investigated in pre-clinical models, and include macrophage depletion, inhibiting macrophage recruitment, and macrophage reprogramming. However, the effectiveness of these drugs in pre-clinical models has not always translated into clinical trials. In this review, we discuss the molecular mechanisms that underpin macrophage heterogeneity within the pancreatic tumor microenvironment, and examine the contribution of macrophages at various stages of PDAC progression. We also provide a comprehensive update of macrophage-targeting therapies that are currently undergoing clinical evaluation, and discuss clinical challenges associated with these treatment modalities in human PDAC patients.

Published

2021

30. A novel BH3-mimetic, AZD0466, targeting BCL-XL and BCL-2 is effective in pre-clinical models of malignant pleural mesothelioma.

Author

Arulananda S, O'Brien M, Evangelista M, Jenkins LJ, Poh AR, Walkiewicz M, Leong T, Mariadason JM, Cebon J, Balachander SB, Cidado JR, Lee EF, John T, and Fairlie WD

Abstract

Malignant pleural mesothelioma (MPM) is an aggressive cancer with treatment limited to Cisplatin and Pemetrexed chemotherapy. Recently, we showed that drugs targeting the BCL-2-regulated apoptosis pathway could kill MPM cell lines in vitro, and control tumor growth in vivo. These studies showed BCL-XL was the dominant pro-survival BCL-2 family member correlating with its high-level expression in cells and patient tumor samples. In this study we show another inhibitor, AZD4320 that targets BCL-XL (and BCL-2), can also potently kill MPM tumor cells in vitro (EC 50 values in the 200 nM range) and this effect is enhanced by co-inhibition of MCL-1 using AZD5991. Moreover, we show that a novel nanoparticle, AZD0466, where AZD4320 is chemically conjugated to a PEGylated poly-lysine dendrimer, was as effective as standard-of-care chemotherapy, Cisplatin, at inhibiting tumor growth in mouse xenograft studies, and this effect was enhanced when both drugs were combined. Critically, the degree of thrombocytopenia, an on-target toxicity associated with BCL-XL inhibition, was significantly reduced throughout the treatment period compared to other BCL-XL-targeting BH3-mimetics. These pre-clinical findings provide a rationale for the future clinical evaluation for novel BH3-mimetic formulations in MPM, and indeed, other solid tumor types dependent on BCL-XL.

Published

2021

31. BCL-XL is an actionable target for treatment of malignant pleural mesothelioma.

Author

Arulananda S, O'Brien M, Evangelista M, Harris TJ, Steinohrt NS, Jenkins LJ, Walkiewicz M, O'Donoghue RJJ, Poh AR, Thapa B, Williams DS, Leong T, Mariadason JM, Li X, Cebon J, Lee EF, John T, and Fairlie WD

Abstract

Despite having one of the lowest survival rates of all cancers, there have been no new approved treatments for malignant pleural mesothelioma (MPM) in over a decade. Standard-of-care treatment relies on Cisplatin plus Pemetrexed chemotherapy. Here, we tested a suite of BH3-mimetic drugs targeting BCL-2 pro-survival proteins of the intrinsic apoptotic pathway. We found BCL-XL is the dominant pro-survival protein in a panel of cell lines in vitro, though potent, synergistic cell killing occurred with MCL-1 co-targeting. This correlates with high-level expression of BCL-XL and MCL-1 in cell lines and a large cohort of patient tumour samples. BCL-XL inhibition combined with Cisplatin also enhanced cell killing. In vivo BCL-XL inhibition was as effective as Cisplatin, and the combination enhanced tumour growth control and survival. Genetic ablation of MCL-1 also enhanced the effects of BCL-XL inhibitors, in vivo. Combined, these data provide a compelling rationale for the clinical investigation of BH3-mimetics targeting BCL-XL in MPM.

Published

2020

32. Inhibition of the SRC Kinase HCK Impairs STAT3-Dependent Gastric Tumor Growth in Mice.

Author

Poh AR, Dwyer AR, Eissmann MF, Chand AL, Baloyan D, Boon L, Murrey MW, Whitehead L, O'Brien M, Lowell CA, Putoczki TL, Pixley FJ, O'Donoghue RJJ, and Ernst M

Subjects

Animals, Female, Humans, Macrophage Activation drug effects, Male, Mice, Mice, Transgenic, Phosphorylation drug effects, Proto-Oncogene Proteins c-hck metabolism, Stomach Neoplasms metabolism, Stomach Neoplasms pathology, Survival Rate, Proto-Oncogene Proteins c-hck antagonists & inhibitors, Pyrimidines pharmacology, Pyrroles pharmacology, STAT3 Transcription Factor metabolism, Stomach Neoplasms drug therapy

Abstract

Persistent activation of the latent transcription factor STAT3 is observed in gastric tumor epithelial and immune cells and is associated with a poor patient prognosis. Although targeting STAT3-activating upstream kinases offers therapeutically viable targets with limited specificity, direct inhibition of STAT3 remains challenging. Here we provide functional evidence that myeloid-specific hematopoietic cell kinase (HCK) activity can drive STAT3-dependent epithelial tumor growth in mice and is associated with alternative macrophage activation alongside matrix remodeling and tumor cell invasion. Accordingly, genetic reduction of HCK expression in bone marrow-derived cells or systemic pharmacologic inhibition of HCK activity suppresses alternative macrophage polarization and epithelial STAT3 activation, and impairs tumor growth. These data validate HCK as a molecular target for the treatment of human solid tumors harboring excessive STAT3 activity., (©2020 American Association for Cancer Research.)

Published

2020

33. Loss of Bcl-G, a Bcl-2 family member, augments the development of inflammation-associated colorectal cancer.

Author

Nguyen PM, Dagley LF, Preaudet A, Lam N, Giam M, Fung KY, Aizel K, van Duijneveldt G, Tan CW, Hirokawa Y, Yip HYK, Love CG, Poh AR, Cruz A, Burstroem C, Feltham R, Abdirahman SM, Meiselbach K, Low RRJ, Palmieri M, Ernst M, Webb AI, Burgess T, Sieber OM, Bouillet P, and Putoczki TL

Subjects

Animals, Colitis metabolism, Colitis pathology, Colorectal Neoplasms pathology, Humans, Inflammation pathology, Mice, Mice, Knockout, Proto-Oncogene Proteins c-bcl-2 deficiency, Proto-Oncogene Proteins c-bcl-2 genetics, Colorectal Neoplasms metabolism, Inflammation metabolism, Proto-Oncogene Proteins c-bcl-2 metabolism

Abstract

Gastrointestinal epithelial cells provide a selective barrier that segregates the host immune system from luminal microorganisms, thereby contributing directly to the regulation of homeostasis. We have shown that from early embryonic development Bcl-G, a Bcl-2 protein family member with unknown function, was highly expressed in gastrointestinal epithelial cells. While Bcl-G was dispensable for normal growth and development in mice, the loss of Bcl-G resulted in accelerated progression of colitis-associated cancer. A label-free quantitative proteomics approach revealed that Bcl-G may contribute to the stability of a mucin network, which when disrupted, is linked to colon tumorigenesis. Consistent with this, we observed a significant reduction in Bcl-G expression in human colorectal tumors. Our study identifies an unappreciated role for Bcl-G in colon cancer.

Published

2020

34. IL-33-mediated mast cell activation promotes gastric cancer through macrophage mobilization.

Author

Eissmann MF, Dijkstra C, Jarnicki A, Phesse T, Brunnberg J, Poh AR, Etemadi N, Tsantikos E, Thiem S, Huntington ND, Hibbs ML, Boussioutas A, Grimbaldeston MA, Buchert M, O'Donoghue RJJ, Masson F, and Ernst M

Subjects

Aminopyridines administration & dosage, Animals, Cell Degranulation drug effects, Cell Degranulation immunology, Cromolyn Sodium administration & dosage, Disease Models, Animal, Epithelium immunology, Epithelium pathology, Female, Gastric Mucosa cytology, Gastric Mucosa immunology, Gastric Mucosa pathology, Humans, Interleukin-1 Receptor-Like 1 Protein immunology, Interleukin-1 Receptor-Like 1 Protein metabolism, Interleukin-33 metabolism, Male, Mice, Mice, Transgenic, Pyrroles administration & dosage, Signal Transduction drug effects, Signal Transduction immunology, Stomach Neoplasms genetics, Stomach Neoplasms mortality, Stomach Neoplasms pathology, Tissue Array Analysis, Tumor Microenvironment immunology, Interleukin-33 immunology, Macrophages immunology, Mast Cells immunology, Stomach Neoplasms immunology

Abstract

The contribution of mast cells in the microenvironment of solid malignancies remains controversial. Here we functionally assess the impact of tumor-adjacent, submucosal mast cell accumulation in murine and human intestinal-type gastric cancer. We find that genetic ablation or therapeutic inactivation of mast cells suppresses accumulation of tumor-associated macrophages, reduces tumor cell proliferation and angiogenesis, and diminishes tumor burden. Mast cells are activated by interleukin (IL)-33, an alarmin produced by the tumor epithelium in response to the inflammatory cytokine IL-11, which is required for the growth of gastric cancers in mice. Accordingly, ablation of the cognate IL-33 receptor St2 limits tumor growth, and reduces mast cell-dependent production and release of the macrophage-attracting factors Csf2, Ccl3, and Il6. Conversely, genetic or therapeutic macrophage depletion reduces tumor burden without affecting mast cell abundance. Therefore, tumor-derived IL-33 sustains a mast cell and macrophage-dependent signaling cascade that is amenable for the treatment of gastric cancer.

Published

2019

35. Repurposing the selective estrogen receptor modulator bazedoxifene to suppress gastrointestinal cancer growth.

Author

Thilakasiri P, Huynh J, Poh AR, Tan CW, Nero TL, Tran K, Parslow AC, Afshar-Sterle S, Baloyan D, Hannan NJ, Buchert M, Scott AM, Griffin MD, Hollande F, Parker MW, Putoczki TL, Ernst M, and Chand AL

Subjects

Adenomatous Polyposis Coli Protein genetics, Animals, Cell Proliferation drug effects, Cytokine Receptor gp130 chemistry, Cytokine Receptor gp130 metabolism, Disease Models, Animal, Female, Gastrointestinal Neoplasms pathology, Humans, Indoles metabolism, Indoles pharmacology, Interleukin-11 chemistry, Interleukin-11 metabolism, Interleukin-11 pharmacology, Male, Mice, Mice, Inbred C57BL, Mice, Transgenic, STAT3 Transcription Factor metabolism, Selective Estrogen Receptor Modulators metabolism, Selective Estrogen Receptor Modulators pharmacology, Signal Transduction drug effects, Xenograft Model Antitumor Assays, beta Catenin metabolism, Drug Repositioning, Gastrointestinal Neoplasms drug therapy, Indoles therapeutic use, Selective Estrogen Receptor Modulators therapeutic use

Abstract

Excessive signaling through gp130, the shared receptor for the interleukin (IL)6 family of cytokines, is a common hallmark in solid malignancies and promotes their progression. Here, we established the in vivo utility of bazedoxifene, a steroid analog clinically approved for the treatment of osteoporosis, to suppress gp130-dependent tumor growth of the gastrointestinal epithelium. Bazedoxifene administration reduced gastric tumor burden in gp130 Y757F mice, where tumors arise exclusively through excessive gp130/STAT3 signaling in response to the IL6 family cytokine IL11. Likewise, in mouse models of sporadic colon and intestinal cancers, which arise from oncogenic mutations in the tumor suppressor gene Apc and the associated β-catenin/canonical WNT pathway, bazedoxifene treatment reduces tumor burden. Consistent with the proposed orthogonal tumor-promoting activity of IL11-dependent gp130/STAT3 signaling, tumors of bazedoxifene -treated Apc -mutant mice retain excessive nuclear accumulation of β-catenin and aberrant WNT pathway activation. Likewise, bazedoxifene treatment of human colon cancer cells harboring mutant APC did not reduce aberrant canonical WNT signaling, but suppressed IL11-dependent STAT3 signaling. Our findings provide compelling proof of concept to support the repurposing of bazedoxifene for the treatment of gastrointestinal cancers in which IL11 plays a tumor-promoting role., (© 2019 The Authors. Published under the terms of the CC BY 4.0 license.)

Published

2019

36. Targeting Macrophages in Cancer: From Bench to Bedside.

Author

Poh AR and Ernst M

Abstract

Macrophages are a major component of the tumor microenvironment and orchestrate various aspects of immunity. Within tumors, macrophages can reversibly alter their endotype in response to environmental cues, including hypoxia and stimuli derived from other immune cells, as well as the extracellular matrix. Depending on their activation status, macrophages can exert dual influences on tumorigenesis by either antagonizing the cytotoxic activity immune cells or by enhancing antitumor responses. In most solid cancers, increased infiltration with tumor-associated macrophages (TAMs) has long been associated with poor patient prognosis, highlighting their value as potential diagnostic and prognostic biomarkers in cancer. A number of macrophage-centered approaches to anticancer therapy have been investigated, and include strategies to block their tumor-promoting activities or exploit their antitumor effector functions. Integrating therapeutic strategies to target TAMs to complement conventional therapies has yielded promising results in preclinical trials and warrants further investigation to determine its translational benefit in human cancer patients. In this review, we discuss the molecular mechanisms underlying the pro-tumorigenic programming of macrophages and provide a comprehensive update of macrophage-targeted therapies for the treatment of solid cancers.

Published

2018

37. Targeting H(i)ck education for cancer therapy?

Author

Ernst M, O'Donoghue RJJ, and Poh AR

Abstract

Competing Interests: CONFLICTS OF INTEREST The authors declare no conflicts of interest.

Published

2017

38. Inhibition of Hematopoietic Cell Kinase Activity Suppresses Myeloid Cell-Mediated Colon Cancer Progression.

Author

Poh AR, Love CG, Masson F, Preaudet A, Tsui C, Whitehead L, Monard S, Khakham Y, Burstroem L, Lessene G, Sieber O, Lowell C, Putoczki TL, O'Donoghue RJJ, and Ernst M

Subjects

Animals, Colonic Neoplasms genetics, Colonic Neoplasms metabolism, Colorectal Neoplasms genetics, Colorectal Neoplasms pathology, Female, Gene Expression Regulation, Neoplastic, Humans, Macrophage Activation genetics, Mice, Inbred C57BL, Mice, Knockout, Proto-Oncogene Proteins c-hck antagonists & inhibitors, Proto-Oncogene Proteins c-hck genetics, Pyrimidines pharmacology, Pyrroles pharmacology, STAT3 Transcription Factor metabolism, Signal Transduction, Stromal Cells metabolism, Xenograft Model Antitumor Assays, Colonic Neoplasms pathology, Colorectal Neoplasms metabolism, Colorectal Neoplasms mortality, Proto-Oncogene Proteins c-hck metabolism

Abstract

Aberrant activation of the SRC family kinase hematopoietic cell kinase (HCK) triggers hematological malignancies as a tumor cell-intrinsic oncogene. Here we find that high HCK levels correlate with reduced survival of colorectal cancer patients. Likewise, increased Hck activity in mice promotes the growth of endogenous colonic malignancies and of human colorectal cancer cell xenografts. Furthermore, tumor-associated macrophages of the corresponding tumors show a pronounced alternatively activated endotype, which occurs independently of mature lymphocytes or of Stat6-dependent Th2 cytokine signaling. Accordingly, pharmacological inhibition or genetic reduction of Hck activity suppresses alternative activation of tumor-associated macrophages and the growth of colon cancer xenografts. Thus, Hck may serve as a promising therapeutic target for solid malignancies., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

39. Mouse models for gastric cancer: Matching models to biological questions.

Author

Poh AR, O'Donoghue RJ, Ernst M, and Putoczki TL

Subjects

Animals, Gastrins, Helicobacter Infections, Helicobacter felis, Helicobacter pylori, Methylnitrosourea, Molecular Targeted Therapy, Stomach Neoplasms classification, Stomach Neoplasms genetics, Stomach Neoplasms therapy, Disease Models, Animal, Mice, Inbred Strains, Mice, Transgenic, Stomach Neoplasms etiology

Abstract

Gastric cancer is the third leading cause of cancer-related mortality worldwide. This is in part due to the asymptomatic nature of the disease, which often results in late-stage diagnosis, at which point there are limited treatment options. Even when treated successfully, gastric cancer patients have a high risk of tumor recurrence and acquired drug resistance. It is vital to gain a better understanding of the molecular mechanisms underlying gastric cancer pathogenesis to facilitate the design of new-targeted therapies that may improve patient survival. A number of chemically and genetically engineered mouse models of gastric cancer have provided significant insight into the contribution of genetic and environmental factors to disease onset and progression. This review outlines the strengths and limitations of current mouse models of gastric cancer and their relevance to the pre-clinical development of new therapeutics., (© 2016 The Authors Journal of Gastroenterology and Hepatology published by Journal of Gastroenterology and Hepatology Foundation and John Wiley & Sons Australia, Ltd.)

Published

2016

40. Hematopoietic cell kinase (HCK) as a therapeutic target in immune and cancer cells.

Author

Poh AR, O'Donoghue RJ, and Ernst M

Subjects

Animals, Cell Proliferation physiology, Humans, Signal Transduction, Neoplasms immunology, Neoplasms therapy, Proto-Oncogene Proteins c-hck immunology

Abstract

The hematopoietic cell kinase (HCK) is a member of the SRC family of cytoplasmic tyrosine kinases (SFKs), and is expressed in cells of the myeloid and B-lymphocyte cell lineages. Excessive HCK activation is associated with several types of leukemia and enhances cell proliferation and survival by physical association with oncogenic fusion proteins, and with functional interactions with receptor tyrosine kinases. Elevated HCK activity is also observed in many solid malignancies, including breast and colon cancer, and correlates with decreased patient survival rates. HCK enhances the secretion of growth factors and pro-inflammatory cytokines from myeloid cells, and promotes macrophage polarization towards a wound healing and tumor-promoting alternatively activated phenotype. Within tumor associated macrophages, HCK stimulates the formation of podosomes that facilitate extracellular matrix degradation, which enhance immune and epithelial cell invasion. By virtue of functional cooperation between HCK and bona fide oncogenic tyrosine kinases, excessive HCK activation can also reduce drug efficacy and contribute to chemo-resistance, while genetic ablation of HCK results in minimal physiological consequences in healthy mice. Given its known crystal structure, HCK therefore provides an attractive therapeutic target to both, directly inhibit the growth of cancer cells, and indirectly curb the source of tumor-promoting changes in the tumor microenvironment.

Published

2015

41. Partial inhibition of gp130-Jak-Stat3 signaling prevents Wnt-β-catenin-mediated intestinal tumor growth and regeneration.

Author

Phesse TJ, Buchert M, Stuart E, Flanagan DJ, Faux M, Afshar-Sterle S, Walker F, Zhang HH, Nowell CJ, Jorissen R, Tan CW, Hirokawa Y, Eissmann MF, Poh AR, Malaterre J, Pearson HB, Kirsch DG, Provero P, Poli V, Ramsay RG, Sieber O, Burgess AW, Huszar D, Vincan E, and Ernst M

Subjects

Animals, Colonic Neoplasms genetics, Cytokine Receptor gp130 metabolism, DNA Primers genetics, Female, Gene Expression Regulation, Neoplastic genetics, Histological Techniques, Immunohistochemistry, Janus Kinase 1 metabolism, Luciferases, Mice, Mice, Inbred BALB C, Microscopy, Fluorescence, Polycomb Repressive Complex 1 metabolism, Proto-Oncogene Proteins metabolism, Reverse Transcriptase Polymerase Chain Reaction, STAT3 Transcription Factor metabolism, Wnt Signaling Pathway genetics, Colonic Neoplasms metabolism, Gene Expression Regulation, Neoplastic physiology, Genes, APC physiology, Intestinal Mucosa physiology, Regeneration physiology, Wnt Signaling Pathway physiology, beta Catenin metabolism

Abstract

Most colon cancers arise from somatic mutations in the tumor suppressor gene APC (adenomatous polyposis coli), and these mutations cause constitutive activation of the Wnt-to-β-catenin pathway in the intestinal epithelium. Because Wnt-β-catenin signaling is required for homeostasis and regeneration of the adult intestinal epithelium, therapeutic targeting of this pathway is challenging. We found that genetic activation of the cytokine-stimulated pathway mediated by the receptor gp130, the associated Jak (Janus kinase) kinases, and the transcription factor Stat3 (signal transducer and activator of transcription 3) was required for intestinal regeneration in response to irradiation-induced damage in wild-type mice and for tumorigenesis in Apc-mutant mice. Systemic pharmacological or partial genetic inhibition of gp130-Jak-Stat3 signaling suppressed intestinal regeneration, the growth of tumors in Apc-mutant mice, and the growth of colon cancer xenografts. The growth of Apc-mutant tumors depended on gp130-Jak-Stat3 signaling for induction of the polycomb repressor Bmi-1, and the associated repression of genes encoding the cell cycle inhibitors p16 and p21. However, suppression of gp130-Jak-Stat3 signaling did not affect Wnt-β-catenin signaling or homeostasis in the intestine. Thus, these data not only suggest a molecular mechanism for how the gp130-Jak-Stat3 pathway can promote cancer but also provide a rationale for therapeutic inhibition of Jak in colon cancer., (Copyright © 2014, American Association for the Advancement of Science.)

Published

2014

42. RIPK1 regulates RIPK3-MLKL-driven systemic inflammation and emergency hematopoiesis.

Author

Rickard JA, O'Donnell JA, Evans JM, Lalaoui N, Poh AR, Rogers T, Vince JE, Lawlor KE, Ninnis RL, Anderton H, Hall C, Spall SK, Phesse TJ, Abud HE, Cengia LH, Corbin J, Mifsud S, Di Rago L, Metcalf D, Ernst M, Dewson G, Roberts AW, Alexander WS, Murphy JM, Ekert PG, Masters SL, Vaux DL, Croker BA, Gerlic M, and Silke J

Subjects

Animals, Animals, Newborn, Caspase 8 metabolism, Cell Death, Liver metabolism, Mice, Mice, 129 Strain, Mice, Inbred C57BL, Myeloid Differentiation Factor 88 genetics, Myeloid Differentiation Factor 88 metabolism, Protein Kinases genetics, Protein Kinases metabolism, Receptor-Interacting Protein Serine-Threonine Kinases genetics, Receptors, Tumor Necrosis Factor, Type I metabolism, Tumor Necrosis Factors metabolism, Genes, Lethal, Hematopoiesis, Inflammation metabolism, Receptor-Interacting Protein Serine-Threonine Kinases metabolism

Abstract

Upon ligand binding, RIPK1 is recruited to tumor necrosis factor receptor superfamily (TNFRSF) and Toll-like receptor (TLR) complexes promoting prosurvival and inflammatory signaling. RIPK1 also directly regulates caspase-8-mediated apoptosis or, if caspase-8 activity is blocked, RIPK3-MLKL-dependent necroptosis. We show that C57BL/6 Ripk1(-/-) mice die at birth of systemic inflammation that was not transferable by the hematopoietic compartment. However, Ripk1(-/-) progenitors failed to engraft lethally irradiated hosts properly. Blocking TNF reversed this defect in emergency hematopoiesis but, surprisingly, Tnfr1 deficiency did not prevent inflammation in Ripk1(-/-) neonates. Deletion of Ripk3 or Mlkl, but not Casp8, prevented extracellular release of the necroptotic DAMP, IL-33, and reduced Myd88-dependent inflammation. Reduced inflammation in the Ripk1(-/-)Ripk3(-/-), Ripk1(-/-)Mlkl(-/-), and Ripk1(-/-)Myd88(-/-) mice prevented neonatal lethality, but only Ripk1(-/-)Ripk3(-/-)Casp8(-/-) mice survived past weaning. These results reveal a key function for RIPK1 in inhibiting necroptosis and, thereby, a role in limiting, not only promoting, inflammation., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014