Your search keyword '"Wong, Kwok"' showing total 45 results

1. Development of a bioengineered Erwinia chrysanthemi asparaginase to enhance its anti-solid tumor potential for treating gastric cancer.

Author

Tam SY, Chung SF, Kim CF, To JC, So PK, Cheung KK, Chung WH, Wong KY, and Leung YC

Subjects

Humans, Animals, Mice, Asparaginase genetics, Asparaginase pharmacology, Asparaginase therapeutic use, Asparagine, Glutamine, Enterobacteriaceae metabolism, Serum Albumin, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Dickeya chrysanthemi genetics, Dickeya chrysanthemi metabolism, Stomach Neoplasms drug therapy

Abstract

Asparaginase has been traditionally applied for only treating acute lymphoblastic leukemia due to its ability to deplete asparagine. However, its ultimate anticancer potential for treating solid tumors has not yet been unleashed. In this study, we bioengineered Erwinia chrysanthemi asparaginase (ErWT), one of the US Food and Drug Administration-approved types of amino acid depleting enzymes, to achieve double amino acid depletions for treating a solid tumor. We constructed a fusion protein by joining an albumin binding domain (ABD) to ErWT via a linker (GGGGS) 5 to achieve ABD-ErS5. The ABD could bind to serum albumin to form an albumin-ABD-ErS5 complex, which could avoid renal clearance and escape from anti-drug antibodies, resulting in a remarkably prolonged elimination half-life of ABD-ErS5. Meanwhile, ABD-ErS5 did not only deplete asparagine but also glutamine for ∼2 weeks. A biweekly administration of ABD-ErS5 (1.5 mg/kg) significantly suppressed tumor growth in an MKN-45 gastric cancer xenograft model, demonstrating a novel approach for treating solid tumor depleting asparagine and glutamine. Multiple administrations of ABD-ErS5 did not cause any noticeable histopathological abnormalities of key organs, suggesting the absence of acute toxicity to mice. Our results suggest ABD-ErS5 is a potential therapeutic candidate for treating gastric cancer., Competing Interests: Declaration of competing interest The authors declare that they have no conflict of interest., (Copyright © 2023. Published by Elsevier B.V.)

Published

2023

2. Combined Inhibition of SHP2 and CXCR1/2 Promotes Antitumor T-cell Response in NSCLC.

Author

Tang KH, Li S, Khodadadi-Jamayran A, Jen J, Han H, Guidry K, Chen T, Hao Y, Fedele C, Zebala JA, Maeda DY, Christensen JG, Olson P, Athanas A, Loomis CA, Tsirigos A, Wong KK, and Neel BG

Subjects

Animals, Antineoplastic Agents therapeutic use, Cell Line, Tumor, Enzyme Inhibitors therapeutic use, Humans, Male, Mice, Mice, Inbred C57BL, Tumor Microenvironment, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Enzyme Inhibitors pharmacology, Lung Neoplasms drug therapy, Protein Tyrosine Phosphatase, Non-Receptor Type 11 antagonists & inhibitors, Receptors, Interleukin-8B antagonists & inhibitors

Abstract

SHP2 inhibitors (SHP2i) alone and in various combinations are being tested in multiple tumors with overactivation of the RAS/ERK pathway. SHP2 plays critical roles in normal cell signaling; hence, SHP2is could influence the tumor microenvironment. We found that SHP2i treatment depleted alveolar and M2-like macrophages, induced tumor-intrinsic CCL5/CXCL10 secretion, and promoted B and T lymphocyte infiltration in Kras - and Egfr -mutant non-small cell lung cancer (NSCLC). However, treatment also increased intratumor granulocytic myeloid-derived suppressor cells (gMDSC) via tumor-intrinsic, NFκB-dependent production of CXCR2 ligands. Other RAS/ERK pathway inhibitors also induced CXCR2 ligands and gMDSC influx in mice, and CXCR2 ligands were induced in tumors from patients on KRAS G12C inhibitor trials. Combined SHP2 (SHP099)/CXCR1/2 (SX682) inhibition depleted a specific cluster of S100a8/9 hi gMDSCs, generated Klrg1 + CD8 + effector T cells with a strong cytotoxic phenotype but expressing the checkpoint receptor NKG2A, and enhanced survival in Kras - and Egfr -mutant models. Our results argue for testing RAS/ERK pathway/CXCR1/2/NKG2A inhibitor combinations in patients with NSCLC. SIGNIFICANCE: Our study shows that inhibiting the SHP2/RAS/ERK pathway triggers NFκB-dependent upregulation of CXCR2 ligands and recruitment of S100A8 hi gMDSCs, which suppress T cells. Combining SHP2/CXCR2 inhibitors blocks gMDSC immigration, resulting in enhanced Th1 polarization, induced CD8 + KLRG1 + effector T cells with high cytotoxic activity, and improved survival in multiple NSCLC models. This article is highlighted in the In This Issue feature, p. 1 ., (©2021 The Authors; Published by the American Association for Cancer Research.)

Published

2022

3. Cellular Origins of EGFR-Driven Lung Cancer Cells Determine Sensitivity to Therapy.

Author

Chen F, Liu J, Flight RM, Naughton KJ, Lukyanchuk A, Edgin AR, Song X, Zhang H, Wong KK, Moseley HNB, Wang C, and Brainson CF

Subjects

Animals, Cell Line, Tumor, Disease Models, Animal, Female, Humans, Male, Mice, Mice, Nude, Precision Medicine methods, Treatment Outcome, Acrylamides therapeutic use, Aniline Compounds therapeutic use, Antineoplastic Agents therapeutic use, ErbB Receptors drug effects, Lung Neoplasms drug therapy, Protein Kinase Inhibitors therapeutic use, Pyrimidines therapeutic use

Abstract

Targeting the epidermal growth factor receptor (EGFR) with tyrosine kinase inhibitors (TKIs) is one of the major precision medicine treatment options for lung adenocarcinoma. Due to common development of drug resistance to first- and second-generation TKIs, third-generation inhibitors, including osimertinib and rociletinib, have been developed. A model of EGFR-driven lung cancer and a method to develop tumors of distinct epigenetic states through 3D organotypic cultures are described here. It is discovered that activation of the EGFR T790M/L858R mutation in lung epithelial cells can drive lung cancers with alveolar or bronchiolar features, which can originate from alveolar type 2 (AT2) cells or bronchioalveolar stem cells, but not basal cells or club cells of the trachea. It is also demonstrated that these clones are able to retain their epigenetic differences through passaging orthotopically in mice and crucially that they have distinct drug vulnerabilities. This work serves as a blueprint for exploring how epigenetics can be used to stratify patients for precision medicine decisions., (© 2021 The Authors. Advanced Science published by Wiley-VCH GmbH.)

Published

2021

4. Mobocertinib (TAK-788): A Targeted Inhibitor of EGFR Exon 20 Insertion Mutants in Non-Small Cell Lung Cancer.

Author

Gonzalvez F, Vincent S, Baker TE, Gould AE, Li S, Wardwell SD, Nadworny S, Ning Y, Zhang S, Huang WS, Hu Y, Li F, Greenfield MT, Zech SG, Das B, Narasimhan NI, Clackson T, Dalgarno D, Shakespeare WC, Fitzgerald M, Chouitar J, Griffin RJ, Liu S, Wong KK, Zhu X, and Rivera VM

Subjects

Aniline Compounds pharmacology, Animals, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung genetics, Cell Line, Tumor drug effects, ErbB Receptors, Humans, Indoles pharmacology, Lung Neoplasms genetics, Mice, Mutagenesis, Insertional, Pyrimidines pharmacology, Xenograft Model Antitumor Assays, Aniline Compounds therapeutic use, Antineoplastic Agents therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Exons, Indoles therapeutic use, Lung Neoplasms drug therapy, Pyrimidines therapeutic use

Abstract

Most EGFR exon 20 insertion ( EGFR ex20ins) driver mutations in non-small cell lung cancer (NSCLC) are insensitive to approved EGFR tyrosine kinase inhibitors (TKI). To address the limitations of existing therapies targeting EGFR -mutated NSCLC, mobocertinib (TAK-788), a novel irreversible EGFR TKI, was specifically designed to potently inhibit oncogenic variants containing activating EGFR ex20ins mutations with selectivity over wild-type EGFR. The in vitro and in vivo activity of mobocertinib was evaluated in engineered and patient-derived models harboring diverse EGFR ex20ins mutations. Mobocertinib inhibited viability of various EGFRex20ins-driven cell lines more potently than approved EGFR TKIs and demonstrated in vivo antitumor efficacy in patient-derived xenografts and murine orthotopic models. These findings support the ongoing clinical development of mobocertinib for the treatment of EGFR ex20ins-mutated NSCLC. SIGNIFICANCE: No oral EGFR-targeted therapies are approved for EGFR exon 20 insertion ( EGFR ex20ins) mutation-driven NSCLC. Mobocertinib is a novel small-molecule EGFR inhibitor specifically designed to target EGFRex20ins mutants. Preclinical data reported here support the clinical development of mobocertinib in patients with NSCLC with EGFR exon 20 insertion mutations. See related commentary by Pacheco, p. 1617 . This article is highlighted in the In This Issue feature, p. 1601 ., (©2021 American Association for Cancer Research.)

Published

2021

5. The KRAS G12C Inhibitor MRTX849 Reconditions the Tumor Immune Microenvironment and Sensitizes Tumors to Checkpoint Inhibitor Therapy.

Author

Briere DM, Li S, Calinisan A, Sudhakar N, Aranda R, Hargis L, Peng DH, Deng J, Engstrom LD, Hallin J, Gatto S, Fernandez-Banet J, Pavlicek A, Wong KK, Christensen JG, and Olson P

Subjects

Animals, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cell Proliferation, Disease Models, Animal, Humans, Immune Checkpoint Inhibitors pharmacology, Mice, Tumor Microenvironment drug effects, Acetonitriles antagonists & inhibitors, Antineoplastic Agents therapeutic use, Immune Checkpoint Inhibitors therapeutic use, Piperazines antagonists & inhibitors, Proto-Oncogene Proteins p21(ras) antagonists & inhibitors, Pyrimidines antagonists & inhibitors

Abstract

KRAS G12C inhibitors, including MRTX849, are promising treatment options for KRAS-mutant non-small cell lung cancer (NSCLC). PD-1 inhibitors are approved in NSCLC; however, strategies to enhance checkpoint inhibitor therapy (CIT) are needed. KRAS G12C mutations are smoking-associated transversion mutations associated with high tumor mutation burden, PD-L1 positivity, and an immunosuppressive tumor microenvironment. To evaluate the potential of MRTX849 to augment CIT, its impact on immune signaling and response to CIT was evaluated. In human tumor xenograft models, MRTX849 increased MHC class I protein expression and decreased RNA and/or plasma protein levels of immunosuppressive factors. In a Kras G12C -mutant CT26 syngeneic mouse model, MRTX849 decreased intratumoral myeloid-derived suppressor cells and increased M1-polarized macrophages, dendritic cells, CD4 + , and CD8 + T cells. Similar results were observed in lung Kras G12C -mutant syngeneic and a genetically engineered mouse (GEM) model. In the CT26 Kras G12C model, MRTX849 demonstrated marked tumor regression when tumors were established in immune-competent BALB/c mice; however, the effect was diminished when tumors were grown in T-cell-deficient nu / nu mice. Tumors progressed following anti-PD-1 or MRTX849 single-agent treatment in immune-competent mice; however, combination treatment demonstrated durable, complete responses (CRs). Tumors did not reestablish in the same mice that exhibited durable CRs when rechallenged with tumor cell inoculum, demonstrating these mice developed adaptive antitumor immunity. In a GEM model, treatment with MRTX849 plus anti-PD-1 led to increased progression-free survival compared with either single agent alone. These data demonstrate KRAS inhibition reverses an immunosuppressive tumor microenvironment and sensitizes tumors to CIT through multiple mechanisms., (©2021 American Association for Cancer Research.)

Published

2021

6. Ground-glass opacity-featured lung adenocarcinoma has no response to chemotherapy.

Author

Zhang Y, Deng C, Ma X, Gao Z, Wang S, Zheng Q, Xia G, Wen Z, Han H, Fu F, Liu Q, Hu H, Li Y, Wong KK, and Chen H

Subjects

Adult, Aged, Female, Humans, Lung drug effects, Lung pathology, Male, Middle Aged, Pneumonectomy, Retrospective Studies, Tomography, X-Ray Computed methods, Adenocarcinoma of Lung drug therapy, Adenocarcinoma of Lung pathology, Antineoplastic Agents therapeutic use, Lung Neoplasms drug therapy, Lung Neoplasms pathology

Abstract

Purpose: We aimed to investigate the treatment effect of chemotherapy on ground-glass opacity (GGO)-featured lung adenocarcinoma radiologically and pathologically., Methods: This retrospective study included patients who met the following criteria: (1) presence of lung GGO lesions before chemotherapy for other concurrent malignancies; (2) underwent surgical resection of GGO-featured primary lung adenocarcinoma. The last computed tomography images before chemotherapy (CT1) and the last images before GGO resection (CT2) were reviewed to assess radiologic response. Specimens of the resected tumors were reviewed to evaluate the histopathologic response. Immunohistochemical staining of ki-67, caspase-3 and β-gal was performed and compared between these tumors and a propensity score-matched (1:1) cohort of GGO-featured lung adenocarcinoma without prior chemotherapy., Results: Forty-four patients with 55 GGO lesions were included. There were 20 mixed GGOs and 22 invasive adenocarcinomas. These patients all received at least three cycles of chemotherapy for other concurrent malignancies in breast, lung, cervix, ovary or rectum. Thirty-four (77%) patients received chemotherapy regimens that contained platinum, pemetrexed, paclitaxel, docetaxel or gemcitabine. The median interval between CT1 and CT2 was 10 months. Radiologically, all the GGO lesions either remained unchanged or enlarged. There was no chemotherapy-induced histopathologic response (necrosis, fibrosis or inflammation) in any of these tumors. The protein expression of ki-67, caspase-3 and β-gal was comparable between GGO-featured lung adenocarcinoma with or without prior chemotherapy., Conclusion: GGO-featured lung adenocarcinoma has no response to chemotherapy. For these patients, chemotherapy should not be a treatment option.

Published

2020

7. Targeting glutamine-addiction and overcoming CDK4/6 inhibitor resistance in human esophageal squamous cell carcinoma.

Author

Qie S, Yoshida A, Parnham S, Oleinik N, Beeson GC, Beeson CC, Ogretmen B, Bass AJ, Wong KK, Rustgi AK, and Diehl JA

Subjects

Animals, Benzeneacetamides pharmacology, Cell Line, Tumor, Cyclin D1 genetics, Cyclin D1 metabolism, Cyclin-Dependent Kinase 4 antagonists & inhibitors, Cyclin-Dependent Kinase 4 genetics, Cyclin-Dependent Kinase 4 metabolism, Cyclin-Dependent Kinase 6 antagonists & inhibitors, Cyclin-Dependent Kinase 6 genetics, Cyclin-Dependent Kinase 6 metabolism, Drug Resistance, Neoplasm genetics, Drug Synergism, Energy Metabolism drug effects, Energy Metabolism genetics, Esophageal Neoplasms genetics, Esophageal Neoplasms metabolism, Esophageal Neoplasms pathology, Esophageal Squamous Cell Carcinoma genetics, Esophageal Squamous Cell Carcinoma metabolism, Esophageal Squamous Cell Carcinoma pathology, F-Box Proteins genetics, F-Box Proteins metabolism, Glutaminase antagonists & inhibitors, Glutaminase genetics, Glutaminase metabolism, Glutamine antagonists & inhibitors, Humans, Male, Mechanistic Target of Rapamycin Complex 1 genetics, Mechanistic Target of Rapamycin Complex 1 metabolism, Metformin pharmacology, Mice, Molecular Targeted Therapy, Phenformin pharmacology, Retinoblastoma Protein genetics, Retinoblastoma Protein metabolism, Signal Transduction, Thiadiazoles pharmacology, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Drug Resistance, Neoplasm drug effects, Esophageal Neoplasms drug therapy, Esophageal Squamous Cell Carcinoma drug therapy, Gene Expression Regulation, Neoplastic, Glutamine metabolism, Hypoglycemic Agents pharmacology, Protein Kinase Inhibitors pharmacology

Abstract

The dysregulation of Fbxo4-cyclin D1 axis occurs at high frequency in esophageal squamous cell carcinoma (ESCC), where it promotes ESCC development and progression. However, defining a therapeutic vulnerability that results from this dysregulation has remained elusive. Here we demonstrate that Rb and mTORC1 contribute to Gln-addiction upon the dysregulation of the Fbxo4-cyclin D1 axis, which leads to the reprogramming of cellular metabolism. This reprogramming is characterized by reduced energy production and increased sensitivity of ESCC cells to combined treatment with CB-839 (glutaminase 1 inhibitor) plus metformin/phenformin. Of additional importance, this combined treatment has potent efficacy in ESCC cells with acquired resistance to CDK4/6 inhibitors in vitro and in xenograft tumors. Our findings reveal a molecular basis for cancer therapy through targeting glutaminolysis and mitochondrial respiration in ESCC with dysregulated Fbxo4-cyclin D1 axis as well as cancers resistant to CDK4/6 inhibitors.

Published

2019

8. Targeting HER2 Aberrations in Non-Small Cell Lung Cancer with Osimertinib.

Author

Liu S, Li S, Hai J, Wang X, Chen T, Quinn MM, Gao P, Zhang Y, Ji H, Cross DAE, and Wong KK

Subjects

Animals, Biomarkers, Tumor, Carcinoma, Non-Small-Cell Lung diagnosis, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung metabolism, Cell Line, Tumor, DNA Copy Number Variations, Disease Models, Animal, Exons, Humans, Lung Neoplasms drug therapy, Lung Neoplasms metabolism, Lung Neoplasms pathology, Magnetic Resonance Imaging, Mice, Molecular Targeted Therapy, Receptor, ErbB-2 antagonists & inhibitors, Xenograft Model Antitumor Assays, Acrylamides pharmacology, Aniline Compounds pharmacology, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung genetics, Lung Neoplasms genetics, Mutation, Protein Kinase Inhibitors pharmacology, Receptor, ErbB-2 genetics

Abstract

Purpose: HER2 (or ERBB2 ) aberrations, including both amplification and mutations, have been classified as oncogenic drivers that contribute to 2% to 6% of lung adenocarcinomas. HER2 amplification is also an important mechanism for acquired resistance to EGFR tyrosine kinase inhibitors (TKI). However, due to limited preclinical studies and clinical trials, currently there is still no available standard of care for lung cancer patients with HER2 aberrations. To fulfill the clinical need for targeting HER2 in patients with non-small cell lung cancer (NSCLC), we performed a comprehensive preclinical study to evaluate the efficacy of a third-generation TKI, osimertinib (AZD9291). Experimental Design: Three genetically modified mouse models (GEMM) mimicking individual HER2 alterations in NSCLC were generated, and osimertinib was tested for its efficacy against these HER2 aberrations in vivo Results: Osimertinib treatment showed robust efficacy in HER2 wt overexpression and EGFR del19/HER2 models, but not in HER2 exon 20 insertion tumors. Interestingly, we further identified that combined treatment with osimertinib and the BET inhibitor JQ1 significantly increased the response rate in HER2 -mutant NSCLC, whereas JQ1 single treatment did not show efficacy. Conclusions: Overall, our data indicated robust antitumor efficacy of osimertinib against multiple HER2 aberrations in lung cancer, either as a single agent or in combination with JQ1. Our study provides a strong rationale for future clinical trials using osimertinib either alone or in combination with epigenetic drugs to target aberrant HER2 in patients with NSCLC. Clin Cancer Res; 24(11); 2594-604. ©2018 AACR See related commentary by Cappuzzo and Landi, p. 2470 ., (©2018 American Association for Cancer Research.)

Published

2018

9. JAK2/IDH-mutant-driven myeloproliferative neoplasm is sensitive to combined targeted inhibition.

Author

McKenney AS, Lau AN, Somasundara AVH, Spitzer B, Intlekofer AM, Ahn J, Shank K, Rapaport FT, Patel MA, Papalexi E, Shih AH, Chiu A, Freinkman E, Akbay EA, Steadman M, Nagaraja R, Yen K, Teruya-Feldstein J, Wong KK, Rampal R, Vander Heiden MG, Thompson CB, and Levine RL

Subjects

Aged, Animals, Disease Progression, Epigenesis, Genetic, Female, Gene Expression Profiling, Humans, Male, Mice, Mice, Mutant Strains, Mice, Transgenic, Middle Aged, Mutation, Phenotype, Stem Cells, Antineoplastic Agents pharmacology, Gene Expression Regulation, Neoplastic, Isocitrate Dehydrogenase genetics, Janus Kinase 2 genetics, Myeloproliferative Disorders drug therapy, Myeloproliferative Disorders genetics

Abstract

Patients with myeloproliferative neoplasms (MPNs) frequently progress to bone marrow failure or acute myeloid leukemia (AML), and mutations in epigenetic regulators such as the metabolic enzyme isocitrate dehydrogenase (IDH) are associated with poor outcomes. Here, we showed that combined expression of Jak2V617F and mutant IDH1R132H or Idh2R140Q induces MPN progression, alters stem/progenitor cell function, and impairs differentiation in mice. Jak2V617F Idh2R140Q-mutant MPNs were sensitive to small-molecule inhibition of IDH. Combined inhibition of JAK2 and IDH2 normalized the stem and progenitor cell compartments in the murine model and reduced disease burden to a greater extent than was seen with JAK inhibition alone. In addition, combined JAK2 and IDH2 inhibitor treatment also reversed aberrant gene expression in MPN stem cells and reversed the metabolite perturbations induced by concurrent JAK2 and IDH2 mutations. Combined JAK2 and IDH2 inhibitor therapy also showed cooperative efficacy in cells from MPN patients with both JAK2mut and IDH2mut mutations. Taken together, these data suggest that combined JAK and IDH inhibition may offer a therapeutic advantage in this high-risk MPN subtype.

Published

2018

10. Noncanonical agonist PPARγ ligands modulate the response to DNA damage and sensitize cancer cells to cytotoxic chemotherapy.

Author

Khandekar MJ, Banks AS, Laznik-Bogoslavski D, White JP, Choi JH, Kazak L, Lo JC, Cohen P, Wong KK, Kamenecka TM, Griffin PR, and Spiegelman BM

Subjects

Amino Acid Motifs, Animals, Apoptosis drug effects, Carboplatin administration & dosage, Cell Line, Tumor, Humans, Ligands, Lung Neoplasms genetics, Lung Neoplasms metabolism, Male, Mice, Mice, Nude, PPAR gamma agonists, PPAR gamma chemistry, PPAR gamma genetics, Phosphorylation, Tumor Suppressor Protein p53 genetics, Tumor Suppressor Protein p53 metabolism, Antineoplastic Agents administration & dosage, DNA Damage drug effects, Lung Neoplasms drug therapy, PPAR gamma metabolism, Thiazolidinediones administration & dosage

Abstract

The peroxisome-proliferator receptor-γ (PPARγ) is expressed in multiple cancer types. Recently, our group has shown that PPARγ is phosphorylated on serine 273 (S273), which selectively modulates the transcriptional program controlled by this protein. PPARγ ligands, including thiazolidinediones (TZDs), block S273 phosphorylation. This activity is chemically separable from the canonical activation of the receptor by agonist ligands and, importantly, these noncanonical agonist ligands do not cause some of the known side effects of TZDs. Here, we show that phosphorylation of S273 of PPARγ occurs in cancer cells on exposure to DNA damaging agents. Blocking this phosphorylation genetically or pharmacologically increases accumulation of DNA damage, resulting in apoptotic cell death. A genetic signature of PPARγ phosphorylation is associated with worse outcomes in response to chemotherapy in human patients. Noncanonical agonist ligands sensitize lung cancer xenografts and genetically induced lung tumors to carboplatin therapy. Moreover, inhibition of this phosphorylation results in deregulation of p53 signaling, and biochemical studies show that PPARγ physically interacts with p53 in a manner dependent on S273 phosphorylation. These data implicate a role for PPARγ in modifying the p53 response to cytotoxic therapy, which can be modulated for therapeutic gain using these compounds., Competing Interests: The authors declare no conflict of interest.

Published

2018

11. Overcoming EGFR(T790M) and EGFR(C797S) resistance with mutant-selective allosteric inhibitors.

Author

Jia Y, Yun CH, Park E, Ercan D, Manuia M, Juarez J, Xu C, Rhee K, Chen T, Zhang H, Palakurthi S, Jang J, Lelais G, DiDonato M, Bursulaya B, Michellys PY, Epple R, Marsilje TH, McNeill M, Lu W, Harris J, Bender S, Wong KK, Jänne PA, and Eck MJ

Subjects

Allosteric Regulation drug effects, Allosteric Site drug effects, Animals, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung enzymology, Carcinoma, Non-Small-Cell Lung pathology, Cell Line, Tumor, Cell Proliferation drug effects, Cetuximab pharmacology, Disease Models, Animal, Drug Resistance, Multiple drug effects, Drug Resistance, Multiple genetics, Drug Resistance, Neoplasm drug effects, Drug Synergism, ErbB Receptors antagonists & inhibitors, ErbB Receptors chemistry, ErbB Receptors metabolism, Lung Neoplasms drug therapy, Lung Neoplasms enzymology, Lung Neoplasms pathology, Mice, Mutant Proteins chemistry, Mutant Proteins genetics, Mutant Proteins metabolism, Protein Conformation drug effects, Protein Multimerization drug effects, Antineoplastic Agents pharmacology, Benzeneacetamides pharmacology, Drug Resistance, Neoplasm genetics, ErbB Receptors genetics, Mutant Proteins antagonists & inhibitors, Protein Kinase Inhibitors pharmacology, Thiazoles pharmacology

Abstract

The epidermal growth factor receptor (EGFR)-directed tyrosine kinase inhibitors (TKIs) gefitinib, erlotinib and afatinib are approved treatments for non-small cell lung cancers harbouring activating mutations in the EGFR kinase, but resistance arises rapidly, most frequently owing to the secondary T790M mutation within the ATP site of the receptor. Recently developed mutant-selective irreversible inhibitors are highly active against the T790M mutant, but their efficacy can be compromised by acquired mutation of C797, the cysteine residue with which they form a key covalent bond. All current EGFR TKIs target the ATP-site of the kinase, highlighting the need for therapeutic agents with alternative mechanisms of action. Here we describe the rational discovery of EAI045, an allosteric inhibitor that targets selected drug-resistant EGFR mutants but spares the wild-type receptor. The crystal structure shows that the compound binds an allosteric site created by the displacement of the regulatory C-helix in an inactive conformation of the kinase. The compound inhibits L858R/T790M-mutant EGFR with low-nanomolar potency in biochemical assays. However, as a single agent it is not effective in blocking EGFR-driven proliferation in cells owing to differential potency on the two subunits of the dimeric receptor, which interact in an asymmetric manner in the active state. We observe marked synergy of EAI045 with cetuximab, an antibody therapeutic that blocks EGFR dimerization, rendering the kinase uniformly susceptible to the allosteric agent. EAI045 in combination with cetuximab is effective in mouse models of lung cancer driven by EGFR(L858R/T790M) and by EGFR(L858R/T790M/C797S), a mutant that is resistant to all currently available EGFR TKIs. More generally, our findings illustrate the utility of purposefully targeting allosteric sites to obtain mutant-selective inhibitors.

Published

2016

12. Intratumoral Heterogeneity in EGFR-Mutant NSCLC Results in Divergent Resistance Mechanisms in Response to EGFR Tyrosine Kinase Inhibition.

Author

Soucheray M, Capelletti M, Pulido I, Kuang Y, Paweletz CP, Becker JH, Kikuchi E, Xu C, Patel TB, Al-Shahrour F, Carretero J, Wong KK, Jänne PA, Shapiro GI, and Shimamura T

Subjects

Animals, Carcinoma, Non-Small-Cell Lung metabolism, Carcinoma, Non-Small-Cell Lung pathology, Cell Line, Tumor, Cluster Analysis, Epithelial-Mesenchymal Transition drug effects, Epithelial-Mesenchymal Transition genetics, Gefitinib, Gene Expression Profiling, Humans, Lung Neoplasms metabolism, Lung Neoplasms pathology, Mice, Phenotype, Quinazolines pharmacology, Receptors, Transforming Growth Factor beta metabolism, Signal Transduction drug effects, Smad Proteins metabolism, Transforming Growth Factor beta1 metabolism, Transforming Growth Factor beta1 pharmacology, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung genetics, Drug Resistance, Neoplasm genetics, Lung Neoplasms genetics, Mutation, Protein Kinase Inhibitors pharmacology

Abstract

Non-small cell lung cancers (NSCLC) that have developed resistance to EGF receptor (EGFR) tyrosine kinase inhibitor (TKI), including gefitinib and erlotinib, are clinically linked to an epithelial-to-mesenchymal transition (EMT) phenotype. Here, we examined whether modulating EMT maintains the responsiveness of EGFR-mutated NSCLCs to EGFR TKI therapy. Using human NSCLC cell lines harboring mutated EGFR and a transgenic mouse model of lung cancer driven by mutant EGFR (EGFR-Del19-T790M), we demonstrate that EGFR inhibition induces TGFβ secretion followed by SMAD pathway activation, an event that promotes EMT. Chronic exposure of EGFR-mutated NSCLC cells to TGFβ was sufficient to induce EMT and resistance to EGFR TKI treatment. Furthermore, NSCLC HCC4006 cells with acquired resistance to gefitinib were characterized by a mesenchymal phenotype and displayed a higher prevalence of the EGFR T790M mutated allele. Notably, combined inhibition of EGFR and the TGFβ receptor in HCC4006 cells prevented EMT but was not sufficient to prevent acquired gefitinib resistance because of an increased emergence of the EGFR T790M allele compared with cells treated with gefitinib alone. Conversely, another independent NSCLC cell line, PC9, reproducibly developed EGFR T790M mutations as the primary mechanism underlying EGFR TKI resistance, even though the prevalence of the mutant allele was lower than that in HCC4006 cells. Thus, our findings underscore heterogeneity within NSCLC cells lines harboring EGFR kinase domain mutations that give rise to divergent resistance mechanisms in response to treatment and anticipate the complexity of EMT suppression as a therapeutic strategy., (©2015 American Association for Cancer Research.)

Published

2015

13. Development of Selective Covalent Janus Kinase 3 Inhibitors.

Author

Tan L, Akahane K, McNally R, Reyskens KM, Ficarro SB, Liu S, Herter-Sprie GS, Koyama S, Pattison MJ, Labella K, Johannessen L, Akbay EA, Wong KK, Frank DA, Marto JA, Look TA, Arthur JS, Eck MJ, and Gray NS

Subjects

Animals, Antineoplastic Agents pharmacokinetics, Biological Availability, Cell Line, Tumor, Cell Survival, Humans, Male, Mice, Models, Molecular, Protein Kinase Inhibitors pharmacokinetics, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Antineoplastic Agents chemical synthesis, Antineoplastic Agents pharmacology, Janus Kinase 3 antagonists & inhibitors, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacology

Abstract

The Janus kinases (JAKs) and their downstream effectors, signal transducer and activator of transcription proteins (STATs), form a critical immune cell signaling circuit, which is of fundamental importance in innate immunity, inflammation, and hematopoiesis, and dysregulation is frequently observed in immune disease and cancer. The high degree of structural conservation of the JAK ATP binding pockets has posed a considerable challenge to medicinal chemists seeking to develop highly selective inhibitors as pharmacological probes and as clinical drugs. Here we report the discovery and optimization of 2,4-substituted pyrimidines as covalent JAK3 inhibitors that exploit a unique cysteine (Cys909) residue in JAK3. Investigation of structure-activity relationship (SAR) utilizing biochemical and transformed Ba/F3 cellular assays resulted in identification of potent and selective inhibitors such as compounds 9 and 45. A 2.9 Å cocrystal structure of JAK3 in complex with 9 confirms the covalent interaction. Compound 9 exhibited decent pharmacokinetic properties and is suitable for use in vivo. These inhibitors provide a set of useful tools to pharmacologically interrogate JAK3-dependent biology.

Published

2015

14. Combined MEK and PI3K inhibition in a mouse model of pancreatic cancer.

Author

Alagesan B, Contino G, Guimaraes AR, Corcoran RB, Deshpande V, Wojtkiewicz GR, Hezel AF, Wong KK, Loda M, Weissleder R, Benes CH, Engelman J, and Bardeesy N

Subjects

Aminopyridines, Animals, Benzimidazoles pharmacology, Cell Line, Tumor, Disease Models, Animal, Drug Screening Assays, Antitumor, Drug Synergism, Erlotinib Hydrochloride, Humans, MAP Kinase Kinase Kinases antagonists & inhibitors, Mice, Transgenic, Morpholines, Phosphoinositide-3 Kinase Inhibitors, Quinazolines pharmacology, Antineoplastic Agents pharmacology, Carcinoma, Pancreatic Ductal drug therapy, Pancreatic Neoplasms drug therapy, Protein Kinase Inhibitors pharmacology

Abstract

Purpose: Improved therapeutic approaches are needed for the treatment of pancreatic ductal adenocarcinoma (PDAC). As dual MEK and PI3K inhibition is presently being used in clinical trials for patients with PDAC, we sought to test the efficacy of combined targeting of these pathways in PDAC using both in vitro drug screens and genetically engineered mouse models (GEMM)., Experimental Design: We performed high-throughput screening of >500 human cancer cell lines (including 46 PDAC lines), for sensitivity to 50 clinically relevant compounds, including MEK and PI3K inhibitors. We tested the top hit in the screen, the MEK1/2 inhibitor, AZD6244, for efficacy alone or in combination with the PI3K inhibitors, BKM120 or GDC-0941, in a Kras(G12D)-driven GEMM that recapitulates the histopathogenesis of human PDAC., Results: In vitro screens revealed that PDAC cell lines are relatively resistant to single-agent therapies. The response profile to the MEK1/2 inhibitor, AZD6244, was an outlier, showing the highest selective efficacy in PDAC. Although MEK inhibition alone was mainly cytostatic, apoptosis was induced when combined with PI3K inhibitors (BKM120 or GDC-0941). When tested in a PDAC GEMM and compared with the single agents or vehicle controls, the combination delayed tumor formation in the setting of prevention and extended survival when used to treat advanced tumors, although no durable responses were observed., Conclusions: Our studies point to important contributions of MEK and PI3K signaling to PDAC pathogenesis and suggest that dual targeting of these pathways may provide benefit in some patients with PDAC. Clin Cancer Res; 21(2); 396-404. ©2014 AACR., (©2014 American Association for Cancer Research.)

Published

2015

15. Targeting transcriptional addictions in small cell lung cancer with a covalent CDK7 inhibitor.

Author

Christensen CL, Kwiatkowski N, Abraham BJ, Carretero J, Al-Shahrour F, Zhang T, Chipumuro E, Herter-Sprie GS, Akbay EA, Altabef A, Zhang J, Shimamura T, Capelletti M, Reibel JB, Cavanaugh JD, Gao P, Liu Y, Michaelsen SR, Poulsen HS, Aref AR, Barbie DA, Bradner JE, George RE, Gray NS, Young RA, and Wong KK

Subjects

Animals, Antineoplastic Agents pharmacology, Cell Line, Tumor, Cyclin-Dependent Kinases antagonists & inhibitors, Enzyme Inhibitors pharmacology, High-Throughput Screening Assays, Humans, Mice, Molecular Sequence Data, Neoplasms, Experimental, Sequence Analysis, DNA, Small Cell Lung Carcinoma, Transcription, Genetic drug effects, Xenograft Model Antitumor Assays, Antineoplastic Agents administration & dosage, Enzyme Inhibitors administration & dosage, Gene Expression Regulation, Neoplastic drug effects, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Transcription Factors metabolism

Abstract

Small cell lung cancer (SCLC) is an aggressive disease with high mortality, and the identification of effective pharmacological strategies to target SCLC biology represents an urgent need. Using a high-throughput cellular screen of a diverse chemical library, we observe that SCLC is sensitive to transcription-targeting drugs, in particular to THZ1, a recently identified covalent inhibitor of cyclin-dependent kinase 7. We find that expression of super-enhancer-associated transcription factor genes, including MYC family proto-oncogenes and neuroendocrine lineage-specific factors, is highly vulnerability to THZ1 treatment. We propose that downregulation of these transcription factors contributes, in part, to SCLC sensitivity to transcriptional inhibitors and that THZ1 represents a prototype drug for tailored SCLC therapy., (Copyright © 2014 Elsevier Inc. All rights reserved.)

Published

2014

16. Preexisting oncogenic events impact trastuzumab sensitivity in ERBB2-amplified gastroesophageal adenocarcinoma.

Author

Kim J, Fox C, Peng S, Pusung M, Pectasides E, Matthee E, Hong YS, Do IG, Jang J, Thorner AR, Van Hummelen P, Rustgi AK, Wong KK, Zhou Z, Tang P, Kim KM, Lee J, and Bass AJ

Subjects

Drug Resistance, Neoplasm, ErbB Receptors genetics, ErbB Receptors metabolism, Female, Humans, Male, Phosphatidylinositol 3-Kinases genetics, Phosphatidylinositol 3-Kinases metabolism, Trastuzumab, Adenocarcinoma drug therapy, Adenocarcinoma enzymology, Adenocarcinoma genetics, Adenocarcinoma pathology, Antibodies, Monoclonal, Humanized administration & dosage, Antineoplastic Agents administration & dosage, Biomarkers, Tumor genetics, Biomarkers, Tumor metabolism, Esophageal Neoplasms diet therapy, Esophageal Neoplasms enzymology, Esophageal Neoplasms genetics, Esophageal Neoplasms pathology, Gene Amplification drug effects, Gene Amplification genetics, Receptor, ErbB-2 genetics, Receptor, ErbB-2 metabolism, Stomach Neoplasms drug therapy, Stomach Neoplasms enzymology, Stomach Neoplasms genetics, Stomach Neoplasms pathology

Abstract

Patients with gastric and esophageal (GE) adenocarcinoma tumors in which the oncogene ERBB2 has been amplified are routinely treated with a combination of cytotoxic chemotherapy and the ERBB2-directed antibody trastuzumab; however, the addition of trastuzumab, even when tested in a selected biomarker-positive patient population, provides only modest survival gains. To investigate the potential reasons for the modest impact of ERBB2-directed therapies, we explored the hypothesis that secondary molecular features of ERBB2-amplified GE adenocarcinomas attenuate the impact of ERBB2 blockade. We analyzed genomic profiles of ERBB2-amplified GE adenocarcinomas and determined that the majority of ERBB2-amplified tumors harbor secondary oncogenic alterations that have the potential to be therapeutically targeted. These secondary events spanned genes involved in cell-cycle regulation as well as phosphatidylinositol-3 kinase and receptor tyrosine kinase signaling. Using ERBB2-amplified cell lines, we demonstrated that secondary oncogenic events could confer resistance to ERBB2-directed therapies. Moreover, this resistance could be overcome by targeting the secondary oncogene in conjunction with ERBB2-directed therapy. EGFR is commonly coamplified with ERBB2, and in the setting of ERBB2 amplification, higher EGFR expression appears to mark tumors with greater sensitivity to dual EGFR/ERBB2 kinase inhibitors. These data suggest that combination inhibitor strategies, guided by secondary events in ERBB2-amplified GE adenocarcinomas, should be evaluated in clinical trials.

Published

2014

17. Targeting the oncogenic MUC1-C protein inhibits mutant EGFR-mediated signaling and survival in non-small cell lung cancer cells.

Author

Kharbanda A, Rajabi H, Jin C, Tchaicha J, Kikuchi E, Wong KK, and Kufe D

Subjects

Carcinoma, Non-Small-Cell Lung genetics, Cell Line, Tumor, Down-Regulation drug effects, Down-Regulation genetics, Humans, Lung Neoplasms genetics, Oncogenes drug effects, Protein Kinase Inhibitors pharmacology, Proto-Oncogene Proteins c-akt genetics, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Cell Survival drug effects, ErbB Receptors metabolism, Lung Neoplasms drug therapy, Mucin-1 metabolism, Signal Transduction drug effects

Abstract

Purpose: Non-small cell lung cancers (NSCLC) that express EGF receptor with activating mutations frequently develop resistance to EGFR kinase inhibitors. The mucin 1 (MUC1) heterodimeric protein is aberrantly overexpressed in NSCLC cells and confers a poor prognosis; however, the functional involvement of MUC1 in mutant EGFR signaling is not known., Experimental Design: Targeting the oncogenic MUC1 C-terminal subunit (MUC1-C) in NSCLC cells harboring mutant EGFR was studied for effects on signaling, growth, clonogenic survival, and tumorigenicity., Results: Stable silencing of MUC1-C in H1975/EGFR(L858R/T790M) cells resulted in downregulation of AKT signaling and inhibition of growth, colony formation, and tumorigenicity. Similar findings were obtained when MUC1-C was silenced in gefitinib-resistant PC9GR cells expressing EGFR(delE746_A750/T790M). The results further show that expression of a MUC1-C(CQC → AQA) mutant, which blocks MUC1-C homodimerization, suppresses EGFR(T790M), AKT and MEK → ERK activation, colony formation, and tumorigenicity. In concert with these results, treatment of H1975 and PC9GR cells with GO-203, a cell-penetrating peptide that blocks MUC1-C homodimerization, resulted in inhibition of EGFR, AKT, and MEK → ERK signaling and in loss of survival. Combination studies of GO-203 and afatinib, an irreversible inhibitor of EGFR, further demonstrate that these agents are synergistic in inhibiting growth of NSCLC cells harboring the activating EGFR(T790M) or EGFR(delE746-A750) mutants., Conclusions: These findings indicate that targeting MUC1-C inhibits mutant EGFR signaling and survival, and thus represents a potential approach alone and in combination for the treatment of NSCLCs resistant to EGFR kinase inhibitors., (©2014 American Association for Cancer Research.)

Published

2014

18. Co-clinical trials demonstrate superiority of crizotinib to chemotherapy in ALK-rearranged non-small cell lung cancer and predict strategies to overcome resistance.

Author

Chen Z, Akbay E, Mikse O, Tupper T, Cheng K, Wang Y, Tan X, Altabef A, Woo SA, Chen L, Reibel JB, Janne PA, Sharpless NE, Engelman JA, Shapiro GI, Kung AL, and Wong KK

Subjects

Anaplastic Lymphoma Kinase, Animals, Antineoplastic Agents administration & dosage, Carcinoma, Non-Small-Cell Lung diagnosis, Carcinoma, Non-Small-Cell Lung mortality, Crizotinib, Disease Models, Animal, Drug Resistance, Neoplasm genetics, HSP90 Heat-Shock Proteins antagonists & inhibitors, Humans, Lung Neoplasms diagnosis, Lung Neoplasms mortality, Magnetic Resonance Imaging, Mice, Oncogene Proteins, Fusion genetics, Positron-Emission Tomography, Protein Kinase Inhibitors administration & dosage, Pyrazoles administration & dosage, Pyridines administration & dosage, Treatment Outcome, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung genetics, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Protein Kinase Inhibitors pharmacology, Pyrazoles pharmacology, Pyridines pharmacology, Receptor Protein-Tyrosine Kinases genetics

Abstract

Purpose: To extend the results of a phase III trial in patients with non-small cell lung cancer with adenocarcinomas harboring EML4-ALK fusion., Experimental Design: We conducted a co-clinical trial in a mouse model comparing the ALK inhibitor crizotinib to the standard-of-care cytotoxic agents docetaxel or pemetrexed., Results: Concordant with the clinical outcome in humans, crizotinib produced a substantially higher response rate compared with chemotherapy, associated with significantly longer progression-free survival. Overall survival was also prolonged in crizotinib- compared with chemotherapy-treated mice. Pemetrexed produced superior overall survival compared with docetaxel, suggesting that this agent may be the preferred chemotherapy in the ALK population. In addition, in the EML4-ALK-driven mouse lung adenocarcinoma model, HSP90 inhibition can overcome both primary and acquired crizotinib resistance. Furthermore, HSP90 inhibition, as well as the second-generation ALK inhibitor TAE684, demonstrated activity in newly developed lung adenocarcinoma models driven by crizotinib-insensitive EML4-ALK L1196M or F1174L., Conclusions: Our findings suggest that crizotinib is superior to standard chemotherapy in ALK inhibitor-naïve disease and support further clinical investigation of HSP90 inhibitors and second-generation ALK inhibitors in tumors with primary or acquired crizotinib resistance., (©2013 AACR)

Published

2014

19. The myeloma drug lenalidomide promotes the cereblon-dependent destruction of Ikaros proteins.

Author

Lu G, Middleton RE, Sun H, Naniong M, Ott CJ, Mitsiades CS, Wong KK, Bradner JE, and Kaelin WG Jr

Subjects

Adaptor Proteins, Signal Transducing, Cell Line, Tumor, HEK293 Cells, Humans, Ikaros Transcription Factor genetics, Lenalidomide, Peptide Hydrolases genetics, Proteolysis, Thalidomide pharmacology, Ubiquitin-Protein Ligases, Antineoplastic Agents pharmacology, Ikaros Transcription Factor metabolism, Multiple Myeloma metabolism, Peptide Hydrolases metabolism, Teratogens pharmacology, Thalidomide analogs & derivatives

Abstract

Thalidomide-like drugs such as lenalidomide are clinically important treatments for multiple myeloma and show promise for other B cell malignancies. The biochemical mechanisms underlying their antitumor activity are unknown. Thalidomide was recently shown to bind to, and inhibit, the cereblon ubiquitin ligase. Cereblon loss in zebrafish causes fin defects reminiscent of the limb defects seen in children exposed to thalidomide in utero. Here we show that lenalidomide-bound cereblon acquires the ability to target for proteasomal degradation two specific B cell transcription factors, Ikaros family zinc finger proteins 1 and 3 (IKZF1 and IKZF3). Analysis of myeloma cell lines revealed that loss of IKZF1 and IKZF3 is both necessary and sufficient for lenalidomide's therapeutic effect, suggesting that the antitumor and teratogenic activities of thalidomide-like drugs are dissociable.

Published

2014

20. Cetuximab response of lung cancer-derived EGF receptor mutants is associated with asymmetric dimerization.

Author

Cho J, Chen L, Sangji N, Okabe T, Yonesaka K, Francis JM, Flavin RJ, Johnson W, Kwon J, Yu S, Greulich H, Johnson BE, Eck MJ, Jänne PA, Wong KK, and Meyerson M

Subjects

Adenocarcinoma metabolism, Amino Acid Substitution, Animals, Cell Transformation, Neoplastic genetics, Cell Transformation, Neoplastic metabolism, Cells, Cultured, Cetuximab, ErbB Receptors chemistry, ErbB Receptors genetics, Humans, Lung Neoplasms metabolism, Mice, NIH 3T3 Cells, Protein Conformation drug effects, Adenocarcinoma genetics, Antibodies, Monoclonal, Humanized pharmacology, Antineoplastic Agents pharmacology, ErbB Receptors metabolism, Lung Neoplasms genetics, Protein Multimerization drug effects

Abstract

Kinase domain mutations of the EGF receptor (EGFR) are common oncogenic events in lung adenocarcinoma. Here, we explore the dependency upon asymmetric dimerization of the kinase domain for activation of lung cancer-derived EGFR mutants. We show that whereas wild-type EGFR and the L858R mutant require dimerization for activation and oncogenic transformation, the exon 19 deletion, exon 20 insertion, and L858R/T790M EGFR mutants do not require dimerization. In addition, treatment with the monoclonal antibody, cetuximab, shrinks mouse lung tumors induced by the dimerization-dependent L858R mutant, but exerts only a modest effect on tumors driven by dimerization-independent EGFR mutants. These data imply that different EGFR mutants show differential requirements for dimerization and that disruption of dimerization may be among the antitumor mechanisms of cetuximab., (©2013 AACR)

Published

2013

21. A multicenter phase II study of ganetespib monotherapy in patients with genotypically defined advanced non-small cell lung cancer.

Author

Socinski MA, Goldman J, El-Hariry I, Koczywas M, Vukovic V, Horn L, Paschold E, Salgia R, West H, Sequist LV, Bonomi P, Brahmer J, Chen LC, Sandler A, Belani CP, Webb T, Harper H, Huberman M, Ramalingam S, Wong KK, Teofilovici F, Guo W, and Shapiro GI

Subjects

Adult, Aged, Aged, 80 and over, Anaplastic Lymphoma Kinase, Antineoplastic Agents administration & dosage, Antineoplastic Agents adverse effects, Carcinoma, Non-Small-Cell Lung genetics, Carcinoma, Non-Small-Cell Lung pathology, Female, Gene Rearrangement, Genotype, HSP90 Heat-Shock Proteins antagonists & inhibitors, Humans, Lung Neoplasms genetics, Lung Neoplasms pathology, Male, Middle Aged, Mutation, Neoplasm Staging, Receptor Protein-Tyrosine Kinases genetics, Treatment Outcome, Triazoles administration & dosage, Triazoles adverse effects, Antineoplastic Agents therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, Triazoles therapeutic use

Abstract

Purpose: Ganetespib is a novel inhibitor of the heat shock protein 90 (Hsp90), a chaperone protein critical to tumor growth and proliferation. In this phase II study, we evaluated the activity and tolerability of ganetespib in previously treated patients with non-small cell lung cancer (NSCLC)., Experimental Design: Patients were enrolled into cohort A (mutant EGFR), B (mutant KRAS), or C (no EGFR or KRAS mutations). Patients were treated with 200 mg/m(2) ganetespib by intravenous infusion once weekly for 3 weeks followed by 1 week of rest, until disease progression. The primary endpoint was progression-free survival (PFS) at 16 weeks. Secondary endpoints included objective response (ORR), duration of treatment, tolerability, median PFS, overall survival (OS), and correlative studies., Results: Ninety-nine patients with a median of 2 prior systemic therapies were enrolled; 98 were assigned to cohort A (n = 15), B (n = 17), or C (n = 66), with PFS rates at 16 weeks of 13.3%, 5.9%, and 19.7%, respectively. Four patients (4%) achieved partial response (PR); all had disease that harbored anaplastic lymphoma kinase (ALK) gene rearrangement, retrospectively detected by FISH (n = 1) or PCR-based assays (n = 3), in crizotinib-naïve patients enrolled to cohort C. Eight patients (8.1%) experienced treatment-related serious adverse events (AE); 2 of these (cardiac arrest and renal failure) resulted in death. The most common AEs were diarrhea, fatigue, nausea, and anorexia., Conclusions: Ganetespib monotherapy showed a manageable side effect profile as well as clinical activity in heavily pretreated patients with advanced NSCLCs, particularly in patients with tumors harboring ALK gene rearrangement., (©2013 AACR)

Published

2013

22. Synthetic lethal interaction of combined BCL-XL and MEK inhibition promotes tumor regressions in KRAS mutant cancer models.

Author

Corcoran RB, Cheng KA, Hata AN, Faber AC, Ebi H, Coffee EM, Greninger P, Brown RD, Godfrey JT, Cohoon TJ, Song Y, Lifshits E, Hung KE, Shioda T, Dias-Santagata D, Singh A, Settleman J, Benes CH, Mino-Kenudson M, Wong KK, and Engelman JA

Subjects

Aniline Compounds therapeutic use, Animals, Antineoplastic Agents therapeutic use, Benzimidazoles therapeutic use, Drug Screening Assays, Antitumor, Humans, Mice, Neoplasms genetics, Proto-Oncogene Proteins p21(ras) metabolism, Sulfonamides therapeutic use, Aniline Compounds pharmacology, Antineoplastic Agents pharmacology, Benzimidazoles pharmacology, MAP Kinase Kinase Kinases antagonists & inhibitors, Neoplasms drug therapy, Proto-Oncogene Proteins p21(ras) genetics, Sulfonamides pharmacology, bcl-X Protein antagonists & inhibitors

Abstract

KRAS is the most commonly mutated oncogene, yet no effective targeted therapies exist for KRAS mutant cancers. We developed a pooled shRNA-drug screen strategy to identify genes that, when inhibited, cooperate with MEK inhibitors to effectively treat KRAS mutant cancer cells. The anti-apoptotic BH3 family gene BCL-XL emerged as a top hit through this approach. ABT-263 (navitoclax), a chemical inhibitor that blocks the ability of BCL-XL to bind and inhibit pro-apoptotic proteins, in combination with a MEK inhibitor led to dramatic apoptosis in many KRAS mutant cell lines from different tissue types. This combination caused marked in vivo tumor regressions in KRAS mutant xenografts and in a genetically engineered KRAS-driven lung cancer mouse model, supporting combined BCL-XL/MEK inhibition as a potential therapeutic approach for KRAS mutant cancers., (Copyright © 2013 Elsevier Inc. All rights reserved.)

Published

2013

23. Comparison of the anti-tumor effects of denosumab and zoledronic acid on the neoplastic stromal cells of giant cell tumor of bone.

Author

Lau CP, Huang L, Wong KC, and Kumta SM

Subjects

Alkaline Phosphatase metabolism, Antibodies, Monoclonal, Humanized pharmacology, Antineoplastic Agents pharmacology, Apoptosis drug effects, Apoptosis genetics, Cell Count, Cell Line, Tumor, Cell Movement drug effects, Cell Proliferation drug effects, Cell Survival drug effects, Cell Survival genetics, Collagen Type I genetics, Collagen Type I metabolism, Denosumab, Diphosphonates pharmacology, Gene Expression Regulation, Neoplastic drug effects, Giant Cell Tumor of Bone genetics, Humans, Imidazoles pharmacology, Macrophage Colony-Stimulating Factor metabolism, Osteoprotegerin genetics, Osteoprotegerin metabolism, RANK Ligand genetics, RANK Ligand metabolism, RNA, Messenger genetics, RNA, Messenger metabolism, Solubility, Stromal Cells drug effects, Stromal Cells metabolism, Stromal Cells pathology, Zoledronic Acid, Antibodies, Monoclonal, Humanized therapeutic use, Antineoplastic Agents therapeutic use, Diphosphonates therapeutic use, Giant Cell Tumor of Bone drug therapy, Giant Cell Tumor of Bone pathology, Imidazoles therapeutic use

Abstract

Denosumab and Zoledronic acid (ZOL) are two antiresorptive drugs currently in use for treating osteoporosis. They have different mechanisms of action but both have been shown to delay the onset of skeletal-related events in patients with giant cell tumor of bone (GCT). However, the anti-tumor mechanisms of denosumab on the neoplastic GCT stromal cells remain unknown. In this study, we focused on the direct effects of denosumab on the neoplastic GCT stromal cells and compared with ZOL. The microscopic view demonstrated a reduced cell growth in ZOL-treated but not in denosumab-treated GCT stromal cells. ZOL was found to exhibit a dose-dependent inhibition in cell growth in all GCT stromal cell lines tested and cause apoptosis in two out of three cell lines. In contrast, denosumab only exerted a minimal inhibitory effect in one cell line and did not induce any apoptosis. ZOL significantly inhibited the mRNA expression of receptor activator of nuclear factor kappa-B ligand (RANKL) and osteoprotegerin (OPG) in two GCT stromal cell lines whereas their protein levels remained unchanged. On the contrary, denosumab did not regulate RANKL and OPG expression at both mRNA and protein levels. Moreover, the protein expression of Macrophage Colony-Stimulating Factor (M-CSF), Alkaline Phosphatase (ALP), and Collagen α1 Type I were not regulated by denosumab and ZOL either. Our findings provide new insights in the anti-tumor effect of denosumab on GCT stromal cells and raise a concern that tumor recurrence may occur after the withdrawal of the drug.

Published

2013

24. Ganetespib (STA-9090), a nongeldanamycin HSP90 inhibitor, has potent antitumor activity in in vitro and in vivo models of non-small cell lung cancer.

Author

Shimamura T, Perera SA, Foley KP, Sang J, Rodig SJ, Inoue T, Chen L, Li D, Carretero J, Li YC, Sinha P, Carey CD, Borgman CL, Jimenez JP, Meyerson M, Ying W, Barsoum J, Wong KK, and Shapiro GI

Subjects

Animals, Antineoplastic Agents therapeutic use, Antineoplastic Agents toxicity, Benzoquinones pharmacology, Carcinoma, Non-Small-Cell Lung metabolism, Cell Line, Tumor, Female, HSP90 Heat-Shock Proteins metabolism, Humans, Intramolecular Oxidoreductases metabolism, Lactams, Macrocyclic pharmacology, Lung Neoplasms metabolism, Mice, Mice, SCID, Prostaglandin-E Synthases, Protein Binding drug effects, Protein Stability drug effects, Triazoles therapeutic use, Triazoles toxicity, Xenograft Model Antitumor Assays, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, HSP90 Heat-Shock Proteins antagonists & inhibitors, Lung Neoplasms drug therapy, Triazoles pharmacology

Abstract

Purpose: We describe the anticancer activity of ganetespib, a novel non-geldanamycin heat shock protein 90 (HSP90) inhibitor, in non-small cell lung cancer (NSCLC) models., Experimental Design: The activity of ganetespib was compared with that of the geldanamycin 17-AAG in biochemical assays, cell lines, and xenografts, and evaluated in an ERBB2 YVMA-driven mouse lung adenocarcinoma model., Results: Ganetespib blocked the ability of HSP90 to bind to biotinylated geldanamycin and disrupted the association of HSP90 with its cochaperone, p23, more potently than 17-AAG. In genomically defined NSCLC cell lines, ganetespib caused depletion of receptor tyrosine kinases, extinguishing of downstream signaling, inhibition of proliferation and induction of apoptosis with IC(50) values ranging 2 to 30 nmol/L, substantially lower than those required for 17-AAG (20-3,500 nmol/L). Ganetespib was also approximately 20-fold more potent in isogenic Ba/F3 pro-B cells rendered IL-3 independent by expression of EGFR and ERBB2 mutants. In mice bearing NCI-H1975 (EGFR L858R/T790M) xenografts, ganetespib was rapidly eliminated from plasma and normal tissues but was maintained in tumor with t(1/2) 58.3 hours, supporting once-weekly dosing experiments, in which ganetespib produced greater tumor growth inhibition than 17-AAG. However, after a single dose, reexpression of mutant EGFR occurred by 72 hours, correlating with reversal of antiproliferative and proapoptotic effects. Consecutive day dosing resulted in xenograft regressions, accompanied by more sustained pharmacodynamic effects. Ganetespib also showed activity against mouse lung adenocarcinomas driven by oncogenic ERBB2 YVMA., Conclusions: Ganetespib has greater potency than 17-AAG and potential efficacy against several NSCLC subsets, including those harboring EGFR or ERBB2 mutation., (©2012 AACR.)

Published

2012

25. Exploiting cancer cell vulnerabilities to develop a combination therapy for ras-driven tumors.

Author

De Raedt T, Walton Z, Yecies JL, Li D, Chen Y, Malone CF, Maertens O, Jeong SM, Bronson RT, Lebleu V, Kalluri R, Normant E, Haigis MC, Manning BD, Wong KK, Macleod KF, and Cichowski K

Subjects

Animals, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung genetics, Carcinoma, Non-Small-Cell Lung metabolism, Endoplasmic Reticulum drug effects, Fluorescent Antibody Technique, Glutathione antagonists & inhibitors, Glutathione biosynthesis, HSP90 Heat-Shock Proteins antagonists & inhibitors, In Situ Nick-End Labeling, Mice, Mitochondria drug effects, Molecular Targeted Therapy, Nerve Sheath Neoplasms metabolism, Oxidative Stress drug effects, Oxidative Stress genetics, Polymerase Chain Reaction, Proto-Oncogene Proteins p21(ras) metabolism, RNA Interference, RNA, Small Interfering, Reactive Oxygen Species metabolism, Tumor Cells, Cultured, Tumor Suppressor Protein p53 metabolism, eIF-2 Kinase antagonists & inhibitors, eIF-2 Kinase genetics, Antineoplastic Agents therapeutic use, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Benzoquinones pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Lactams, Macrocyclic pharmacology, Nerve Sheath Neoplasms drug therapy, Sirolimus pharmacology, ras Proteins metabolism

Abstract

Ras-driven tumors are often refractory to conventional therapies. Here we identify a promising targeted therapeutic strategy for two Ras-driven cancers: Nf1-deficient malignancies and Kras/p53 mutant lung cancer. We show that agents that enhance proteotoxic stress, including the HSP90 inhibitor IPI-504, induce tumor regression in aggressive mouse models, but only when combined with rapamycin. These agents synergize by promoting irresolvable ER stress, resulting in catastrophic ER and mitochondrial damage. This process is fueled by oxidative stress, which is caused by IPI-504-dependent production of reactive oxygen species, and the rapamycin-dependent suppression of glutathione, an important endogenous antioxidant. Notably, the mechanism by which these agents cooperate reveals a therapeutic paradigm that can be expanded to develop additional combinations., (Copyright © 2011 Elsevier Inc. All rights reserved.)

Published

2011

26. Mitigation of hematologic radiation toxicity in mice through pharmacological quiescence induced by CDK4/6 inhibition.

Author

Johnson SM, Torrice CD, Bell JF, Monahan KB, Jiang Q, Wang Y, Ramsey MR, Jin J, Wong KK, Su L, Zhou D, and Sharpless NE

Subjects

Animals, Cell Cycle drug effects, Cell Line, Cyclin-Dependent Kinase 4 antagonists & inhibitors, Cyclin-Dependent Kinase Inhibitor p18 metabolism, Hematopoietic Stem Cells metabolism, Mice, Mice, Inbred C3H, Mice, Inbred C57BL, Mice, Knockout, Radiation, Antineoplastic Agents pharmacology

Abstract

Total body irradiation (TBI) can induce lethal myelosuppression, due to the sensitivity of proliferating hematopoietic stem/progenitor cells (HSPCs) to ionizing radiation (IR). No effective therapy exists to mitigate the hematologic toxicities of TBI. Here, using selective and structurally distinct small molecule inhibitors of cyclin-dependent kinase 4 (CDK4) and CDK6, we have demonstrated that selective cellular quiescence increases radioresistance of human cell lines in vitro and mice in vivo. Cell lines dependent on CDK4/6 were resistant to IR and other DNA-damaging agents when treated with CDK4/6 inhibitors. In contrast, CDK4/6 inhibitors did not protect cell lines that proliferated independently of CDK4/6 activity. Treatment of wild-type mice with CDK4/6 inhibitors induced reversible pharmacological quiescence (PQ) of early HSPCs but not most other cycling cells in the bone marrow or other tissues. Selective PQ of HSPCs decreased the hematopoietic toxicity of TBI, even when the CDK4/6 inhibitor was administered several hours after TBI. Moreover, PQ at the time of administration of therapeutic IR to mice harboring autochthonous cancers reduced treatment toxicity without compromising the therapeutic tumor response. These results demonstrate an effective method to mitigate the hematopoietic toxicity of IR in mammals, which may be potentially useful after radiological disaster or as an adjuvant to anticancer therapy.

Published

2010

27. Targeting the PI3K signaling pathway in cancer.

Author

Wong KK, Engelman JA, and Cantley LC

Subjects

Antineoplastic Combined Chemotherapy Protocols therapeutic use, Humans, MAP Kinase Kinase Kinases, Phosphatidylinositol 3-Kinases genetics, Receptor, ErbB-2 antagonists & inhibitors, Signal Transduction drug effects, Antineoplastic Agents therapeutic use, Neoplasms drug therapy, Phosphoinositide-3 Kinase Inhibitors

Abstract

The phosphoinositide 3-kinase (PI3K) pathway is activated in a variety of different human cancers, and inhibitors of this pathway are under active development as anti-cancer therapeutics. In this review, we discuss the data supporting the use of PI3K pathway inhibitors in genetically and clinically defined cancers. This review focuses on their efficacy as single agents and in combination with other targeted therapies, specifically those targeting the MEK-ERK signaling pathway., (Copyright 2009 Elsevier Ltd. All rights reserved.)

Published

2010

28. Novel mutant-selective EGFR kinase inhibitors against EGFR T790M.

Author

Zhou W, Ercan D, Chen L, Yun CH, Li D, Capelletti M, Cortot AB, Chirieac L, Iacob RE, Padera R, Engen JR, Wong KK, Eck MJ, Gray NS, and Jänne PA

Subjects

Animals, Antineoplastic Agents chemistry, Antineoplastic Agents toxicity, Cell Line, Tumor, Cell Proliferation drug effects, Drug Evaluation, Preclinical, Drug Resistance, Neoplasm genetics, Lung drug effects, Mice, Models, Chemical, Models, Molecular, NIH 3T3 Cells, Phosphorylation drug effects, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors toxicity, Antineoplastic Agents pharmacology, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Mutation genetics, Protein Kinase Inhibitors pharmacology

Abstract

The clinical efficacy of epidermal growth factor receptor (EGFR) kinase inhibitors in EGFR-mutant non-small-cell lung cancer (NSCLC) is limited by the development of drug-resistance mutations, including the gatekeeper T790M mutation. Strategies targeting EGFR T790M with irreversible inhibitors have had limited success and are associated with toxicity due to concurrent inhibition of wild-type EGFR. All current EGFR inhibitors possess a structurally related quinazoline-based core scaffold and were identified as ATP-competitive inhibitors of wild-type EGFR. Here we identify a covalent pyrimidine EGFR inhibitor by screening an irreversible kinase inhibitor library specifically against EGFR T790M. These agents are 30- to 100-fold more potent against EGFR T790M, and up to 100-fold less potent against wild-type EGFR, than quinazoline-based EGFR inhibitors in vitro. They are also effective in murine models of lung cancer driven by EGFR T790M. Co-crystallization studies reveal a structural basis for the increased potency and mutant selectivity of these agents. These mutant-selective irreversible EGFR kinase inhibitors may be clinically more effective and better tolerated than quinazoline-based inhibitors. Our findings demonstrate that functional pharmacological screens against clinically important mutant kinases represent a powerful strategy to identify new classes of mutant-selective kinase inhibitors.

Published

2009

29. Predicting drug susceptibility of non-small cell lung cancers based on genetic lesions.

Author

Sos ML, Michel K, Zander T, Weiss J, Frommolt P, Peifer M, Li D, Ullrich R, Koker M, Fischer F, Shimamura T, Rauh D, Mermel C, Fischer S, Stückrath I, Heynck S, Beroukhim R, Lin W, Winckler W, Shah K, LaFramboise T, Moriarty WF, Hanna M, Tolosi L, Rahnenführer J, Verhaak R, Chiang D, Getz G, Hellmich M, Wolf J, Girard L, Peyton M, Weir BA, Chen TH, Greulich H, Barretina J, Shapiro GI, Garraway LA, Gazdar AF, Minna JD, Meyerson M, Wong KK, and Thomas RK

Subjects

Animals, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung pathology, Cell Line, Tumor, Drug Evaluation, Preclinical, ErbB Receptors chemistry, ErbB Receptors genetics, ErbB Receptors metabolism, Gene Expression Profiling, Humans, Magnetic Resonance Imaging, Mice, Models, Molecular, Mutation genetics, Phenotype, Protein Structure, Tertiary, Substrate Specificity, Antineoplastic Agents therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung genetics

Abstract

Somatic genetic alterations in cancers have been linked with response to targeted therapeutics by creation of specific dependency on activated oncogenic signaling pathways. However, no tools currently exist to systematically connect such genetic lesions to therapeutic vulnerability. We have therefore developed a genomics approach to identify lesions associated with therapeutically relevant oncogene dependency. Using integrated genomic profiling, we have demonstrated that the genomes of a large panel of human non-small cell lung cancer (NSCLC) cell lines are highly representative of those of primary NSCLC tumors. Using cell-based compound screening coupled with diverse computational approaches to integrate orthogonal genomic and biochemical data sets, we identified molecular and genomic predictors of therapeutic response to clinically relevant compounds. Using this approach, we showed that v-Ki-ras2 Kirsten rat sarcoma viral oncogene homolog (KRAS) mutations confer enhanced Hsp90 dependency and validated this finding in mice with KRAS-driven lung adenocarcinoma, as these mice exhibited dramatic tumor regression when treated with an Hsp90 inhibitor. In addition, we found that cells with copy number enhancement of v-abl Abelson murine leukemia viral oncogene homolog 2 (ABL2) and ephrin receptor kinase and v-src sarcoma (Schmidt-Ruppin A-2) viral oncogene homolog (avian) (SRC) kinase family genes were exquisitely sensitive to treatment with the SRC/ABL inhibitor dasatinib, both in vitro and when it xenografted into mice. Thus, genomically annotated cell-line collections may help translate cancer genomics information into clinical practice by defining critical pathway dependencies amenable to therapeutic inhibition.

Published

2009

30. A phase I study with neratinib (HKI-272), an irreversible pan ErbB receptor tyrosine kinase inhibitor, in patients with solid tumors.

Author

Wong KK, Fracasso PM, Bukowski RM, Lynch TJ, Munster PN, Shapiro GI, Jänne PA, Eder JP, Naughton MJ, Ellis MJ, Jones SF, Mekhail T, Zacharchuk C, Vermette J, Abbas R, Quinn S, Powell C, and Burris HA

Subjects

Adult, Aged, Aged, 80 and over, Antineoplastic Agents pharmacokinetics, Antineoplastic Agents therapeutic use, ErbB Receptors antagonists & inhibitors, Female, Humans, Male, Maximum Tolerated Dose, Middle Aged, Neoplasms diagnosis, Protein Kinase Inhibitors pharmacokinetics, Protein Kinase Inhibitors therapeutic use, Quinolines pharmacokinetics, Quinolines therapeutic use, Receptor, ErbB-2 antagonists & inhibitors, Antineoplastic Agents adverse effects, Neoplasms drug therapy, Protein Kinase Inhibitors adverse effects, Quinolines adverse effects

Abstract

Purpose: The dose-limiting toxicities, maximum tolerated dose, pharmacokinetic profile, and preliminary antitumor activity of neratinib (HKI-272), an irreversible pan ErbB inhibitor, were determined in patients with advanced solid tumors., Experimental Design: Neratinib was administered orally as a single dose, followed by a 1-week observation period, and then once daily continuously. Planned dose escalation was 40, 80, 120, 180, 240, 320, 400, and 500 mg. For pharmacokinetic analysis, timed blood samples were collected after administration of the single dose and after the first 14 days of continuous daily administration., Results: Dose-limiting toxicity was grade 3 diarrhea, which occurred in one patient treated with 180 mg and in four patients treated with 400 mg neratinib; hence, the maximum tolerated dose was determined to be 320 mg. Other common neratinib-related toxicities included nausea, vomiting, fatigue, and anorexia. Exposure to neratinib was dose dependent, and the pharmacokinetic profile of neratinib supports a once-a-day dosing regimen. Partial response was observed for 8 (32%) of the 25 evaluable patients with breast cancer. Stable disease >or=24 weeks was observed in one evaluable breast cancer patient and 6 (43%) of the 14 evaluable non-small cell lung cancer patients., Conclusion: The maximum tolerated dose of once-daily oral neratinib is 320 mg. The most common neratinib-related toxicity was diarrhea. Antitumor activity was observed in patients with breast cancer who had previous treatment with trastuzumab, anthracyclines, and taxanes, and tumors with a baseline ErbB-2 immunohistochemical staining intensity of 2+ or 3+. The antitumor activity, tolerable toxicity profile, and pharmacokinetic properties of neratinib warrant its further evaluation.

Published

2009

31. Regression of drug-resistant lung cancer by the combination of rosiglitazone and carboplatin.

Author

Girnun GD, Chen L, Silvaggi J, Drapkin R, Chirieac LR, Padera RF, Upadhyay R, Vafai SB, Weissleder R, Mahmood U, Naseri E, Buckley S, Li D, Force J, McNamara K, Demetri G, Spiegelman BM, and Wong KK

Subjects

Animals, Cell Proliferation drug effects, Cell Survival drug effects, Drug Therapy, Combination, ErbB Receptors physiology, Genes, ras physiology, Humans, Lung Neoplasms metabolism, Lung Neoplasms pathology, Magnetic Resonance Imaging, Mice, Mice, Transgenic, PPAR gamma agonists, Protein Kinase Inhibitors adverse effects, Rosiglitazone, Uteroglobin physiology, Antineoplastic Agents therapeutic use, Carboplatin therapeutic use, Drug Resistance, Neoplasm drug effects, Hypoglycemic Agents therapeutic use, Lung Neoplasms drug therapy, Thiazolidinediones therapeutic use

Abstract

Purpose: Current therapy for lung cancer involves multimodality therapies. However, many patients are either refractory to therapy or develop drug resistance. KRAS and epidermal growth factor receptor (EGFR) mutations represent some of the most common mutations in lung cancer, and many studies have shown the importance of these mutations in both carcinogenesis and chemoresistance. Genetically engineered murine models of mutant EGFR and KRAS have been developed that more accurately recapitulate human lung cancer. Recently, using cell-based experiments, we showed that platinum-based drugs and the antidiabetic drug rosiglitazone (PPARgamma ligand) interact synergistically to reduce cancer cell and tumor growth. Here, we directly determined the efficacy of the PPARgamma/carboplatin combination in these more relevant models of drug resistant non-small cell lung cancer., Experimental Design: Tumorigenesis was induced by activation of either mutant KRAS or EGFR. Mice then received either rosiglitazone or carboplatin monotherapy, or a combination of both drugs. Change in tumor burden, pathology, and evidence of apoptosis and cell growth were assessed., Results: Tumor burden remained unchanged or increased in the mice after monotherapy with either rosiglitazone or carboplatin. In striking contrast, we observed significant tumor shrinkage in mice treated with these drugs in combination. Immunohistochemical analyses showed that this synergy was mediated via both increased apoptosis and decreased proliferation. Importantly, this synergy between carboplatin and rosiglitazone did not increase systemic toxicity., Conclusions: These data show that the PPARgamma ligand/carboplatin combination is a new therapy worthy of clinical investigation in lung cancers, including those cancers that show primary resistance to platinum therapy or acquired resistance to targeted therapy.

Published

2008

32. Magnetic resonance imaging of the response of a mouse model of non-small cell lung cancer to tyrosine kinase inhibitor treatment.

Author

Zhou X, Bao H, Al-Hashem R, Ji H, Albert M, Wong KK, and Sun Y

Subjects

Animals, Doxycycline therapeutic use, Magnetic Resonance Imaging, Mice, Mice, Transgenic, Antineoplastic Agents therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, Protein Kinase Inhibitors therapeutic use, Protein-Tyrosine Kinases antagonists & inhibitors

Abstract

Mutational activation of the gene for epidermal growth factor receptor (EGFR) is 1 of the main ways by which this receptor induces non-small cell lung cancers (NSCLC). Variant III EGFR (EGFRvIII) is a potential therapeutic target in NSCLC treatment because of the high frequency of deletion mutations in this protein. This study used noninvasive magnetic resonance imaging (MRI) to investigate the role of an EGFRvIII mutant in lung tumorigenesis and tumor maintenance as well as its response to the EGFR small molecule inhibitor erlotinib (Tarceva) on bitransgenic mice. Both spin-echo and gradient-echo sequences with and without cardiac and respiratory gating were performed to image the invasive mouse lung tumor driven by EGFRvIII mutation. Tumor volumes were measured based on 2-dimensional axial MRI; 3-dimensional rendering of the images were obtained to demonstrate the spatial location and distribution of the tumor in the lung. The MRI results indicated that the tumor driven by the EGFRvIII mutation was generated and maintained in the bitransgenic mice with the use of doxycycline. Tumor monitoring via MRI showed that Erlotinib can significantly inhibit the growth of tumor in vivo. MRI has the ability to image mouse lung tumor with different sequences focusing on tissue contrasts between tumor and surroundings. The MRI approaches in this work can be applied on other antitumor drug treatment evaluation in vivo when appropriate sequences are chosen.

Published

2008

33. Searching for a magic bullet in NSCLC: the role of epidermal growth factor receptor mutations and tyrosine kinase inhibitors.

Author

Wong KK

Subjects

Drug Resistance, Neoplasm genetics, Humans, Antineoplastic Agents pharmacology, Carcinoma, Non-Small-Cell Lung drug therapy, Carcinoma, Non-Small-Cell Lung genetics, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Lung Neoplasms drug therapy, Lung Neoplasms genetics, Mutation genetics, Protein Kinase Inhibitors pharmacology

Abstract

The epidermal growth factor receptor (EGFR) has been implicated in the pathophysiology of various cancers, including non-small cell lung cancer (NSCLC). Inhibitors targeting the tyrosine kinase domain of this receptor have been seen to elicit favourable responses in a subset of NSCLC patients. Mutational analysis of the EGFR has revealed that the response to reversible tyrosine kinase inhibitors (TKIs) is a result of the presence of activating mutations present between exons 18 and 21, most frequently the exon 19 deletion and the L858R mutations. After a prolonged treatment with reversible TKIs, patients have been seen to develop resistance that results, in part, from the presence of the secondary T790M mutation in exon 20. Preclinical data suggest that second-generation TKIs may be able to overcome T790M resistance by virtue of their irreversible mode of binding. In addition to the predominant mutations in the EGFR gene, alternative genetic changes between exons 18 and 21 have been observed. Experimental models have demonstrated that TKIs exhibit differential efficacy depending on which mutations are present. Such information may result in the design of highly specific agents that target specific mutations, which could result in more efficacious treatments.

Published

2008

34. Discovery of a drug-like G-quadruplex binding ligand by high-throughput docking.

Author

Ma DL, Lai TS, Chan FY, Chung WH, Abagyan R, Leung YC, and Wong KY

Subjects

Binding Sites, Binding, Competitive, Circular Dichroism, Computer Simulation, DNA drug effects, Databases as Topic, Drug Screening Assays, Antitumor, Fluorescence Resonance Energy Transfer, Ligands, Models, Molecular, Nucleic Acid Conformation drug effects, Structure-Activity Relationship, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Drug Design, G-Quadruplexes drug effects, Hydrazones chemistry, Hydrazones pharmacology, Pyrazoles chemistry, Pyrazoles pharmacology

Published

2008

35. G-quadruplexes: targets in anticancer drug design.

Author

Ou TM, Lu YJ, Tan JH, Huang ZS, Wong KY, and Gu LQ

Subjects

Antineoplastic Agents pharmacology, Calorimetry, Differential Scanning, DNA chemistry, Genes, bcl-2, Genes, myc, Genome, Human, Humans, Ligands, Models, Molecular, Nucleic Acid Conformation, Porphyrins chemistry, Proto-Oncogene Proteins c-kit genetics, Telomere, Antineoplastic Agents chemistry, Drug Design, G-Quadruplexes

Abstract

G-quadruplexes are special secondary structures adopted in some guanine-rich DNA sequences. As guanine-rich sequences are present in important regions of the eukaryotic genome, such as telomeres and the regulatory regions of many genes, such structures may play important roles in the regulation of biological events in the body. G-quadruplexes have become valid targets for new anticancer drugs in the past few decades. Many leading compounds that target these structures have been reported, and a few of them have entered preclinical or clinical trials. Nonetheless, the selectivity of this kind of antitumor compound has yet to be improved in order to suppress the side effects caused by nonselective binding. As drug design targets, the topology and structural characteristics of quadruplexes, their possible biological roles, and the modes and sites of small-ligand binding to these structures should be understood clearly. Herein we provide a summary of published research that has set out to address the above problem to provide useful information on the design of small ligands that target G-quadruplexes. This review also covers research methodologies that have been developed to study the binding of ligands to G-quadruplexes.

Published

2008

36. PF00299804, an irreversible pan-ERBB inhibitor, is effective in lung cancer models with EGFR and ERBB2 mutations that are resistant to gefitinib.

Author

Engelman JA, Zejnullahu K, Gale CM, Lifshits E, Gonzales AJ, Shimamura T, Zhao F, Vincent PW, Naumov GN, Bradner JE, Althaus IW, Gandhi L, Shapiro GI, Nelson JM, Heymach JV, Meyerson M, Wong KK, and Jänne PA

Subjects

Adaptor Proteins, Signal Transducing drug effects, Animals, Cell Division, Cell Line, Tumor, Cloning, Molecular, ErbB Receptors drug effects, Gefitinib, Humans, Lung Neoplasms, Mice, Mice, Nude, Adaptor Proteins, Signal Transducing genetics, Antineoplastic Agents therapeutic use, ErbB Receptors genetics, Oncogene Proteins v-erbB antagonists & inhibitors, Quinazolines pharmacology, Quinazolinones therapeutic use

Abstract

Epidermal growth factor receptor (EGFR) tyrosine kinase inhibitors gefitinib and erlotinib are effective treatments for a subset of non-small cell lung cancers. In particular, cancers with specific EGFR-activating mutations seem to be the most sensitive to these agents. However, despite their initial response, such cancers almost invariably develop resistance. In 50% of such cancers, a secondary EGFR mutation, T790M, has been identified that renders gefitinib and erlotinib ineffective inhibitors of EGFR kinase activity. Thus, there is a clinical need to develop novel EGFR inhibitors that can effectively inactivate T790M-containing EGFR proteins. In this study, we evaluate the effectiveness of a novel compound, PF00299804, an irreversible pan-ERBB inhibitor. The results from these studies show that PF00299804 is a potent inhibitor of EGFR-activating mutations as well as the EGFR T790M resistance mutation both in vitro and in vivo. Additionally, PF00299804 is a highly effective inhibitor of both the wild-type ERBB2 and the gefitinib-resistant oncogenic ERBB2 mutation identified in lung cancers. These preclinical evaluations support further clinical development of PF00299804 for cancers with mutations and/or amplifications of ERBB family members.

Published

2007

37. HKI-272 in non small cell lung cancer.

Author

Wong KK

Subjects

Animals, Clinical Trials as Topic, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Genetic Predisposition to Disease, Humans, Antineoplastic Agents therapeutic use, Carcinoma, Non-Small-Cell Lung drug therapy, Lung Neoplasms drug therapy, Quinolines therapeutic use

Abstract

Somatic mutations in the kinase domain of the epidermal growth factor receptor (EGFR) gene are found in approximately 10% of lung adenocarcinomas sequenced in the United States and in approximately 30% sequenced in Asia. These mutations are associated with sensitivity to the EGFR inhibitors gefitinib and erlotinib. Many patients who initially respond to erlotinib or gefitinib subsequently relapse. Studies have identified EGFR T790M mutations in tumors from patients who initially responded and then relapsed. The T790M mutation, when combined in vitro with treatment-sensitizing EGFR mutations, permits the continued growth of tumor cells in the presence of erlotinib and gefitinib. HKI-272 is an irreversible EGFR/HER/ErbB inhibitor that has been shown to inhibit the growth of T790M mutant cells in vitro in human lung cancer cell lines and in murine cells transfected with sensitizing EGFR mutations. A phase I HKI-272 monotherapy trial in patients with solid tumors is close to completion. Preliminary analyses of the trial, presented at the 2006 annual meeting of American Society of Clinical Oncology, showed that HKI-272 can achieve stable disease control for over 6 months in some patients with non-small cell lung cancer that has progressed after treatment with gefitinib or erlotinib. A phase II trial of HKI-272 in non-small cell lung cancer patients has been initiated. HKI-272 might offer benefits to non-small cell lung cancer patients who have relapsed after an initial response to erlotinib.

Published

2007

38. Novel agents in the treatment of lung cancer: Fourth Cambridge Conference.

Author

Lynch TJ, Bonomi PD, Butts C, Davies AM, Engelman J, Govindan R, Herbst RS, Heymach JV, Johnson BE, Martins RG, Perez-Soler R, Riely GJ, Sandler AB, Sequist LV, Socinski MA, Wong KK, and Hart CS

Subjects

Animals, Clinical Trials as Topic, Humans, Antineoplastic Agents therapeutic use, Lung Neoplasms drug therapy

Abstract

The Fourth Cambridge Conference on Novel Agents in the Treatment of Lung Cancer was held in Cambridge, Massachusetts on September 29 to 30, 2006, to discuss ongoing clinical research of novel targeted agents for the treatment of non-small cell lung cancer, along with supportive basic and translational research into the molecular pathways implicated in cancer growth and resistance. New information, conclusions, and recommendations considered significant for the field by the program faculty are summarized below and presented at greater length in the individual articles and accompanying discussions that comprise the full conference proceedings.

Published

2007

39. Stabilization of G-quadruplex DNA and down-regulation of oncogene c-myc by quindoline derivatives.

Author

Ou TM, Lu YJ, Zhang C, Huang ZS, Wang XD, Tan JH, Chen Y, Ma DL, Wong KY, Tang JC, Chan AS, and Gu LQ

Subjects

Alkaloids pharmacology, Antineoplastic Agents pharmacology, Base Sequence, Cell Line, Tumor, Cell Proliferation drug effects, Circular Dichroism, DNA chemistry, Dialysis, Humans, Indoles pharmacology, Isomerism, Models, Molecular, Promoter Regions, Genetic, Proto-Oncogene Proteins c-myc genetics, Quinolines pharmacology, Static Electricity, Structure-Activity Relationship, Thermodynamics, Alkaloids chemistry, Antineoplastic Agents chemistry, DNA genetics, Guanine chemistry, Indoles chemistry, Nucleic Acid Conformation, Proto-Oncogene Proteins c-myc biosynthesis, Quinolines chemistry

Abstract

Stabilization of G-quadruplex structures in the promoter region of certain oncogenes is an emerging field in anticancer drug design. Human c-myc gene is one of these oncogenes, and G-quadruplexes have been proven to be the transcriptional controller of this gene. In the present study, the interaction of quindoline derivatives with G-quadruplexes in c-myc was investigated. The experimental results indicated that these derivatives have the ability to induce/stabilize the G-quadruplexes in c-myc, which lead to down-regulation of the c-myc in the Hep G2 cell line. It was found that derivatives with terminal amino groups in their side chains would selectively bind to the isomers with the double nucleotide loops in the absence of K+. Molecular modeling studies revealed the binding mode between the derivatives and the G-quadruplexes is end-stacking at the 3'-position, and the positively charged side chain on the quindoline derivatives may contribute to the selectivity to certain loop isomers of topological quadruplexes as well as the improved stabilization action.

Published

2007

40. DNA binding and cytotoxicity of ruthenium(II) and rhenium(I) complexes of 2-amino-4-phenylamino-6-(2-pyridyl)-1,3,5-triazine.

Author

Ma DL, Che CM, Siu FM, Yang M, and Wong KY

Subjects

Animals, Antineoplastic Agents chemical synthesis, Apoptosis drug effects, Binding Sites, Binding, Competitive, Cell Line, Tumor, Crystallography, X-Ray, Humans, Hydrogen Bonding, Nucleic Acid Denaturation, Oligonucleotides chemistry, Spectrophotometry, Ultraviolet, Temperature, Antineoplastic Agents chemistry, DNA chemistry, Ruthenium Compounds chemistry

Abstract

[Ru(tBu2bpy)2(2-appt)](PF6)2 [1.(PF6)2, tBu2bpy = 4,4'-di-tert-butyl-2,2'-bipyridine, 2-appt = 2-amino-4-phenylamino-6-(2-pyridyl)-1,3,5-triazine] and [Re(CO)3(2-appt)Cl] (2) were prepared and characterized by X-ray crystal analysis. The binding of 1.(PF6)2 and 2 to calf thymus DNA (ct DNA) led to increases in the DNA melting temperature (Delta Tm = +12 degrees C), modest hypochromism (29% and 5% of the absorption bands at lambda max = 450 and 376 nm, respectively), and insignificant shifts in the absorption maxima. The binding constants of 1.(PF6)2 and 2 with ct DNA, as determined by absorption titration, are (8.9 +/- 0.5) x 104 and (3.6 +/- 0.1) x 104 dm3 mol-1, respectively. UV-vis absorption titration, DNA melting studies, and competition dialysis using synthetic oligonucleotides [poly(dA-dT)2 and poly(dG-dC)2] revealed that 1.(PF6)2 and 2 exhibit a binding preference for AT sequences. A modeling study on the interaction between 1 or 2 and B-DNA revealed that the minor groove is the most favored binding site and an extensive hydrogen-bonding network is formed. As determined by MTT assays, 1.(PF6)2 and 2 exhibited moderate cytotoxicities toward several human cancer cell lines (KB-3-1, HepG2, and HeLa), as well as a multi-drug-resistant cancer cell line (KB-V-1). According to confocal microscopic and flow cytometric studies, 1.(PF6)2 and 2 induced apoptosis (50-60%) in cancer cells with <5% necrosis detected.

Published

2007

41. The impact of human EGFR kinase domain mutations on lung tumorigenesis and in vivo sensitivity to EGFR-targeted therapies.

Author

Ji H, Li D, Chen L, Shimamura T, Kobayashi S, McNamara K, Mahmood U, Mitchell A, Sun Y, Al-Hashem R, Chirieac LR, Padera R, Bronson RT, Kim W, Jänne PA, Shapiro GI, Tenen D, Johnson BE, Weissleder R, Sharpless NE, and Wong KK

Subjects

Adenocarcinoma drug therapy, Adenocarcinoma pathology, Adenocarcinoma, Bronchiolo-Alveolar drug therapy, Adenocarcinoma, Bronchiolo-Alveolar genetics, Adenocarcinoma, Bronchiolo-Alveolar pathology, Animals, Antibodies, Monoclonal therapeutic use, Antibodies, Monoclonal, Humanized, Cetuximab, Enzyme Activation, ErbB Receptors antagonists & inhibitors, ErbB Receptors genetics, Erlotinib Hydrochloride, Exons, Humans, Lung metabolism, Lung Neoplasms drug therapy, Lung Neoplasms pathology, Mice, Mice, Transgenic, Mutation, Protein Structure, Tertiary, Quinazolines therapeutic use, Quinolines therapeutic use, Adenocarcinoma genetics, Antineoplastic Agents therapeutic use, ErbB Receptors metabolism, Lung Neoplasms genetics

Abstract

To understand the role of human epidermal growth factor receptor (hEGFR) kinase domain mutations in lung tumorigenesis and response to EGFR-targeted therapies, we generated bitransgenic mice with inducible expression in type II pneumocytes of two common hEGFR mutants seen in human lung cancer. Both bitransgenic lines developed lung adenocarcinoma after sustained hEGFR mutant expression, confirming their oncogenic potential. Maintenance of these lung tumors was dependent on continued expression of the EGFR mutants. Treatment with small molecule inhibitors (erlotinib or HKI-272) as well as prolonged treatment with a humanized anti-hEGFR antibody (cetuximab) led to dramatic tumor regression. These data suggest that persistent EGFR signaling is required for tumor maintenance in human lung adenocarcinomas expressing EGFR mutants.

Published

2006

42. Complications of gastrectomy following CPT-11-based neoadjuvant chemotherapy for gastric cancer.

Author

Marcus SG, Cohen D, Lin K, Wong K, Thompson S, Rothberger A, Potmesil M, Hiotis S, and Newman E

Subjects

Adenocarcinoma drug therapy, Adenocarcinoma pathology, Adult, Aged, Aged, 80 and over, Cisplatin adverse effects, Female, Humans, Irinotecan, Male, Middle Aged, Neoadjuvant Therapy, Neoplasm Staging, Stomach Neoplasms drug therapy, Stomach Neoplasms pathology, Treatment Outcome, Adenocarcinoma surgery, Antineoplastic Agents adverse effects, Camptothecin adverse effects, Camptothecin analogs & derivatives, Gastrectomy mortality, Postoperative Complications mortality, Stomach Neoplasms surgery

Abstract

Potential benefits of neoadjuvant therapy for locally advanced gastric cancer include tumor downstaging and an increased R0 resection rate. Potential disadvantages include increased surgical complications. This study assesses postoperative morbidity and mortality by comparing patients undergoing gastrectomy with and without neoadjuvant chemotherapy. From October 1998 to July 2002, a total of 34 patients with locally advanced gastric cancer were placed on a phase II neoadjuvant chemotherapy protocol consisting of two cycles of CPT-11 (75 mg/m(2)) with cisplatin (25 mg/m(2)). Demographic, clinical, morbidity, and mortality data were compared for these patients (CHEMO) versus 85 patients undergoing gastrectomy without neoadjuvant chemotherapy (SURG). The CHEMO patients were more likely to be less than 70 years of age (P< or =0.01), have proximal tumors (P< or =0.01), and undergo proximal gastrectomy (P< or =0.025). Fifty-two percent of SURG patients had T3/T4 tumors compared to 19% of CHEMO patients, consistent with tumor downstaging. The R0 resection rate was similar (80%). Morbidity was 41% in CHEMO patients and 39% in SURG patients. There were five postoperative deaths (4.4%), two in the CHEMO group and three in the SURG group (P=NS). It was concluded that neoadjuvant chemotherapy with CPT-11 and cisplatin is not associated with increased postoperative morbidity compared to surgery alone. CPT-11-based neoadjuvant chemotherapy should be tested further in combined-modality treatment of gastric cancer.

Published

2003

43. Overcoming Resistance to Dual Innate Immune and MEK Inhibition Downstream of KRAS

Author

Kitajima, Shunsuke, Asahina, Hajime, Chen, Ting, Guo, Sujuan, Quiceno, Laura Gutierrez, Cavanaugh, Jillian D, Merlino, Ashley A, Tange, Shoichiro, Terai, Hideki, Kim, Jong Wook, Wang, Xiaoen, Zhou, Shan, Xu, Man, Wang, Stephen, Zhu, Zehua, Thai, Tran C, Takahashi, Chiaki, Wang, Yujin, Neve, Richard, Stinson, Susanna, Tamayo, Pablo, Watanabe, Hideo, Kirschmeier, Paul T, Wong, Kwok-Kin, and Barbie, David A

Subjects

Cancer, Lung, Lung Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, AMP-Activated Protein Kinase Kinases, AMP-Activated Protein Kinases, Adaptor Proteins, Signal Transducing, Animals, Antineoplastic Agents, Immunological, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Disease Models, Animal, Drug Resistance, Neoplasm, HEK293 Cells, Humans, Immunity, Innate, Insulin-Like Growth Factor I, Lung Neoplasms, Mice, Mice, Transgenic, Mitogen-Activated Protein Kinase Kinases, Phosphoproteins, Protein Kinase Inhibitors, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins p21(ras), Transcription Factors, YAP-Signaling Proteins, BET inhibitor, IL-6, KRAS, MEK inhibitor, STK11/LKB1, TBK1 inhibitor, TP53, YAP1 signaling, innate immune signaling, non-small-cell lung cancer, Neurosciences, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Despite extensive efforts, oncogenic KRAS remains resistant to targeted therapy. Combined downstream RAL-TBK1 and MEK inhibition induces only transient lung tumor shrinkage in KRAS-driven genetically engineered mouse models (GEMMs). Using the sensitive KRAS;LKB1 (KL) mutant background, we identify YAP1 upregulation and a therapy-induced secretome as mediators of acquired resistance. This program is reversible, associated with H3K27 promoter acetylation, and suppressed by BET inhibition, resensitizing resistant KL cells to TBK1/MEK inhibition. Constitutive YAP1 signaling promotes intrinsic resistance in KRAS;TP53 (KP) mutant lung cancer. Intermittent treatment with the BET inhibitor JQ1 thus overcomes resistance to combined pathway inhibition in KL and KP GEMMs. Using potent and selective TBK1 and BET inhibitors we further develop an effective therapeutic strategy with potential translatability to the clinic.

Published

2018

44. STK11/LKB1 Mutations and PD-1 Inhibitor Resistance in KRAS-Mutant Lung Adenocarcinoma.

Author

Skoulidis, Ferdinandos, Goldberg, Michael, Greenawalt, Danielle, Hellmann, Matthew, Awad, Mark, Gainor, Justin, Schrock, Alexa, Hartmaier, Ryan, Trabucco, Sally, Gay, Laurie, Ali, Siraj, Elvin, Julia, Singal, Gaurav, Ross, Jeffrey, Fabrizio, David, Szabo, Peter, Chang, Han, Sasson, Ariella, Srinivasan, Sujaya, Kirov, Stefan, Szustakowski, Joseph, Vitazka, Patrik, Edwards, Robin, Bufill, Jose, Sharma, Neelesh, Ou, Sai-Hong, Peled, Nir, Spigel, David, Rizvi, Hira, Aguilar, Elizabeth, Carter, Brett, Erasmus, Jeremy, Halpenny, Darragh, Plodkowski, Andrew, Long, Niamh, Nishino, Mizuki, Denning, Warren, Galan-Cobo, Ana, Hamdi, Haifa, Hirz, Taghreed, Tong, Pan, Wang, Jing, Rodriguez-Canales, Jaime, Villalobos, Pamela, Parra, Edwin, Kalhor, Neda, Sholl, Lynette, Sauter, Jennifer, Jungbluth, Achim, Mino-Kenudson, Mari, Azimi, Roxana, Elamin, Yasir, Zhang, Jianjun, Leonardi, Giulia, Wong, Kwok-Kin, Lee, J, Papadimitrakopoulou, Vassiliki, Wistuba, Ignacio, Miller, Vincent, Frampton, Garrett, Wolchok, Jedd, Shaw, Alice, Jänne, Pasi, Stephens, Philip, Rudin, Charles, Geese, William, Albacker, Lee, Heymach, John, and Jiang, Fei

Subjects

AMP-Activated Protein Kinase Kinases, Adenocarcinoma of Lung, Adult, Aged, Aged, 80 and over, Animals, Antineoplastic Agents, Immunological, Disease Models, Animal, Drug Resistance, Neoplasm, Humans, Immunotherapy, Lung Neoplasms, Male, Mice, Middle Aged, Mutation, Nivolumab, Prognosis, Programmed Cell Death 1 Receptor, Progression-Free Survival, Protein Serine-Threonine Kinases, Proto-Oncogene Proteins p21(ras)

Abstract

KRAS is the most common oncogenic driver in lung adenocarcinoma (LUAC). We previously reported that STK11/LKB1 (KL) or TP53 (KP) comutations define distinct subgroups of KRAS-mutant LUAC. Here, we examine the efficacy of PD-1 inhibitors in these subgroups. Objective response rates to PD-1 blockade differed significantly among KL (7.4%), KP (35.7%), and K-only (28.6%) subgroups (P < 0.001) in the Stand Up To Cancer (SU2C) cohort (174 patients) with KRAS-mutant LUAC and in patients treated with nivolumab in the CheckMate-057 phase III trial (0% vs. 57.1% vs. 18.2%; P = 0.047). In the SU2C cohort, KL LUAC exhibited shorter progression-free (P < 0.001) and overall (P = 0.0015) survival compared with KRASMUT;STK11/LKB1WT LUAC. Among 924 LUACs, STK11/LKB1 alterations were the only marker significantly associated with PD-L1 negativity in TMBIntermediate/High LUAC. The impact of STK11/LKB1 alterations on clinical outcomes with PD-1/PD-L1 inhibitors extended to PD-L1-positive non-small cell lung cancer. In Kras-mutant murine LUAC models, Stk11/Lkb1 loss promoted PD-1/PD-L1 inhibitor resistance, suggesting a causal role. Our results identify STK11/LKB1 alterations as a major driver of primary resistance to PD-1 blockade in KRAS-mutant LUAC.Significance: This work identifies STK11/LKB1 alterations as the most prevalent genomic driver of primary resistance to PD-1 axis inhibitors in KRAS-mutant lung adenocarcinoma. Genomic profiling may enhance the predictive utility of PD-L1 expression and tumor mutation burden and facilitate establishment of personalized combination immunotherapy approaches for genomically defined LUAC subsets. Cancer Discov; 8(7); 822-35. ©2018 AACR.See related commentary by Etxeberria et al., p. 794This article is highlighted in the In This Issue feature, p. 781.

Published

2018

45. Magnetic Resonance Imaging of the Response of a Mouse Model of Non-Small Cell Lung Cancer to Tyrosine Kinase Inhibitor Treatment

Author

Zhou, Xiangzhi, Bao, Haihua, Al-Hashem, Ruqayyah, Ji, Hongbin, Albert, Mitchell, Wong, Kwok-Kin, and Sun, Yanping

Subjects

Mice, Lung Neoplasms, Carcinoma, Non-Small-Cell Lung, Doxycycline, Animals, Mouse Models, Antineoplastic Agents, Mice, Transgenic, Protein-Tyrosine Kinases, Magnetic Resonance Imaging, Protein Kinase Inhibitors, respiratory tract diseases

Abstract

Mutational activation of the gene for epidermal growth factor receptor (EGFR) is 1 of the main ways by which this receptor induces non-small cell lung cancers (NSCLC). Variant III EGFR (EGFRvIII) is a potential therapeutic target in NSCLC treatment because of the high frequency of deletion mutations in this protein. This study used noninvasive magnetic resonance imaging (MRI) to investigate the role of an EGFRvIII mutant in lung tumorigenesis and tumor maintenance as well as its response to the EGFR small molecule inhibitor erlotinib (Tarceva) on bitransgenic mice. Both spin-echo and gradient-echo sequences with and without cardiac and respiratory gating were performed to image the invasive mouse lung tumor driven by EGFRvIII mutation. Tumor volumes were measured based on 2-dimensional axial MRI; 3-dimensional rendering of the images were obtained to demonstrate the spatial location and distribution of the tumor in the lung. The MRI results indicated that the tumor driven by the EGFRvIII mutation was generated and maintained in the bitransgenic mice with the use of doxycycline. Tumor monitoring via MRI showed that Erlotinib can significantly inhibit the growth of tumor in vivo. MRI has the ability to image mouse lung tumor with different sequences focusing on tissue contrasts between tumor and surroundings. The MRI approaches in this work can be applied on other antitumor drug treatment evaluation in vivo when appropriate sequences are chosen.

Published

2008