Your search keyword '"Xenograft Model Antitumor Assays"' showing total 87,417 results

1. Targeting Patient-Derived Orthotopic Gastric Cancers with a Fluorescent Humanized Anti-CEA Antibody

Author

Cox, Kristin E, Turner, Michael A, Lwin, Thinzar M, Amirfakhri, Siamak, Kelly, Kaitlyn J, Hosseini, Mojgan, Ghosh, Pradipta, Obonyo, Marygorret, Hoffman, Robert M, Yazaki, Paul J, and Bouvet, Michael

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Orphan Drug, Rare Diseases, Digestive Diseases, 5.1 Pharmaceuticals, Stomach Neoplasms, Animals, Humans, Mice, Carcinoembryonic Antigen, Adenocarcinoma, Xenograft Model Antitumor Assays, Antibodies, Monoclonal, Humanized, Fluorescent Dyes, Tumor Cells, Cultured, Female, Indoles, Optical Imaging, Gastrectomy, Mice, Nude, Cell Line, Tumor, Gastric cancer, Patient-derived orthotopic xenograft, PDOX, Fluorescence, Fluorescent antibody, CEA, Tumor targeting, Tumor labeling, Gastric cancer, Oncology & Carcinogenesis, Oncology and carcinogenesis

Abstract

BackgroundGastric cancer poses a major diagnostic and therapeutic challenge as surgical resection provides the only opportunity for a cure. Specific labeling of gastric cancer could distinguish resectable and nonresectable disease and facilitate an R0 resection, which could improve survival.MethodsTwo patient-derived gastric cancer lines, KG8 and KG10, were established from surgical specimens of two patients who underwent gastrectomy for gastric adenocarcinoma. Harvested tumor fragments were implanted into the greater curvature of the stomach to establish patient-derived orthotopic xenograft (PDOX) models. M5A (humanized anti-CEA antibody) or IgG control antibodies were conjugated with the near-infrared dye IRDye800CW. Mice received 50 µg of M5A-IR800 or 50 µg of IgG-IR800 intravenously and were imaged after 72 hr. Fluorescence imaging was performed by using the LI-COR Pearl Imaging System. A tumor-to-background ratio (TBR) was calculated by dividing the mean fluorescence intensity of the tumor versus adjacent stomach tissue.ResultsM5A-IR800 administration resulted in bright labeling of both KG8 and K10 tumors. In the KG8 PDOX models, the TBR for M5A-IR800 was 5.85 (SE ± 1.64) compared with IgG-IR800 at 0.70 (SE ± 0.17). The K10 PDOX models had a TBR of 3.71 (SE ± 0.73) for M5A-IR800 compared with 0.66 (SE ± 0.12) for IgG-IR800.ConclusionsHumanized anti-CEA (M5A) antibodies conjugated to fluorescent dyes provide bright and specific labeling of gastric cancer PDOX models. This tumor-specific fluorescent antibody is a promising potential clinical tool to detect the extent of disease for the determination of resectability as well as to visualize tumor margins during gastric cancer resection.

Published

2024

2. Entinostat as a combinatorial therapeutic for rhabdomyosarcoma.

Author

Chauhan, Shefali, Lian, Emily, Habib, Iman, Liu, Qianqian, Anders, Nicole, Bugg, Megan, Federman, Noah, Reid, Joel, Stewart, Clinton, Cates, Tristan, Michalek, Joel, and Keller, Charles

Subjects

Alveolar rhabdomyosarcoma, Embryonal rhabdomyosarcoma, Entinostat, HDAC inhibitor, Mocetinostat, Rhabdomyosarcoma, Humans, Pyridines, Animals, Benzamides, Mice, Rhabdomyosarcoma, Xenograft Model Antitumor Assays, Cell Line, Tumor, Histone Deacetylase Inhibitors, Antineoplastic Combined Chemotherapy Protocols

Abstract

Rhabdomyosarcoma (RMS) is the most common childhood soft tissue sarcoma. For the alveolar subtype (ARMS), the presence of the PAX3::FOXO1 fusion gene and/or metastases are strong predictors of poor outcome. Metastatic PAX3::FOXO1+ ARMS often responds to chemotherapies initially, only to subsequently relapse and become resistant with most patients failing to survive beyond 8 years post-diagnosis. No curative intent phase II or phase III clinical trial has been available for patients in the past 10 years (ARST0921). Thus, metastatic ARMS represents a significantly unmet clinical need. Chemotherapy resistance in ARMS has previously been attributed to PAX3::FOXO1-mediated cell cycle checkpoint adaptation, which is mediated by an HDAC3-SMARCA4-miR-27a-PAX3::FOXO1 circuit that can be disrupted by HDAC3 inhibition. In this study, we investigated the therapeutic efficacy of combining the epigenetic regulator entinostat, a Class I Histone Deacetylase (HDAC1-3) inhibitor, with RMS-specific chemotherapies in patient derived xenograft (PDX) models of RMS. We identified single agent, additive or synergistic relationships between relapse-specific chemotherapies and clinically relevant drug exposures of entinostat in three PAX3::FOXO1+ ARMS mouse models. This preclinical data provides further rationale for clinical investigation of entinostat, already known to be well tolerated in a pediatric phase I clinical trial (ADVL1513).

Published

2024

3. Manzamine A reduces androgen receptor transcription and synthesis by blocking E2F8-DNA interactions and effectively inhibits prostate tumor growth in mice.

Author

Karan, Dev, Dubey, Seema, Gunewardena, Sumedha, Iczkowski, Kenneth, Singh, Manohar, Liu, Pengyuan, Poletti, Angelo, Choo, Yeun-Mun, Chen, Hui-Zi, and Hamann, Mark

Subjects

E2F8, androgen receptor, manzamine A, prostate cancer, Male, Animals, Receptors, Androgen, Humans, Mice, Cell Line, Tumor, Prostatic Neoplasms, Transcription, Genetic, Xenograft Model Antitumor Assays, Cell Proliferation, Gene Expression Regulation, Neoplastic, Mice, Nude, DNA

Abstract

The androgen receptor (AR) is the main driver in the development of castration-resistant prostate cancer, where the emergence of AR splice variants leads to treatment-resistant disease. Through detailed molecular studies of the marine alkaloid manzamine A (MA), we identified transcription factor E2F8 as a previously unknown regulator of AR transcription that prevents AR synthesis in prostate cancer cells. MA significantly inhibited the growth of various prostate cancer cell lines and was highly effective in inhibiting xenograft tumor growth in mice without any pathophysiological perturbations in major organs. MA suppressed the full-length AR (AR-FL), its spliced variant AR-V7, and the AR-regulated prostate-specific antigen (PSA; also known as KLK3) and human kallikrein 2 (hK2; also known as KLK2) genes. RNA sequencing (RNA-seq) analysis and protein modeling studies revealed E2F8 interactions with DNA as a potential novel target of MA, suppressing AR transcription and its synthesis. This novel mechanism of blocking AR biogenesis via E2F8 may provide an opportunity to control therapy-resistant prostate cancer over the currently used AR antagonists designed to target different parts of the AR gene.

Published

2024

4. Development and application of genetic ancestry reconstruction methods to study diversity of patient-derived models in the NCI PDXNet Consortium

Author

Lott, Paul C, Chiu, Katherine, Quino, Juanita Elizabeth, Vang, April Pangia, Lloyd, Michael W, Srivastava, Anuj, Chuang, Jeffrey H, Consortium, for the PDXNet, and Carvajal-Carmona, Luis G

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Genetics, Health Services and Systems, Health Sciences, Human Genome, Social Determinants of Health, Health Disparities, Precision Medicine, Cancer Genomics, Cancer, Minority Health, Good Health and Well Being, Humans, United States, Neoplasms, Animals, National Cancer Institute (U.S.), Genomics, Mice, Xenograft Model Antitumor Assays, PDXNet Consortium

Abstract

Precision medicine holds great promise for improving cancer outcomes. Yet, there are large inequities in the demographics of patients from whom genomic data and models, including patient-derived xenografts (PDX), are developed and for whom treatments are optimized. In this study, we developed a genetic ancestry pipeline for the Cancer Genomics Cloud, which we used to assess the diversity of models currently available in the National Cancer Institute-supported PDX Development and Trial Centers Research Network (PDXNet). We showed that there is an under-representation of models derived from patients of non-European ancestry, consistent with other cancer model resources. We discussed these findings in the context of disparities in cancer incidence and outcomes among demographic groups in the US, as well as power analyses for biomarker discovery, to highlight the immediate need for developing models from minority populations to address cancer health equity in precision medicine. Our analyses identified key priority disparity-associated cancer types for which new models should be developed.SignificanceUnderstanding whether and how tumor genetic factors drive differences in outcomes among U.S. minority groups is critical to addressing cancer health disparities. Our findings suggest that many additional models will be necessary to understand the genome-driven sources of these disparities.

Published

2024

5. Plexin D1 emerges as a novel target in the development of neural lineage plasticity in treatment-resistant prostate cancer

Author

Chen, Bo, Xu, Pengfei, Yang, Joy C, Nip, Christopher, Wang, Leyi, Shen, Yuqiu, Ning, Shu, Shang, Yufeng, Corey, Eva, Gao, Allen C, Gestwicki, Jason E, Wei, Qiang, Liu, Liangren, and Liu, Chengfei

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Cancer, Genetics, Biotechnology, Prostate Cancer, Urologic Diseases, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Humans, Male, Animals, Mice, Drug Resistance, Neoplasm, Cell Line, Tumor, Prostatic Neoplasms, Cell Proliferation, Gene Expression Regulation, Neoplastic, Cell Lineage, Nerve Tissue Proteins, Xenograft Model Antitumor Assays, Cell Plasticity, Receptors, Cell Surface, Prognosis, Membrane Glycoproteins, Intracellular Signaling Peptides and Proteins, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Treatment-induced neuroendocrine prostate cancer (t-NEPC) often arises from adenocarcinoma via lineage plasticity in response to androgen receptor signaling inhibitors, such as enzalutamide. However, the specific regulators and targets involved in the transition to NEPC are not well understood. Plexin D1 (PLXND1) is a cellular receptor of the semaphorin (SEMA) family that plays important roles in modulating the cytoskeleton and cell adhesion. Here, we found that PLXND1 was highly expressed and positively correlated with neuroendocrine markers in patients with NEPC. High PLXND1 expression was associated with poorer prognosis in prostate cancer patients. Additionally, PLXND1 was upregulated and negatively regulated by androgen receptor signaling in enzalutamide-resistant cells. Knockdown or knockout of PLXND1 inhibited neural lineage pathways, thereby suppressing NEPC cell proliferation, patient derived xenograft (PDX) tumor organoid viability, and xenograft tumor growth. Mechanistically, the heat shock protein 70 (HSP70) regulated PLXND1 protein stability through degradation, and inhibition of HSP70 decreased PLXND1 expression and NEPC organoid growth. In summary, our findings indicate that PLXND1 could serve as a promising therapeutic target and molecular marker for NEPC.

Published

2024

6. Assessment of Patient-Derived Xenograft Growth and Antitumor Activity: The NCI PDXNet Consensus Recommendations.

Author

Meric-Bernstam, Funda, Lloyd, Michael, Koc, Soner, Evrard, Yvonne, McShane, Lisa, Lewis, Michael, Evans, Kurt, Li, Dali, Rubinstein, Lawrence, Welm, Alana, Dean, Dennis, Srivastava, Anuj, Grover, Jeffrey, Ha, Min, Chen, Huiqin, Huang, Xuelin, Varadarajan, Kaushik, Wang, Jing, Roth, Jack, Welm, Bryan, Govinden, Ramaswamy, Ding, Li, Kaochar, Salma, Mitsiades, Nicholas, Carvajal-Carmona, Luis, Herylyn, Meenhard, Davies, Michael, Shapiro, Geoffrey, Fields, Ryan, Trevino, Jose, Harrell, Joshua, Doroshow, James, Chuang, Jeffrey, and Moscow, Jeffrey

Subjects

Humans, Animals, Xenograft Model Antitumor Assays, Neoplasms, National Cancer Institute (U.S.), United States, Mice, Antineoplastic Agents, Consensus

Abstract

Although patient-derived xenografts (PDX) are commonly used for preclinical modeling in cancer research, a standard approach to in vivo tumor growth analysis and assessment of antitumor activity is lacking, complicating the comparison of different studies and determination of whether a PDX experiment has produced evidence needed to consider a new therapy promising. We present consensus recommendations for assessment of PDX growth and antitumor activity, providing public access to a suite of tools for in vivo growth analyses. We expect that harmonizing PDX study design and analysis and assessing a suite of analytical tools will enhance information exchange and facilitate identification of promising novel therapies and biomarkers for guiding cancer therapy.

Published

2024

7. A deep learning model of tumor cell architecture elucidates response and resistance to CDK4/6 inhibitors.

Author

Park, Sungjoon, Silva, Erica, Singhal, Akshat, Kelly, Marcus, Licon, Kate, Panagiotou, Isabella, Fogg, Catalina, Fong, Samson, Lee, John, Zhao, Xiaoyu, Bachelder, Robin, Parker, Barbara, Yeung, Kay, and Ideker, Trey

Subjects

Humans, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, Drug Resistance, Neoplasm, Deep Learning, Animals, Protein Kinase Inhibitors, Pyridines, Female, Piperazines, Mice, Cell Line, Tumor, Breast Neoplasms, Xenograft Model Antitumor Assays

Abstract

Cyclin-dependent kinase 4 and 6 inhibitors (CDK4/6is) have revolutionized breast cancer therapy. However,

Published

2024

8. A Kinome-Wide Synthetic Lethal CRISPR/Cas9 Screen Reveals That mTOR Inhibition Prevents Adaptive Resistance to CDK4/CDK6 Blockade in HNSCC.

Author

Goto, Yusuke, Koshizuka, Keiichi, Ando, Toshinori, Izumi, Hiroki, Wu, Xingyu, Sato, Kuniaki, Ishikawa, Tomohiko, Ford, Kyle, Feng, Xiaodong, Wang, Zhiyong, Arang, Nadia, Allevato, Michael, Kishore, Ayush, Mali, Prashant, and Gutkind, Jorge

Subjects

Humans, Cyclin-Dependent Kinase 4, Cyclin-Dependent Kinase 6, CRISPR-Cas Systems, Squamous Cell Carcinoma of Head and Neck, Piperazines, Pyridines, Mice, Animals, Drug Resistance, Neoplasm, Head and Neck Neoplasms, Cell Line, Tumor, MTOR Inhibitors, Protein Kinase Inhibitors, TOR Serine-Threonine Kinases, Cyclin E, Xenograft Model Antitumor Assays, Synthetic Lethal Mutations, Oncogene Proteins

Abstract

UNLABELLED: The comprehensive genomic analysis of the head and neck squamous cell carcinoma (HNSCC) oncogenome revealed the frequent loss of p16INK4A (CDKN2A) and amplification of cyclin D1 genes in most human papillomavirus-negative HNSCC lesions. However, cyclin-dependent kinase 4 and 6 (CDK4/6) inhibitors have shown modest effects in the clinic. The aberrant activation of the PI3K/mTOR pathway is highly prevalent in HNSCC, and recent clinical trials have shown promising clinical efficacy of mTOR inhibitors (mTORi) in the neoadjuvant and adjuvant settings but not in patients with advanced HNSCC. By implementing a kinome-wide CRISPR/Cas9 screen, we identified cell-cycle inhibition as a synthetic lethal target for mTORis. A combination of mTORi and palbociclib, a CDK4/6-specific inhibitor, showed strong synergism in HNSCC-derived cells in vitro and in vivo. Remarkably, we found that an adaptive increase in cyclin E1 (CCNE1) expression upon palbociclib treatment underlies the rapid acquired resistance to this CDK4/6 inhibitor. Mechanistically, mTORi inhibits the formation of eIF4G-CCNE1 mRNA complexes, with the consequent reduction in mRNA translation and CCNE1 protein expression. Our findings suggest that mTORi reverts the adaptive resistance to palbociclib. This provides a multimodal therapeutic option for HNSCC by cotargeting mTOR and CDK4/6, which in turn may halt the emergence of palbociclib resistance. SIGNIFICANCE: A kinome-wide CRISPR/Cas9 screen identified cell-cycle inhibition as a synthetic lethal target of mTORis. A combination of mTORi and palbociclib, a CDK4/6-specific inhibitor, showed strong synergistic effects in HNSCC. Mechanistically, mTORis inhibited palbociclib-induced increase in CCNE1.

Published

2024

9. N-Myristoytransferase Inhibition Causes Mitochondrial Iron Overload and Parthanatos in TIM17A-Dependent Aggressive Lung Carcinoma

Author

Geroyska, Sofia, Mejia, Isabel, Chan, Alfred A, Navarrete, Marian, Pandey, Vijaya, Kharpatin, Samuel, Noguti, Juliana, Wang, Feng, Srole, Daniel, Chou, Tsui-Fen, Wohlschlegel, James, Nemeth, Elizabeta, Damoiseaux, Robert, Shackelford, David B, Lee, Delphine J, and Díaz, Begoña

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Digestive Diseases, Cancer, Lung, Genetics, Lung Cancer, Orphan Drug, Rare Diseases, 5.1 Pharmaceuticals, 2.1 Biological and endogenous factors, Humans, Lung Neoplasms, Animals, Mitochondrial Precursor Protein Import Complex Proteins, Mitochondria, Acyltransferases, Mice, Iron Overload, Cell Line, Tumor, Kelch-Like ECH-Associated Protein 1, Membrane Transport Proteins, Protein Serine-Threonine Kinases, AMP-Activated Protein Kinase Kinases, Proto-Oncogene Proteins p21(ras), Xenograft Model Antitumor Assays, Mutation, Oxidative Stress

Abstract

Myristoylation is a type of protein acylation by which the fatty acid myristate is added to the N-terminus of target proteins, a process mediated by N-myristoyltransferases (NMT). Myristoylation is emerging as a promising cancer therapeutic target; however, the molecular determinants of sensitivity to NMT inhibition or the mechanism by which it induces cancer cell death are not completely understood. We report that NMTs are a novel therapeutic target in lung carcinoma cells with LKB1 and/or KEAP1 mutations in a KRAS-mutant background. Inhibition of myristoylation decreases cell viability in vitro and tumor growth in vivo. Inhibition of myristoylation causes mitochondrial ferrous iron overload, oxidative stress, elevated protein poly (ADP)-ribosylation, and death by parthanatos. Furthermore, NMT inhibitors sensitized lung carcinoma cells to platinum-based chemotherapy. Unexpectedly, the mitochondrial transporter translocase of inner mitochondrial membrane 17 homolog A (TIM17A) is a critical target of myristoylation inhibitors in these cells. TIM17A silencing recapitulated the effects of NMT inhibition at inducing mitochondrial ferrous iron overload and parthanatos. Furthermore, sensitivity of lung carcinoma cells to myristoylation inhibition correlated with their dependency on TIM17A. This study reveals the unexpected connection between protein myristoylation, the mitochondrial import machinery, and iron homeostasis. It also uncovers myristoylation inhibitors as novel inducers of parthanatos in cancer, and the novel axis NMT-TIM17A as a potential therapeutic target in highly aggressive lung carcinomas.SignificanceKRAS-mutant lung carcinomas with LKB1 and/or KEAP1 co-mutations have intrinsic therapeutic resistance. We show that these tumors are sensitive to NMT inhibitors, which slow tumor growth in vivo and sensitize cells to platinum-based chemotherapy in vitro. Inhibition of myristoylation causes death by parthanatos and thus has the potential to kill apoptosis and ferroptosis-resistant cancer cells. Our findings warrant investigation of NMT as a therapeutic target in highly aggressive lung carcinomas.

Published

2024

10. Discovery of CDC42 Inhibitors with a Favorable Pharmacokinetic Profile and Anticancer In Vivo Efficacy.

Author

Brindani, Nicoletta, Vuong, Linh, La Serra, Maria, Salvador, Noel, Menichetti, Andrea, Acquistapace, Isabella, Ortega, Jose, Veronesi, Marina, Bertozzi, Sine, Summa, Maria, Girotto, Stefania, Bertorelli, Rosalia, Armirotti, Andrea, Ganesan, Anand, and De Vivo, Marco

Subjects

Animals, Antineoplastic Agents, Humans, Mice, cdc42 GTP-Binding Protein, Cell Line, Tumor, Drug Discovery, Structure-Activity Relationship, Xenograft Model Antitumor Assays, Pyrimidines, Female

Abstract

We previously reported trisubstituted pyrimidine lead compounds, namely, ARN22089 and ARN25062, which block the interaction between CDC42 with its specific downstream effector, a PAK protein. This interaction is crucial for the progression of multiple tumor types. Such inhibitors showed anticancer efficacy in vivo. Here, we describe a second class of CDC42 inhibitors with favorable drug-like properties. Out of the 25 compounds here reported, compound 15 (ARN25499) stands out as the best lead compound with an improved pharmacokinetic profile, increased bioavailability, and efficacy in an in vivo PDX tumor mouse model. Our results indicate that these CDC42 inhibitors represent a promising chemical class toward the discovery of anticancer drugs, with ARN25499 as an additional lead candidate for preclinical development.

Published

2024

11. Activation of the Mevalonate Pathway in Response to Anti-cancer Treatments Drives Glioblastoma Recurrences Through Activation of Rac-1

Author

He, Ling, Ioannidis, Angeliki, Hoffman, Carter J, Arambula, Evelyn, Joshi, Purva, Whitelegge, Julian, Liau, Linda M, Kornblum, Harley I, and Pajonk, Frank

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Rare Diseases, Stem Cell Research - Nonembryonic - Human, Stem Cell Research - Nonembryonic - Non-Human, Brain Disorders, Brain Cancer, Orphan Drug, Neurosciences, Cancer, Stem Cell Research, Glioblastoma, Mevalonic Acid, Humans, Animals, rac1 GTP-Binding Protein, Mice, Brain Neoplasms, Cell Line, Tumor, Temozolomide, Hydroxymethylglutaryl-CoA Reductase Inhibitors, Neoplasm Recurrence, Local, Xenograft Model Antitumor Assays, Neoplastic Stem Cells, Signal Transduction, Dopamine Antagonists

Abstract

Glioblastoma (GBM) is the deadliest adult brain cancer. Under the current standard of care, almost all patients succumb to the disease and novel treatments are urgently needed. Recognizing that GBMs are addicted to cholesterol, past clinical trials have repurposed statins against GBM but failed. The purpose of this study was to test whether treatments that upregulate the cholesterol biosynthesis pathway in GBM would generate a metabolic vulnerability that can be exploited using statins and to determine the underlying mechanisms.Effects of radiotherapy and temozolomide or dopamine receptor antagonists on the mevalonate pathway in GBM were assessed in vitro and in vivo. The impact of statins on self-renewal of glioma stem cells and median survival was studied. Branches of the mevalonate pathway were probed to identify relevant effector proteins.Cells surviving combination treatments that converge in activating the immediate early response, universally upregulated the mevalonate pathway and increased stemness of GBM cells through activation of the Rho-GTPase Rac-1. Activation of the mevalonate pathway and Rac-1 was inhibited by statins, which led to improved survival in mouse models of glioblastoma when combined with radiation and drugs that target the glioma stem cell pool and plasticity of glioma cells.We conclude that a combination of dopamine receptor antagonists and statins could potentially improve radiotherapy outcome and warrants further investigation.SignificanceCombination therapies that activate the mevalonate pathway in GBM cells after sublethal treatment enhance self-renewal and migratory capacity through Rac-1 activation, which creates a metabolic vulnerability that can be further potentially exploited using statins.

Published

2024

12. PLX038A, a long-acting SN-38, penetrates the blood-tumor-brain-barrier, accumulates and releases SN-38 in brain tumors to increase survival of tumor bearing mice.

Author

Jung, Jinkyu, Schneider, Eric, Zhang, Wei, Song, Hua, Zhang, Meili, Chou, William, Meher, Niranjan, VanBrocklin, Henry, Barcellos-Hoff, Mary Helen, Ozawa, Tomoko, Gilbert, Mark, and Santi, Daniel

Subjects

Animals, Brain Neoplasms, Irinotecan, Blood-Brain Barrier, Mice, Prodrugs, Humans, Cell Line, Tumor, Female, Xenograft Model Antitumor Assays, Glioblastoma, Camptothecin

Abstract

Central nervous system tumors have resisted effective chemotherapy because most therapeutics do not penetrate the blood-tumor-brain-barrier. Nanomedicines between  ~ 10 and 100 nm accumulate in many solid tumors by the enhanced permeability and retention effect, but it is controversial whether the effect can be exploited for treatment of brain tumors. PLX038A is a long-acting prodrug of the topoisomerase 1 inhibitor SN-38. It is composed of a 15 nm 4-arm 40 kDa PEG tethered to four SN-38 moieties by linkers that slowly cleave to release the SN-38. The prodrug was remarkably effective at suppressing growth of intracranial breast cancer and glioblastoma (GBM), significantly increasing the life span of mice harboring them. We addressed the important issue of whether the prodrug releases SN-38 systemically and then penetrates the brain to exert anti-tumor effects, or whether it directly penetrates the blood-tumor-brain-barrier and releases the SN-38 cargo within the tumor. We argue that the amount of SN-38 formed systemically is insufficient to inhibit the tumors, and show by PET imaging that a close surrogate of the 40 kDa PEG carrier in PLX038A accumulates and is retained in the GBM. We conclude that the prodrug penetrates the blood-tumor-brain-barrier, accumulates in the tumor microenvironment and releases its SN-38 cargo from within. Based on our results, we pose the provocative question as to whether the 40 kDa nanomolecule PEG carrier might serve as a Trojan horse to carry other drugs past the blood-tumor-brain-barrier and release them into brain tumors.

Published

2024

13. IRX4204 Induces Senescence and Cell Death in HER2-positive Breast Cancer and Synergizes with Anti-HER2 Therapy.

Author

Moyer, Cassandra, Lanier, Amanda, Qian, Jing, Coleman, Darian, Hill, Jamal, Vuligonda, Vidyasagar, Sanders, Martin, Mazumdar, Abhijit, and Brown, Powel

Subjects

Humans, Animals, Breast Neoplasms, Female, Receptor, ErbB-2, Mice, Cell Line, Tumor, Xenograft Model Antitumor Assays, Drug Synergism, Cellular Senescence, Cell Proliferation, Apoptosis, Trastuzumab, Drug Resistance, Neoplasm, Retinoids

Abstract

PURPOSE: Rexinoids, agonists of nuclear retinoid X receptor (RXR), have been used for the treatment of cancers and are well tolerated in both animals and humans. However, the usefulness of rexinoids in treatment of breast cancer remains unknown. This study examines the efficacy of IRX4204, a highly specific rexinoid, in breast cancer cell lines and preclinical models to identify a biomarker for response and potential mechanism of action. EXPERIMENTAL DESIGN: IRX4204 effects on breast cancer cell growth and viability were determined using cell lines, syngeneic mouse models, and primary patient-derived xenograft (PDX) tumors. In vitro assays of cell cycle, apoptosis, senescence, and lipid metabolism were used to uncover a potential mechanism of action. Standard anti-HER2 therapies were screened in combination with IRX4204 on a panel of breast cancer cell lines to determine drug synergy. RESULTS: IRX4204 significantly inhibits the growth of HER2-positive breast cancer cell lines, including trastuzumab and lapatinib-resistant JIMT-1 and HCC1954. Treatment with IRX4204 reduced tumor growth rate in the MMTV-ErbB2 mouse and HER2-positive PDX model by 49% and 44%, respectively. Mechanistic studies revealed IRX4204 modulates lipid metabolism and induces senescence of HER2-positive cells. In addition, IRX4204 demonstrates additivity and synergy with HER2-targeted mAbs, tyrosine kinase inhibitors, and antibody-drug conjugates. CONCLUSIONS: These findings identify HER2 as a biomarker for IRX4204 treatment response and demonstrate a novel use of RXR agonists to synergize with current anti-HER2 therapies. Furthermore, our results suggest that RXR agonists can be useful for the treatment of anti-HER2 resistant and metastatic HER2-positive breast cancer.

Published

2024

14. Mediator kinase inhibition reverses castration resistance of advanced prostate cancer

Author

Li, Jing, Hilimire, Thomas A, Yueying, Liu, Wang, Lili, Liang, Jiaxin, Győrffy, Balázs, Sikirzhytski, Vitali, Ji, Hao, Zhang, Li, Cheng, Chen, Ding, Xiaokai, Kerr, Kendall R, Dowling, Charles E, Chumanevich, Alexander A, Mack, Zachary T, Schools, Gary P, Lim, Chang-uk, Ellis, Leigh, Zi, Xiaolin, Porter, Donald C, Broude, Eugenia V, McInnes, Campbell, Wilding, George, Lilly, Michael B, Roninson, Igor B, and Chen, Mengqian

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Urologic Diseases, Genetics, Prostate Cancer, Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Male, Humans, Animals, Prostatic Neoplasms, Castration-Resistant, Mice, Cyclin-Dependent Kinases, Cyclin-Dependent Kinase 8, Cell Line, Tumor, Xenograft Model Antitumor Assays, Protein Kinase Inhibitors, Gene Expression Regulation, Neoplastic, Tumor Microenvironment, Oncology, Therapeutics, Transcription, Medical and Health Sciences, Immunology, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

Mediator kinases CDK19 and CDK8, pleiotropic regulators of transcriptional reprogramming, are differentially regulated by androgen signaling, but both kinases are upregulated in castration-resistant prostate cancer (CRPC). Genetic or pharmacological inhibition of CDK8 and CDK19 reverses the castration-resistant phenotype and restores the sensitivity of CRPC xenografts to androgen deprivation in vivo. Prolonged CDK8/19 inhibitor treatment combined with castration not only suppressed the growth of CRPC xenografts but also induced tumor regression and cures. Transcriptomic analysis revealed that Mediator kinase inhibition amplified and modulated the effects of castration on gene expression, disrupting CRPC adaptation to androgen deprivation. Mediator kinase inactivation in tumor cells also affected stromal gene expression, indicating that Mediator kinase activity in CRPC molded the tumor microenvironment. The combination of castration and Mediator kinase inhibition downregulated the MYC pathway, and Mediator kinase inhibition suppressed a MYC-driven CRPC tumor model even without castration. CDK8/19 inhibitors showed efficacy in patient-derived xenograft models of CRPC, and a gene signature of Mediator kinase activity correlated with tumor progression and overall survival in clinical samples of metastatic CRPC. These results indicate that Mediator kinases mediated androgen-independent in vivo growth of CRPC, supporting the development of CDK8/19 inhibitors for the treatment of this presently incurable disease.

Published

2024

15. Repurposing mebendazole against triple-negative breast cancer CNS metastasis

Author

Rodrigues, Adrian J, Chernikova, Sophia B, Wang, Yuelong, Trinh, Thy TH, Solow-Cordero, David E, Alexandrova, Ludmila, Casey, Kerriann M, Alli, Elizabeth, Aggarwal, Abhishek, Quill, Tyler, Koegel, Ashley K, Feldman, Brian J, Ford, James M, and Hayden-Gephart, Melanie

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Breast Cancer, Neurosciences, Cancer, Women's Health, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Triple Negative Breast Neoplasms, Animals, Humans, Drug Repositioning, Female, Mebendazole, Mice, Mice, Nude, Mice, Inbred BALB C, Cell Movement, Xenograft Model Antitumor Assays, Cell Line, Tumor, Central Nervous System Neoplasms, Cell Proliferation, Breast cancer, Leptomeningeal disease, Drug repurposing, Oncology & Carcinogenesis, Oncology and carcinogenesis

Abstract

PurposeTriple-negative breast cancer (TNBC) often metastasizes to the central nervous system (CNS) and has the highest propensity among breast cancer subtypes to develop leptomeningeal disease (LMD). LMD is a spread of cancer into leptomeningeal space that speeds up the disease progression and severely aggravates the prognosis. LMD has limited treatment options. We sought to test whether the common anti-helminthic drug mebendazole (MBZ) may be effective against murine TNBC LMD.MethodsA small-molecule screen involving TNBC cell lines identified benzimidazoles as potential therapeutic agents for further study. In vitro migration assays were used to evaluate cell migration capacity and the effect of MBZ. For in vivo testing, CNS metastasis was introduced into BALB/c athymic nude mice through internal carotid artery injections of brain-tropic MDA-MB-231-BR or MCF7-BR cells. Tumor growth and spread was monitored by bioluminescence imaging and immunohistochemistry. MBZ was given orally at 50 and 100 mg/kg doses. MBZ bioavailability was assayed by mass spectrometry.ResultsBioinformatic analysis and migration assays revealed higher migratory capacity of TNBC compared to other breast cancer subtypes. MBZ effectively slowed down migration of TNBC cell line MDA-MB-231 and its brain tropic derivative MDA-MB-231-BR. In animal studies, MBZ reduced leptomeningeal spread, and extended survival in brain metastasis model produced by MDA-MB-231-BR cells. MBZ did not have an effect in the non-migratory MCF7-BR model.ConclusionsWe demonstrated that MBZ is a safe and effective oral agent in an animal model of TNBC CNS metastasis. Our findings are concordant with previous efforts involving MBZ and CNS pathology and support the drug's potential utility to slow down leptomeningeal spread.

Published

2024

16. Enhancing CAR-T cell metabolism to overcome hypoxic conditions in the brain tumor microenvironment

Author

Hatae, Ryusuke, Kyewalabye, Keith, Yamamichi, Akane, Chen, Tiffany, Phyu, Su, Chuntova, Pavlina, Nejo, Takahide, Levine, Lauren S, Spitzer, Matthew H, and Okada, Hideho

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Brain Cancer, Rare Diseases, Brain Disorders, Neurosciences, Mice, Humans, Animals, Tumor Microenvironment, AMP-Activated Protein Kinases, Xenograft Model Antitumor Assays, Cell Line, Tumor, Brain, Glioma, T-Lymphocytes, TOR Serine-Threonine Kinases, Brain cancer, Cancer immunotherapy, Hypoxia, Otology, Biomedical and clinical sciences, Health sciences

Abstract

The efficacy of chimeric antigen receptor T cell (CAR-T) therapy has been limited against brain tumors to date. CAR-T cells infiltrating syngeneic intracerebral SB28 EGFRvIII gliomas revealed impaired mitochondrial ATP production and a markedly hypoxic status compared with ones migrating to subcutaneous tumors. Drug screenings to improve metabolic states of T cells under hypoxic conditions led us to evaluate the combination of the AMPK activator metformin and the mTOR inhibitor rapamycin (Met+Rap). Met+Rap-pretreated mouse CAR-T cells showed activated PPAR-γ coactivator 1α (PGC-1α) through mTOR inhibition and AMPK activation, and a higher level of mitochondrial spare respiratory capacity than those pretreated with individual drugs or without pretreatment. Moreover, Met+Rap-pretreated CAR-T cells demonstrated persistent and effective antiglioma cytotoxic activities in the hypoxic condition. Furthermore, a single intravenous infusion of Met+Rap-pretreated CAR-T cells significantly extended the survival of mice bearing intracerebral SB28 EGFRvIII gliomas. Mass cytometric analyses highlighted increased glioma-infiltrating CAR-T cells in the Met+Rap group, with fewer Ly6c+CD11b+ monocytic myeloid-derived suppressor cells in the tumors. Finally, human CAR-T cells pretreated with Met+Rap recapitulated the observations with murine CAR-T cells, demonstrating improved functions under in vitro hypoxic conditions. These findings advocate for translational and clinical exploration of Met+Rap-pretreated CAR-T cells in human trials.

Published

2024

17. Osteosarcoma PDX-Derived Cell Line Models for Preclinical Drug Evaluation Demonstrate Metastasis Inhibition by Dinaciclib through a Genome-Targeted Approach

Author

Schott, Courtney R, Koehne, Amanda L, Sayles, Leanne C, Young, Elizabeth P, Luck, Cuyler, Yu, Katherine, Lee, Alex G, Breese, Marcus R, Leung, Stanley G, Xu, Hang, Shah, Avanthi Tayi, Liu, Heng-Yi, Spillinger, Aviv, Behroozfard, Inge H, Marini, Kieren D, Dinh, Phuong T, Ventura, María V Pons, Vanderboon, Emma N, Hazard, Florette K, Cho, Soo-Jin, Avedian, Raffi S, Mohler, David G, Zimel, Melissa, Wustrack, Rosanna, Curtis, Christina, Sirota, Marina, and Sweet-Cordero, E Alejandro

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Pediatric, Biotechnology, Genetics, Rare Diseases, Pediatric Cancer, Cancer, Cancer Genomics, Human Genome, Orphan Drug, Good Health and Well Being, Humans, Animals, Mice, Disease Models, Animal, Drug Evaluation, Preclinical, Xenograft Model Antitumor Assays, Osteosarcoma, Cell Line, Tumor, Bone Neoplasms, Cyclic N-Oxides, Indolizines, Pyridinium Compounds, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

PurposeModels to study metastatic disease in rare cancers are needed to advance preclinical therapeutics and to gain insight into disease biology. Osteosarcoma is a rare cancer with a complex genomic landscape in which outcomes for patients with metastatic disease are poor. As osteosarcoma genomes are highly heterogeneous, multiple models are needed to fully elucidate key aspects of disease biology and to recapitulate clinically relevant phenotypes.Experimental designMatched patient samples, patient-derived xenografts (PDX), and PDX-derived cell lines were comprehensively evaluated using whole-genome sequencing and RNA sequencing. The in vivo metastatic phenotype of the PDX-derived cell lines was characterized in both an intravenous and an orthotopic murine model. As a proof-of-concept study, we tested the preclinical effectiveness of a cyclin-dependent kinase inhibitor on the growth of metastatic tumors in an orthotopic amputation model.ResultsPDXs and PDX-derived cell lines largely maintained the expression profiles of the patient from which they were derived despite the emergence of whole-genome duplication in a subset of cell lines. The cell lines were heterogeneous in their metastatic capacity, and heterogeneous tissue tropism was observed in both intravenous and orthotopic models. Single-agent dinaciclib was effective at dramatically reducing the metastatic burden.ConclusionsThe variation in metastasis predilection sites between osteosarcoma PDX-derived cell lines demonstrates their ability to recapitulate the spectrum of the disease observed in patients. We describe here a panel of new osteosarcoma PDX-derived cell lines that we believe will be of wide use to the osteosarcoma research community.

Published

2024

18. Manuka Honey Inhibits Human Breast Cancer Progression in Preclinical Models

Author

Márquez-Garbán, Diana C, Yanes, Cristian D, Llarena, Gabriela, Elashoff, David, Hamilton, Nalo, Hardy, Mary, Wadehra, Madhuri, McCloskey, Susan A, and Pietras, Richard J

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Women's Health, Breast Cancer, Cancer, 5.1 Pharmaceuticals, Humans, Honey, Breast Neoplasms, Female, Animals, Apoptosis, MCF-7 Cells, Cell Proliferation, Signal Transduction, Mice, Xenograft Model Antitumor Assays, Mice, Nude, Leptospermum, TOR Serine-Threonine Kinases, Proto-Oncogene Proteins c-akt, Antineoplastic Agents, STAT3 Transcription Factor, Disease Progression, AMP-Activated Protein Kinases, Cell Line, Tumor, Phosphorylation, Manuka honey, breast cancer, estrogen receptor-positive breast cancer, triple-negative breast cancer, in vivo xenografts, AMP kinase signaling, mTOR, STAT3, Food Sciences, Nutrition and Dietetics, Clinical sciences, Nutrition and dietetics, Public health

Abstract

Manuka honey (MH) exhibits potential antitumor activity in preclinical models of a number of human cancers. Treatment in vitro with MH at concentrations ranging from 0.3 to 5.0% (w/v) led to significant dose-dependent inhibition of proliferation of human breast cancer MCF-7 cells, but anti-proliferative effects of MH were less pronounced in MDA-MB-231 breast cancer cells. Effects of MH were also tested on non-malignant human mammary epithelial cells (HMECs) at 2.5% w/v, and it was found that MH reduced the proliferation of MCF-7 cells but not that of HMECs. Notably, the antitumor activity of MH was in the range of that exerted by treatment of MCF-7 cells with the antiestrogen tamoxifen. Further, MH treatment stimulated apoptosis of MCF-7 cells in vitro, with most cells exhibiting acute and significant levels of apoptosis that correlated with PARP activation. Additionally, the effects of MH induced the activation of AMPK and inhibition of AKT/mTOR downstream signaling. Treatment of MCF7 cells with increased concentrations of MH induced AMPK phosphorylation in a dose-dependent manner that was accompanied by inhibition of phosphorylation of AKT and mTOR downstream effector protein S6. In addition, MH reduced phosphorylated STAT3 levels in vitro, which may correlate with MH and AMPK-mediated anti-inflammatory properties. Further, in vivo, MH administered alone significantly inhibited the growth of established MCF-7 tumors in nude mice by 84%, resulting in an observable reduction in tumor volume. Our findings highlight the need for further research into the use of natural compounds, such as MH, for antitumor efficacy and potential chemoprevention and investigation of molecular pathways underlying these actions.

Published

2024

19. Development of a Simple and Reproducible Cell-derived Orthotopic Xenograft Murine Model for Neuroblastoma

Author

Doyle, Kathleen, Hassan, Abd-Elrahman, Sutter, Maria, Rodriguez, Monica, Kumar, Priyadarsini, and Brown, Erin

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Neuroblastoma, Pediatric Cancer, Pediatric, Neurosciences, Cancer, Biotechnology, Bioengineering, Orphan Drug, Rare Diseases, Child, Humans, Animals, Mice, Disease Models, Animal, Heterografts, Mice, SCID, Adrenal Gland Neoplasms, Xenograft Model Antitumor Assays, Cell Line, Tumor, orthotopic murine model, PDOX, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Dentistry, Oncology and carcinogenesis

Abstract

Background/aimNeuroblastoma is a common childhood cancer with poor survival for children with high-risk disease, and ongoing research to improve outcomes is needed. Patient-derived xenografts (PDX) and genetically engineered mouse models (GEMM) are reliable models for oncologic research; however, they are resource-intensive, expensive, and require significant expertise to develop and maintain. We developed an orthotopic xenograft murine model of neuroblastoma that utilizes cryopreserved banks of human neuroblastoma cell lines, requires minimal equipment, and is easily reproducible.Materials and methodsThe neuroblastoma cell line NB1643 was obtained from the Children's Oncology Group (COG) Childhood Cancer Repository. Nod-SCID-gamma (NSG) mice underwent orthotopic injection of 2x106 NB1643 cells suspended in 10 μl of collagen hydrogel directly into the adrenal gland via an open retroperitoneal surgical approach. Mice were monitored by ultrasound and in vivo imaging system (IVIS) until the tumor reached the volume of the ipsilateral kidney. Tumor identity was confirmed by necropsy and histologic analysis.ResultsA total of 55 mice underwent surgery. Eight died due to anesthetic or surgical complications. 39/47 (78%) survivors grew primary adrenal tumors. Average anesthesia time was 30 min. Ultrasound and IVIS successfully characterized tumor growth in all mice. Average time to target tumor size was 5 weeks (range=3-9). Gross pathologic and histologic analysis confirmed adrenal tumors consistent with neuroblastoma in all mice with adrenal masses.ConclusionA cell-derived orthotopic xenograft murine model can be successfully used to create an in vivo model of neuroblastoma. This model can be utilized in environments where PDX or GEMM models are not feasible.

Published

2024

20. Single protein encapsulated SN38 for tumor-targeting treatment.

Author

Yu, Changjun, Huang, Faqing, Wang, Kinsley, Liu, Mengmeng, Chow, Warren, Ling, Xiang, Li, Fengzhi, Causey, Jason, Huang, Xiuzhen, Cook-Wiens, Galen, and Cui, Xiaojiang

Subjects

Colorectal cancer, FcRn, SN38, SPESN38-5, SPESN38-8, Single protein encapsulation, Soft tissue sarcoma, Topoisomerase I inhibitor, Humans, Mice, Animals, Irinotecan, Xenograft Model Antitumor Assays, Camptothecin, Antineoplastic Agents, Colorectal Neoplasms, Disease Models, Animal, Water, Cell Line, Tumor, Antineoplastic Agents, Phytogenic

Abstract

BACKGROUND: The alkaloid camptothecin analog SN38 is a potent antineoplastic agent, but cannot be used directly for clinical application due to its poor water solubility. Currently, the prodrug approach on SN38 has resulted in 3 FDA-approved cancer therapeutics, irinotecan, ONIVYDE, and Trodelvy. However, only 2-8% of irinotecan can be transformed enzymatically in vivo into the active metabolite SN38, which severely limits the drugs efficacy. While numerous drug delivery systems have been attempted to achieve effective SN38 delivery, none have produced drug products with antitumor efficacy better than irinotecan in clinical trials. Therefore, novel approaches are urgently needed for effectively delivering SN38 to cancer cells with better efficacy and lower toxicity. METHODS: Based on the unique properties of human serum albumin (HSA), we have developed a novel single protein encapsulation (SPE) technology to formulate cancer therapeutics for improving their pharmacokinetics (PK) and antitumor efficacy and reducing their side effects. Previous application of SPE technology to doxorubicin (DOX) formulation has led to a promising drug candidate SPEDOX-6 (FDA IND #, 152154), which will undergo a human phase I clinical trial. Using the same SPE platform on SN38, we have now produced two SPESN38 complexes, SPESN38-5 and SPESN38-8. We conducted their pharmacological evaluations with respect to maximum tolerated dose, PK, and in vivo efficacy against colorectal cancer (CRC) and soft tissue sarcoma (STS) in mouse models. RESULTS: The lyophilized SPESN38 complexes can dissolve in aqueous media to form clear and stable solutions. Maximum tolerated dose (MTD) of SPESN38-5 is 250 mg/kg by oral route (PO) and 55 mg/kg by intravenous route (IV) in CD-1 mice. SPESN38-8 has the MTD of 45 mg/kg by IV in the same mouse model. PK of SPESN38-5 by PO at 250 mg/kg gave mouse plasma AUC0-∞ of 0.05 and 4.5 nmol × h/mL for SN38 and SN38 glucuronidate (SN38G), respectively, with a surprisingly high molar ratio of SN38G:SN38 = 90:1. However, PK of SPESN38-5 by IV at 55 mg/kg yielded much higher mouse plasma AUC0-∞ of 19 and 28 nmol × h/mL for SN38 and SN38G, producing a much lower molar ratio of SN38G:SN38 = 1.5:1. Antitumor efficacy of SPESN38-5 and irinotecan (control) was evaluated against HCT-116 CRC xenograft tumors. The data indicates that SPESN38-5 by IV at 55 mg/kg is more effective in suppressing HCT-116 tumor growth with lower systemic toxicity compared to irinotecan at 50 mg/kg. Additionally, SPESN38-8 and DOX (control) by IV were evaluated in the SK-LMS-1 STS mouse model. The results show that SPESN38-8 at 33 mg/kg is highly effective for inhibiting SK-LMS-1 tumor growth with low toxicity, in contrast to DOXs insensitivity to SK-LMS-1 with high toxicity. CONCLUSION: SPESN38 complexes provide a water soluble SN38 formulation. SPESN38-5 and SPESN38-8 demonstrate better PK values, lower toxicity, and superior antitumor efficacy in mouse models, compared with irinotecan and DOX.

Published

2023

21. Targeting de novo lipid synthesis induces lipotoxicity and impairs DNA damage repair in glioblastoma mouse models.

Author

Jha, Roshani, Mnatsakanyan, Hayk, Pechdimaljian, Caline, Carvalho, Litia, Neustadt, Rudolph, Moses, Charlotte, Alnasser, Ahmad, Tardiff, Daniel, Su, Baolong, Williams, Kevin, Chung, Chee, Badr, Christian, Eyme, Katharina, Bensinger, Steven, and Sammarco, Alessandro

Subjects

Animals, Mice, Glioblastoma, AMP-Activated Protein Kinases, Cell Line, Tumor, Brain Neoplasms, Xenograft Model Antitumor Assays, DNA Damage, Lipids, Neoplastic Stem Cells

Abstract

Deregulated de novo lipid synthesis (DNLS) is a potential druggable vulnerability in glioblastoma (GBM), a highly lethal and incurable cancer. Yet the molecular mechanisms that determine susceptibility to DNLS-targeted therapies remain unknown, and the lack of brain-penetrant inhibitors of DNLS has prevented their clinical evaluation as GBM therapeutics. Here, we report that YTX-7739, a clinical-stage inhibitor of stearoyl CoA desaturase (SCD), triggers lipotoxicity in patient-derived GBM stem-like cells (GSCs) and inhibits fatty acid desaturation in GSCs orthotopically implanted in mice. When administered as a single agent, or in combination with temozolomide (TMZ), YTX-7739 showed therapeutic efficacy in orthotopic GSC mouse models owing to its lipotoxicity and ability to impair DNA damage repair. Leveraging genetic, pharmacological, and physiological manipulation of key signaling nodes in gliomagenesis complemented with shotgun lipidomics, we show that aberrant MEK/ERK signaling and its repression of the energy sensor AMP-activated protein kinase (AMPK) primarily drive therapeutic vulnerability to SCD and other DNLS inhibitors. Conversely, AMPK activation mitigates lipotoxicity and renders GSCs resistant to the loss of DNLS, both in culture and in vivo, by decreasing the saturation state of phospholipids and diverting toxic lipids into lipid droplets. Together, our findings reveal mechanisms of metabolic plasticity in GSCs and provide a framework for the rational integration of DNLS-targeted GBM therapies.

Published

2023

22. A dendritic/tumor fusion cell vaccine enhances efficacy of nanobody-based CAR-T cells against solid tumor

Author

Sun, Shuyang, Ding, Ziqiang, Gao, Li, Hammock, Bruce D, Huang, Xianing, Xu, Zhi Ping, Wang, Xuan, Cheng, Qihong, Mo, Fengzhen, Shi, Wei, Xie, Shenxia, Liu, Aiqun, Li, Haixia, Yang, Xiaomei, and Lu, Xiaoling

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Orphan Drug, Immunization, Vaccine Related, Immunotherapy, Rare Diseases, Gene Therapy, Genetics, Biotechnology, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Humans, Animals, Mice, Receptors, Chimeric Antigen, Cell Line, Tumor, T-Lymphocytes, Immunotherapy, Adoptive, Cell Proliferation, Xenograft Model Antitumor Assays, nanobody, CAR-T cells, DC/tumor fusion vaccines, EGFRvIII, solid tumor, Oncology and carcinogenesis

Abstract

Background: Chimeric antigen receptor (CAR) T-cell therapy is practical in treating cancers of hematopoietic origin, but of that in solid tumors compromises efficacy for the loss of the antigen recognized by the CAR. However, dendritic cell (DC)/tumor fusion vaccines present a spectrum of known or unknown tumor antigens to stimulate T cell expansion and enhanced T cell response. Developing a new strategy of enhanced nanobody-based CAR-T (Nb-CAR-T) cells antitumor activity by DC/tumor fusion vaccines stimulation would provide guidance for more effective CAR-T cell therapies. Methods: Considering the therapeutic potential of nanobody (Nb), we first screened EGFRvIII Nb, then constructed and verified the function of EGFRvIII Nb-CAR-T cells in vitro and in vivo. We further combined DC/tumor fusion vaccines to boost EGFRvIII Nb-CAR-T cells antitumor effect, which was evaluated in vitro Nb-CAR-T cell function and in the tumor-bearing xenograft mouse models. Results: We had for the first time successfully selected EGFRvIII Nb for the generation of the novel EGFRvIII Nb-CAR-T cells. Importantly, our results suggested that DC/tumor fusion vaccines stimulate Nb-CAR-T cells response not only in improving T cell proliferation, T cell activation, cytokine secretion and tumor-specific cytotoxicity in vitro, but also significantly reducing tumor burden, prolonging survival and improving Nb-CAR-T cells infiltration. Conclusions: We have innovatively shown that DC/tumor fusion vaccines significantly enhance the efficacy of Nb-CAR-T cells against solid tumors. This new strategy has provided a promising therapeutic platform for promoting the clinical treatment of CAR-T cells therapy.

Published

2023

23. SF3B1 inhibition disrupts malignancy and prolongs survival in glioblastoma patients through BCL2L1 splicing and mTOR/ß-catenin pathways imbalances

Author

Fuentes-Fayos, Antonio C, Pérez-Gómez, Jesús M, G-García, Miguel E, Jiménez-Vacas, Juan M, Blanco-Acevedo, Cristóbal, Sánchez-Sánchez, Rafael, Solivera, Juan, Breunig, Joshua J, Gahete, Manuel D, Castaño, Justo P, and Luque, Raúl M

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Genetics, Rare Diseases, Brain Disorders, Neurosciences, Brain Cancer, Clinical Research, Cancer, 2.1 Biological and endogenous factors, Aetiology, Animals, Apoptosis, Cell Line, Tumor, Cell Proliferation, Disease Models, Animal, Glioblastoma, Humans, Mice, Phosphoproteins, RNA Splicing Factors, Survival Analysis, TOR Serine-Threonine Kinases, Transfection, Xenograft Model Antitumor Assays, bcl-X Protein, beta Catenin, Splicing factor SF3B1, Glioma mouse models, Antitumor therapy, BCL2L1 splicing variants, Oncology and carcinogenesis

Abstract

BackgroundGlioblastoma is one of the most devastating cancer worldwide based on its locally aggressive behavior and because it cannot be cured by current therapies. Defects in alternative splicing process are frequent in cancer. Recently, we demonstrated that dysregulation of the spliceosome is directly associated with glioma development, progression, and aggressiveness.MethodsDifferent human cohorts and a dataset from different glioma mouse models were analyzed to determine the mutation frequency as well as the gene and protein expression levels between tumor and control samples of the splicing-factor-3B-subunit-1 (SF3B1), an essential and druggable spliceosome component. SF3B1 expression was also explored at the single-cell level across all cell subpopulations and transcriptomic programs. The association of SF3B1 expression with relevant clinical data (e.g., overall survival) in different human cohorts was also analyzed. Different functional (proliferation/migration/tumorspheres and colonies formation/VEGF secretion/apoptosis) and mechanistic (gene expression/signaling pathways) assays were performed in three different glioblastomas cell models (human primary cultures and cell lines) in response to SF3B1 blockade (using pladienolide B treatment). Moreover, tumor progression and formation were monitored in response to SF3B1 blockade in two preclinical xenograft glioblastoma mouse models.ResultsOur data provide novel evidence demonstrating that the splicing-factor-3B-subunit-1 (SF3B1, an essential and druggable spliceosome component) is low-frequency mutated in human gliomas (~ 1 %) but widely overexpressed in glioblastoma compared with control samples from the different human cohorts and mouse models included in the present study, wherein SF3B1 levels are associated with key molecular and clinical features (e.g., overall survival, poor prognosis and/or drug resistance). Remarkably, in vitro and in vivo blockade of SF3B1 activity with pladienolide B drastically altered multiple glioblastoma pathophysiological processes (i.e., reduction in proliferation, migration, tumorspheres formation, VEGF secretion, tumor initiation and increased apoptosis) likely by suppressing AKT/mTOR/ß-catenin pathways, and an imbalance of BCL2L1 splicing.ConclusionsTogether, we highlight SF3B1 as a potential diagnostic and prognostic biomarker and an efficient pharmacological target in glioblastoma, offering a clinically relevant opportunity worth to be explored in humans.

Published

2022

24. CBFA2T3-GLIS2 model of pediatric acute megakaryoblastic leukemia identifies FOLR1 as a CAR T cell target

Author

Le, Quy, Hadland, Brandon, Smith, Jenny L, Leonti, Amanda, Huang, Benjamin J, Ries, Rhonda, Hylkema, Tiffany A, Castro, Sommer, Tang, Thao T, McKay, Cyd N, Perkins, LaKeisha, Pardo, Laura, Sarthy, Jay, Beckman, Amy K, Williams, Robin, Idemmili, Rhonda, Furlan, Scott, Ishida, Takashi, Call, Lindsey, Srivastava, Shivani, Loeb, Anisha M, Milano, Filippo, Imren, Suzan, Morris, Shelli M, Pakiam, Fiona, Olson, James M, Loken, Michael R, Brodersen, Lisa Eidenschink, Riddell, Stanley R, Tarlock, Katherine, Bernstein, Irwin D, Loeb, Keith R, and Meshinchi, Soheil

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Pediatric Research Initiative, Pediatric, Cancer, Genetics, Pediatric Cancer, Stem Cell Research, Stem Cell Research - Nonembryonic - Human, Stem Cell Research - Nonembryonic - Non-Human, Biotechnology, Hematology, Rare Diseases, Childhood Leukemia, Orphan Drug, 2.1 Biological and endogenous factors, Aetiology, Animals, Child, Child, Preschool, Humans, Infant, Disease Models, Animal, Folate Receptor 1, Immunotherapy, Adoptive, Leukemia, Megakaryoblastic, Acute, Oncogene Proteins, Fusion, T-Lymphocytes, Transcriptome, Xenograft Model Antitumor Assays, Cancer immunotherapy, Leukemias, Oncogenes, Oncology, Therapeutics, Medical and Health Sciences, Biological sciences, Biomedical and clinical sciences, Health sciences

Abstract

The CBFA2T3-GLIS2 (C/G) fusion is a product of a cryptic translocation primarily seen in infants and early childhood and is associated with dismal outcome. Here, we demonstrate that the expression of the C/G oncogenic fusion protein promotes the transformation of human cord blood hematopoietic stem and progenitor cells (CB HSPCs) in an endothelial cell coculture system that recapitulates the transcriptome, morphology, and immunophenotype of C/G acute myeloid leukemia (AML) and induces highly aggressive leukemia in xenograft models. Interrogating the transcriptome of C/G-CB cells and primary C/G AML identified a library of C/G-fusion-specific genes that are potential targets for therapy. We developed chimeric antigen receptor (CAR) T cells directed against one of the targets, folate receptor α (FOLR1), and demonstrated their preclinical efficacy against C/G AML using in vitro and xenograft models. FOLR1 is also expressed in renal and pulmonary epithelium, raising concerns for toxicity that must be addressed for the clinical application of this therapy. Our findings underscore the role of the endothelial niche in promoting leukemic transformation of C/G-transduced CB HSPCs. Furthermore, this work has broad implications for studies of leukemogenesis applicable to a variety of oncogenic fusion-driven pediatric leukemias, providing a robust and tractable model system to characterize the molecular mechanisms of leukemogenesis and identify biomarkers for disease diagnosis and targets for therapy.

Published

2022

25. A Genomically and Clinically Annotated Patient-Derived Xenograft (PDX) Resource for Preclinical Research in Non-Small Cell Lung Cancer

Author

Woo, Xing Yi, Srivastava, Anuj, Mack, Philip C, Graber, Joel H, Sanderson, Brian J, Lloyd, Michael W, Chen, Mandy, Domanskyi, Sergii, Gandour-Edwards, Regina, Tsai, Rebekah A, Keck, James, Cheng, Mingshan, Bundy, Margaret, Jocoy, Emily L, Riess, Jonathan W, Holland, William, Grubb, Stephen C, Peterson, James G, Stafford, Grace A, Paisie, Carolyn, Neuhauser, Steven B, Karuturi, R Krishna Murthy, George, Joshy, Simons, Allen K, Chavaree, Margaret, Tepper, Clifford G, Goodwin, Neal, Airhart, Susan D, Lara, Primo N, Openshaw, Thomas H, Liu, Edison T, Gandara, David R, and Bult, Carol J

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Orphan Drug, Lung Cancer, Biotechnology, Genetics, Human Genome, Rare Diseases, Cancer, Lung, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Good Health and Well Being, Humans, Animals, Carcinoma, Non-Small-Cell Lung, Lung Neoplasms, Heterografts, Xenograft Model Antitumor Assays, Adenocarcinoma of Lung, Disease Models, Animal, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

Patient-derived xenograft (PDX) models are an effective preclinical in vivo platform for testing the efficacy of novel drugs and drug combinations for cancer therapeutics. Here we describe a repository of 79 genomically and clinically annotated lung cancer PDXs available from The Jackson Laboratory that have been extensively characterized for histopathologic features, mutational profiles, gene expression, and copy-number aberrations. Most of the PDXs are models of non-small cell lung cancer (NSCLC), including 37 lung adenocarcinoma (LUAD) and 33 lung squamous cell carcinoma (LUSC) models. Other lung cancer models in the repository include four small cell carcinomas, two large cell neuroendocrine carcinomas, two adenosquamous carcinomas, and one pleomorphic carcinoma. Models with both de novo and acquired resistance to targeted therapies with tyrosine kinase inhibitors are available in the collection. The genomic profiles of the LUAD and LUSC PDX models are consistent with those observed in patient tumors from The Cancer Genome Atlas and previously characterized gene expression-based molecular subtypes. Clinically relevant mutations identified in the original patient tumors were confirmed in engrafted PDX tumors. Treatment studies performed in a subset of the models recapitulated the responses expected on the basis of the observed genomic profiles. These models therefore serve as a valuable preclinical platform for translational cancer research.SignificancePatient-derived xenografts of lung cancer retain key features observed in the originating patient tumors and show expected responses to treatment with standard-of-care agents, providing experimentally tractable and reproducible models for preclinical investigations.

Published

2022

26. STAT3 Activation as a Predictive Biomarker for Ruxolitinib Response in Head and Neck Cancer.

Author

Qureshy, Zoya, Li, Hua, Zeng, Yan, Rivera, Jose, Cheng, Ning, Peterson, Christopher N, Kim, Mi-Ok, Ryan, William R, Ha, Patrick K, Bauman, Julie E, Wang, Steven J, Long, Steven R, Johnson, Daniel E, and Grandis, Jennifer R

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Cancer, Dental/Oral and Craniofacial Disease, Rare Diseases, Orphan Drug, Clinical Research, Good Health and Well Being, Humans, Mice, Animals, Squamous Cell Carcinoma of Head and Neck, Carcinoma, Squamous Cell, Xenograft Model Antitumor Assays, Head and Neck Neoplasms, STAT3 Transcription Factor, Biomarkers, Cell Line, Tumor, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

PurposeIncreased activity of STAT3 is associated with progression of head and neck squamous cell carcinoma (HNSCC). Upstream activators of STAT3, such as JAKs, represent potential targets for therapy of solid tumors, including HNSCC. In this study, we investigated the anticancer effects of ruxolitinib, a clinical JAK1/2 inhibitor, in HNSCC preclinical models, including patient-derived xenografts (PDX) from patients treated on a window-of-opportunity trial.Experimental designHNSCC cell lines were treated with ruxolitinib, and the impact on activated STAT3 levels, cell growth, and colony formation was assessed. PDXs were generated from patients with HNSCC who received a brief course of neoadjuvant ruxolitinib on a clinical trial. The impact of ruxolitinib on tumor growth and STAT3 activation was assessed.ResultsRuxolitinib inhibited STAT3 activation, cellular growth, and colony formation of HNSCC cell lines. Ruxolitinib treatment of mice bearing an HNSCC cell line-derived xenograft significantly inhibited tumor growth compared with vehicle-treated controls. The response of HNSCC PDXs derived from patients on the clinical trial mirrored the responses seen in the neoadjuvant setting. Baseline active STAT3 (pSTAT3) and total STAT3 levels were lower, and ruxolitinib inhibited STAT3 activation in a PDX from a patient whose disease was stable on ruxolitinib, compared with a PDX from a patient whose disease progressed on ruxolitinib and where ruxolitinib treatment had minimal impact on STAT3 activation.ConclusionsRuxolitinib exhibits antitumor effects in HNSCC preclinical models. Baseline pSTAT3 or total STAT3 levels in the tumor may serve as predictive biomarkers to identify patients most likely to respond to ruxolitinib.

Published

2022

27. Brain-restricted mTOR inhibition with binary pharmacology

Author

Zhang, Ziyang, Fan, Qiwen, Luo, Xujun, Lou, Kevin, Weiss, William A, and Shokat, Kevan M

Subjects

Biomedical and Clinical Sciences, Medicinal and Biomolecular Chemistry, Chemical Sciences, Biological Psychology, Psychology, Pharmacology and Pharmaceutical Sciences, Neurosciences, Orphan Drug, Cancer, Rare Diseases, Brain Disorders, Brain Cancer, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Neurological, Humans, Brain, Drug Therapy, Combination, Glioblastoma, Ligands, MTOR Inhibitors, Sirolimus, Tacrolimus Binding Protein 1A, TOR Serine-Threonine Kinases, Xenograft Model Antitumor Assays, General Science & Technology

Abstract

On-target-off-tissue drug engagement is an important source of adverse effects that constrains the therapeutic window of drug candidates1,2. In diseases of the central nervous system, drugs with brain-restricted pharmacology are highly desirable. Here we report a strategy to achieve inhibition of mammalian target of rapamycin (mTOR) while sparing mTOR activity elsewhere through the use of the brain-permeable mTOR inhibitor RapaLink-1 and the brain-impermeable FKBP12 ligand RapaBlock. We show that this drug combination mitigates the systemic effects of mTOR inhibitors but retains the efficacy of RapaLink-1 in glioblastoma xenografts. We further present a general method to design cell-permeable, FKBP12-dependent kinase inhibitors from known drug scaffolds. These inhibitors are sensitive to deactivation by RapaBlock, enabling the brain-restricted inhibition of their respective kinase targets.

Published

2022

28. RASA2 ablation in T cells boosts antigen sensitivity and long-term function

Author

Carnevale, Julia, Shifrut, Eric, Kale, Nupura, Nyberg, William A, Blaeschke, Franziska, Chen, Yan Yi, Li, Zhongmei, Bapat, Sagar P, Diolaiti, Morgan E, O’Leary, Patrick, Vedova, Shane, Belk, Julia, Daniel, Bence, Roth, Theodore L, Bachl, Stefanie, Anido, Alejandro Allo, Prinzing, Brooke, Ibañez-Vega, Jorge, Lange, Shannon, Haydar, Dalia, Luetke-Eversloh, Marie, Born-Bony, Maelys, Hegde, Bindu, Kogan, Scott, Feuchtinger, Tobias, Okada, Hideho, Satpathy, Ansuman T, Shannon, Kevin, Gottschalk, Stephen, Eyquem, Justin, Krenciute, Giedre, Ashworth, Alan, and Marson, Alexander

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Biotechnology, Immunotherapy, Gene Therapy, Genetics, Cancer, Development of treatments and therapeutic interventions, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, 5.2 Cellular and gene therapies, Aetiology, Animals, Antigens, Neoplasm, Bone Marrow, CRISPR-Cas Systems, Disease Models, Animal, Gene Knockdown Techniques, Humans, Immunotherapy, Adoptive, Leukemia, Mice, Neoplasms, Receptors, Antigen, T-Cell, Receptors, Chimeric Antigen, T-Lymphocytes, Time Factors, Xenograft Model Antitumor Assays, ras GTPase-Activating Proteins, General Science & Technology

Abstract

The efficacy of adoptive T cell therapies for cancer treatment can be limited by suppressive signals from both extrinsic factors and intrinsic inhibitory checkpoints1,2. Targeted gene editing has the potential to overcome these limitations and enhance T cell therapeutic function3-10. Here we performed multiple genome-wide CRISPR knock-out screens under different immunosuppressive conditions to identify genes that can be targeted to prevent T cell dysfunction. These screens converged on RASA2, a RAS GTPase-activating protein (RasGAP) that we identify as a signalling checkpoint in human T cells, which is downregulated upon acute T cell receptor stimulation and can increase gradually with chronic antigen exposure. RASA2 ablation enhanced MAPK signalling and chimeric antigen receptor (CAR) T cell cytolytic activity in response to target antigen. Repeated tumour antigen stimulations in vitro revealed that RASA2-deficient T cells show increased activation, cytokine production and metabolic activity compared with control cells, and show a marked advantage in persistent cancer cell killing. RASA2-knockout CAR T cells had a competitive fitness advantage over control cells in the bone marrow in a mouse model of leukaemia. Ablation of RASA2 in multiple preclinical models of T cell receptor and CAR T cell therapies prolonged survival in mice xenografted with either liquid or solid tumours. Together, our findings highlight RASA2 as a promising target to enhance both persistence and effector function in T cell therapies for cancer treatment.

Published

2022

29. Engineered IL13 variants direct specificity of IL13Rα2-targeted CAR T cell therapy

Author

Stern, Lawrence A, Gholamin, Sharareh, Moraga, Ignacio, Yang, Xin, Saravanakumar, Supraja, Cohen, Joseph R, Starr, Renate, Aguilar, Brenda, Salvary, Vanessa, Hibbard, Jonathan C, Kalbasi, Anusha, Shepphird, Jennifer K, O’Hearn, James, Garcia, K Christopher, and Brown, Christine E

Subjects

Biological Sciences, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Genetics, Rare Diseases, Cancer, 5.2 Cellular and gene therapies, Development of treatments and therapeutic interventions, Animals, Cell Line, Tumor, Humans, Immunotherapy, Adoptive, Interleukin-13, Interleukin-13 Receptor alpha2 Subunit, Mice, Neoplasms, Protein Engineering, Tissue Distribution, Xenograft Model Antitumor Assays, chimeric antigen receptors, CARs, T cells, IL13R alpha 2, glioblastoma, IL13Rα2

Abstract

IL13Rα2 is an attractive target due to its overexpression in a variety of cancers and rare expression in healthy tissue, motivating expansion of interleukin 13 (IL13)-based chimeric antigen receptor (CAR) T cell therapy from glioblastoma into systemic malignancies. IL13Rα1, the other binding partner of IL13, is ubiquitously expressed in healthy tissue, raising concerns about the therapeutic window of systemic administration. IL13 mutants with diminished binding affinity to IL13Rα1 were previously generated by structure-guided protein engineering. In this study, two such variants, termed C4 and D7, are characterized for their ability to mediate IL13Rα2-specific response as binding domains for CAR T cells. Despite IL13Rα1 and IL13Rα2 sharing similar binding interfaces on IL13, mutations to IL13 that decrease binding affinity for IL13Rα1 did not drastically change binding affinity for IL13Rα2. Micromolar affinity to IL13Rα1 was sufficient to pacify IL13-mutein CAR T cells in the presence of IL13Rα1-overexpressing cells in vitro. Interestingly, effector activity of D7 CAR T cells, but not C4 CAR T cells, was demonstrated when cocultured with IL13Rα1/IL4Rα-coexpressing cancer cells. While low-affinity interactions with IL13Rα1 did not result in observable toxicities in mice, in vivo biodistribution studies demonstrated that C4 and D7 CAR T cells were better able to traffic away from IL13Rα1+ lung tissue than were wild-type (WT) CAR T cells. These results demonstrate the utility of structure-guided engineering of ligand-based binding domains with appropriate selectivity while validating IL13-mutein CARs with improved selectivity for application to systemic IL13Rα2-expressing malignancies.

Published

2022

30. Spatial organization of heterogeneous immunotherapy target antigen expression in high-grade glioma

Author

Barish, Michael E, Weng, Lihong, Awabdeh, Dina, Zhai, Yubo, Starr, Renate, D'Apuzzo, Massimo, Rockne, Russell C, Li, Haiqing, Badie, Behnam, Forman, Stephen J, and Brown, Christine E

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Cancer, Clinical Research, Vaccine Related, Brain Disorders, Immunization, Brain Cancer, Rare Diseases, Development of treatments and therapeutic interventions, 5.2 Cellular and gene therapies, Cell Line, Tumor, ErbB Receptors, Glioblastoma, Glioma, Humans, Immunotherapy, Immunotherapy, Adoptive, Interleukin-13 Receptor alpha2 Subunit, Receptors, Antigen, T-Cell, T-Lymphocytes, Xenograft Model Antitumor Assays, tumor heterogeneity, spatial organization of glioblastoma, antigen escape, immunotherapy, CART cells, IL13R alpha 2, HER2, EGFR, CAR T cells, IL13Rα2, Clinical Sciences, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

High-grade (WHO grades III-IV) glioma remains one of the most lethal human cancers. Adoptive transfer of tumor-targeting chimeric antigen receptor (CAR)-redirected T cells for high-grade glioma has revealed promising indications of anti-tumor activity, but objective clinical responses remain elusive for most patients. A significant challenge to effective immunotherapy is the highly heterogeneous structure of these tumors, including large variations in the magnitudes and distributions of target antigen expression, observed both within individual tumors and between patients. To obtain a more detailed understanding of immunotherapy target antigens within patient tumors, we immunochemically mapped at single cell resolution three clinically-relevant targets, IL13Rα2, HER2 and EGFR, on tumor samples drawn from a 43-patient cohort. We observed that within individual tumor samples, expression of these antigens was neither random nor uniform, but rather that they mapped into local neighborhoods - phenotypically similar cells within regions of cellular tumor - reflecting not well understood properties of tumor cells and their milieu. Notably, tumor cell neighborhoods of high antigen expression were not arranged independently within regions. For example, in cellular tumor regions, neighborhoods of high IL13Rα2 and HER2 expression appeared to be reciprocal to those of EGFR, while in areas of pseudopalisading necrosis, expression of IL13Rα2 and HER2, but not EGFR, appeared to reflect the radial organization of tumor cells around hypoxic cores. Other structural features affecting expression of immunotherapy target antigens remain to be elucidated. This structured but heterogeneous organization of antigen expression in high grade glioma is highly permissive for antigen escape, and combinatorial antigen targeting is a commonly suggested potential mitigating strategy. Deeper understanding of antigen expression within and between patient tumors will enhance optimization of combination immunotherapies, the most immediate clinical application of the observations presented here being the importance of including (wild-type) EGFR as a target antigen.

Published

2022

31. Translocon-associated Protein Subunit SSR3 Determines and Predicts Susceptibility to Paclitaxel in Breast Cancer and Glioblastoma.

Author

Dmello, Crismita, Sonabend, Aarón, Arrieta, Victor A, Zhang, Daniel Y, Kanojia, Deepak, Chen, Li, Gould, Andrew, Zhang, Jiangshan, Kang, Seong Jae, Winter, Jan, Horbinski, Craig, Amidei, Christina, Győrffy, Balázs, Cordero, Alex, Chang, Catalina Lee, Castro, Brandyn, Hsu, Patrick, Ahmed, Atique U, Lesniak, Maciej S, Stupp, Roger, and Sonabend, Adam M

Subjects

Neurosciences, Genetics, Breast Cancer, Brain Disorders, Rare Diseases, Cancer, Brain Cancer, Animals, Antineoplastic Agents, Phytogenic, Biomarkers, Pharmacological, Brain Neoplasms, Breast Neoplasms, Calcium-Binding Proteins, Cell Line, Tumor, Drug Resistance, Neoplasm, Endoribonucleases, Female, Glioblastoma, Humans, Membrane Glycoproteins, Mice, Paclitaxel, Prospective Studies, Protein Serine-Threonine Kinases, Receptors, Cytoplasmic and Nuclear, Receptors, Peptide, Xenograft Model Antitumor Assays, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

PurposePaclitaxel (PTX) is one of the most potent and commonly used chemotherapies for breast and pancreatic cancer. Several ongoing clinical trials are investigating means of enhancing delivery of PTX across the blood-brain barrier for glioblastomas. Despite the widespread use of PTX for breast cancer, and the initiative to repurpose this drug for gliomas, there are no predictive biomarkers to inform which patients will likely benefit from this therapy.Experimental designTo identify predictive biomarkers for susceptibility to PTX, we performed a genome-wide CRISPR knockout (KO) screen using human glioma cells. The genes whose KO was most enriched in the CRISPR screen underwent further selection based on their correlation with survival in the breast cancer patient cohorts treated with PTX and not in patients treated with other chemotherapies, a finding that was validated on a second independent patient cohort using progression-free survival.ResultsCombination of CRISPR screen results with outcomes from patients with taxane-treated breast cancer led to the discovery of endoplasmic reticulum (ER) protein SSR3 as a putative predictive biomarker for PTX. SSR3 protein levels showed positive correlation with susceptibility to PTX in breast cancer cells, glioma cells, and in multiple intracranial glioma xenografts models. KO of SSR3 turned the cells resistant to PTX while its overexpression sensitized the cells to PTX. Mechanistically, SSR3 confers susceptibility to PTX through regulation of phosphorylation of ER stress sensor IRE1α.ConclusionsOur hypothesis generating study showed SSR3 as a putative biomarker for susceptibility to PTX, warranting its prospective clinical validation.

Published

2022

32. RESEARCH PROGRESS IN INDIVIDUALIZED DRUG SCREENING TECHNOLOGY FOR PATIENTS WITH TUMORS

Author

WU Xiao-xiao, LIU Meiyou, PENG Li, CHENG Lianghua, WANG Fan, WANG Jingwen, JIA Yanyan

Subjects

neoplasms, drug screening assays, antitumor, genome aequencing, organoids, xenograft model antitumor assays, precision medicine, disease models, animal, review, Medicine

Abstract

In China, the incidence of tumors is increasing year by year, with the number of patients with new tumors ranking first in the world. Currently, tumors are usually treated with surgery combined with radiotherapy, chemotherapy, targeted therapy, or immunotherapy. However, individuals with tumors vary substantially in response to chemotherapeutic drugs. Therefore, selecting the drugs that patients are most sensitive to through the in vitro drug sensitivity screening technology is of great importance to guide personalized drug treatment of patients with tumors. Currently, there are various techniques for personalized anti-tumor drug screening, each with its own advantages and disadvantages. This article reviews the application progress on several commonly used techniques, with the aim to provide a reference for the selection of personalized anti-tumor drug screening techno-logy.

Published

2023

33. Targeted siRNA nanocarrier: a platform technology for cancer treatment

Author

Bäumer, Nicole, Tiemann, Jessica, Scheller, Annika, Meyer, Theresa, Wittmann, Lisa, Suburu, Matias Ezequiel Gutierrez, Greune, Lilo, Peipp, Matthias, Kellmann, Neele, Gumnior, Annika, Brand, Caroline, Hartmann, Wolfgang, Rossig, Claudia, Müller-Tidow, Carsten, Neri, Dario, Strassert, Cristian A, Rüter, Christian, Dersch, Petra, Lenz, Georg, Koeffler, H Phillip, Berdel, Wolfgang E, and Bäumer, Sebastian

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Biological Sciences, Medical Biotechnology, Oncology and Carcinogenesis, Rare Diseases, Lung Cancer, Genetics, Biotechnology, Lung, Nanotechnology, Cancer, Bioengineering, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Gene Expression Regulation, Neoplastic, Humans, Lung Neoplasms, Male, Oncogene Proteins, Fusion, Protamines, Proto-Oncogene Protein c-fli-1, RNA, Small Interfering, RNA-Binding Protein EWS, Technology, Xenograft Model Antitumor Assays, Clinical Sciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

The small arginine-rich protein protamine condenses complete genomic DNA into the sperm head. Here, we applied its high RNA binding capacity for spontaneous electrostatic assembly of therapeutic nanoparticles decorated with tumour-cell-specific antibodies for efficiently targeting siRNA. Fluorescence microscopy and DLS measurements of these nanocarriers revealed the formation of a vesicular architecture that requires presence of antibody-protamine, defined excess of free SMCC-protamine, and anionic siRNA to form. Only these complex nanoparticles were efficient in the treatment of non-small-cell lung cancer (NSCLC) xenograft models, when the oncogene KRAS was targeted via EGFR-mediated delivery. To show general applicability, we used the modular platform for IGF1R-positive Ewing sarcomas. Anti-IGR1R-antibodies were integrated into an antibody-protamine nanoparticle with an siRNA specifically against the oncogenic translocation product EWS/FLI1. Using these nanoparticles, EWS/FLI1 knockdown blocked in vitro and in vivo growth of Ewing sarcoma cells. We conclude that these antibody-protamine-siRNA nanocarriers provide a novel platform technology to specifically target different cell types and yet undruggable targets in cancer therapy by RNAi.

Published

2022

34. Alternative Splicing of EZH2 pre-mRNA by SF3B3 Contributes to the Tumorigenic Potential of Renal CancerEZH2 Gene Is Regulated by SF3B3

Author

Chen, Ke, Xiao, Haibing, Zeng, Jin, Yu, Gan, Zhou, Hui, Huang, Chunhua, Yao, Weimin, Xiao, Wei, Hu, Junhui, Guan, Wei, Wu, Lily, Huang, Jiaoti, Huang, Qihong, Xu, Hua, and Ye, Zhangqun

Subjects

Genetics, Kidney Disease, Cancer, Rare Diseases, Alternative Splicing, Animals, Carcinogenesis, Carcinoma, Renal Cell, Cell Line, Tumor, Cell Movement, Cell Proliferation, Enhancer of Zeste Homolog 2 Protein, Gene Expression Regulation, Neoplastic, Humans, Mice, Protein Isoforms, RNA Precursors, RNA Splicing Factors, Xenograft Model Antitumor Assays, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Purpose: Deregulation or mutation of the EZH2 gene causes various tumors, including clear cell renal cell carcinoma (ccRCC). Although several splice variants of EZH2 have been identified, little is known about how EZH2 splicing is regulated or the contribution of alternative splicing to its protumorigenic functions.Experimental Design: We conducted RT-PCR, Western blot analysis, and IHC techniques to examine EZH2 and its alternative splicing transcript expression in renal cancer tissue and renal cancer cell lines. Proliferation, migration, clonogenicity, and tumorigenicity of renal cancer cells either exhibiting knockdown of EZH2 or its splicing factor SF3B3 were assessed by CCK8, Transwell assay, and murine xenograft experiments.Results: We found that the inclusion of alternative EZH2 exon 14 was significantly increased in ccRCC samples and renal cancer cell lines. In ccRCC lines, enforced expression of EZH2Δ14 inhibited, and EZH2 promoted, cell growth, migration, proliferation, and tumorigenicity in a xenograft model. Mechanistic studies demonstrated that EZH2Δ14 isoform functions as a dominant-negative inhibitor of full-length EZH2. Coexpression of EZH2Δ14 variant with full-length EZH2 not only abrogated DAB2IP and HOXA9 suppression but also inhibited EZH2-driven tumorigenesis. Strikingly, the splicing factor SF3B3 stimulates inclusion of exon14 and has pro-proliferative activity. Importantly, the upregulation of SF3B3 expression observed in clinical ccRCC samples parallels the increased inclusion of EZH2 exon14, and the SF3B3 level is associated with higher tumor stage and poor overall survival.Conclusions: These results suggest SF3B3 as a key regulator of EZH2 pre-mRNA splicing and SF3B3 may represent a novel prognostic factor and potential therapeutic target in ccRCC. Clin Cancer Res; 23(13); 3428-41. ©2016 AACR.

Published

2022

35. HLA-independent T cell receptors for targeting tumors with low antigen density.

Author

Mansilla-Soto, Jorge, Eyquem, Justin, Haubner, Sascha, Hamieh, Mohamad, Feucht, Judith, Paillon, Noémie, Zucchetti, Andrés, Li, Zhuoning, Sjöstrand, Maria, Lindenbergh, Pieter, Saetersmoen, Michelle, Dobrin, Anton, Maurin, Mathieu, Iyer, Archana, Garcia Angus, Andreina, Miele, Matthew, Zhao, Zeguo, Giavridis, Theodoros, van der Stegen, Sjoukje, Tamzalit, Fella, Rivière, Isabelle, Huse, Morgan, Hendrickson, Ronald, Hivroz, Claire, and Sadelain, Michel

Subjects

Animals, Antigens, CD19, Histocompatibility Antigens, Humans, Immunotherapy, Adoptive, Leukemia, Myeloid, Acute, Mice, Receptors, Antigen, T-Cell, Receptors, Chimeric Antigen, Xenograft Model Antitumor Assays

Abstract

Chimeric antigen receptors (CARs) are receptors for antigen that direct potent immune responses. Tumor escape associated with low target antigen expression is emerging as one potential limitation of their efficacy. Here we edit the TRAC locus in human peripheral blood T cells to engage cell-surface targets through their T cell receptor-CD3 complex reconfigured to utilize the same immunoglobulin heavy and light chains as a matched CAR. We demonstrate that these HLA-independent T cell receptors (HIT receptors) consistently afford high antigen sensitivity and mediate tumor recognition beyond what CD28-based CARs, the most sensitive design to date, can provide. We demonstrate that the functional persistence of HIT T cells can be augmented by constitutive coexpression of CD80 and 4-1BBL. Finally, we validate the increased antigen sensitivity afforded by HIT receptors in xenograft mouse models of B cell leukemia and acute myeloid leukemia, targeting CD19 and CD70, respectively. Overall, HIT receptors are well suited for targeting cell surface antigens of low abundance.

Published

2022

36. Phospho-Aspirin (MDC-22) inhibits pancreatic cancer growth in patient-derived tumor xenografts and KPC mice by targeting EGFR: Enhanced efficacy in combination with irinotecan

Author

Lanzi, Cecilia Rodriguez, Wei, Ran, Luo, Dingyuan, and Mackenzie, Gerardo G

Subjects

Cancer, Rare Diseases, Pancreatic Cancer, Digestive Diseases, Orphan Drug, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Animals, Antineoplastic Agents, Aspirin, Disease Models, Animal, Drug Therapy, Combination, ErbB Receptors, Humans, Irinotecan, Mice, Pancreatic Neoplasms, Treatment Outcome, Xenograft Model Antitumor Assays, Pancreatic cancer, KPC, Phospho-Aspirin, EGFR, irinotecan, FAK, MDC-22, Clinical Sciences, Oncology & Carcinogenesis

Abstract

Novel therapeutic strategies are needed in the fight against pancreatic cancer. We have previously documented the chemopreventive effect of MDC-22 in preclinical models of pancreatic cancer. In the present work, we examined the therapeutic effects of MDC-22 in patient-derived tumor xenografts (PDTXs) and in LSL-KrasG12D/+, LSL-Trp53R172H/+, Pdx1-Cre (KPC) genetically engineered mice, two complementary and clinically relevant animal models of pancreatic cancer. In addition, we evaluated whether MDC-22 could synergize with current chemotherapeutic drugs used in the clinic. MDC-22 reduced the growth of various human pancreatic cancer cell lines in a concentration-dependent manner. In vivo, MDC-22 strongly reduced patient-derived pancreatic tumor xenograft growth by 50%, and extended survival of LSL-KrasG12D/+; LSL-Trp53R172H/+; Pdx1-Cre (KPC) mice by over a month (5.3 months versus 7.0 months). In both models, MDC-22 inhibited EGFR activation and its downstream signals, including ERK and FAK phosphorylation. In human pancreatic cancer cell lines, MDC-22 enhanced the growth inhibitory effect of irinotecan, and to a lesser degree those of gemcitabine and nab-paclitaxel. Normal human pancreatic epithelial cells were more resistant to the cytotoxic effects of, both, MDC-22 alone or in combination with irinotecan, indicating selectivity. Furthermore, MDC-22 enhanced irinotecan's effect on cell migration, in part, by inhibiting EGFR/FAK signaling. Collectively, our results indicate that MDC-22 is an effective anticancer drug in preclinical models of pancreatic cancer, and suggest that MDC-22 plus irinotecan as drug combination strategy for pancreatic cancer treatment, which warrants further evaluation.

Published

2022

37. Reprogramming of nucleotide metabolism by interferon confers dependence on the replication stress response pathway in pancreatic cancer cells

Author

Abt, Evan R, Le, Thuc M, Dann, Amanda M, Capri, Joseph R, Poddar, Soumya, Lok, Vincent, Li, Luyi, Liang, Keke, Creech, Amanda L, Rashid, Khalid, Kim, Woosuk, Wu, Nanping, Cui, Jing, Cho, Arthur, Lee, Hailey Rose, Rosser, Ethan W, Link, Jason M, Czernin, Johannes, Wu, Ting-Ting, Damoiseaux, Robert, Dawson, David W, Donahue, Timothy R, and Radu, Caius G

Subjects

Biochemistry and Cell Biology, Biological Sciences, Rare Diseases, Genetics, Cancer, Digestive Diseases, Human Genome, Pancreatic Cancer, Good Health and Well Being, Adenocarcinoma, Animals, Ataxia Telangiectasia Mutated Proteins, Carcinoma, Pancreatic Ductal, Cell Cycle Checkpoints, Cell Line, Tumor, DNA Damage, Female, Humans, Interferon Type I, Male, Membrane Proteins, Mice, Mice, Inbred NOD, Nucleotides, Pancreatic Neoplasms, Protein Kinase Inhibitors, Signal Transduction, Xenograft Model Antitumor Assays, STING, interferon, nucleotide metabolism, pancreas cancer, replication stress, Medical Physiology, Biological sciences

Abstract

We determine that type I interferon (IFN) response biomarkers are enriched in a subset of pancreatic ductal adenocarcinoma (PDAC) tumors; however, actionable vulnerabilities associated with IFN signaling have not been systematically defined. Integration of a phosphoproteomic analysis and a chemical genomics synergy screen reveals that IFN activates the replication stress response kinase ataxia telangiectasia and Rad3-related protein (ATR) in PDAC cells and sensitizes them to ATR inhibitors. IFN triggers cell-cycle arrest in S-phase, which is accompanied by nucleotide pool insufficiency and nucleoside efflux. In combination with IFN, ATR inhibitors induce lethal DNA damage and downregulate nucleotide biosynthesis. ATR inhibition limits the growth of PDAC tumors in which IFN signaling is driven by stimulator of interferon genes (STING). These results identify a cross talk between IFN, DNA replication stress response networks, and nucleotide metabolism while providing the rationale for targeted therapeutic interventions that leverage IFN signaling in tumors.

Published

2022

38. Fluorescent Anti-MUC5AC Brightly Targets Pancreatic Cancer in a Patient-derived Orthotopic Xenograft

Author

Turner, Michael A, Hollandsworth, Hannah M, Nishino, Hiroto, Amirfakhri, Siamak, Lwin, Thinzar M, Lowy, Andrew M, Kaur, Sukhwinder, Natarajan, Gopalakrishnan, Mallya, Kavita, Hoffman, Robert M, Batra, Surinder K, and Bouvet, Michael

Subjects

Rare Diseases, Orphan Drug, Biotechnology, Digestive Diseases, Pancreatic Cancer, Cancer, 2.1 Biological and endogenous factors, Aetiology, Good Health and Well Being, Animals, Fluorescent Dyes, Heterografts, Humans, Mice, Mice, Nude, Pancreatic Neoplasms, Xenograft Model Antitumor Assays, Pancreatic cancer, mucin, MUC5AC, antibody, tumor-specific imaging, fluorescence guided surgery, PDOX, Clinical Sciences, Oncology & Carcinogenesis

Abstract

BackgroundOverexpression of mucin-5AC (MUC5AC) makes it a targetable biomarker in pancreatic cancer. The present study evaluated tumor targeting with a MUC5AC antibody conjugated to a near-infrared dye in a patient-derived orthotopic xenograft (PDOX) mouse model.Materials and methodsMUC5AC monoclonal antibody was conjugated to the near-infrared dye IRDye800CW to synthesize MUC5AC-IR800. PDOX models were established by implanting a high-MUC5AC-expressing patient-derived pancreatic tumor on the pancreas of nude mice. After 4 weeks of PDOX tumor growth, mice were imaged after receiving MUC5AC-IR800 (75 μg) intravenously.ResultsIn the PDOX models, MUC5AC-IR800 selectively and brightly targeted the pancreatic tumor (tumor to background ratio: 2.46±0.465).ConclusionMUC5AC-IR800 provides distinct visualization of pancreatic tumors. MUC5AC-IR800 may be used clinically in the future to improve pancreatic cancer resection. This novel fluorescent probe is also promising for targeting of pre-malignant pancreatic lesions with subsequent resection under fluorescence guidance.

Published

2022

39. Receptor-interacting protein kinase 2 (RIPK2) stabilizes c-Myc and is a therapeutic target in prostate cancer metastasis

Author

Yan, Yiwu, Zhou, Bo, Qian, Chen, Vasquez, Alex, Kamra, Mohini, Chatterjee, Avradip, Lee, Yeon-Joo, Yuan, Xiaopu, Ellis, Leigh, Di Vizio, Dolores, Posadas, Edwin M, Kyprianou, Natasha, Knudsen, Beatrice S, Shah, Kavita, Murali, Ramachandran, Gertych, Arkadiusz, You, Sungyong, Freeman, Michael R, and Yang, Wei

Subjects

Aging, Biotechnology, Prostate Cancer, Urologic Diseases, Cancer, Development of treatments and therapeutic interventions, Aetiology, 2.1 Biological and endogenous factors, 5.1 Pharmaceuticals, Animals, Cell Line, Tumor, Cell Proliferation, Gene Expression Regulation, Neoplastic, Gene Knockout Techniques, HEK293 Cells, Humans, Imidazoles, Kaplan-Meier Estimate, Male, Mice, SCID, Neoplasm Metastasis, PC-3 Cells, Prostatic Neoplasms, Protein Kinase Inhibitors, Protein Stability, Proto-Oncogene Proteins c-myc, Pyridazines, Receptor-Interacting Protein Serine-Threonine Kinase 2, Xenograft Model Antitumor Assays

Abstract

Despite progress in prostate cancer (PC) therapeutics, distant metastasis remains a major cause of morbidity and mortality from PC. Thus, there is growing recognition that preventing or delaying PC metastasis holds great potential for substantially improving patient outcomes. Here we show receptor-interacting protein kinase 2 (RIPK2) is a clinically actionable target for inhibiting PC metastasis. RIPK2 is amplified/gained in ~65% of lethal metastatic castration-resistant PC. Its overexpression is associated with disease progression and poor prognosis, and its genetic knockout substantially reduces PC metastasis. Multi-level proteomics analyses reveal that RIPK2 strongly regulates the stability and activity of c-Myc (a driver of metastasis), largely via binding to and activating mitogen-activated protein kinase kinase 7 (MKK7), which we identify as a direct c-Myc-S62 kinase. RIPK2 inhibition by preclinical and clinical drugs inactivates the noncanonical RIPK2/MKK7/c-Myc pathway and effectively impairs PC metastatic outgrowth. These results support targeting RIPK2 signaling to extend metastasis-free and overall survival.

Published

2022

40. MAPK4 promotes triple negative breast cancer growth and reduces tumor sensitivity to PI3K blockade

Author

Wang, Wei, Han, Dong, Cai, Qinbo, Shen, Tao, Dong, Bingning, Lewis, Michael T, Wang, Runsheng, Meng, Yanling, Zhou, Wolong, Yi, Ping, Creighton, Chad J, Moore, David D, and Yang, Feng

Subjects

Cancer, Breast Cancer, Human Genome, Genetics, Animals, Breast Neoplasms, Cell Line, Tumor, Female, Gene Expression Regulation, Neoplastic, Humans, Mice, Mice, SCID, Mitogen-Activated Protein Kinases, PTEN Phosphohydrolase, Phosphatidylinositol 3-Kinases, Phosphoinositide-3 Kinase Inhibitors, Proto-Oncogene Proteins c-akt, RNA Helicases, Signal Transduction, TOR Serine-Threonine Kinases, Triple Negative Breast Neoplasms, Xenograft Model Antitumor Assays

Abstract

About 15-20% of breast cancer (BCa) is triple-negative BCa (TNBC), a devastating disease with limited therapeutic options. Aberrations in the PI3K/PTEN signaling pathway are common in TNBC. However, the therapeutic impact of PI3K inhibitors in TNBC has been limited and the mechanism(s) underlying this lack of efficacy remain elusive. Here, we demonstrate that a large subset of TNBC expresses significant levels of MAPK4, and this expression is critical for driving AKT activation independent of PI3K and promoting TNBC cell and xenograft growth. The ability of MAPK4 to bypass PI3K for AKT activation potentially provides a direct mechanism regulating tumor sensitivity to PI3K inhibition. Accordingly, repressing MAPK4 greatly sensitizes TNBC cells and xenografts to PI3K blockade. Altogether, we conclude that high MAPK4 expression defines a large subset or subtype of TNBC responsive to MAPK4 blockage. Targeting MAPK4 in this subset/subtype of TNBC both represses growth and sensitizes tumors to PI3K blockade.

Published

2022

41. Transcriptional Reprogramming Differentiates Active from Inactive ESR1 Fusions in Endocrine Therapy-Refractory Metastatic Breast Cancer.

Author

Anurag, Meenakshi, Lei, Jonathan, Kim, Beom-Jun, Singh, Purba, Seker, Sinem, Fandino, Diana, Han, Airi, Rehman, Saif, Hu, Jianhong, Korchina, Viktoriya, Doddapaneni, Harshavardhan, Dobrolecki, Lacey, Mitsiades, Nicholas, Lewis, Michael, Welm, Alana, Li, Shunqiang, Lee, Adrian, Robinson, Dan, Foulds, Charles, Ellis, Matthew, and Gou, Xuxu

Subjects

Animals, Antineoplastic Agents, Hormonal, Apoptosis, Biomarkers, Tumor, Breast Neoplasms, Cell Proliferation, Drug Resistance, Neoplasm, Estrogen Receptor alpha, Female, Gene Expression Regulation, Neoplastic, Humans, Mice, Mice, Nude, Mutation, Oncogene Proteins, Fusion, Prognosis, Survival Rate, Transcriptome, Tumor Cells, Cultured, Xenograft Model Antitumor Assays

Abstract

Genomic analysis has recently identified multiple ESR1 gene translocations in estrogen receptor alpha-positive (ERα+) metastatic breast cancer (MBC) that encode chimeric proteins whereby the ESR1 ligand binding domain (LBD) is replaced by C-terminal sequences from many different gene partners. Here we functionally screened 15 ESR1 fusions and identified 10 that promoted estradiol-independent cell growth, motility, invasion, epithelial-to-mesenchymal transition, and resistance to fulvestrant. RNA sequencing identified a gene expression pattern specific to functionally active ESR1 gene fusions that was subsequently reduced to a diagnostic 24-gene signature. This signature was further examined in 20 ERα+ patient-derived xenografts and in 55 ERα+ MBC samples. The 24-gene signature successfully identified cases harboring ESR1 gene fusions and also accurately diagnosed the presence of activating ESR1 LBD point mutations. Therefore, the 24-gene signature represents an efficient approach to screening samples for the presence of diverse somatic ESR1 mutations and translocations that drive endocrine treatment failure in MBC. SIGNIFICANCE: This study identifies a gene signature diagnostic for functional ESR1 fusions that drive poor outcome in advanced breast cancer, which could also help guide precision medicine approaches in patients harboring ESR1 mutations.

Published

2021

42. Activation of Notch and Myc signaling via B cell-restricted depletion of Dnmt3a generates a consistent murine model of chronic lymphocytic leukemia

Author

Biran, Anat, Yin, Shanye, Kretzmer, Helene, Ten Hacken, Elisa, Parvin, Salma, Lucas, Fabienne, Uduman, Mohamed, Gutierrez, Catherine, Dangle, Nathan, Billington, Leah, Regis, Fara Faye, Rassenti, Laura Z, Mohammad, Arman, Hoffmann, Gabriela Brunsting, Stevenson, Kristen, Zheng, Mei, Witten, Elizabeth, Fernandes, Stacey M, Tausch, Eugen, Sun, Clare, Stilgenbauer, Stephan, Brown, Jennifer R, Kipps, Thomas J, Aster, John C, Gnirke, Andreas, Neuberg, Donna S, Letai, Anthony, Wang, Lili, Carrasco, Ruben D, Meissner, Alexander, and Wu, Catherine J

Subjects

Genetics, Lymphoma, Cancer, Rare Diseases, Hematology, Aetiology, 2.1 Biological and endogenous factors, Animals, Anti-Bacterial Agents, Apoptosis, Biomarkers, Tumor, Cell Proliferation, DNA Methyltransferase 3A, Daptomycin, Disease Models, Animal, Drug Resistance, Neoplasm, Female, Gene Expression Regulation, Neoplastic, Humans, Leukemia, Lymphocytic, Chronic, B-Cell, Male, Mice, Mice, Inbred NOD, Mice, Knockout, Mice, SCID, Prognosis, Proto-Oncogene Proteins c-myc, RNA-Seq, Receptors, Notch, Survival Rate, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Oncology and Carcinogenesis, Oncology & Carcinogenesis

Abstract

Chronic lymphocytic leukemia (CLL) is characterized by disordered DNA methylation, suggesting these epigenetic changes might play a critical role in disease onset and progression. The methyltransferase DNMT3A is a key regulator of DNA methylation. Although DNMT3A somatic mutations in CLL are rare, we found that low DNMT3A expression is associated with more aggressive disease. A conditional knockout mouse model showed that homozygous depletion of Dnmt3a from B cells results in the development of CLL with 100% penetrance at a median age of onset of 5.3 months, and heterozygous Dnmt3a depletion yields a disease penetrance of 89% with a median onset at 18.5 months, confirming its role as a haploinsufficient tumor suppressor. B1a cells were confirmed as the cell of origin of disease in this model, and Dnmt3a depletion resulted in focal hypomethylation and activation of Notch and Myc signaling. Amplification of chromosome 15 containing the Myc gene was detected in all CLL mice tested, and infiltration of high-Myc-expressing CLL cells in the spleen was observed. Notably, hyperactivation of Notch and Myc signaling was exclusively observed in the Dnmt3a CLL mice, but not in three other CLL mouse models tested (Sf3b1-Atm, Ikzf3, and MDR), and Dnmt3a-depleted CLL were sensitive to pharmacologic inhibition of Notch signaling in vitro and in vivo. Consistent with these findings, human CLL samples with lower DNMT3A expression were more sensitive to Notch inhibition than those with higher DNMT3A expression. Altogether, these results suggest that Dnmt3a depletion induces CLL that is highly dependent on activation of Notch and Myc signaling. SIGNIFICANCE: Loss of DNMT3A expression is a driving event in CLL and is associated with aggressive disease, activation of Notch and Myc signaling, and enhanced sensitivity to Notch inhibition.

Published

2021

43. Human iPSC-derived fallopian tube organoids with BRCA1 mutation recapitulate early-stage carcinogenesis.

Author

Yucer, Nur, Ahdoot, Rodney, Workman, Michael J, Laperle, Alexander H, Recouvreux, Maria S, Kurowski, Kathleen, Naboulsi, Diana J, Liang, Victoria, Qu, Ying, Plummer, Jasmine T, Gayther, Simon A, Orsulic, Sandra, Karlan, Beth Y, and Svendsen, Clive N

Subjects

Fallopian Tubes, Organoids, Tumor Cells, Cultured, Animals, Humans, Mice, Mice, Nude, Ovarian Neoplasms, BRCA1 Protein, Case-Control Studies, Xenograft Model Antitumor Assays, Apoptosis, Cell Differentiation, Cell Proliferation, Germ-Line Mutation, Female, Induced Pluripotent Stem Cells, Carcinogenesis, carcinogenesis, disease modeling, fallopian tube, induced pluripotent stem cell, ovarian cancer, Breast Cancer, Stem Cell Research - Induced Pluripotent Stem Cell - Human, Stem Cell Research, Prevention, Clinical Research, Ovarian Cancer, Rare Diseases, Stem Cell Research - Induced Pluripotent Stem Cell, Cancer, Aetiology, 2.1 Biological and endogenous factors, Good Health and Well Being, Biochemistry and Cell Biology, Medical Physiology

Abstract

Germline pathogenic mutations in BReast CAncer (BRCA1) genes are thought to drive normal fallopian tube epithelial (FTE) cell transformation to high-grade serous ovarian cancer. No human models capture the sequence of events for disease initiation and progression. Here, we generate induced pluripotent stem cells (iPSCs) from healthy individuals and young ovarian cancer patients with germline pathogenic BRCA1 mutations (BRCA1mut). Following differentiation into FTE organoids, BRCA1mut lines exhibit cellular abnormalities consistent with neoplastic transformation compared to controls. BRCA1mut organoids show an increased production of cancer-specific proteins and survival following transplantation into mice. Organoids from women with the most aggressive ovarian cancer show the greatest pathology, indicating the potential value to predict clinical severity prior to disease onset. These human FTE organoids from BRCA1mut carriers provide a faithful physiological in vitro model of FTE lesion generation and early carcinogenesis. This platform can be used for personalized mechanistic and drug screening studies.

Published

2021

44. Selective targeting of MYC mRNA by stabilized antisense oligonucleotides

Author

Gill, Taylor, Wang, Haichuan, Bandaru, Raj, Lawlor, Matthew, Lu, Chenyue, Nieman, Linda T, Tao, Junyan, Zhang, Yixian, Anderson, Daniel G, Ting, David T, Chen, Xin, Bradner, James E, and Ott, Christopher J

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Rare Diseases, Genetics, Biotechnology, Liver Disease, Orphan Drug, Cancer, Digestive Diseases, Development of treatments and therapeutic interventions, 5.1 Pharmaceuticals, Animals, Apoptosis, Carcinoma, Hepatocellular, Cell Proliferation, Female, Humans, Liver Neoplasms, Mice, Mice, Inbred C57BL, Oligonucleotides, Antisense, Proto-Oncogene Proteins c-myc, RNA Stability, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, Clinical Sciences, Oncology & Carcinogenesis, Biochemistry and cell biology, Oncology and carcinogenesis

Abstract

MYC is a prolific proto-oncogene driving the malignant behaviors of numerous common cancers, yet potent and selective cell-permeable inhibitors of MYC remain elusive. In order to ultimately realize the goal of therapeutic MYC inhibition in cancer, we have initiated discovery chemistry efforts aimed at inhibiting MYC translation. Here we describe a series of conformationally stabilized synthetic antisense oligonucleotides designed to target MYC mRNA (MYCASOs). To support bioactivity, we designed and synthesized this focused library of MYCASOs incorporating locked nucleic acid (LNA) bases at the 5'- and 3'-ends, a phosphorothioate backbone, and internal DNA bases. Treatment of MYC-expressing cancer cells with MYCASOs leads to a potent decrease in MYC mRNA and protein levels. Cleaved MYC mRNA in MYCASO-treated cells is detected with a sensitive 5' Rapid Amplification of cDNA Ends (RACE) assay. MYCASO treatment of cancer cell lines leads to significant inhibition of cellular proliferation while specifically perturbing MYC-driven gene expression signatures. In a MYC-induced model of hepatocellular carcinoma, MYCASO treatment decreases MYC protein levels within tumors, decreases tumor burden, and improves overall survival. MYCASOs represent a new chemical tool for in vitro and in vivo modulation of MYC activity, and promising therapeutic agents for MYC-addicted tumors.

Published

2021

45. Targeting glioblastoma signaling and metabolism with a re-purposed brain-penetrant drug

Author

Bi, Junfeng, Khan, Atif, Tang, Jun, Armando, Aaron M, Wu, Sihan, Zhang, Wei, Gimple, Ryan C, Reed, Alex, Jing, Hui, Koga, Tomoyuki, Wong, Ivy Tsz-Lo, Gu, Yuchao, Miki, Shunichiro, Yang, Huijun, Prager, Briana, Curtis, Ellis J, Wainwright, Derek A, Furnari, Frank B, Rich, Jeremy N, Cloughesy, Timothy F, Kornblum, Harley I, Quehenberger, Oswald, Rzhetsky, Andrey, Cravatt, Benjamin F, and Mischel, Paul S

Subjects

Biological Sciences, Cancer, Brain Cancer, Mental Health, Brain Disorders, Rare Diseases, Neurosciences, Depression, 6.1 Pharmaceuticals, Evaluation of treatments and therapeutic interventions, Animals, Antineoplastic Agents, Antineoplastic Combined Chemotherapy Protocols, Blood-Brain Barrier, Brain Neoplasms, Cell Line, Tumor, Drug Repositioning, Electronic Health Records, Energy Metabolism, ErbB Receptors, Female, Fluoxetine, Glioblastoma, Humans, Mice, Nude, Permeability, Retrospective Studies, Signal Transduction, Sphingomyelin Phosphodiesterase, Sphingomyelins, Temozolomide, Tumor Burden, Tumor Cells, Cultured, Xenograft Model Antitumor Assays, EGFR signaling, Membrane lipids, SMPD1, combination therapy, electronic medical records, fluoxetine, glioblastoma, real-world evidence, sphingolipid metabolism, Biochemistry and Cell Biology, Medical Physiology, Biological sciences

Abstract

The highly lethal brain cancer glioblastoma (GBM) poses a daunting challenge because the blood-brain barrier renders potentially druggable amplified or mutated oncoproteins relatively inaccessible. Here, we identify sphingomyelin phosphodiesterase 1 (SMPD1), an enzyme that regulates the conversion of sphingomyelin to ceramide, as an actionable drug target in GBM. We show that the highly brain-penetrant antidepressant fluoxetine potently inhibits SMPD1 activity, killing GBMs, through inhibition of epidermal growth factor receptor (EGFR) signaling and via activation of lysosomal stress. Combining fluoxetine with temozolomide, a standard of care for GBM, causes massive increases in GBM cell death and complete tumor regression in mice. Incorporation of real-world evidence from electronic medical records from insurance databases reveals significantly increased survival in GBM patients treated with fluoxetine, which was not seen in patients treated with other selective serotonin reuptake inhibitor (SSRI) antidepressants. These results nominate the repurposing of fluoxetine as a potentially safe and promising therapy for patients with GBM and suggest prospective randomized clinical trials.

Published

2021

46. A patch of positively charged residues regulates the efficacy of clinical DR5 antibodies in solid tumors.

Author

Shivange, Gururaj, Mondal, Tanmoy, Lyerly, Evan, Bhatnagar, Sanchita, Landen, Charles N, Reddy, Shivani, Kim, Jonathan, Doan, Britney, Riddle, Paula, and Tushir-Singh, Jogender

Subjects

Animals, Mice, Inbred C57BL, Mice, Inbred NOD, Humans, Mice, SCID, Neoplasms, Antibodies, Monoclonal, Epitopes, Tumor Burden, Xenograft Model Antitumor Assays, Signal Transduction, Apoptosis, Antibody Specificity, Receptors, TNF-Related Apoptosis-Inducing Ligand, Antibodies, Monoclonal, Humanized, A549 Cells, Antineoplastic Agents, Immunological, TNBC, TNF superfamily, death receptor, death receptor agonist antibodies, ovarian tumors, receptor clustering, solid tumors, Biotechnology, Generic health relevance, Biochemistry and Cell Biology, Medical Physiology

Abstract

Receptor clustering is the first and critical step to activate apoptosis by death receptor-5 (DR5). The recent discovery of the autoinhibitory DR5 ectodomain has challenged the long-standing view of its mechanistic activation by the natural ligand Apo2L. Because the autoinhibitory residues have remained unknown, here we characterize a crucial patch of positively charged residues (PPCR) in the highly variable domain of DR5. The PPCR electrostatically separates DR5 receptors to autoinhibit their clustering in the absence of ligand and antibody binding. Mutational substitution and antibody-mediated PPCR interference resulted in increased apoptotic cytotoxic function. A dually specific antibody that enables sustained tampering with PPCR function exceptionally enhanced DR5 clustering and apoptotic activation and distinctively improved the survival of animals bearing aggressive metastatic and recurrent tumors, whereas clinically tested DR5 antibodies without PPCR blockade function were largely ineffective. Our study provides mechanistic insights into DR5 activation and a therapeutic analytical design for potential clinical success.

Published

2021

47. A protein network map of head and neck cancer reveals PIK3CA mutant drug sensitivity

Author

Swaney, Danielle L, Ramms, Dana J, Wang, Zhiyong, Park, Jisoo, Goto, Yusuke, Soucheray, Margaret, Bhola, Neil, Kim, Kyumin, Zheng, Fan, Zeng, Yan, McGregor, Michael, Herrington, Kari A, O'Keefe, Rachel, Jin, Nan, VanLandingham, Nathan K, Foussard, Helene, Von Dollen, John, Bouhaddou, Mehdi, Jimenez-Morales, David, Obernier, Kirsten, Kreisberg, Jason F, Kim, Minkyu, Johnson, Daniel E, Jura, Natalia, Grandis, Jennifer R, Gutkind, J Silvio, Ideker, Trey, and Krogan, Nevan J

Subjects

Biochemistry and Cell Biology, Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Biological Sciences, Cancer, Genetics, Rare Diseases, Dental/Oral and Craniofacial Disease, 2.1 Biological and endogenous factors, Aetiology, Animals, Carcinoma, Squamous Cell, Cell Line, Tumor, Cell Movement, Class I Phosphatidylinositol 3-Kinases, Drug Resistance, Neoplasm, Female, Head and Neck Neoplasms, Humans, Intracellular Signaling Peptides and Proteins, Mice, Mice, Nude, Microfilament Proteins, Mutation, Protein Interaction Maps, Receptor, Fibroblast Growth Factor, Type 3, Xenograft Model Antitumor Assays, General Science & Technology

Abstract

We outline a framework for elucidating tumor genetic complexity through multidimensional protein-protein interaction maps and apply it to enhancing our understanding of head and neck squamous cell carcinoma. This network uncovers 771 interactions from cancer and noncancerous cell states, including WT and mutant protein isoforms. Prioritization of cancer-enriched interactions reveals a previously unidentified association of the fibroblast growth factor receptor tyrosine kinase 3 with Daple, a guanine-nucleotide exchange factor, resulting in activation of Gαi- and p21-activated protein kinase 1/2 to promote cancer cell migration. Additionally, we observe mutation-enriched interactions between the human epidermal growth factor receptor 3 (HER3) receptor tyrosine kinase and PIK3CA (the alpha catalytic subunit of phosphatidylinositol 3-kinase) that can inform the response to HER3 inhibition in vivo. We anticipate that the application of this framework will be valuable for translating genetic alterations into a molecular and clinical understanding of the underlying biology of many disease areas.

Published

2021

48. Plant Viral Nanoparticle Conjugated with Anti-PD-1 Peptide for Ovarian Cancer Immunotherapy.

Author

Gautam, Aayushma, Beiss, Veronique, Wang, Chao, Wang, Lu, and Steinmetz, Nicole

Subjects

anti-PD-1 blockade, cancer immunotherapy, checkpoint inhibitor therapy, cowpea mosaic virus, in situ vaccine, Amino Acid Sequence, Animals, B7-H1 Antigen, Cancer Vaccines, Comovirus, Disease Models, Animal, Female, Humans, Immunotherapy, Mice, Nanoparticles, Ovarian Neoplasms, Peptides, Plant Viruses, Vaccines, Virus-Like Particle, Xenograft Model Antitumor Assays

Abstract

Immunotherapy holds tremendous potential in cancer therapy, in particular, when treatment regimens are combined to achieve synergy between pathways along the cancer immunity cycle. In previous works, we demonstrated that in situ vaccination with the plant virus cowpea mosaic virus (CPMV) activates and recruits innate immune cells, therefore reprogramming the immunosuppressive tumor microenvironment toward an immune-activated state, leading to potent anti-tumor immunity in tumor mouse models and canine patients. CPMV therapy also increases the expression of checkpoint regulators on effector T cells in the tumor microenvironment, such as PD-1/PD-L1, and we demonstrated that combination with immune checkpoint therapy improves therapeutic outcomes further. In the present work, we tested the hypothesis that CPMV could be combined with anti-PD-1 peptides to replace expensive antibody therapies. Specifically, we set out to test whether a multivalent display of anti-PD-1 peptides (SNTSESF) would enhance efficacy over a combination of CPMV and soluble peptide. Efficacy of the approaches were tested using a syngeneic mouse model of intraperitoneal ovarian cancer. CPMV combination with anti-PD-1 peptides (SNTSESF) resulted in increased efficacy; however, increased potency against metastatic ovarian cancer was only observed when SNTSESF was conjugated to CPMV, and not added as a free peptide. This can be explained by the differences in the in vivo fates of the nanoparticle formulation vs. the free peptide; the larger nanoparticles are expected to exhibit prolonged tumor residence and favorable intratumoral distribution. Our study provides new design principles for plant virus-based in situ vaccination strategies.

Published

2021

49. STING-driven interferon signaling triggers metabolic alterations in pancreas cancer cells visualized by [18F]FLT PET imaging

Author

Liang, Keke, Abt, Evan R, Le, Thuc M, Cho, Arthur, Dann, Amanda M, Cui, Jing, Li, Luyi, Rashid, Khalid, Creech, Amanda L, Wei, Liu, Ghukasyan, Razmik, Rosser, Ethan W, Wu, Nanping, Carlucci, Giuseppe, Czernin, Johannes, Donahue, Timothy R, and Radu, Caius G

Subjects

Biomedical and Clinical Sciences, Oncology and Carcinogenesis, Immunology, Rare Diseases, Genetics, Cancer, Pancreatic Cancer, Biomedical Imaging, Digestive Diseases, Animals, Cell Line, Tumor, Dideoxynucleosides, Female, Fluorine Radioisotopes, Humans, Interferon Type I, Male, Membrane Proteins, Mice, Mice, Inbred NOD, Pancreatic Neoplasms, Positron-Emission Tomography, Signal Transduction, Xenograft Model Antitumor Assays, interferon, STING, PET imaging, nucleotide metabolism, pancreatic cancer

Abstract

Type I interferons (IFNs) are critical effectors of emerging cancer immunotherapies designed to activate pattern recognition receptors (PRRs). A challenge in the clinical translation of these agents is the lack of noninvasive pharmacodynamic biomarkers that indicate increased intratumoral IFN signaling following PRR activation. Positron emission tomography (PET) imaging enables the visualization of tissue metabolic activity, but whether IFN signaling-induced alterations in tumor cell metabolism can be detected using PET has not been investigated. We found that IFN signaling augments pancreatic ductal adenocarcinoma (PDAC) cell nucleotide metabolism via transcriptional induction of metabolism-associated genes including thymidine phosphorylase (TYMP). TYMP catalyzes the first step in the catabolism of thymidine, which competitively inhibits intratumoral accumulation of the nucleoside analog PET probe 3'-deoxy-3'-[18F]fluorothymidine ([18F]FLT). Accordingly, IFN treatment up-regulates cancer cell [18F]FLT uptake in the presence of thymidine, and this effect is dependent upon TYMP expression. In vivo, genetic activation of stimulator of interferon genes (STING), a PRR highly expressed in PDAC, enhances the [18F]FLT avidity of xenograft tumors. Additionally, small molecule STING agonists trigger IFN signaling-dependent TYMP expression in PDAC cells and increase tumor [18F]FLT uptake in vivo following systemic treatment. These findings indicate that [18F]FLT accumulation in tumors is sensitive to IFN signaling and that [18F]FLT PET may serve as a pharmacodynamic biomarker for STING agonist-based therapies in PDAC and possibly other malignancies characterized by elevated STING expression.

Published

2021

50. mTORC2-mediated direct phosphorylation regulates YAP activity promoting glioblastoma growth and invasive characteristics

Author

Holmes, Brent, Benavides-Serrato, Angelica, Saunders, Jacquelyn T, Kumar, Sunil, Nishimura, Robert N, and Gera, Joseph

Subjects

Biomedical and Clinical Sciences, Clinical Sciences, Oncology and Carcinogenesis, Cancer, Brain Cancer, Neurosciences, Brain Disorders, Genetics, Rare Diseases, 2.1 Biological and endogenous factors, Animals, Brain Neoplasms, Cell Line, Tumor, Female, Glioblastoma, Hippo Signaling Pathway, Humans, Mechanistic Target of Rapamycin Complex 2, Mice, Mice, SCID, Neoplasm Invasiveness, Phosphorylation, Tumor Burden, Xenograft Model Antitumor Assays, YAP-Signaling Proteins, mTORC2, YAP, Signal transduction, Oncology & Carcinogenesis, Clinical sciences, Oncology and carcinogenesis

Abstract

The Hippo and mTOR signaling cascades are major regulators of cell growth and division. Aberrant regulation of these pathways has been demonstrated to contribute to gliomagenesis and result in enhanced glioblastoma proliferation and invasive characteristics. Several crosstalk mechanisms have been described between these two pathways, although a complete picture of these signaling interactions is lacking and is required for effective therapeutic targeting. Here we report the ability of mTORC2 to directly phosphorylate YAP at serine 436 (Ser436) positively regulating YAP activity. We show that mTORC2 activity enhances YAP transcriptional activity and the induction of YAP-dependent target gene expression while its ablation via genetic or pharmacological means has the opposite affects on YAP function. mTORC2 interacts with YAP via Sin1 and mutational analysis of serine 436 demonstrates that this phosphorylation event affects several properties of YAP leading to enhanced transactivation potential. Moreover, YAP serine 436 mutants display altered glioblastoma growth, migratory capacity and invasiveness both in vitro and in xenograft experiments. We further demonstrate that mTORC2 is able to regulate a Hippo pathway resistant allele of YAP suggesting that mTORC2 can regulate YAP independent of Hippo signaling. Correlative associations between the expression of these components in GBM patient samples also supported the presence of this signaling relationship. These results advance a direct mTORC2/YAP signaling axis driving GBM growth, motility and invasiveness.

Published

2021