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1. Proteostasis Modulation in Germline Missense von Hippel Lindau Disease

Author

Prashant Chittiboina, Debjani Mandal, Alejandro Bugarini, David T. Asuzu, Dustin Mullaney, Panagiotis Mastorakos, Stefan Stoica, Reinier Alvarez, Gretchen Scott, Dragan Maric, Abdel Elkahloun, Zhengping Zhuang, Emily Y. Chew, Chunzhang Yang, Marston Linehan, and Russell R. Lonser

Subjects
Cancer Research, Oncology
Abstract

Purpose: Missense mutated von Hippel Lindau (VHL) protein (pVHL) maintains intrinsic function but undergoes proteasomal degradation and tumor initiation and/or progression in VHL disease. Vorinostat can rescue missense mutated pVHL and arrest tumor growth in preclinical models. We asked whether short-term oral vorinostat could rescue pVHL in central nervous system hemangioblastomas in patients with germline missense VHL. Patients and Methods: We administered oral vorinostat to 7 subjects (ages 46.0 ± 14.5 years) and then removed symptomatic hemangioblastomas surgically (ClinicalTrials.gov identifier NCT02108002). Results: Vorinostat was tolerated without serious adverse events by all patients. pVHL expression was elevated in neoplastic stromal cells compared with untreated hemangioblastomas from same patients. We found transcriptional suppression of downstream hypoxia-inducible factor (HIF) effectors. Mechanistically, vorinostat prevented Hsp90 recruitment to mutated pVHL in vitro. The effects of vorinostat on the Hsp90–pVHL interaction, pVHL rescue, and transcriptional repression of downstream HIF effectors was independent of the location of the missense mutation on the VHL locus. We confirmed a neoplastic stromal cell–specific effect in suppression of protumorigenic pathways with single-nucleus transcriptomic profiling. Conclusions: We found that oral vorinostat treatment in patients with germline missense VHL mutations has a potent biologic effect that warrants further clinical study. These results provide biologic evidence to support the use of proteostasis modulation for the treatment of syndromic solid tumors involving protein misfolding. Proteostasis modulation with vorinostat rescues missense mutated VHL protein. Further clinical trials are needed to demonstrate tumor growth arrest.

Published
2023

3. Targeting PP2A for cancer therapeutic modulation

Author

Halle Ronk, Jared S. Rosenblum, Timothy Kung, and Zhengping Zhuang

Subjects
Cancer Research, Clinical Trials, Phase II as Topic, Clinical Trials, Phase I as Topic, Oncology, Neoplasms, Humans, Protein Phosphatase 2
Abstract

Protein phosphatases play essential roles as negative regulators of kinases and signaling cascades involved in cytoskeletal organization. Protein phosphatase 2A (PP2A) is highly conserved and is the predominant serine/threonine phosphatase in the nervous system, constituting more than 70% of all neuronal phosphatases. PP2A is involved in diverse regulatory functions, including cell cycle progression, apoptosis, and DNA repair. Although PP2A has historically been identified as a tumor suppressor, inhibition of PP2A has paradoxically demonstrated potential as a therapeutic target for various cancers. LB100, a water-soluble, small-molecule competitive inhibitor of PP2A, has shown particular promise as a chemo- and radio-sensitizing agent. Preclinical success has led to a profusion of clinical trials on LB100 adjuvant therapies, including a phase I trial in extensive-stage small-cell lung cancer, a phase I/II trial in myelodysplastic syndrome, a phase II trial in recurrent glioblastoma, and a completed phase I trial assessing the safety of LB100 and docetaxel in various relapsed solid tumors. Herein, we review the development of LB100, the role of PP2A in cancer biology, and recent advances in targeting PP2A inhibition in immunotherapy.

Published
2022

4. Intratumoral immunotherapy of murine pheochromocytoma shows no age-dependent differences in its efficacy

Author

Ondrej Uher, Katerina Hadrava Vanova, Radka Lencova, Andrea Frejlachova, Herui Wang, Zhengping Zhuang, Jan Zenka, and Karel Pacak

Subjects
Endocrinology, Diabetes and Metabolism
Abstract

Cancer immunotherapy has shown remarkable clinical progress in recent years. Although age is one of the biggest leading risk factors for cancer development and older adults represent a majority of cancer patients, only a few new cancer immunotherapeutic interventions have been preclinically tested in aged animals. Thus, the lack of preclinical studies focused on age-dependent effect during cancer immunotherapy could lead to different therapeutic outcomes in young and aged animals and future modifications of human clinical trials. Here, we compare the efficacy of previously developed and tested intratumoral immunotherapy, based on the combination of polysaccharide mannan, toll-like receptor ligands, and anti-CD40 antibody (MBTA immunotherapy), in young (6 weeks) and aged (71 weeks) mice bearing experimental pheochromocytoma (PHEO). The presented results point out that despite faster growth of PHEO in aged mice MBTA intratumoral immunotherapy is effective approach without age dependence and could be one of the possible therapeutic interventions to enhance immune response to pheochromocytoma and perhaps other tumor types in aged and young hosts.

Published
2023

13. Data from The Protein Phosphatase 2A Inhibitor LB100 Sensitizes Ovarian Carcinoma Cells to Cisplatin-Mediated Cytotoxicity

Author

Michael M. Gottesman, Zhengping Zhuang, R. Mark Simpson, Matthew D. Hall, James P. Madigan, Bih-Rong Wei, and Ki-Eun Chang

Abstract

Despite early positive response to platinum-based chemotherapy, the majority of ovarian carcinomas develop resistance and progress to fatal disease. Protein phosphatase 2A (PP2A) is a ubiquitous phosphatase involved in the regulation of DNA-damage response (DDR) and cell-cycle checkpoint pathways. Recent studies have shown that LB100, a small-molecule inhibitor of PP2A, sensitizes cancer cells to radiation-mediated DNA damage. We hypothesized that LB100 could sensitize ovarian cancer cells to cisplatin treatment. We performed in vitro studies in SKOV-3, OVCAR-8, and PEO1, -4, and -6 ovarian cancer lines to assess cytotoxicity potentiation, cell-death mechanism(s), cell-cycle regulation, and DDR signaling. In vivo studies were conducted in an intraperitoneal metastatic mouse model using SKOV-3/f-Luc cells. LB100 sensitized ovarian carcinoma lines to cisplatin-mediated cell death. Sensitization via LB100 was mediated by abrogation of cell-cycle arrest induced by cisplatin. Loss of the cisplatin-induced checkpoint correlated with decreased Wee1 expression, increased cdc2 activation, and increased mitotic entry (p-histone H3). LB100 also induced constitutive hyperphosphorylation of DDR proteins (BRCA1, Chk2, and γH2AX), altered the chronology and persistence of JNK activation, and modulated the expression of 14-3-3 binding sites. In vivo, cisplatin sensitization via LB100 significantly enhanced tumor growth inhibition and prevented disease progression after treatment cessation. Our results suggest that LB100 sensitizes ovarian cancer cells to cisplatin in vitro and in vivo by modulation of the DDR pathway and cell-cycle checkpoint abrogation. Mol Cancer Ther; 14(1); 90–100. ©2014 AACR.

Published
2023

14. Supplementary figures S1-S5 from The Protein Phosphatase 2A Inhibitor LB100 Sensitizes Ovarian Carcinoma Cells to Cisplatin-Mediated Cytotoxicity

Author

Michael M. Gottesman, Zhengping Zhuang, R. Mark Simpson, Matthew D. Hall, James P. Madigan, Bih-Rong Wei, and Ki-Eun Chang

Abstract

Supplementary figures S1-S5. Supplementary Figure S1. Western blot showing differential expression of PP2A-C (catalytic subunit) and PP2A-A (scaffold subunit) in different ovarian cancer cell lines; Supplementary Figure S2. LB100 is not a substrate for ATP-binding cassette (ABC) efflux transporters; Supplementary Figure S3. LB100 has minimal cross-resistance with cisplatin; Supplementary Figure S4. Inhibition of PP2A by LB100 sensitizes resistant ovarian cancer cells to cisplatin; Supplementary Figure S5. Western blots showing effect of LB100 on cell-cycle dependent kinases.

Published
2023

16. Data from Acetylation within the N- and C-Terminal Domains of Src Regulates Distinct Roles of STAT3-Mediated Tumorigenesis

Author

Y. Eugene Chin, Guohong Hu, Xiaoren Zhang, Zhengping Zhuang, Gautam U. Mehta, Chunzhang Yang, Jinsong Gao, Yimei Hao, Ting C. Zhao, Marina K. Ayrapetov, Hank W. Lee, Lihan Chen, Zhe Zhang, and Chao Huang

Abstract

Posttranslational modifications of mammalian c-Src N-terminal and C-terminal domains regulate distinct functions. Myristoylation of G2 controls its cell membrane association and phosphorylation of Y419/Y527 controls its activation or inactivation, respectively. We provide evidence that Src–cell membrane association–dissociation and catalytic activation–inactivation are both regulated by acetylation. In EGF-treated cells, CREB binding protein (CBP) acetylates an N-terminal lysine cluster (K5, K7, and K9) of c-Src to promote dissociation from the cell membrane. CBP also acetylates the C-terminal K401, K423, and K427 of c-Src to activate intrinsic kinase activity for STAT3 recruitment and activation. N-terminal domain phosphorylation (Y14, Y45, and Y68) of STAT3 by c-Src activates transcriptionally active dimers of STAT3. Moreover, acetyl-Src translocates into nuclei, where it forms the Src-STAT3 enhanceosome for gene regulation and cancer cell proliferation. Thus, c-Src acetylation in the N-terminal and C-terminal domains play distinct roles in Src activity and regulation.Significance: CBP-mediated acetylation of lysine clusters in both the N-terminal and C-terminal regions of c-Src provides additional levels of control over STAT3 transcriptional activity. Cancer Res; 78(11); 2825–38. ©2018 AACR.

Published
2023

18. Supplemental Experimental Procedures, Supplementary Tables 1-3, Supplementary Figures 1-9 from Global Metabolic Profiling Identifies a Pivotal Role of Proline and Hydroxyproline Metabolism in Supporting Hypoxic Response in Hepatocellular Carcinoma

Author

Yang Liu, Guowang Xu, Zhengping Zhuang, Enyou Li, Peng Gao, Jane Yu, Lei Guo, Chunxiu Hu, Peiyuan Yin, Jiao Wang, Changsong Wang, Mingju Sun, Yang Wang, Chengnan Fang, Pengyu Geng, Jun Zeng, and Ling Tang

Abstract

Table S1. Clinical information of enrolled subjects for discovery; Table S2. Clinical information of enrolled hepatic carcinoma subjects for validation; TableS3. Differential metabolites obtained from tissue specimens in metabolomics discovery; Figure S1. Scheme of the metabolic characterization study of hepatic carcinoma; Figure S2. Metabolic pathway analysis for HCC. Figure S3. Refining of important differential metabolites; Figure S4. The correlation between hydroxyproline and clinical parameters for discovery specimens; Figure S5. Proliferation assay in tumor xenografts; Figure S6. mRNA levels of PRODH2 and ALDH18A1 in HCC under hypoxia; Figure S7. 13C5 glutamine tracer analysis for glutamate and proline production under hypoxic condition in SMMC-7721 cell line. (mean± SE); Figure S8. Knockdown of MYC has no effect on expression of prolidase in HCC cell; Figure S9. Knockdown of ALDH18A1 induced apoptosis in the presence of sorafenib under hypoxia.

Published
2023

20. Data from Global Metabolic Profiling Identifies a Pivotal Role of Proline and Hydroxyproline Metabolism in Supporting Hypoxic Response in Hepatocellular Carcinoma

Author

Yang Liu, Guowang Xu, Zhengping Zhuang, Enyou Li, Peng Gao, Jane Yu, Lei Guo, Chunxiu Hu, Peiyuan Yin, Jiao Wang, Changsong Wang, Mingju Sun, Yang Wang, Chengnan Fang, Pengyu Geng, Jun Zeng, and Ling Tang

Abstract

Purpose: Metabolic reprogramming is frequently identified in hepatocellular carcinoma (HCC), which is the most common type of liver malignancy. The reprogrammed cellular metabolisms promote tumor cell survival, proliferation, angiogenesis, and metastasis. However, the mechanisms of this process remain unclear in HCC.Experimental Design: The global nontargeted metabolic study in 69 paired hepatic carcinomas and adjacent tissue specimens was performed using capillary electrophoresis-time of flight mass spectrometry–based approach. Key findings were validated by targeted metabolomic approach. Biological studies were also performed to investigate the role of proline biosynthesis in HCC pathogenesis.Results: Proline metabolism was markedly changed in HCC tumor tissue, characterized with accelerated consumption of proline and accumulation of hydroxyproline, which significantly correlated with α-fetoprotein levels and poor prognosis in HCC. In addition, we found that hydroxyproline promoted hypoxia- and HIF-dependent phenotype in HCC. Moreover, we demonstrated that hypoxia activated proline biosynthesis via upregulation of ALDH18A1, subsequently leading to accumulation of hydroxyproline via attenuated PRODH2 activity. More importantly, we showed that glutamine, proline, and hydroxyproline metabolic axis supported HCC cell survival through modulating HIF1α stability in response to hypoxia. Finally, inhibition of proline biosynthesis significantly enhanced cytotoxicity of sorafenib in vitro and in vivo.Conclusions: Our results demonstrate that hypoxic microenvironment activates proline metabolism, resulting in accumulation of hydroxyproline that promotes HCC tumor progression and sorafenib resistance through modulating HIF1α. These findings provide the proof of concept for targeting proline metabolism as a potential therapeutic strategy for HCC. Clin Cancer Res; 24(2); 474–85. ©2017 AACR.

Published
2023

27. Data from Novel Targeting of Transcription and Metabolism in Glioblastoma

Author

Jing Wu, Mark R. Gilbert, Chunzhang Yang, Zhengping Zhuang, Mones Abu-Asab, Mioara Larion, Thomas Estok, Kristan Meetze, Wei Zhang, Orieta Celiku, Aiguo Li, Dragan Maric, Adrian Lita, Gabriel Vasconcelos, Hallie Lappin, Li-Yuan Chen, Qi Zhang, Hua Song, Herui Wang, Robert Chen, and Yu-Ting Su

Abstract

Purpose: Glioblastoma (GBM) is highly resistant to treatment, largely due to disease heterogeneity and resistance mechanisms. We sought to investigate a promising drug that can inhibit multiple aspects of cancer cell survival mechanisms and become an effective therapeutic for GBM patients.Experimental Design: To investigate TG02, an agent with known penetration of the blood–brain barrier, we examined the effects as single agent and in combination with temozolomide, a commonly used chemotherapy in GBM. We used human GBM cells and a syngeneic mouse orthotopic GBM model, evaluating survival and the pharmacodynamics of TG02. Mechanistic studies included TG02-induced transcriptional regulation, apoptosis, and RNA sequencing in treated GBM cells as well as the investigation of mitochondrial and glycolytic function assays.Results: We demonstrated that TG02 inhibited cell proliferation, induced cell death, and synergized with temozolomide in GBM cells with different genetic background but not in astrocytes. TG02-induced cytotoxicity was blocked by the overexpression of phosphorylated CDK9, suggesting a CDK9-dependent cell killing. TG02 suppressed transcriptional progression of antiapoptotic proteins and induced apoptosis in GBM cells. We further demonstrated that TG02 caused mitochondrial dysfunction and glycolytic suppression and ultimately ATP depletion in GBM. A prolonged survival was observed in GBM mice receiving combined treatment of TG02 and temozolomide. The TG02-induced decrease of CDK9 phosphorylation was confirmed in the brain tumor tissue.Conclusions: TG02 inhibits multiple survival mechanisms and synergistically decreases energy production with temozolomide, representing a promising therapeutic strategy in GBM, currently under investigation in an ongoing clinical trial. Clin Cancer Res; 24(5); 1124–37. ©2017 AACR.

Published
2023

29. 'Tumor Treating Fields' delivered via electromagnetic induction have varied effects across glioma cell lines and electric field amplitudes

Author

Rea Ravin, Teddy X. Cai, Aiguo Li, Nicole Briceno, Randall H. Pursley, Marcial Garmendia-Cedillos, Tom Pohida, Herui Wang, Zhengping Zhuang, Jing Cui, Nicole Y. Morgan, Nathan H. Williamson, Mark R. Gilbert, and Peter J. Basser

Subjects
Article
Abstract

Previous studies reported that alternating electric fields (EFs) in the intermediate frequency (100 – 300 kHz) and low intensity (1 – 3 V/cm) regime — termed “Tumor Treating Fields” (TTFields) — have a specific, anti-proliferative effect on glioblastoma multiforme (GBM) cells. However, the mechanism(s) of action remain(s) incompletely understood, hindering the clinical adoption of treatments based on TTFields. To advance the study of such treatmentin vitro, we developed an inductive device to deliver EFs to cell cultures which improves thermal and osmolar regulation compared to prior devices. Using this inductive device, we applied continuous, 200 kHz electromagnetic fields (EMFs) with a radial EF amplitude profile spanning 0 – 6.5 V/cm to cultures of primary rat astrocytes and several human GBM cell lines — U87, U118, GSC827, and GSC923 — for a duration of 72 hours. Cell density was assessed via segmented pixel densities from GFP expression (U87, U118) or from staining (astrocytes, GSC827, GSC923). Further RNA-Seq analyses were performed on GSC827 and GSC923 cells. Treated cultures of all cell lines exhibited little to no change in proliferation at lower EF amplitudes (0 – 3 V/cm). At higher amplitudes (> 4 V/cm), different effects were observed. Apparent cell densities increased (U87), decreased (GSC827, GSC923), or showed little change (U118, astrocytes). RNA-Seq analyses on treated and untreated GSC827 and GSC923 cells revealed differentially expressed gene sets of interest, such as those related to cell cycle control. Up- and down-regulation, however, was not consistent across cell lines nor EF amplitudes. Our results indicate no consistent, anti-proliferative effect of 200 kHz EMFs across GBM cell lines and thus contradict previousin vitrofindings. Rather, effects varied across different cell lines and EF amplitude regimes, highlighting the need to assess the effect(s) of TTFields and similar treatments on a per cell line basis.

Published
2023

31. A 13-Year-Old Male With Left Eye Swelling

Author

Matthew A, Nazari, Jared S, Rosenblum, Zhengping, Zhuang, Archana, Malik, Russell R, Lonser, Karel, Pacak, and Stephen, Aronoff

Subjects
Male, Adolescent, Pediatrics, Perinatology and Child Health, Humans, Edema, Pain, Eye
Abstract

A 13-year-old male presented with a 10-day history of left eye swelling and pain. These symptoms prompted presentation to the emergency department. He had no significant past medical history and no preceding fevers or chills. He was found on examination of the eyes and the orbit to have left supraorbital erythema, edema, and pain with upward and medial gaze. Examination of the globe, fundus, and visual fields were normal. His white blood cell count was 6.2 (x1000/mm3) with an erythrocyte sedimentation rate of 4 (mm/hr). Diagnostic endoscopic biopsy was performed. Here we present this case alongside clinical reasoning and diagnostic evaluation with relevant input from respective experts. This case discussion reviews the final diagnosis, as well as the corresponding evaluation and management. Diagnostic algorithms based on literature review and clinical experience are also included.

Published
2022

32. Acute worsening of CADASIL in a patient with COVID-19 infection: illustrative case

Author

Jared S. Rosenblum, Jessa M. Tunacao, Matthew A. Nazari, Halle Ronk, Danielle D. Dang, Chad Downing, Zhengping Zhuang, John D. Heiss, James G. Smirniotopoulos, Avraham Bluestone, James Badia, and Joseph White

Subjects
General Medicine
Abstract

BACKGROUND Reports of cerebrovascular ischemia and stroke occurring as predominant neurological sequelae of severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection, which causes coronavirus disease 2019 (COVID-19), are increasingly evident within the literature. While various pathophysiological mechanisms have been postulated, including hypercoagulability, endothelial invasion, and systemic inflammation, discrete mechanisms for viral neurotropism remain unclear and controversial. OBSERVATIONS The authors present a unique case study of a 64-year-old male with acute COVID-19 infection and acute worsening of previously stable cerebral autosomal dominant arteriopathy with subcortical infarcts and leukoencephalopathy (CADASIL), a rare heritable arteriopathy due to mutation in the Notch3 gene, which is critical for vascular development and tone. Delayed cranial neuropathies, brainstem fluid-attenuated inversion recovery signal, and enhancement of olfactory and vagus nerves on magnetic resonance neurography in this patient further support viral neurotropism via cranial nerves in addition to cerebral vasculature. LESSONS To the authors’ knowledge, this is the first case in the literature that not only demonstrates the consequences of COVID-19 infection in a patient with altered cerebrovascular autoregulation such as CADASIL but also highlights the tropism of SARS-CoV-2 for (1) cranial nerves as a mode of entry to the central nervous system and (2) vessels as a cause of cerebrovascular ischemia.

Published
2022

33. Mannan-BAM, TLR ligands, and anti-CD40 immunotherapy in established murine pancreatic adenocarcinoma: understanding therapeutic potentials and limitations

Author

Marketa Skalickova, Ondrej Uher, Andrea Frejlachova, Per Hansen, Karolina Kvardova, Veronika Caisova, Jan Zenka, Adéla Chlastáková, Karel Pacak, Jindrich Chmelar, Zhengping Zhuang, Jan Kopecky, Lucie Padoukova, Kamila Masakova, Radka Lencova, and Anna Venhauerova

Subjects
Lipopolysaccharides, Cancer Research, T-Lymphocytes, medicine.medical_treatment, Immunology, Adenocarcinoma, Ligands, Article, Mannans, Pheochromocytoma, Mice, Cancer immunotherapy, Antineoplastic Combined Chemotherapy Protocols, Animals, Immunology and Allergy, Medicine, CD40 Antigens, Receptor, biology, business.industry, Melanoma, Toll-Like Receptors, Imidazoles, Immunotherapy, medicine.disease, Pancreatic Neoplasms, Teichoic Acids, Poly I-C, Oncology, Cancer research, biology.protein, Antibody, business, CD8
Abstract

Pancreatic adenocarcinoma is one of the leading causes of cancer-related deaths, and its therapy remains a challenge. Our proposed therapeutic approach is based on the intratumoral injections of mannan-BAM, toll-like receptor ligands, and anti-CD40 antibody (thus termed MBTA therapy), and has shown promising results in the elimination of subcutaneous murine melanoma, pheochromocytoma, colon carcinoma, and smaller pancreatic adenocarcinoma (Panc02). Here, we tested the short- and long-term effects of MBTA therapy in established subcutaneous Panc02 tumors two times larger than in previous study and bilateral Panc02 models as well as the roles of CD4(+) and CD8(+) T lymphocytes in this therapy. The MBTA therapy resulted in eradication of 67% of Panc02 tumors with the development of long-term memory as evidenced by the rejection of Panc02 cells after subcutaneous and intracranial transplantations. The initial Panc02 tumor elimination is not dependent on the presence of CD4(+) T lymphocytes, although these cells seem to be important in long-term survival and resistance against tumor retransplantation. The resistance was revealed to be antigen-specific due to its inability to reject B16-F10 melanoma cells. In the bilateral Panc02 model, MBTA therapy manifested a lower therapeutic response. Despite numerous combinations of MBTA therapy with other therapeutic approaches, our results show that only simultaneous application of MBTA therapy into both tumors has potential for the treatment of the bilateral Panc02 model.

Published
2021

34. Metformin enhances anti-cancer effects of cisplatin in meningioma through AMPK-mTOR signaling pathways

Author

Xiaohua Zhang, Liemei Guo, Jing Cui, Zhengping Zhuang, Yingying Lin, Herui Wang, Rogelio Medina, and Shilei Zhang

Subjects
AMPK, 0301 basic medicine, Cancer Research, endocrine system diseases, cisplatin, lcsh:RC254-282, meningioma, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, medicine, Chemosensitizing agent, Pharmacology (medical), Protein kinase A, PI3K/AKT/mTOR pathway, Cisplatin, business.industry, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Metformin, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, mTOR, Cancer research, Molecular Medicine, Original Article, Signal transduction, metformin, business, medicine.drug
Abstract

Cisplatin is currently used to treat inoperable recurrent meningiomas, but its side effects and drug resistance limit its use. Metformin has recently been identified as a chemosensitizing agent. However, the combined treatment of cisplatin and metformin in high-grade meningiomas has not been reported. Herein, our findings demonstrate metformin significantly enhanced cisplatin-induced inhibition of proliferation in meningioma cells, which was associated with the induction of G0/G1 cell cycle arrest. Additionally, metformin activated adenosine monophosphate activated protein kinase (AMPK) and repressed the mammalian target of rapamycin (mTOR) signaling pathways via an AMPK-dependent mechanism. Furthermore, our xenograft murine model confirmed that metformin enhanced cisplatin’s anti-cancer effect by upregulation of AMPK and downregulation of mTOR signaling pathways. In addition, in 63 patients with atypical meningiomas, the activation of AMPK was significantly associated with tumor recurrence and short disease-free survival (DFS). These results demonstrate metformin enhanced the anti-cancer effect of cisplatin in meningioma in vitro and in vivo, an effect mediated through the activation of AMPK and repression of mTOR signaling pathways. Our study suggests the combined treatment of metformin and cisplatin is an effective and safe treatment for high-grade meningiomas., Graphical Abstract, Lin, Zhuang, and their scholars confirmed for the first time that metformin combined with cisplatin is a safe and effective treatment for high-grade meningioma. This study illuminates a new direction for treating high-grade meningioma.

Published
2021

35. Epigenetic Regulation in Primary CNS Tumors: An Opportunity to Bridge Old and New WHO Classifications

Author

Danielle D. Dang, Jared S. Rosenblum, Ashish H. Shah, Zhengping Zhuang, and Tara T. Doucet-O’Hare

Subjects
Cancer Research, Oncology
Abstract

Originally approved in 1979, a specific grading classification for central nervous system (CNS) tumors was devised by the World Health Organization (WHO) in an effort to guide cancer treatment and better understand prognosis. These “blue books” have since undergone several iterations based on tumor location, advancements in histopathology, and most recently, diagnostic molecular pathology in its fifth edition. As new research methods have evolved to elucidate complex molecular mechanisms of tumorigenesis, a need to update and integrate these findings into the WHO grading scheme has become apparent. Epigenetic tools represent an area of burgeoning interest that encompasses all non-Mendelian inherited genetic features affecting gene expression, including but not limited to chromatin remodeling complexes, DNA methylation, and histone regulating enzymes. The SWItch/Sucrose non-fermenting (SWI/SNF) chromatin remodeling complex is the largest mammalian family of chromatin remodeling proteins and is estimated to be altered in 20–25% of all human malignancies; however, the ways in which it contributes to tumorigenesis are not fully understood. We recently discovered that CNS tumors with SWI/SNF mutations have revealed an oncogenic role for endogenous retroviruses (ERVs), remnants of exogenous retroviruses that integrated into the germline and are inherited like Mendelian genes, several of which retain open reading frames for proteins whose expression putatively contributes to tumor formation. Herein, we analyzed the latest WHO classification scheme for all CNS tumors with documented SWI/SNF mutations and/or aberrant ERV expression, and we summarize this information to highlight potential research opportunities that could be integrated into the grading scheme to better delineate diagnostic criteria and therapeutic targets.

Published
2023

36. Abstract 6800: Unique autologous cancer vaccine comprised of irradiated whole tumor cells and MBTA (rWTC-MBTA) triggers antitumor immune response to prevent metastasis

Author

Juan Ye, Herui Wang, Mitchell Sun, Ondrej Uher, Mark R. Gilbert, Karel Pacak, Zhengping Zhuang, Rogelio Medina, Samik Chakraborty, and Jan Zenka

Subjects
Cancer Research, Oncology
Abstract

Despite the advances made in cancer treatment over the past decades, one statistic has remained unchanged: metastatic cancer accounts for 90 percent of annual cancer deaths in the United States. Our group previously demonstrated that an autologous whole tumor cell vaccine (rWTC-MBTA: irradiated autologous whole tumor cells pulsed with Mannan-BAM, TLR ligands, and anti-CD40 antibody) had a potent anti-tumor immune response and prolonged survival in a mouse colon carcinoma model. To investigate whether rWTC-MBTA would work in “cold” tumor models, we evaluated the vaccine’s effect on preventing and treating tumor metastasis in 4T1 breast tumors. Our data showed that vaccinated mice could significantly prevent lung metastasis in both intravenous injection and mammary pad subcutaneous implantation animal models. Further, we used another metastasis model that more closely mimics clinical practice by resecting the primary tumor after metastasis development. The data showed that vaccinated mice could prevent tumor recurrence, increase T-cell infiltration in the metastatic tumor, and prolong the survival curve. The mechanistic investigation by immunophenotyping revealed that rWTC-MBTA vaccination induced both effector memory (CD44+CD62L−) and center memory (CD44+CD62L+) T cells as well as increased overall CD4+ and CD8+ T-cell count while depletion experiments demonstrated that CD8+ T cells were required for vaccine efficacy. Isolated splenocytes co-cultured with 4T1 cells showed rWTC-MBTA significantly increased T-cell mediated cytotoxicity through TNF-a and IFN-γ in CD107a+CD4+ T cells and Granzyme B and IFN-γ in CD107a+CD8+ T cells. In all experiments, vaccination exerted negligible systemic toxicity. Collectively, our study demonstrates that the rWTC-MBTA vaccine is a safe and promising therapeutic option to prevent and treat tumor metastasis by triggering an antitumor immune response. Citation Format: Juan Ye, Herui Wang, Mitchell Sun, Ondrej Uher, Mark R. Gilbert, Karel Pacak, Zhengping Zhuang, Rogelio Medina, Samik Chakraborty, Jan Zenka. Unique autologous cancer vaccine comprised of irradiated whole tumor cells and MBTA (rWTC-MBTA) triggers antitumor immune response to prevent metastasis. [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 6800.

Published
2023

37. Abstract 691: Irradiated whole tumor cells pulsed with mannan-BAM, TLR ligands and anti-CD40 antibody serve as a potent tumor cell vaccine against glioblastoma

Author

Herui Wang, Rogelio Medina, Juan Ye, Samik Chakraborty, Ondrej Uher, Mitchell Sun, Jan Zenka, Mark R. Gilbert, Karel Pacak, and Zhengping Zhuang

Subjects
Cancer Research, Oncology
Abstract

Despite numerous therapeutic advances in cancers, the treatment of glioblastoma multiforme (GBM) remains a challenge. Boosting T-lymphocyte mediated responses against GBM offers a promising approach towards solving this problem. Herein, we present a therapeutic vaccination strategy that promotes the phagocytosis of tumor cells, enhances tumor antigen presentation, and induces a tumor-specific adaptive immune response with subsequent tumor eradication. This strategy consists of subcutaneous injection of irradiated whole tumor cells (rWTC) pulsed with phagocytic agonists (Mannan-BAM), TLR ligands (LTA, Poly (I:C), and R-848), and anti-CD40 agonistic antibody (collectively abbreviated as rWTC-MBTA). We evaluated the therapeutic efficacy of rWTC-MBTA strategy in mouse syngeneic GBM tumor models with GL261 and SB28 cells. In GL261 GBM model, complete regression (CR) of intracranial tumors was achieved in 70% (7/10) of rWTC-MBTA treated animals while none survived in the control group. Of note, the therapeutic efficacy of rWTC-MBTA was abolished in CD4-T and/or CD8-T lymphocyte depleted mice. Immunophenotyping analyses of peripheral lymph nodes and brain tumors of rWTC-MBTA treated mice demonstrated increased antigen presenting cells (dendritic cells and MHC II+ monocytes) and increased cytotoxic IFNγ, TNFα, and granzyme B-secreting CD4-T and CD8-T cells. All three CR mice that were rechallenged with GL261 cells intracranially 14 months after their last rWTC-MBTA treatment resisted tumor development, confirming the establishment of long-term immunological memory. In SB28 GBM model, 80% (8/10) rWTC-MBTA treated mice survived past 95 days after tumor cell implantation without any GBM-related symptoms, with median survival being only 35 days in control groups. In summary, our study demonstrated that rWTC-MBTA strategy can induce potent adaptive immune response against GBM in pre-clinical models. Citation Format: Herui Wang, Rogelio Medina, Juan Ye, Samik Chakraborty, Ondrej Uher, Mitchell Sun, Jan Zenka, Mark R. Gilbert, Karel Pacak, Zhengping Zhuang. Irradiated whole tumor cells pulsed with mannan-BAM, TLR ligands and anti-CD40 antibody serve as a potent tumor cell vaccine against glioblastoma [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2023; Part 1 (Regular and Invited Abstracts); 2023 Apr 14-19; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2023;83(7_Suppl):Abstract nr 691.

Published
2023

39. Somatic Mosaicism of EPAS1 Mutations in Pacak-Zhuang Syndrome

Author

Herui Wang, Zhengping Zhuang, Jared S. Rosenblum, and Karel Pacak

Subjects
Adolescent, Whole Genome Sequencing, Mosaicism, Endocrinology, Diabetes and Metabolism, Adrenal Gland Neoplasms, Polycythemia, Syndrome, Magnetic Resonance Imaging, Article, Normetanephrine, Paraganglioma, Endocrinology, Indenes, Gain of Function Mutation, Adrenal Glands, Mutation, Basic Helix-Loop-Helix Transcription Factors, Chromogranins, Humans, Female, Biomarkers, Signal Transduction
Abstract

The integration of genomic testing into clinical care enables the use of individualized approaches to the management of rare diseases. We describe the use of belzutifan, a potent and selective small-molecule inhibitor of the protein hypoxia-inducible factor 2α (HIF2α), in a patient with polycythemia and multiple paragangliomas (the Pacak-Zhuang syndrome). The syndrome was caused in this patient by somatic mosaicism for an activating mutation in

Published
2022

40. Non-invasive

Author

Jared S, Rosenblum, Anthony J, Cappadona, Pashayar P, Lookian, Vikram, Chandrashekhar, Jean-Paul, Bryant, Vibhu, Chandrashekhar, David Y, Zhao, Russell H, Knutsen, Danielle R, Donahue, Dorian B, McGavern, Beth, Kozel, John D, Heiss, and Zhengping, Zhuang

Abstract

Understanding physiologic and pathologic central nervous system function depends on our ability to map the entire

Published
2022

41. C‐Terminal, but Not Intact, <scp>FGF23</scp> and <scp>EPO</scp> Are Strongly Correlatively Elevated in Patients With Gain‐of‐Function Mutations in <scp>HIF2A</scp> : Clinical Evidence for <scp>EPO</scp> Regulating <scp>FGF23</scp>

Author

Thanh Huynh, Ying Pang, Karel Pacak, Sydney M Brown, Michael T. Collins, Kelly L Roszko, and Zhengping Zhuang

Subjects
0301 basic medicine, Fibroblast growth factor 23, medicine.medical_specialty, Hormone activity, Chemistry, Endocrinology, Diabetes and Metabolism, EPAS1, 030209 endocrinology & metabolism, urologic and male genital diseases, In vitro, stomatognathic diseases, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Endocrinology, In vivo, Erythropoietin, Internal medicine, medicine, Orthopedics and Sports Medicine, Post-translational regulation, Hormone, medicine.drug
Abstract

Fibroblast growth factor 23 (FGF23) is a key phosphate- and vitamin D-regulating hormone. FGF23 circulates as an intact 251 amino acid protein or N- and C-terminal degradation products. Hormone activity resides in the intact molecule, but it has been suggested that high levels of the C-terminal protein can interfere with intact FGF23 (iFGF23) activity. New evidence points to involvement of the hypoxia-inducible factor (HIF)/erythropoietin (EPO)/iron pathway as important in FGF23 physiology. Exactly how this pathway regulates FGF23 is not clear. Various in vitro, in vivo, and clinical studies involving perturbations in this pathway at various points have yielded conflicting results. Many of these studies are complicated by the confounding, independent effect of renal insufficiency on FGF23. To gain insight into FGF23 physiology, we studied 8 patients with a rare paraganglioma/somatostatinoma syndrome who had elevated blood EPO levels as a result of somatic gain-of-function mutations in HIF2A (EPAS1) that stimulate tumoral EPO production. All patients had normal renal function. EPO levels varied; most were very elevated and highly correlated with C-terminal FGF23 (cFGF23) levels that were also markedly elevated. Blood phosphate and intact FGF23 levels were normal. These data from patients with normal renal function in whom HIF activation was the inciting event suggest a direct role of the HIF/EPO pathway in FGF23 transcription and translation. They also demonstrate that posttranslational regulation was finely tuned to maintain normal blood phosphate levels. Additionally, normal phosphate and intact FGF23 levels in the setting of markedly increased C-terminal FGF23 levels suggest intact FGF23 action is not attenuated by C-terminal FGF23. Published 2020. This article is a U.S. Government work and is in the public domain in the USA. Journal of Bone and Mineral Research published by Wiley Periodicals LLC on behalf of American Society for Bone and Mineral Research (ASBMR).

Published
2020

42. Blocking lncRNA MALAT1/miR-199a/ZHX1 Axis Inhibits Glioblastoma Proliferation and Progression

Author

Pauline Dmitriev, Zhipeng Xiao, Xiaochun Zhao, Yingying Lin, Zhengping Zhuang, Weizhen Gao, Yongming Qiu, Jianwei Ge, Liemei Guo, Keman Liao, Xiaohua Zhang, Rogelio Medina, and Jing Cui

Subjects
0301 basic medicine, Biology, medicine.disease_cause, Article, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Glioma, Drug Discovery, medicine, competing endogenous RNA, MALAT1, Gene knockdown, long non-coding RNA, Competing endogenous RNA, Cell growth, lcsh:RM1-950, glioblastoma, ZHX1, medicine.disease, Long non-coding RNA, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Molecular Medicine, Carcinogenesis
Abstract

Zinc fingers and homeoboxes 1 (ZHX1) is a transcription repressor that has been implicated in the tumorigenesis and progression of diverse tumors. The functional role and regulating mechanism of ZHX1 has not been elucidated in glioblastoma (GBM). Previous reports have suggested that a large number of non-coding RNAs play a vital role in glioma initiation and progression. This study aimed to investigate the functional role and co-regulatory mechanisms of the metastasis-associated lung adenocarcinoma transcript-1 (MALAT1)/ microRNA-199a (miR-199a)/ZHX1 axis in GBM. We analyzed the expression of the MALAT1/miR-199a/ZHX1 axis and its correlation with patients’ overall survival using two different glioma gene-expression datasets. A series of in vitro and in vivo studies including dual luciferase reporter assay, fluorescence in situ hybridization (FISH), RNA immunoprecipitation, and pull-down experiments were completed to elucidate the biological significance of the MALAT1/miR-199a/ZHX1 axis in promoting glioma proliferation and progression. Elevated ZHX1 expression correlated with poor prognosis in GBM patients, and in vitro studies demonstrated that ZHX1 attenuated GBM cell apoptosis by downregulation of pro-apoptotic protein (Bax) and upregulation of anti-apoptotic protein (Bcl-2). Furthermore, knockdown of MALAT1 inhibited GBM proliferation and progression in vitro and reduced tumor volume and prolonged survival in an orthotopic GBM murine model. Finally, we demonstrated that MALAT1 promoted ZHX1 expression via acting as a competing endogenous RNA by sponging miR-199a. The MALAT1/miR-199a/ZHX1 axis promotes GBM cell proliferation and progression in vitro and in vivo, and its expression negatively correlates with GBM patient survival. Blocking the MALAT1/miR-199a/ZHX1 axis can serve as a novel therapeutic strategy for treating GBM. Keywords: MALAT1, ZHX1, glioblastoma, competing endogenous RNA, long non-coding RNA

Published
2019

43. Targeting selenoprotein H in the nucleolus suppresses tumors and metastases by Isovalerylspiramycin I

Author

Jing Cui, Jingcheng Zhou, Weiqing He, Juan Ye, Timothy Westlake, Rogelio Medina, Herui Wang, Bhushan L. Thakur, Juanjuan Liu, Mingyu Xia, Zhonggui He, Fred E. Indig, Aiguo Li, Yan Li, Robert J. Weil, Mirit I. Aladjem, Laiping Zhong, Mark R. Gilbert, and Zhengping Zhuang

Subjects
Cancer Research, Oncology, RNA, Ribosomal, Humans, Nuclear Proteins, Reactive Oxygen Species, Selenoproteins, Cell Nucleolus, Genomic Instability
Abstract

Background Compared to normal cells, cancer cells exhibit a higher level of oxidative stress, which primes key cellular and metabolic pathways and thereby increases their resilience under oxidative stress. This higher level of oxidative stress also can be exploited to kill tumor cells while leaving normal cells intact. In this study we have found that isovalerylspiramycin I (ISP I), a novel macrolide antibiotic, suppresses cancer cell growth and tumor metastases by targeting the nucleolar protein selenoprotein H (SELH), which plays critical roles in keeping redox homeostasis and genome stability in cancer cells. Methods We developed ISP I through genetic recombination and tested the antitumor effects using primary and metastatic cancer models. The drug target was identified using the drug affinity responsive target stability (DARTS) and mass spectrum assays. The effects of ISP I were assessed for reactive oxygen species (ROS) generation, DNA damage, R-loop formation and its impact on the JNK2/TIF-IA/RNA polymerase I (POLI) transcription pathway. Results ISP I suppresses cancer cell growth and tumor metastases by targeting SELH. Suppression of SELH induces accumulation of ROS and cancer cell-specific genomic instability. The accumulation of ROS in the nucleolus triggers nucleolar stress and blocks ribosomal RNA transcription via the JNK2/TIF-IA/POLI pathway, causing cell cycle arrest and apoptosis in cancer cells. Conclusions We demonstrated that ISP I links cancer cell vulnerability to oxidative stress and RNA biogenesis by targeting SELH. This suggests a potential new cancer treatment paradigm, in which the primary therapeutic agent has minimal side-effects and hence may be useful for long-term cancer chemoprevention.

Published
2021

44. Isovalerylspiramycin I suppresses non-small cell lung carcinoma growth through ROS-mediated inhibition of PI3K/AKT signaling pathway

Author

Zeyu Liu, Moli Huang, Yue Hong, Shaoyang Wang, Yongle Xu, Cheng Zhong, Jingyuan Zhang, Zhengping Zhuang, Shan Shan, and Tao Ren

Subjects
Lung Neoplasms, Apoptosis, Cell Biology, Applied Microbiology and Biotechnology, G2 Phase Cell Cycle Checkpoints, Phosphatidylinositol 3-Kinases, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, Carcinoma, Squamous Cell, Humans, Mouth Neoplasms, Reactive Oxygen Species, Molecular Biology, Proto-Oncogene Proteins c-akt, Ecology, Evolution, Behavior and Systematics, Developmental Biology, Cell Proliferation, Signal Transduction
Abstract

Novel drugs are required for non-small cell lung cancer (NSCLC) treatment urgently. Repurposing old drugs as new treatments is a practicable approach with time and cost savings. Some studies have shown that carrimycin, a Chinese Food and Drug Administration (CFDA)-approved macrolide antibiotic, possesses potent anti-tumor effects against oral squamous cell carcinoma. However, its detailed component and underlying mechanisms in anti-NSCLC remain unknown. In our study, isovalerylspiramycin I (ISP-I) was isolated from carrimycin and demonstrated a remarkable anti-NSCLC efficacy in vitro and in vivo with a favorable safety profile. It has been proven that in NSCLC cell lines H460 and A549, ISP-I could induce G2/M arrest and apoptosis, which was mainly attributed to ROS accumulation and subsequently PI3K/AKT signaling pathway inhibition. Numerous downstream genes including mTOR and FOXOs were also changed correspondingly. An observation of NAC-induced reverse effect on ISP-I-leading cell death and PI3K/AKT pathway inhibition, emphasized the necessity of ROS signaling in this event. Moreover, we identified ROS accumulation and PI3K/AKT pathway inhibition in tumor xenograft models in vivo as well. Taken together, our study firstly reveals that ISP-I is a novel ROS inducer and may act as a promising candidate with multi-target and low biological toxicity for anti-NSCLC treatment.

Published
2021

45. Tentorial venous anatomy of mice and humans

Author

John D. Heiss, Anthony J. Cappadona, Danielle R. Donahue, Jared S. Rosenblum, Jessa M Tunacao, Zhengping Zhuang, Jeeva Munasinghe, James G. Smirniotopoulos, Pashayar P. Lookian, Vibhu Chandrashekhar, Jean-Paul Bryant, and Vikram Chandrashekhar

Subjects
Plexus, medicine.diagnostic_test, business.industry, Bone development, Neuroimaging, Magnetic resonance imaging, Venous plexus, General Medicine, Anatomy, Development, Brain cancer, Tentorium, Veins, Mice, Murine embryo, Vascular Biology, medicine, Animals, Humans, Choroid plexus, business, Venous anatomy, Research Article
Abstract

We recently described a previously unknown trans-tentorial venous system (TTVS) connecting venous drainage throughout the brain in humans. Prior to this finding, it was believed that the embryologic tentorial plexus regresses, resulting in a largely avascular tentorium. Our finding contradicted this understanding and necessitated further investigation into the development of the newly described TTVS. Herein we sought to investigate mice as a model to study the development of this system. First, using vascular casting and ex vivo micro-computed tomography (micro-CT), we demonstrate that this TTVS is conserved in adult mice. Next, using high-resolution magnetic resonance imaging (MRI), we found the primitive tentorial venous plexus in murine embryo at day 14.5. We also found that, at this embryologic stage, the tentorial plexus drains the choroid plexus. Finally, using vascular casting and micro-CT, we found that the TTVS is the dominant venous drainage in the early postnatal period (P8). Herein, we demonstrate that the TTVS is conserved between mice and humans and present a longitudinal study of its development. In addition, our findings establish mice as a translational model for further study of this newly described system and its relationship to intracranial physiology.

Published
2021

46. MODL-42. ESTABLISHMENT AND CHARACTERIZATION OF A NOVEL MOUSE SYNGENEIC GLIOBLASTOMA CELL LINE

Author

Juan Ye, Herui Wang, Chunzhang Yang, and Zhengping Zhuang

Subjects
Cancer Research, Oncology, Neurology (clinical)
Abstract

Glioblastoma (GBM) is the most common and the deadliest type of brain tumor affecting the adult central nervous system, carrying a median survival of 14 months. In vivo syngeneic animal models of GBM that recapitulate human GBM are urgently needed to decipher glioma biology and develop novel therapeutics, including immunotherapy. Here, we generated a syngeneic mouse glioblastoma stem cell line (RCAS-TVA-GSC01) through repeated in-vitro passages of stem-like tumor cells isolated from the RCAS-TVA glioma mouse model, which overexpresses PDGFA and carries a homozygous deletion of Ink4a-Arf locus. We characterized this new GSC line both in vitro and in vivo. This cell line expresses stemness markers CD133 and Nestin, and is able to differentiate into astrocyte, neuron, and oligodendrocyte-like cells in 2% FBS differentiating medium with markers GFAP, β-III tubulin, and O4, respectively. Transcriptomic and genomic profiling of RCAS-TVA-GSC01 cells revealed molecular heterogeneity comparable to human glioblastoma. When intracranially transplanted into wild-type C57BL/6 mice, this cell line formed high-grade gliomas with a median survival time of 56.5 days. The differentiation potential and molecular heterogeneity make RCAS-TVA GSC01 line a unique and useful tool for studying multiple aspects of glioblastoma pathogenesis and a promising platform for testing new GBM therapeutics study, especially for immunotherapy that requires a syngeneic mouse model.

Published
2022

47. SMARCB1 deletion in atypical teratoid rhabdoid tumors results in human endogenous retrovirus K (HML-2) expression

Author

Lisa J. Henderson, Saeed Fathi, Wenxue Li, Tongguang Wang, Myoung Hwa Lee, Sariah Allen, Kory R. Johnson, Kevon Sampson, Zhengping Zhuang, Tara T. Doucet-O'Hare, Avindra Nath, Jared S. Rosenblum, Catherine DeMarino, Marta Garcia-Montojo, Abigail L Atkinson, Jeffrey A. Kowalak, Brianna DiSanza, Mariarita Santi, and Brent A. Orr

Subjects
Epigenomics, Neuroblastoma RAS viral oncogene homolog, Tumor suppressor gene, Science, Biology, medicine.disease_cause, Article, GTP Phosphohydrolases, Paediatric cancer, Small hairpin RNA, Cell-Derived Microparticles, Cell Line, Tumor, Genetics, Biomarkers, Tumor, medicine, Humans, Transcription factor, Rhabdoid Tumor, Cancer, Cell Proliferation, Repetitive Sequences, Nucleic Acid, Sequence Deletion, Multidisciplinary, Endogenous Retroviruses, Membrane Proteins, SMARCB1 Protein, medicine.disease, Cell Transformation, Neoplastic, Gene Expression Regulation, Atypical teratoid rhabdoid tumor, Cancer research, Medicine, Virus Activation, Disease Susceptibility, Stem cell, Carcinogenesis, Chromatin immunoprecipitation, Signal Transduction
Abstract

Atypical Teratoid Rhabdoid Tumor (AT/RT) is a rare pediatric central nervous system cancer often characterized by deletion or mutation of SMARCB1, a tumor suppressor gene. In this study, we found that SMARCB1 regulates Human Endogenous Retrovirus K (HERV-K, subtype HML-2) expression. HML-2 is a repetitive element scattered throughout the human genome, encoding several intact viral proteins that have been associated with stem cell maintenance and tumorigenesis. We found HML-2 env expression in both the intracellular and extracellular compartments in all AT/RT cell lines (n = 4) and in 95% of AT/RT patient tissues (n = 37) evaluated. SMARCB1 knock-down in neural stem cells (NSCs) led to an upregulation of HML-2 transcription. We found that SMARCB1 binds adjacent to the HML-2 promoter, repressing its transcription via chromatin immunoprecipitation; restoration of SMARCB1 expression in AT/RT cell lines significantly downregulated HML-2 expression. Further, targeted downregulation of HML-2 transcription via CRISPR-dCas9 coupled with suppressor proteins led to cellular dispersion, decreased proliferation, and cell death in vitro. HML-2 knock-down with shRNA, siRNA, and CRISPR-dCas9 significantly decreased Ras expression as measured by qRT-PCR, suggesting that HML-2 modulates MAPK/ERK signaling in AT/RT cells. Overexpression of NRAS was sufficient to restore cellular proliferation, and MYC, a transcription factor downstream of NRAS, was bound to the HERV-K LTR significantly more in the absence of SMARCB1 expression in AT/RT cells. We show a mechanism by which these undifferentiated tumors remain pluripotent, and we demonstrate that their formation is aided by aberrant HML-2 activation, which is dependent on SMARCB1 and its interaction with MYC.

Published
2021

48. Coley's immunotherapy revived: Innate immunity as a link in priming cancer cells for an attack by adaptive immunity

Author

Jan Zenka, Veronika Caisova, Zhengping Zhuang, Jan Kopecky, Jindrich Chmelar, Ondrej Uher, Per Hansen, and Karel Pacak

Subjects
0301 basic medicine, medicine.medical_treatment, Adaptive Immunity, Ligands, Article, Immunomodulation, 03 medical and health sciences, Antineoplastic Agents, Immunological, 0302 clinical medicine, Immune system, Phagocytosis, Neoplasms, Tumor Microenvironment, medicine, Animals, Humans, Innate immune system, biology, business.industry, Melanoma, Toll-Like Receptors, Hematology, Immunotherapy, medicine.disease, Acquired immune system, Combined Modality Therapy, Immunity, Innate, Treatment Outcome, 030104 developmental biology, Oncology, Immune System, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, biology.protein, Adenocarcinoma, Antibody, business
Abstract

There is no doubt that immunotherapy lies in the spotlight of current cancer research and clinical trials. However, there are still limitations in the treatment response in certain types of tumors largely due to the presence of the complex network of immunomodulatory and immunosuppressive pathways. These limitations are not likely to be overcome by current immunotherapeutic options, which often target isolated steps in immune pathways preferentially involved in adaptive immunity. Recently, we have developed an innovative anti-cancer immunotherapeutic strategy that initially elicits a strong innate immune response with subsequent activation of adaptive immunity in mouse models. Robust primary innate immune response against tumor cells is induced by toll-like receptor ligands and anti-CD40 agonistic antibodies combined with the phagocytosis-stimulating ligand mannan, anchored to a tumor cell membrane by biocompatible anchor for membrane. This immunotherapeutic approach results in a dramatic therapeutic response in large established murine subcutaneous tumors including melanoma, sarcoma, pancreatic adenocarcinoma, and pheochromocytoma. Additionally, eradication of metastases and/or long-lasting resistance to subsequent re-challenge with tumor cells was also accomplished. Current and future advantages of this immunotherapeutic approach and its possible combinations with other available therapies are discussed in this review.

Published
2019

49. Targeting hypoxia downstream signaling protein, CAIX, for CAR T-cell therapy against glioblastoma

Author

Yu Yao, Herui Wang, Chunxia Ji, Jared S. Rosenblum, Liemei Guo, Xiaoyu Cao, Dongqing Cao, Yang Wang, Zhengping Zhuang, Pauline Dmitriev, Kaiyong Yang, Mark R. Gilbert, Jing Cui, Qi Song, Iris H Indig, Qi Zhang, and Mitchell Sun

Subjects
Cancer Research, medicine.medical_treatment, Apoptosis, Mice, SCID, Immunotherapy, Adoptive, Mice, Lymphocytes, Tumor-Infiltrating, Antigen, Antigens, Neoplasm, Mice, Inbred NOD, In vivo, Biomarkers, Tumor, Tumor Cells, Cultured, Tumor Microenvironment, medicine, Animals, Humans, Interferon gamma, Carbonic Anhydrase IX, Cell Proliferation, Tumor-infiltrating lymphocytes, business.industry, Immunotherapy, Prognosis, Xenograft Model Antitumor Assays, Chimeric antigen receptor, Gene Expression Regulation, Neoplastic, Oncology, Basic and Translational Investigations, Cancer research, Chimeric Antigen Receptor T-Cell Therapy, Tumor necrosis factor alpha, Neurology (clinical), Glioblastoma, business, Signal Transduction, medicine.drug
Abstract

Background Glioblastoma survival remains unchanged despite continuing therapeutic innovation. Herein, we aim to (i) develop chimeric antigen receptor (CAR) T cells with a specificity to a unique antigen, carbonic anhydrase IX (CAIX), which is expressed in the hypoxic microenvironment characteristic of glioblastoma, and (ii) demonstrate its efficacy with limited off-target effects. Methods First we demonstrated expression of CAIX in patient-derived glioblastoma samples and available databases. CAR T cells were generated against CAIX and efficacy was assessed in 4 glioblastoma cell lines and 2 glioblastoma stem cell lines. Cytotoxicity of anti-CAIX CAR T cells was assessed via interferon gamma, tumor necrosis factor alpha, and interleukin-2 levels when co-cultured with tumor cells. Finally, we assessed efficacy of direct intratumoral injection of the anti-CAIX CAR T cells on an in vivo xenograft mouse model using the U251 luciferase cell line. Tumor infiltrating lymphocyte analyses were performed. Results We confirm that CAIX is highly expressed in glioblastoma from patients. We demonstrate that CAIX is a suitable target for CAR T-cell therapy using anti-CAIX CAR T cells against glioblastoma in vitro and in vivo. In our mouse model, a 20% cure rate was observed without detectable systemic effects. Conclusions By establishing the specificity of CAIX under hypoxic conditions in glioblastoma and highlighting its efficacy as a target for CAR T-cell therapy, our data suggest that anti-CAIX CAR T may be a promising strategy to treat glioblastoma. Direct intratumoral injection increases anti-CAIX CAR T-cell potency while limiting its off-target effects.

Published
2019

50. CHCHD10 is involved in the development of Parkinson's disease caused by CHCHD2 loss-of-function mutation p.T61I

Author

Yaohe Wang, Shuo Zhang, Huisha Xu, Zhengping Zhuang, Zhilei Wang, Chengyuan Mao, Xiang Wang, Shu-yu Zhang, Mibo Tang, Matthew J. Shepard, Changhe Shi, Qi Zhang, Haiyang Luo, Jared S. Rosenblum, Herui Wang, and Yuming Xu

Subjects
0301 basic medicine, Aging, Parkinson's disease, Mutant, Disease, Mitochondrion, Biology, Article, Mitochondrial Proteins, Loss of function mutation, 03 medical and health sciences, 0302 clinical medicine, Asian People, medicine, Humans, Genetic Association Studies, Messenger RNA, Mechanism (biology), General Neuroscience, Parkinson Disease, medicine.disease, Mitochondria, DNA-Binding Proteins, 030104 developmental biology, Mutation, Mutation (genetic algorithm), Cancer research, Neurology (clinical), Geriatrics and Gerontology, 030217 neurology & neurosurgery, Transcription Factors, Developmental Biology
Abstract

Previously we identified the p.Thr61Ile mutation in coiled-coil-helix-coiled-coil-helix domain containing 2 (CHCHD2) in a Chinese family with autosomal dominant Parkinson’s disease. But the mechanism is still unclear. In this study, we explored the effects of CHCHD2 p.Thr61Ile mutation in cells and its association with coiled-coil-helix-coiled-coil-helix domain containing 10 (CHCHD10). We found that overexpression of Parkinson’s disease–associated T61I mutant CHCHD2 did not produce mitochondrial dysfunction. Rather, its protective effect from stress was abrogated. And, the level of the CHCHD2 protein and mRNA in patient fibroblasts was not significantly different from control. In addition, CHCHD2 T61I mutation caused increased interaction with CHCHD10 and reduced CHCHD10 level. The mitochondrial ultrastructural alterations in CHCHD2 T61I mutant patient fibroblasts are similar to that of CHCHD10 mutations. We therefore propose that CHCHD10 is involved in the development of Parkinson’s disease caused by CHCHD2 loss-of-function mutation p.T61I.

Published
2019

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