Your search keyword '"G. Esteban Fernandez"' showing total 47 results

1. Prominin-1 promotes restitution of the murineMAQ:Editorial Office/AASLD: Please indicate if a visual abstract will be forthcoming for this article. extrahepatic biliary luminal epithelium following cholestatic liver injury

Author

Allen Zhong, Celia Short, Jiabo Xu, G. Esteban Fernandez, Nicolas Malkoff, Nicolas Noriega, Theresa Yeo, Larry Wang, Nirmala Mavila, Kinji Asahina, and Kasper S. Wang

Subjects

Diseases of the digestive system. Gastroenterology, RC799-869

Abstract

Background and Aims:. Restitution of the extrahepatic biliary luminal epithelium in cholangiopathies is poorly understood. Prominin-1 (Prom1) is a key component of epithelial ciliary body of stem/progenitor cells. Given that intrahepatic Prom1-expressing progenitor cells undergo cholangiocyte differentiation, we hypothesized that Prom1 may promote restitution of the extrahepatic bile duct (EHBD) epithelium following injury. Approach and Results:. Utilizing various murine biliary injury models, we identified Prom1-expressing cells in the peribiliary glands of the EHBD. These Prom1-expressing cells are progenitor cells which give rise to cholangiocytes as part of the normal maintenance of the EHBD epithelium. Following injury, these cells proliferate significantly more rapidly to re-populate the biliary luminal epithelium. Null mutation of Prom1 leads to significantly >10-fold dilated peribiliary glands following rhesus rotavirus–mediated biliary injury. Cultured organoids derived from Prom1 knockout mice are comprised of biliary progenitor cells with altered apical-basal cellular polarity, significantly fewer and shorter cilia, and decreased organoid proliferation dynamics consistent with impaired cell motility. Conclusions:. We, therefore, conclude that Prom1 is involved in biliary epithelial restitution following biliary injury in part through its role in supporting cell polarity.

Published

2023

2. Fibroblasts and macrophages cooperate to create a pro-tumorigenic and immune resistant environment via activation of TGF-β/IL-6 pathway in neuroblastoma

Author

Kevin Louault, Tania Porras, Meng-Hua Lee, Sakunthala Muthugounder, Rebekah J. Kennedy, Laurence Blavier, Emily Sarte, G. Esteban Fernandez, Fusheng Yang, Bruce R. Pawel, Hiroyuki Shimada, Shahab Asgharzadeh, and Yves A. DeClerck

Subjects

tumor microenvironment, neuroblastoma, cancer-associated fibroblasts, tumor-associated macrophages, mesenchymal stromal cells, cytokines/chemokines, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Tumor-associated macrophages (TAM) and cancer-associated fibroblasts (CAF) and their precursor mesenchymal stromal cells (MSC) are often detected together in tumors, but how they cooperate is not well understood. Here, we show that TAM and CAF are the most abundant nonmalignant cells and are present together in untreated human neuroblastoma (NB) tumors that are also poorly infiltrated with T and natural killer (NK) cells. We then show that MSC and CAF-MSC harvested from NB tumors protected human monocytes (MN) from spontaneous apoptosis in an interleukin (IL)-6 dependent mechanism. The interactions of MN and MSC with NB cells resulted in a significant induction or increase in the expression of several pro-tumorigenic cytokines/chemokines (TGF-β1, MCP-1, IL-6, IL-8, and IL-4) but not of anti-tumorigenic cytokines (TNF-α, IL-12) by MN or MSC, while also inducing cytokine expression in quiescent NB cells. We then identified a TGF-β1/IL-6 pathway where TGF-β1 stimulated the expression of IL-6 in NB cells and MSC, promoting TAM survival. Evidence for the contribution of TAM and MSC to the activation of this pathway was then provided in xenotransplanted NB tumors and patients with primary tumors by demonstrating a direct correlation between the presence of CAF and p-SMAD2 and p-STAT3. The data highlight a new mechanism of interaction between TAM and CAF supporting their pro-tumorigenic function in cancer.

Published

2022

3. Combined immune checkpoint blockade increases CD8+CD28+PD-1+ effector T cells and provides a therapeutic strategy for patients with neuroblastoma

Author

Soheila Shirinbak, Randall Y. Chan, Shilpa Shahani, Sakunthala Muthugounder, Rebekah Kennedy, Long T. Hung, G. Esteban Fernandez, Michael D. Hadjidaniel, Babak Moghimi, Michael A. Sheard, Alan L. Epstein, Muller Fabbri, Hiroyuki Shimada, and Shahab Asgharzadeh

Subjects

neuroblastoma, immune checkpoint therapy, tumor microenvironment, dual immune checkpoint therapy, tumor-associated macrophages, Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Immune checkpoint therapy has resulted in minimal clinical response in many pediatric cancers. We sought to understand the influence of immune checkpoint inhibition using anti-PD-1 and anti-CTLA-4 antibodies individually, in combination, and after chemotherapy on immune responses in minimal and established murine neuroblastoma models. We also sought to understand the role of the tumor microenvironment (TME) and PD-L1 expression and their alteration post-chemotherapy in our models and human tissues. PD-L1 expression was enriched in human tumor-associated macrophages and up-regulated after chemotherapy. In a murine minimal disease model, single and dual immune checkpoint blockade promoted tumor rejection, improved survival, and established immune memory with long-term anti-tumor immunity against re-challenge. In an established tumor model, only dual immune checkpoint blockade showed efficacy. Interestingly, dual immune checkpoint therapy distinctly influenced adaptive and innate immune responses, with significant increase in CD8+CD28+PD-1+ T cells and inflammatory macrophages (CD11bhiCD11c−F4/80+Ly6Chi) in tumor-draining lymph nodes. Adding chemotherapy before immunotherapy provided significant survival benefit for mice with established tumors receiving anti-PD-1 or dual immune checkpoint blockade. Our findings demonstrate anti-PD-1 and anti-CTLA-4 therapy induces a novel subset of effector T cells, and support administration of induction chemotherapy immediately prior to immune checkpoint blockade in children with high-risk neuroblastoma.

Published

2021

4. SERCA directs cell migration and branching across species and germ layers

Author

Danielle V. Bower, Nick Lansdale, Sonia Navarro, Thai V. Truong, Dan J. Bower, Neil C. Featherstone, Marilyn G. Connell, Denise Al Alam, Mark R. Frey, Le A. Trinh, G. Esteban Fernandez, David Warburton, Scott E. Fraser, Daimark Bennett, and Edwin C. Jesudason

Subjects

Branching morphogenesis, Cell migration, SERCA, Calcium dynamics, Science, Biology (General), QH301-705.5

Abstract

Branching morphogenesis underlies organogenesis in vertebrates and invertebrates, yet is incompletely understood. Here, we show that the sarco-endoplasmic reticulum Ca2+ reuptake pump (SERCA) directs budding across germ layers and species. Clonal knockdown demonstrated a cell-autonomous role for SERCA in Drosophila air sac budding. Live imaging of Drosophila tracheogenesis revealed elevated Ca2+ levels in migratory tip cells as they form branches. SERCA blockade abolished this Ca2+ differential, aborting both cell migration and new branching. Activating protein kinase C (PKC) rescued Ca2+ in tip cells and restored cell migration and branching. Likewise, inhibiting SERCA abolished mammalian epithelial budding, PKC activation rescued budding, while morphogens did not. Mesoderm (zebrafish angiogenesis) and ectoderm (Drosophila nervous system) behaved similarly, suggesting a conserved requirement for cell-autonomous Ca2+ signaling, established by SERCA, in iterative budding.

Published

2017

5. PID1 increases chemotherapy-induced apoptosis in medulloblastoma and glioblastoma cells in a manner that involves NFκB

Author

Jingying Xu, Xiuhai Ren, Anup Singh Pathania, G. Esteban Fernandez, Anthony Tran, Yifu Zhang, Rex A. Moats, Gregory M. Shackleford, and Anat Erdreich-Epstein

Subjects

Medicine, Science

Abstract

Abstract Phosphotyrosine Interaction Domain containing 1 (PID1; NYGGF4) inhibits growth of medulloblastoma, glioblastoma and atypical teratoid rhabdoid tumor cell lines. PID1 tumor mRNA levels are highly correlated with longer survival in medulloblastoma and glioma patients, suggesting their tumors may have been more sensitive to therapy. We hypothesized that PID1 sensitizes brain tumors to therapy. We found that PID1 increased the apoptosis induced by cisplatin and etoposide in medulloblastoma and glioblastoma cell lines. PID1 siRNA diminished cisplatin-induced apoptosis, suggesting that PID1 is required for cisplatin-induced apoptosis. Etoposide and cisplatin increased NFκB promoter reporter activity and etoposide induced nuclear translocation of NFκB. Etoposide also increased PID1 promoter reporter activity, PID1 mRNA, and PID1 protein, which were diminished by NFκB inhibitors JSH-23 and Bay117082. However, while cisplatin increased PID1 mRNA, it decreased PID1 protein. This decrease in PID1 protein was mitigated by the proteasome inhibitor, bortezomib, suggesting that cisplatin induced proteasome dependent degradation of PID1. These data demonstrate for the first time that etoposide- and cisplatin-induced apoptosis in medulloblastoma and glioblastoma cell lines is mediated in part by PID1, involves NFκB, and may be regulated by proteasomal degradation. This suggests that PID1 may contribute to responsiveness to chemotherapy.

Published

2017

6. Plasminogen Activator Inhibitor-1 Promotes the Recruitment and Polarization of Macrophages in Cancer

Author

Marta Helena Kubala, Vasu Punj, Veronica Rae Placencio-Hickok, Hua Fang, G. Esteban Fernandez, Richard Sposto, and Yves Albert DeClerck

Subjects

Biology (General), QH301-705.5

Abstract

Summary: Plasminogen activator inhibitor-1 (PAI-1) has a pro-tumorigenic function via its pro-angiogenic and anti-apoptotic activities. Here, we demonstrate that PAI-1 promotes the recruitment and M2 polarization of monocytes/macrophages through different structural domains. Its LRP1 interacting domain regulated macrophage migration, while its C-terminal uPA interacting domain promoted M2 macrophage polarization through activation of p38MAPK and nuclear factor κB (NF-κB) and induction of an autocrine interleukin (IL)-6/STAT3 activation pathway. We then show in several experiments in mice that expression of PAI-1 is associated with increased tumorigenicity, increased presence of M2 macrophages, higher levels of IL-6, and increased STAT3 phosphorylation in macrophages. Strong positive correlations between PAI-1, IL-6, and CD163 (M2 marker) expression were also found by meta-analysis of transcriptome data in many human cancers. Altogether, these data provide evidence for a mechanism explaining the paradoxical pro-tumorigenic function of PAI-1 in cancer. : The serine protease inhibitor plasminogen activator inhibitor-1 (PAI-1) has a paradoxical pro-angiogenic and protective effect on cancer cells. Kubala et al. provide evidence for a third pro-tumorigenic function by demonstrating that PAI-1 promotes recruitment and polarization toward a pro-tumorigenic phenotype of tumor-associated macrophages. Keywords: plasminogen activator inhibitor-1, PAI-1, tumor-associated macrophages, M2 polarization, interleukin 6, STAT3, tumor microenvironment

Published

2018

7. Contribution of neuroblastoma-derived exosomes to the production of pro-tumorigenic signals by bone marrow mesenchymal stromal cells

Author

Rie Nakata, Hiroyuki Shimada, G. Esteban Fernandez, Rob Fanter, Muller Fabbri, Jemily Malvar, Pascale Zimmermann, and Yves A. DeClerck

Subjects

Exosomes, mesenchymal stromal cells, cell–cell interaction, extracellular vesicles, extracellular-signal-regulated kinase, neuroblastoma, Cytology, QH573-671

Abstract

The bone marrow (BM) niche is a microenvironment promoting survival, dormancy and therapeutic resistance in tumor cells. Central to this function are mesenchymal stromal cells (MSCs). Here, using neuroblastoma (NB) as a model, we demonstrate that NB cells release an extracellular vesicle (EVs) whose protein cargo is enriched in exosomal proteins but lacks cytokines and chemokines. Using three different purification methods, we then demonstrate that NB-derived exosomes were captured by MSCs and induced the production of pro-tumorigenic cytokines and chemokines, including interleukin-6 (IL-6), IL-8/CXCL8, vascular endothelial cell growth factor and monocyte-chemotactic protein-1, with exosomes prepared by size exclusion chromatography having the highest activity. We found no correlation between the IL-6 and IL-8/CXCL8 stimulatory activity of exosomes from eight NB cell lines and their origin, degree of MYCN amplification, drug resistance and disease status. We then demonstrate that the uptake of NB exosomes by MSCs was associated with a rapid increase in ERK1/2 and AKT activation, and that blocking ERK1/2 but not AKT activation inhibited the IL-6 and IL-8/CXCL8 production by MSCs without affecting exosome uptake. Thus, we describe a new mechanism by which NB cells induce in MSCs an inflammatory reaction that contributes to a favorable microenvironment in the BM.

Published

2017

8. Supplementary Figure S2. from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

CAF isolated from patients with NB share characteristics with MSC.

Published

2023

9. Supplementary Figure 6 from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

Cytokines and chemokines not up-regulated by NB-MSC interaction and lack of inhibition of STAT3 activation by anti-IL-6/IL-6R

Published

2023

10. Supplementary Tables from Anti-CD105 Antibody Eliminates Tumor Microenvironment Cells and Enhances Anti-GD2 Antibody Immunotherapy of Neuroblastoma with Activated Natural Killer Cells

Author

Robert C. Seeger, Richard Sposto, Charles P. Theuer, Hiroyuki Shimada, Laurence Blavier, Yves A. DeClerck, G. Esteban Fernandez, Jemily Malvar, Michael A. Sheard, and Hong-Wei Wu

Abstract

Supplementary Tables

Published

2023

11. Table A and B from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

A: List of antibodies used in the study B: Clinical characteristics of patients from which CAF-MSC and BM-MSC were isolated.

Published

2023

12. permission letter from Anti-CD105 Antibody Eliminates Tumor Microenvironment Cells and Enhances Anti-GD2 Antibody Immunotherapy of Neuroblastoma with Activated Natural Killer Cells

Author

Robert C. Seeger, Richard Sposto, Charles P. Theuer, Hiroyuki Shimada, Laurence Blavier, Yves A. DeClerck, G. Esteban Fernandez, Jemily Malvar, Michael A. Sheard, and Hong-Wei Wu

Abstract

Permission letter regarding inclusion of information of CHLA-255 C-Myc over-expression

Published

2023

13. Data from Anti-CD105 Antibody Eliminates Tumor Microenvironment Cells and Enhances Anti-GD2 Antibody Immunotherapy of Neuroblastoma with Activated Natural Killer Cells

Author

Robert C. Seeger, Richard Sposto, Charles P. Theuer, Hiroyuki Shimada, Laurence Blavier, Yves A. DeClerck, G. Esteban Fernandez, Jemily Malvar, Michael A. Sheard, and Hong-Wei Wu

Abstract

Purpose:We determined whether elimination of CD105+ cells in the tumor microenvironment (TME) with anti-CD105 antibodies enhanced anti-disialoganglioside (GD2) antibody dinutuximab therapy of neuroblastoma when combined with activated natural killer (aNK) cells.Experimental Design:The effect of MSCs and monocytes on antibody-dependent cellular cytotoxicity (ADCC) mediated by dinutuximab with aNK cells against neuroblastoma cells was determined in vitro. ADCC with anti-CD105 mAb TRC105 and aNK cells against MSCs, monocytes, and endothelial cells, which express CD105, was evaluated. Anti-neuroblastoma activity in immunodeficient NSG mice of dinutuximab with aNK cells without or with anti-CD105 mAbs was determined using neuroblastoma cell lines and a patient-derived xenograft.Results:ADCC mediated by dinutuximab with aNK cells against neuroblastoma cells in vitro was suppressed by addition of MSCs and monocytes, and dinutuximab with aNK cells was less effective against neuroblastomas formed with coinjected MSCs and monocytes in NSG mice than against those formed by tumor cells alone. Anti-CD105 antibody TRC105 with aNK cells mediated ADCC against MSCs, monocytes, and endothelial cells. Neuroblastomas formed in NSG mice by two neuroblastoma cell lines or a patient-derived xenograft coinjected with MSCs and monocytes were most effectively treated with dinutuximab and aNK cells when anti-human (TRC105) and anti-mouse (M1043) CD105 antibodies were added, which depleted human MSCs and murine endothelial cells and macrophages from the TME.Conclusions:Immunotherapy of neuroblastoma with anti-GD2 antibody dinutuximab and aNK cells is suppressed by CD105+ cells in the TME, but suppression is overcome by adding anti-CD105 antibodies to eliminate CD105+ cells.

Published

2023

14. Supplementary Figure 4 from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

CAF-MSC and BM-MSC enhance cell viability of NB cells in vitro and protect tumor cells from drug-induced apoptosis in vitro.

Published

2023

15. Supplementary Fig. 1-8 from Anti-CD105 Antibody Eliminates Tumor Microenvironment Cells and Enhances Anti-GD2 Antibody Immunotherapy of Neuroblastoma with Activated Natural Killer Cells

Author

Robert C. Seeger, Richard Sposto, Charles P. Theuer, Hiroyuki Shimada, Laurence Blavier, Yves A. DeClerck, G. Esteban Fernandez, Jemily Malvar, Michael A. Sheard, and Hong-Wei Wu

Abstract

Targeting CD105+ Microenvironment cells enhances immunotherpy of Dinutuxmab with aNK cells against neuroblastoma

Published

2023

16. Supplementary Figure 5 from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

CAF-MSC and BM-MSC induce activation of STAT3 and ERK1/2 signaling in NB cells

Published

2023

17. Data from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

Cancer-associated fibroblasts (CAF) have been suggested to originate from mesenchymal stromal cells (MSC), but their relationship with MSCs is not clear. Here, we have isolated from primary human neuroblastoma tumors a population of αFAP- and FSP-1–expressing CAFs that share phenotypic and functional characteristics with bone marrow–derived MSCs (BM-MSC). Analysis of human neuroblastoma tumors also confirmed the presence of αFAP- and FSP-1–positive cells in the tumor stroma, and their presence correlated with that of M2 tumor-associated macrophages. These cells (designated CAF-MSCs) enhanced in vitro neuroblastoma cell proliferation, survival, and resistance to chemotherapy and stimulated neuroblastoma tumor engraftment and growth in immunodeficient mice, indicating an effect independent of the immune system. The protumorigenic activity of MSCs in vitro and in xenografted mice was dependent on the coactivation of JAK2/STAT3 and MEK/ERK1/2 in neuroblastoma cells. In a mouse model of orthotopically implanted neuroblastoma cells, inhibition of JAK2/STAT3 and MEK/ERK/1/2 by ruxolitinib and trametinib potentiated tumor response to etoposide and increased overall survival. These data point to a new type of protumorigenic CAF in the tumor microenvironment of neuroblastoma and to STAT3 and ERK1/2 as mediators of their activity. Cancer Res; 77(18); 5142–57. ©2017 AACR.

Published

2023

18. Supplementary Figure 7 from Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Robert C. Seeger, Shahab Asgharzadeh, Hiroyuki Shimada, Laurence Blavier, Jemily Malvar, Richard Sposto, G. Esteban Fernandez, Michael A. Sheard, Rie Nakata, and Lucia Borriello

Abstract

Combination of ruxolitinib and trametinib inhibits the growth of subcutaneous NB tumors, cell proliferation and STAT3 and ERK1/2 activation in vivo.

Published

2023

19. Data from MYCN-Dependent Expression of Sulfatase-2 Regulates Neuroblastoma Cell Survival

Author

Yves A. DeClerck, Jeremy E. Turnbull, Edwin A. Yates, Shahab Asgharzadeh, G. Esteban Fernandez, Richard Sposto, Hiroyuki Shimada, Gianluca Turcatel, Lucia Borriello, and Valeria Solari

Abstract

Heparan sulfate proteoglycans (HSPG) play a critical role in the interaction of tumor cells and their microenvironment. HSPG activity is dictated by sulfation patterns controlled by sulfotransferases, which add sulfate groups, and sulfatases (Sulf), which remove 6-O-sulfates. Here, we report altered expression of these enzymes in human neuroblastoma cells with higher levels of Sulf-2 expression, a specific feature of MYCN-amplified cells (MYCN-A cells) that represent a particularly aggressive subclass. Sulf-2 overexpression in neuroblastoma cells lacking MYCN amplification (MYCN-NA cells) increased their in vitro survival. Mechanistic investigations revealed evidence of a link between Sulf-2 expression and MYCN pathogenicity in vitro and in vivo. Analysis of Sulf-2 protein expression in 65 human neuroblastoma tumors demonstrated a higher level of Sulf-2 expression in MYCN-A tumors than in MYCN-NA tumors. In two different patient cohorts, we confirmed the association in expression patterns of Sulf-2 and MYCN and determined that Sulf-2 overexpression predicted poor outcomes in a nonindependent manner with MYCN. Our findings define Sulf-2 as a novel positive regulator of neuroblastoma pathogenicity that contributes to MYCN oncogenicity. Cancer Res; 74(21); 5999–6009. ©2014 AACR.

Published

2023

20. Supplemental Figure 1 from MYCN-Dependent Expression of Sulfatase-2 Regulates Neuroblastoma Cell Survival

Author

Yves A. DeClerck, Jeremy E. Turnbull, Edwin A. Yates, Shahab Asgharzadeh, G. Esteban Fernandez, Richard Sposto, Hiroyuki Shimada, Gianluca Turcatel, Lucia Borriello, and Valeria Solari

Abstract

Analysis of enzyme expression in other non -neuroblastoma cell lines.

Published

2023

21. Supplemental Figure 2 from MYCN-Dependent Expression of Sulfatase-2 Regulates Neuroblastoma Cell Survival

Author

Yves A. DeClerck, Jeremy E. Turnbull, Edwin A. Yates, Shahab Asgharzadeh, G. Esteban Fernandez, Richard Sposto, Hiroyuki Shimada, Gianluca Turcatel, Lucia Borriello, and Valeria Solari

Abstract

Negative control for figure 2.

Published

2023

22. Supplementary Table 1 from MYCN-Dependent Expression of Sulfatase-2 Regulates Neuroblastoma Cell Survival

Author

Yves A. DeClerck, Jeremy E. Turnbull, Edwin A. Yates, Shahab Asgharzadeh, G. Esteban Fernandez, Richard Sposto, Hiroyuki Shimada, Gianluca Turcatel, Lucia Borriello, and Valeria Solari

Abstract

Sequences of primers used for RT-PCR.

Published

2023

23. Individual red blood cell nitric oxide production in sickle cell anemia: Nitric oxide production is increased and sickle shaped cells have unique morphologic change compared to discoid cells

Author

Matthew Borzage, Pinar Ulker, Silvie Suriany, Jon A Detterich, Rosalinda B. Wenby, Richard Sposto, Herbert J. Meiselman, Honglei Liu, Iris Xu, Thomas D. Coates, Henry Jay Forman, and G. Esteban Fernandez

Subjects

0301 basic medicine, Basal rate, Erythrocytes, Anemia, Sickle Cell, Nitric Oxide, Biochemistry, Nitric oxide, Andrology, 03 medical and health sciences, chemistry.chemical_compound, Basal (phylogenetics), 0302 clinical medicine, Erythrocyte Deformability, Physiology (medical), medicine, Humans, Deoxygenated Hemoglobin, biology, Microcirculation, hemic and immune systems, medicine.disease, Sickle cell anemia, Nitric oxide synthase, Red blood cell, 030104 developmental biology, medicine.anatomical_structure, chemistry, biology.protein, Hemoglobin, 030217 neurology & neurosurgery, circulatory and respiratory physiology

Abstract

Sickle cell anemia (SCA) is characterized by decreased red blood cell (RBC) deformability due to polymerization of deoxygenated hemoglobin, leading to abnormal mechanical properties of RBC, increased cellular adhesion, and microcirculatory obstruction. Prior work has demonstrated that NO• influences RBC hydration and deformability and is produced at a basal rate that increases under shear stress in normal RBC. Nevertheless, the origin and physiological relevance of nitric oxide (NO•) production and scavenging in RBC remains unclear. We aimed to assess the basal and shear-mediated production of NO• in RBC from SCA patients and control (CTRL) subjects. RBCs loaded with a fluorescent NO• detector, DAF-FM (4-Amino-5-methylamino- 2',7'-difluorofluorescein diacetate), were imaged in microflow channels over 30-min without shear stress, followed by a 30-min period under 0.5Pa shear stress. We utilized non-specific nitric oxide synthase (NOS) blockade and carbon monoxide (CO) saturation of hemoglobin to assess the contribution of NOS and hemoglobin, respectively, to NO• production. Quantification of DAF-FM fluorescence intensity in individual RBC showed an increase in NO• in SCA RBC at the start of the basal period; however, both SCA and CTRL RBC increased NO• by a similar quantity under shear. A subpopulation of sickle-shaped RBC exhibited lower basal NO• production compared to discoid RBC from SCA group, and under shear became more circular in the direction of shear when compared to discoid RBC from SCA and CTRL, which elongated. Both CO and NOS inhibition caused a decrease in basal NO• production. Shear-mediated NO• production was decreased by CO in all RBC, but was decreased by NOS blockade only in SCA. In conclusion, total NO• production is increased and shear-mediated NO• production is preserved in SCA RBC in a NOS-dependent manner. Sickle shaped RBC with inclusions have higher NO• production and they become more circular rather than elongated with shear.

Published

2021

24. An immature, dedifferentiated, and lineage-deconstrained cone precursor origin of N-Myc–initiated retinoblastoma

Author

Hardeep P. Singh, Dominic W. H. Shayler, G. Esteban Fernandez, Matthew E. Thornton, Cheryl Mae Craft, Brendan H. Grubbs, and David Cobrinik

Subjects

N-Myc Proto-Oncogene Protein, Multidisciplinary, Carcinogenesis, Retinal Neoplasms, Cell Cycle, Retinal Cone Photoreceptor Cells, Retinoblastoma, Humans

Abstract

Most retinoblastomas develop from maturing cone precursors in response to biallelic RB1 loss and are dependent on cone maturation-related signaling. Additionally, ∼2% lack RB1 mutations but have MYCN amplification ( MYCN A ), N-Myc protein overexpression, and more rapid and invasive growth, yet the MYCN A retinoblastoma cell of origin and basis for its responses to deregulated N-Myc are unknown. Here, using explanted cultured retinae, we show that ectopic N-Myc induces cell cycle entry in cells expressing markers of several retinal types yet induces continuous proliferation and tumorigenesis only in cone precursors. Unlike the response to RB1 loss, both immature cone arrestin-negative (ARR3 – ) and maturing ARR3 + cone precursors proliferate, and maturing cone precursors rapidly dedifferentiate, losing ARR3 as well as L/M-opsin expression. N-Myc–overexpressing retinal cells also lose cell lineage constraints, occasionally coexpressing the cone-specific RXRγ with the rod-specific NRL or amacrine-specific AP2α and widely coexpressing RXRγ with the progenitor and Müller cell–specific SOX9 and retinal ganglion cell-specific BRN3 and GAP43. Mechanistically, N-Myc induced Cyclin D2 and CDK4 overexpression, pRB phosphorylation, and SOX9-dependent proliferation without a retinoma-like stage that characterizes pRB-deficient retinoblastoma, despite continuous p16 INK4A expression. Orthotopic xenografts of N-Myc–overexpressing retinal cells formed tumors with retinal cell marker expression similar to those in MYCN -transduced retinae and MYCN A retinoblastomas in patients. These findings demonstrate the MYCN A retinoblastoma origin from immature and lineage-deconstrained cone precursors, reveal their opportunistic use of an undifferentiated retinal progenitor cell feature, and illustrate that different cancer-initiating mutations cooperate with distinct developmental stage–specific cell signaling circuitries to drive retinoblastoma tumorigenesis.

Published

2022

25. Characterization and staging of outer plexiform layer development in human retina and retinal organoids

Author

David Cobrinik, Angela Ferrario, Jennifer G. Aparicio, Sumitha Prameela Bharathan, G. Esteban Fernandez, Brendan H. Grubbs, Matthew E. Thornton, Carolyn Marks, Kayla Stepanian, Mark W. Reid, Justin S. Kim, Chloe Hutchens, Narine Harutyunyan, and Aaron Nagiel

Subjects

Retina, Human Development, Human Embryonic Stem Cells, Induced Pluripotent Stem Cells, Synaptogenesis, Outer plexiform layer, Retinal, Ribbon synapse, Biology, Protein subcellular localization prediction, Embryonic stem cell, Cell Line, Cell biology, Organoids, stomatognathic diseases, chemistry.chemical_compound, medicine.anatomical_structure, chemistry, medicine, Humans, sense organs, Induced pluripotent stem cell, Molecular Biology, Developmental Biology

Abstract

The development of the first synapse of the visual system between photoreceptors and bipolar cells in the outer plexiform layer (OPL) of the human retina is crucial for visual processing but poorly understood. By studying the maturation state and spatial organization of photoreceptors, depolarizing bipolar cells and horizontal cells in the human fetal retina, we establish a pseudo-temporal staging system for OPL development that we term OPL-Stages 0 to 4. This was validated through quantification of increasingly precise subcellular localization of bassoon to the OPL with each stage (P

Published

2021

26. Extended culture and imaging of normal and regenerating adult zebrafish hearts in a fluidic device

Author

Ching-Ling Lien, Andrew P. Petersen, Michael R. Harrison, G. Esteban Fernandez, Jessi Villafuerte, Joycelyn K. Yip, and Megan L. McCain

Subjects

Biomedical Engineering, Bioengineering, Human myocardium, Biochemistry, Article, Tissue Culture Techniques, 03 medical and health sciences, 0302 clinical medicine, In vivo, Live cell imaging, Lab-On-A-Chip Devices, Animals, Zebrafish, 030304 developmental biology, 0303 health sciences, biology, Regeneration (biology), Heart, General Chemistry, biology.organism_classification, Cell biology, Cardiac repair, Perfusion, 030217 neurology & neurosurgery, Ex vivo

Abstract

Myocardial infarction and heart failure are leading causes of death worldwide, in large part because adult human myocardium has extremely limited regeneration capacity. Zebrafish are a powerful model for identifying new strategies for human cardiac repair because their hearts regenerate after relatively severe injuries. Zebrafish are also relatively scalable and compatible with many genetic tools. However, characterizing the regeneration process in live adult zebrafish hearts has proved challenging because adult fish are opaque, preventing live imaging in vivo. An alternative strategy is to explant and culture intact adult zebrafish hearts and investigate them ex vivo. However, explanted hearts maintained in conventional culture conditions experience rapid declines in morphology and physiology. To overcome these limitations, we designed and fabricated a fluidic device for culturing explanted adult zebrafish hearts with constant media perfusion that is also compatible with live imaging. We then compared the morphology and calcium activity of hearts cultured in the device, hearts cultured statically in dishes, and freshly explanted hearts. After one week of culture, hearts in the device experienced significantly less morphological degradation compared to hearts cultured in dishes. Hearts cultured in devices for one week also maintained capture rates similar to fresh hearts, unlike hearts cultured in dishes. We then cultured explanted injured hearts in the device and used live imaging techniques to continuously record the myocardial revascularization process over several days, demonstrating how our device is compatible with long-term live imaging and thereby enables unprecedented visual access to the multi-day process of adult zebrafish heart regeneration.

Published

2020

27. In Vivo Clonal Analysis of Cardiomyocytes

Author

Tzung K. Hsiai, Yichen Ding, Ngoc B. Nguyen, Reza Ardehali, and G. Esteban Fernandez

Subjects

0301 basic medicine, Regulation of gene expression, Cell type, Tissue clearing, Cell growth, Cell, Clone (cell biology), Biology, Clonal analysis, Cell biology, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, In vivo, medicine, 030217 neurology & neurosurgery

Abstract

The development of the CreER/LoxP system has enabled temporal control and cell type specificity of gene activation or repression. A common application of this system involves lineage tracing and examining the proliferative capacity of cells of interest through clonal analysis. Here, we describe a method of performing 2- and 3-dimensional clonal analysis of cardiomyocytes (CMs) using the Rainbow reporter mouse model. We outline the process of using the Cell Counter plug-in tool in ImageJ to quantify the number of clones as well as the number of cells within each clone. For 3-dimensional analysis, we describe the tissue clearing technique, CLARITY, in conjunction with light-sheet imaging to obtain digital slices of the whole heart that can be reconstructed and clone volumes quantified using the Imaris software.

Published

2020

28. In Vivo Clonal Analysis of Cardiomyocytes

Author

Ngoc B, Nguyen, G Esteban, Fernandez, Yichen, Ding, Tzung, Hsiai, and Reza, Ardehali

Subjects

Pluripotent Stem Cells, Disease Models, Animal, Mice, Genes, Reporter, Animals, Regeneration, Cell Differentiation, Cell Lineage, Myocytes, Cardiac, Cell Separation, Clone Cells

Abstract

The development of the CreER/LoxP system has enabled temporal control and cell type specificity of gene activation or repression. A common application of this system involves lineage tracing and examining the proliferative capacity of cells of interest through clonal analysis. Here, we describe a method of performing 2- and 3-dimensional clonal analysis of cardiomyocytes (CMs) using the Rainbow reporter mouse model. We outline the process of using the Cell Counter plug-in tool in ImageJ to quantify the number of clones as well as the number of cells within each clone. For 3-dimensional analysis, we describe the tissue clearing technique, CLARITY, in conjunction with light-sheet imaging to obtain digital slices of the whole heart that can be reconstructed and clone volumes quantified using the Imaris software.

Published

2020

29. Ub-1 Optical Clearing of the Murine Liver v1

Author

Michelle A Hough, Michael Fenlon, Alison Glazier, Celia Short, G. Esteban Fernandez, Jiabo Xu, Elaa Mahdi, Kinji Asahina, and Kasper Wang

Abstract

We report a urea-amino sugar clearing reagent for the murine liver that rapidly renders the tissue clear with preservation of native architecture, fluorescent proteins and lipophilic dyes. Optical clearing protocols for three-dimensional (3D) imaging, such as confocal or light sheet microscopy, can consist of several steps and solutions, complex apparatuses, or days to weeks for whole-organ clearing. Established protocols that demonstrate efficient clearing can unfortunately quench endogenous proteins, whereas some methods formulated to preserve protein fluorophores can be underwhelming in clearing capability. Many clearing methods have been optimized for neural tissue, with little described for the liver. Our method, a single step modified protocol of the UbasM protocol created by Chen et al., uses Ub-1 to clear the murine liver with only 24 hours incubation and one simple solution. We additionally describe a technique for labeling the murine intrahepatic biliary tree and vasculature. Our methods can benefit investigations of tissue composition and structural relationships in 3D.

Published

2020

30. Cancer-Associated Fibroblasts Share Characteristics and Protumorigenic Activity with Mesenchymal Stromal Cells

Author

Yves A. DeClerck, Hiroyuki Shimada, Rie Nakata, Lucia Borriello, G. Esteban Fernandez, Robert C. Seeger, Michael A. Sheard, Shahab Asgharzadeh, Laurence Blavier, Richard Sposto, and Jemily Malvar

Subjects

Male, 0301 basic medicine, MAPK/ERK pathway, Cancer Research, Pathology, MAP Kinase Kinase 1, Apoptosis, Mice, SCID, Mice, Neuroblastoma, 0302 clinical medicine, Cancer-Associated Fibroblasts, Mice, Inbred NOD, Tumor Cells, Cultured, Tumor Microenvironment, Mitogen-Activated Protein Kinase 1, Trametinib, education.field_of_study, Mitogen-Activated Protein Kinase 3, Cell Differentiation, Gene Expression Regulation, Neoplastic, Oncology, 030220 oncology & carcinogenesis, Female, STAT3 Transcription Factor, medicine.medical_specialty, Pyridones, Population, Antineoplastic Agents, Bone Marrow Cells, Pyrimidinones, Biology, Article, 03 medical and health sciences, Immune system, Nitriles, Biomarkers, Tumor, medicine, Animals, Humans, education, Cell Proliferation, Tumor microenvironment, Mesenchymal stem cell, Mesenchymal Stem Cells, Janus Kinase 2, medicine.disease, Xenograft Model Antitumor Assays, Pyrimidines, 030104 developmental biology, Culture Media, Conditioned, Cancer research, Pyrazoles

Abstract

Cancer-associated fibroblasts (CAF) have been suggested to originate from mesenchymal stromal cells (MSC), but their relationship with MSCs is not clear. Here, we have isolated from primary human neuroblastoma tumors a population of αFAP- and FSP-1–expressing CAFs that share phenotypic and functional characteristics with bone marrow–derived MSCs (BM-MSC). Analysis of human neuroblastoma tumors also confirmed the presence of αFAP- and FSP-1–positive cells in the tumor stroma, and their presence correlated with that of M2 tumor-associated macrophages. These cells (designated CAF-MSCs) enhanced in vitro neuroblastoma cell proliferation, survival, and resistance to chemotherapy and stimulated neuroblastoma tumor engraftment and growth in immunodeficient mice, indicating an effect independent of the immune system. The protumorigenic activity of MSCs in vitro and in xenografted mice was dependent on the coactivation of JAK2/STAT3 and MEK/ERK1/2 in neuroblastoma cells. In a mouse model of orthotopically implanted neuroblastoma cells, inhibition of JAK2/STAT3 and MEK/ERK/1/2 by ruxolitinib and trametinib potentiated tumor response to etoposide and increased overall survival. These data point to a new type of protumorigenic CAF in the tumor microenvironment of neuroblastoma and to STAT3 and ERK1/2 as mediators of their activity. Cancer Res; 77(18); 5142–57. ©2017 AACR.

Published

2017

31. Anti-CD105 Antibody Eliminates Tumor Microenvironment Cells and Enhances Anti-GD2 Antibody Immunotherapy of Neuroblastoma with Activated Natural Killer Cells

Author

Hong-Wei Wu, Robert C. Seeger, Charles P. Theuer, Richard Sposto, G. Esteban Fernandez, Jemily Malvar, Laurence Blavier, Michael A. Sheard, Hiroyuki Shimada, and Yves A. DeClerck

Subjects

0301 basic medicine, Cancer Research, medicine.drug_class, medicine.medical_treatment, Antineoplastic Agents, Mice, SCID, Monoclonal antibody, Article, 03 medical and health sciences, Mice, Neuroblastoma, 0302 clinical medicine, Mice, Inbred NOD, Cell Line, Tumor, Gangliosides, medicine, Animals, Humans, Antibody-dependent cell-mediated cytotoxicity, Tumor microenvironment, biology, Chemistry, Mesenchymal stem cell, Antibody-Dependent Cell Cytotoxicity, Endoglin, Dinutuximab, Antibodies, Monoclonal, Immunotherapy, medicine.disease, Xenograft Model Antitumor Assays, Killer Cells, Natural, 030104 developmental biology, Oncology, 030220 oncology & carcinogenesis, Cancer research, biology.protein, Antibody

Abstract

Purpose: We determined whether elimination of CD105+ cells in the tumor microenvironment (TME) with anti-CD105 antibodies enhanced anti-disialoganglioside (GD2) antibody dinutuximab therapy of neuroblastoma when combined with activated natural killer (aNK) cells. Experimental Design: The effect of MSCs and monocytes on antibody-dependent cellular cytotoxicity (ADCC) mediated by dinutuximab with aNK cells against neuroblastoma cells was determined in vitro. ADCC with anti-CD105 mAb TRC105 and aNK cells against MSCs, monocytes, and endothelial cells, which express CD105, was evaluated. Anti-neuroblastoma activity in immunodeficient NSG mice of dinutuximab with aNK cells without or with anti-CD105 mAbs was determined using neuroblastoma cell lines and a patient-derived xenograft. Results: ADCC mediated by dinutuximab with aNK cells against neuroblastoma cells in vitro was suppressed by addition of MSCs and monocytes, and dinutuximab with aNK cells was less effective against neuroblastomas formed with coinjected MSCs and monocytes in NSG mice than against those formed by tumor cells alone. Anti-CD105 antibody TRC105 with aNK cells mediated ADCC against MSCs, monocytes, and endothelial cells. Neuroblastomas formed in NSG mice by two neuroblastoma cell lines or a patient-derived xenograft coinjected with MSCs and monocytes were most effectively treated with dinutuximab and aNK cells when anti-human (TRC105) and anti-mouse (M1043) CD105 antibodies were added, which depleted human MSCs and murine endothelial cells and macrophages from the TME. Conclusions: Immunotherapy of neuroblastoma with anti-GD2 antibody dinutuximab and aNK cells is suppressed by CD105+ cells in the TME, but suppression is overcome by adding anti-CD105 antibodies to eliminate CD105+ cells.

Published

2019

32. Spatial and temporal changes in extracellular elastin and laminin distribution during lung alveolar development

Author

Nan Li, Gloria S. Pryhuber, Hui Chen, Yongfeng Luo, Wei Shi, David Warburton, Rex Moats, G. Esteban Fernandez, Daria Krenitsky, and Robert P. Mecham

Subjects

0301 basic medicine, Organogenesis, lcsh:Medicine, Inbred C57BL, Article, Elastic recoil, Extracellular matrix, 03 medical and health sciences, Mice, Young Adult, Spatio-Temporal Analysis, Laminin, Extracellular, medicine, Animals, Humans, lcsh:Science, Child, Preschool, Lung, Extracellular Matrix Proteins, Multidisciplinary, biology, Cell growth, Chemistry, lcsh:R, Infant, Newborn, Ring fibers, Endothelial Cells, Infant, respiratory system, Newborn, Extracellular Matrix, Elastin, Mice, Inbred C57BL, Pulmonary Alveoli, 030104 developmental biology, medicine.anatomical_structure, Animals, Newborn, Child, Preschool, biology.protein, Biophysics, lcsh:Q, Generic health relevance

Abstract

Lung alveolarization requires precise coordination of cell growth with extracellular matrix (ECM) synthesis and deposition. The role of extracellular matrices in alveogenesis is not fully understood, because prior knowledge is largely extrapolated from two-dimensional structural analysis. Herein, we studied temporospatial changes of two important ECM proteins, laminin and elastin that are tightly associated with alveolar capillary growth and lung elastic recoil respectively, during both mouse and human lung alveolarization. By combining protein immunofluorescence staining with two- and three-dimensional imaging, we found that the laminin network was simplified along with the thinning of septal walls during alveogenesis, and more tightly associated with alveolar endothelial cells in matured lung. In contrast, elastin fibers were initially localized to the saccular openings of nascent alveoli, forming a ring-like structure. Then, throughout alveolar growth, the number of such alveolar mouth ring-like structures increased, while the relative ring size decreased. These rings were interconnected via additional elastin fibers. The apparent patches and dots of elastin at the tips of alveolar septae found in two-dimensional images were cross sections of elastin ring fibers in the three-dimension. Thus, the previous concept that deposition of elastin at alveolar tips drives septal inward growth may potentially be conceptually challenged by our data.

Published

2018

33. Plasminogen Activator Inhibitor-1 Promotes the Recruitment and Polarization of Macrophages in Cancer

Author

G. Esteban Fernandez, Veronica Rae Placencio-Hickok, Marta Helena Kubala, Yves A. DeClerck, Hua Fang, Richard Sposto, and Vasu Punj

Subjects

0301 basic medicine, STAT3 Transcription Factor, Transplantation, Heterologous, Antigens, Differentiation, Myelomonocytic, Receptors, Cell Surface, p38 Mitogen-Activated Protein Kinases, General Biochemistry, Genetics and Molecular Biology, Monocytes, Article, 03 medical and health sciences, chemistry.chemical_compound, Protein Domains, Antigens, CD, Cell Movement, Neoplasms, Plasminogen Activator Inhibitor 1, Animals, Humans, Autocrine signalling, Interleukin 6, lcsh:QH301-705.5, biology, Interleukin-6, Macrophages, NF-kappa B, Interleukin, Cell Polarity, M2 Macrophage, LRP1, Cell biology, Mice, Inbred C57BL, 030104 developmental biology, HEK293 Cells, Phenotype, lcsh:Biology (General), chemistry, A549 Cells, Plasminogen activator inhibitor-1, biology.protein, Plasminogen activator, CD163

Abstract

Summary: Plasminogen activator inhibitor-1 (PAI-1) has a pro-tumorigenic function via its pro-angiogenic and anti-apoptotic activities. Here, we demonstrate that PAI-1 promotes the recruitment and M2 polarization of monocytes/macrophages through different structural domains. Its LRP1 interacting domain regulated macrophage migration, while its C-terminal uPA interacting domain promoted M2 macrophage polarization through activation of p38MAPK and nuclear factor κB (NF-κB) and induction of an autocrine interleukin (IL)-6/STAT3 activation pathway. We then show in several experiments in mice that expression of PAI-1 is associated with increased tumorigenicity, increased presence of M2 macrophages, higher levels of IL-6, and increased STAT3 phosphorylation in macrophages. Strong positive correlations between PAI-1, IL-6, and CD163 (M2 marker) expression were also found by meta-analysis of transcriptome data in many human cancers. Altogether, these data provide evidence for a mechanism explaining the paradoxical pro-tumorigenic function of PAI-1 in cancer. : The serine protease inhibitor plasminogen activator inhibitor-1 (PAI-1) has a paradoxical pro-angiogenic and protective effect on cancer cells. Kubala et al. provide evidence for a third pro-tumorigenic function by demonstrating that PAI-1 promotes recruitment and polarization toward a pro-tumorigenic phenotype of tumor-associated macrophages. Keywords: plasminogen activator inhibitor-1, PAI-1, tumor-associated macrophages, M2 polarization, interleukin 6, STAT3, tumor microenvironment

Published

2017

34. Contribution of neuroblastoma-derived exosomes to the production of pro-tumorigenic signals by bone marrow mesenchymal stromal cells

Author

Muller Fabbri, Rie Nakata, Pascale Zimmermann, Rob Fanter, Yves A. DeClerck, Hiroyuki Shimada, G. Esteban Fernandez, Jemily Malvar, The Saban Research Institute of Children’s Hospital Los Angeles [Los Angeles, CA, USA], University of Southern California (USC), Division of Hematology, Oncology, and Blood & Marrow Transplantation [Los Angeles, CA, USA], Department of Pediatrics [Los Angeles, CA, USA], Department of Pathology and Laboratory Medicine [UCLA], University of California [Los Angeles] (UCLA), University of California (UC)-University of California (UC)-School of Medicine, Department of Molecular Microbiology and Immunology [Los Angeles, CA, USA], Centre de Recherche en Cancérologie de Marseille (CRCM), Aix Marseille Université (AMU)-Institut Paoli-Calmettes, Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Department of Biochemistry and Molecular Biology [Los Angeles], Keck School of Medicine [Los Angeles], University of Southern California (USC)-University of Southern California (USC), This work was supported by grants P01 CA81403 and U54 CA163117 (to YAD) from the National Institutes of Health, and a grant (to YAD) from the St. Baldrick’s foundation. The work in PZ laboratory was supported by the French Foundation for Cancer Research (ARC, PJA 20161204584), Institut National du Cancer (INCa, subvention 2013-105) and National Research Agency (ANR, Investissements d’Avenir, A*MIDEX project ANR-11-IDEX-0001-02), and by the Research Foundation – Flanders (FWO G.0846.15)., ANR-11-IDEX-0001,Amidex,INITIATIVE D'EXCELLENCE AIX MARSEILLE UNIVERSITE(2011), Ghossoub, Rania, INITIATIVE D'EXCELLENCE AIX MARSEILLE UNIVERSITE - - Amidex2011 - ANR-11-IDEX-0001 - IDEX - VALID, University of California-University of California-School of Medicine, Centre National de la Recherche Scientifique (CNRS)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Institut Paoli-Calmettes, and Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Fédération nationale des Centres de lutte contre le Cancer (FNCLCC)-Aix Marseille Université (AMU)

Subjects

0301 basic medicine, Chemokine, Histology, cell–cell interaction, [SDV]Life Sciences [q-bio], extracellular-signal- regulated kinase, Exosomes, Exosome, 03 medical and health sciences, neuroblastoma, Cell–cell interaction, medicine, lcsh:QH573-671, Protein kinase B, biology, lcsh:Cytology, Mesenchymal stem cell, Cell Biology, Extracellular vesicle, Microvesicles, Cell biology, [SDV] Life Sciences [q-bio], 030104 developmental biology, medicine.anatomical_structure, biology.protein, Bone marrow, extracellular-signal-regulated kinase, mesenchymal stromal cells, extracellular vesicles, Research Article

Abstract

International audience; The bone marrow (BM) niche is a microenvironment promoting survival, dormancy and therapeutic resistance in tumor cells. Central to this function are mesenchymal stromal cells (MSCs). Here, using neuroblastoma (NB) as a model, we demonstrate that NB cells release an extracellular vesicle (EVs) whose protein cargo is enriched in exosomal proteins but lacks cytokines and chemokines. Using three different purification methods, we then demonstrate that NB-derived exosomes were captured by MSCs and induced the production of pro-tumorigenic cytokines and chemokines, including interleukin-6 (IL-6), IL-8/CXCL8, vascular endothelial cell growth factor and monocyte-chemotactic protein-1, with exosomes prepared by size exclusion chromatography having the highest activity. We found no correlation between the IL-6 and IL-8/CXCL8 stimulatory activity of exosomes from eight NB cell lines and their origin, degree of MYCN amplification, drug resistance and disease status. We then demonstrate that the uptake of NB exosomes by MSCs was associated with a rapid increase in ERK1/2 and AKT activation, and that blocking ERK1/2 but not AKT activation inhibited the IL-6 and IL-8/CXCL8 production by MSCs without affecting exosome uptake. Thus, we describe a new mechanism by which NB cells induce in MSCs an inflammatory reaction that contributes to a favorable microenvir-onment in the BM.

Published

2017

35. Cellular uptake and cytotoxicity of a near-IR fluorescent corrole–TiO2 nanoconjugate

Author

Harry B. Gray, Bryce Sadtler, Robert H. Grubbs, G. Esteban Fernandez, Felix Alonso-Valenteen, Nathan S. Lewis, Cathie Nguyen, Rex Moats, Lily Dara, Lali K. Medina-Kauwe, Karn Sorasaenee, and Carl M. Blumenfeld

Subjects

Porphyrins, Absorption spectroscopy, Analytical chemistry, Biochemistry, Article, Inorganic Chemistry, Mice, chemistry.chemical_compound, Microscopy, Electron, Transmission, Fluorescence microscope, Animals, Humans, Viability assay, Corrole, Cytotoxicity, Cells, Cultured, Titanium, Spectroscopy, Near-Infrared, Chemistry, Fluorescence, In vitro, Nanostructures, Microscopy, Fluorescence, Transmission electron microscopy, Hepatocytes, Nuclear chemistry

Abstract

We are investigating the biological and biomedical imaging roles and impacts of fluorescent metallocorrole–TiO_2 nanoconjugates as potential near-infrared optical contrast agents in vitro in cancer and normal cell lines. The TiO_2 nanoconjugate labeled with the small molecule 2,17-bis(chlorosulfonyl)-5,10,15-tris(pentafluorophenyl)corrolato aluminum(III) (1-Al–TiO_2) was prepared. The nanoparticle 1-Al–TiO_2 was characterized by transmission electron microscopy (TEM) and integrating-sphere electronic absorption spectroscopy. TEM images of three different samples of TiO_2 nanoparticles (bare, H_2O_2 etched, and 1-Al functionalized) showed similarity in shapes and sizes with an average diameter of 29 nm for 1-Al–TiO_2. Loading of 1-Al on the TiO_2 surfaces was determined to be ca. 20–40 mg 1-Al/g TiO_2. Confocal fluorescence microscopy (CFM) studies of luciferase-transfected primary human glioblastoma U87-Luc cells treated with the nanoconjugate 1-Al–TiO_2 as the contrast agent in various concentrations were performed. The CFM images revealed that 1-Al–TiO_2 was found inside the cancer cells even at low doses (0.02–2 μg/mL) and localized in the cytosol. Bioluminescence studies of the U87-Luc cells exposed to various amounts of 1-Al–TiO_2 showed minimal cytotoxic effects even at higher doses (2–2000 μg/mL) after 24 h. A similar observation was made using primary mouse hepatocytes (PMH) treated with 1-Al–TiO_2 at low doses (0.0003–3 μg/mL). Longer incubation times (after 48 and 72 h for U87-Luc) and higher doses (> 20 μg/mL 1-Al–TiO_2 for U87-Luc and > 3 μg/mL 1-Al–TiO_2 for PMH) showed decreased cell viability.

Published

2014

36. Low doses of Celecoxib attenuate gut barrier failure during experimental peritonitis

Author

Elizabeth M. Pontarelli, Stephanie Papillon, Henri R. Ford, G. Esteban Fernandez, Jin Wang, Shannon L. Castle, Michael J. Zobel, Scott S. Short, Anatoly Grishin, and Nancy Smiley

Subjects

Peritonitis, Ileum, Pharmacology, Biology, Systemic inflammation, Dinoprostone, Permeability, Article, gut origin sepsis, Pathology and Forensic Medicine, Sepsis, Mice, 03 medical and health sciences, 0302 clinical medicine, Intestinal mucosa, medicine, Animals, Intestinal Mucosa, Prostaglandin E2, Molecular Biology, 030304 developmental biology, Sulfonamides, prostaglandin E2, 0303 health sciences, Cyclooxygenase 2 Inhibitors, Tight junction, Cell Biology, medicine.disease, Intestinal epithelium, 3. Good health, Mice, Inbred C57BL, Disease Models, Animal, gut barrier failure, medicine.anatomical_structure, Celecoxib, cyclooxygenase-2, 030220 oncology & carcinogenesis, Immunology, Pyrazoles, medicine.symptom, medicine.drug

Abstract

The intestinal barrier becomes compromised during systemic inflammation, leading to the entry of luminal bacteria into the host and gut origin sepsis. Pathogenesis and treatment of inflammatory gut barrier failure is an important problem in critical care. In this study, we examined the role of cyclooxygenase-2 (COX-2), a key enzyme in the production of inflammatory prostanoids, in gut barrier failure during experimental peritonitis in mice. I.p. injection of LPS or cecal ligation and puncture (CLP) increased the levels of COX-2 and its product prostaglandin E2 (PGE2) in the ileal mucosa, caused pathologic sloughing of the intestinal epithelium, increased passage of FITC-dextran and bacterial translocation across the barrier, and increased internalization of the tight junction (TJ)-associated proteins junction-associated molecule-A and zonula occludens-1. Luminal instillation of PGE2 in an isolated ileal loop increased transepithelial passage of FITC-dextran. Low doses (0.5-1 mg/kg), but not a higher dose (5 mg/kg) of the specific COX-2 inhibitor Celecoxib partially ameliorated the inflammatory gut barrier failure. These results demonstrate that high levels of COX-2-derived PGE2 seen in the mucosa during peritonitis contribute to gut barrier failure, presumably by compromising TJs. Low doses of specific COX-2 inhibitors may blunt this effect while preserving the homeostatic function of COX-2-derived prostanoids. Low doses of COX-2 inhibitors may find use as an adjunct barrier-protecting therapy in critically ill patients.

Published

2013

37. SERCA directs cell migration and branching across species and germ layers

Author

Scott E. Fraser, Nick Lansdale, Le A. Trinh, Daimark Bennett, David Warburton, Danielle V. Bower, Neil C. Featherstone, G. Esteban Fernandez, Denise Al Alam, Dan J. Bower, Sonia Navarro, Mark R. Frey, EC Jesudason, Thai V. Truong, and Marilyn G. Connell

Subjects

0301 basic medicine, Mesoderm, SERCA, animal structures, QH301-705.5, Science, Organogenesis, Ectoderm, 610 Medicine & health, Germ layer, Biology, General Biochemistry, Genetics and Molecular Biology, Calcium dynamics, 03 medical and health sciences, medicine, Branching morphogenesis, Cell migration, Biology (General), Protein kinase C, Genetics, Budding, 520 Astronomy, fungi, Cell biology, 030104 developmental biology, medicine.anatomical_structure, cardiovascular system, General Agricultural and Biological Sciences, Research Article

Abstract

Branching morphogenesis underlies organogenesis in vertebrates and invertebrates, yet is incompletely understood. Here, we show that the sarco-endoplasmic reticulum Ca2+ reuptake pump (SERCA) directs budding across germ layers and species. Clonal knockdown demonstrated a cell-autonomous role for SERCA in Drosophila air sac budding. Live imaging of Drosophila tracheogenesis revealed elevated Ca2+ levels in migratory tip cells as they form branches. SERCA blockade abolished this Ca2+ differential, aborting both cell migration and new branching. Activating protein kinase C (PKC) rescued Ca2+ in tip cells and restored cell migration and branching. Likewise, inhibiting SERCA abolished mammalian epithelial budding, PKC activation rescued budding, while morphogens did not. Mesoderm (zebrafish angiogenesis) and ectoderm (Drosophila nervous system) behaved similarly, suggesting a conserved requirement for cell-autonomous Ca2+ signaling, established by SERCA, in iterative budding., Summary: Dynamic imaging of living embryos demonstrates that SERCA is a conserved regulator that controls cell migration and branching across species and germ layers, and PKC activation can rescue SERCA inhibition. This article has an associated First Person interview with the first author of the paper as part of the supplementary information.

Published

2017

38. PID1 increases chemotherapy-induced apoptosis in medulloblastoma and glioblastoma cells in a manner that involves NFκB

Author

Anup Singh Pathania, Gregory M. Shackleford, G. Esteban Fernandez, Anat Erdreich-Epstein, Anthony Tran, Rex Moats, Xiuhai Ren, Yifu Zhang, and Jingying Xu

Subjects

0301 basic medicine, Science, Antineoplastic Agents, Apoptosis, Biology, Article, 03 medical and health sciences, Glioma, Cell Line, Tumor, medicine, Humans, neoplasms, Etoposide, Medulloblastoma, Cisplatin, Multidisciplinary, Bortezomib, NF-kappa B, medicine.disease, 030104 developmental biology, HEK293 Cells, Proteasome, Immunology, Cancer research, Proteasome inhibitor, Medicine, Carrier Proteins, Glioblastoma, medicine.drug

Abstract

Phosphotyrosine Interaction Domain containing 1 (PID1; NYGGF4) inhibits growth of medulloblastoma, glioblastoma and atypical teratoid rhabdoid tumor cell lines. PID1 tumor mRNA levels are highly correlated with longer survival in medulloblastoma and glioma patients, suggesting their tumors may have been more sensitive to therapy. We hypothesized that PID1 sensitizes brain tumors to therapy. We found that PID1 increased the apoptosis induced by cisplatin and etoposide in medulloblastoma and glioblastoma cell lines. PID1 siRNA diminished cisplatin-induced apoptosis, suggesting that PID1 is required for cisplatin-induced apoptosis. Etoposide and cisplatin increased NFκB promoter reporter activity and etoposide induced nuclear translocation of NFκB. Etoposide also increased PID1 promoter reporter activity, PID1 mRNA, and PID1 protein, which were diminished by NFκB inhibitors JSH-23 and Bay117082. However, while cisplatin increased PID1 mRNA, it decreased PID1 protein. This decrease in PID1 protein was mitigated by the proteasome inhibitor, bortezomib, suggesting that cisplatin induced proteasome dependent degradation of PID1. These data demonstrate for the first time that etoposide- and cisplatin-induced apoptosis in medulloblastoma and glioblastoma cell lines is mediated in part by PID1, involves NFκB, and may be regulated by proteasomal degradation. This suggests that PID1 may contribute to responsiveness to chemotherapy.

Published

2016

39. IQGAP1 mediates the disruption of adherens junctions to promoteEscherichia coliK1 invasion of brain endothelial cells

Author

Subramanian Krishnan, David B. Sacks, G. Esteban Fernandez, and Nemani V. Prasadarao

Subjects

Tight junction, Immunology, Biology, Microbiology, Molecular biology, Cell biology, Adherens junction, IQGAP1, Virology, Phosphorylation, Transcellular, Receptor, Actin, Protein kinase C

Abstract

Summary The transcellular entry of Escherichia coli K1 through human brain microvascular endothelial cells (HBMEC) is responsible for tight junction disruption, leading to brain oedema in neonatal meningitis. Previous studies demonstrated that outer membrane protein A (OmpA) of E. coli K1 interacts with its receptor, Ecgp96, to induce PKC-α phosphorylation, adherens junction (AJ) disassembly (by dislodging β-catenin from VE-cadherin), and remodelling of actin in HBMEC. We report here that IQGAP1 mediates β-catenin dissociation from AJs to promote actin polymerization required for E. coli K1 invasion of HBMEC. Overexpression of C-terminal truncated IQGAP1 (IQΔC) that cannot bind β-catenin prevents both AJ disruption and E. coli K1 entry. Of note, phospho-PKC-α interacts with the C-terminal portion of Ecgp96 as well as with VE-cadherin after IQGAP1-mediated AJ disassembly. HBMEC overexpressing either C-terminal truncated Ecgp96 (Ecgp96Δ200) or IQΔC upon infection with E. coli showed no interaction ofphospho-PKC-α with Ecgp96. These data indicate that the binding of OmpA to Ecgp96 induces PKC-α phosphorylation and association of phospho-PKC-α with Ecgp96, and then signals IQGAP1 to detach β-catenin from AJs. Subsequently, IQGAP1/β-catenin bound actin translocates to the site of E. coli K1 attachment to promote invasion.

Published

2012

40. Distinct Roles for TGN/Endosome Epsin-like Adaptors Ent3p and Ent5p

Author

Grace H. Huang, Mara C. Duncan, G. Esteban Fernandez, Gregory S. Payne, and Giancarlo Costaguta

Subjects

Saccharomyces cerevisiae Proteins, Epsin, Endosome, Adaptor Protein Complex 1, Molecular Sequence Data, Endosomes, Saccharomyces cerevisiae, Biology, Models, Biological, Clathrin, symbols.namesake, Amino Acid Sequence, Lipid bilayer, Molecular Biology, Alleles, ADP-Ribosylation Factors, Vesicle, Temperature, Articles, Cell Biology, Golgi apparatus, Protein Structure, Tertiary, Transport protein, Cell biology, Adaptor Proteins, Vesicular Transport, Protein Transport, Biochemistry, symbols, biology.protein, Clathrin adaptor proteins, Gene Deletion, trans-Golgi Network

Abstract

Clathrin adaptors are key factors in clathrin-coated vesicle formation, coupling clathrin to cargo and/or the lipid bilayer. A physically interacting network of three classes of adaptors participate in clathrin-mediated traffic between the trans-Golgi network (TGN) and endosomes: AP-1, Gga proteins, and epsin-like proteins. Here we investigate functional relationships within this network through transport assays and protein localization analysis in living yeast cells. We observed that epsin-like protein Ent3p preferentially localized with Gga2p, whereas Ent5p distributed equally between AP-1 and Gga2p. Ent3p was mislocalized in Gga-deficient but not in AP-1-deficient cells. In contrast, Ent5p retained localization in cells lacking either or both AP-1 and Gga proteins. The Ent proteins were dispensable for AP-1 or Gga localization. Synthetic genetic growth and alpha-factor maturation defects were observed when ent5Delta but not ent3Delta was introduced together with deletions of the GGA genes. In AP-1-deficient cells, ent3Delta and to a lesser extent ent5Delta caused minor alpha-factor maturation defects, but together resulted in a near-lethal phenotype. Deletions of ENT3 and ENT5 also displayed synthetic defects similar to, but less severe than, synthetic effects of AP-1 and Gga inactivation. These results differentiate Ent3p and Ent5p function in vivo, suggesting that Ent3p acts primarily with Gga proteins, whereas Ent5p acts with both AP-1 and Gga proteins but is more critical for AP-1-mediated transport. The data also support a model in which the Ent adaptors provide important accessory functions to AP-1 and Gga proteins in TGN/endosome traffic.

Published

2006

41. Exploring the Mode-of-Action of Bioactive Compounds by Chemical-Genetic Profiling in Yeast

Author

Richelle Sopko, Julie A. Brill, Gordon Chua, Inmar E. Givoni, Renee L. Brost, Satoru Ishihara, Brendan J. Frey, Cheuk-Hei Ho, Todd C. Lorenz, Christopher A. Gray, Raymond J. Andersen, Yoshikazu Ohya, Gregory S. Payne, Charles Brenner, David E. Williams, Ainslie B. Parsons, Timothy P. Hughes, Brenda J. Andrews, Justin Porter, Charles Boone, Troy Ketela, Andres Lopez, Todd R. Graham, G. Esteban Fernandez, and Jiyi Wang

Subjects

Antineoplastic Agents, Hormonal, Drug Evaluation, Preclinical, Drug Resistance, Phosphatidylserines, Pharmacology, Biology, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Fungal Proteins, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Depsipeptides, Yeasts, Cluster Analysis, Gene, 030304 developmental biology, 0303 health sciences, Natural product, Molecular Structure, Biochemistry, Genetics and Molecular Biology(all), Drug discovery, Gene Expression Profiling, Lipopeptide, Phosphatidylserine, Yeast, 3. Good health, Papuamide B, Tamoxifen, Pharmaceutical Preparations, DNA profiling, chemistry, Biochemistry, 030220 oncology & carcinogenesis, Mutation, Signal Transduction

Abstract

SummaryDiscovering target and off-target effects of specific compounds is critical to drug discovery and development. We generated a compendium of “chemical-genetic interaction” profiles by testing the collection of viable yeast haploid deletion mutants for hypersensitivity to 82 compounds and natural product extracts. To cluster compounds with a similar mode-of-action and to reveal insights into the cellular pathways and proteins affected, we applied both a hierarchical clustering and a factorgram method, which allows a gene or compound to be associated with more than one group. In particular, tamoxifen, a breast cancer therapeutic, was found to disrupt calcium homeostasis and phosphatidylserine (PS) was recognized as a target for papuamide B, a cytotoxic lipopeptide with anti-HIV activity. Further, the profile of crude extracts resembled that of its constituent purified natural product, enabling detailed classification of extract activity prior to purification. This compendium should serve as a valuable key for interpreting cellular effects of novel compounds with similar activities.

Published

2006

42. Fibroblast growth factor 10 alters the balance between goblet and Paneth cells in the adult mouse small intestine

Author

Senta Georgia, Henri R. Ford, Soula Danopoulos, Tracy C. Grikscheit, Saverio Bellusci, Dana Almohazey, Frederic G. Sala, G. Esteban Fernandez, Denise Al Alam, Kathy A. Schall, and Mark R. Frey

Subjects

medicine.medical_specialty, Programmed cell death, Paneth Cells, Time Factors, Physiology, Cellular differentiation, Mice, Transgenic, Biology, Epithelial cell migration, digestive system, Tissue Culture Techniques, Physiology (medical), Internal medicine, Intestine, Small, medicine, Animals, Humans, Receptor, Fibroblast Growth Factor, Type 1, Receptor, Fibroblast Growth Factor, Type 2, Cell Proliferation, FGF10, Hepatology, Cell Death, Cell growth, Gastroenterology, Cell Differentiation, Small intestine, Epithelium, Cell biology, Mice, Inbred C57BL, stomatognathic diseases, Endocrinology, medicine.anatomical_structure, Call for Papers, Goblet Cells, Signal transduction, Fibroblast Growth Factor 10, Biomarkers, Signal Transduction

Abstract

Intestinal epithelial cell renewal relies on the right balance of epithelial cell migration, proliferation, differentiation, and apoptosis. Intestinal epithelial cells consist of absorptive and secretory lineage. The latter is comprised of goblet, Paneth, and enteroendocrine cells. Fibroblast growth factor 10 (FGF10) plays a central role in epithelial cell proliferation, survival, and differentiation in several organs. The expression pattern of FGF10 and its receptors in both human and mouse intestine and their role in small intestine have yet to be investigated. First, we analyzed the expression of FGF10, FGFR1, and FGFR2, in the human ileum and throughout the adult mouse small intestine. We found that FGF10, FGFR1b, and FGFR2b are expressed in the human ileum as well as in the mouse small intestine. We then used transgenic mouse models to overexpress Fgf10 and a soluble form of Fgfr2b, to study the impact of gain or loss of Fgf signaling in the adult small intestine. We demonstrated that overexpression of Fgf10 in vivo and in vitro induces goblet cell differentiation while decreasing Paneth cells. Moreover, FGF10 decreases stem cell markers such as Lgr5, Lrig1, Hopx, Ascl2, and Sox9. FGF10 inhibited Hes1 expression in vitro, suggesting that FGF10 induces goblet cell differentiation likely through the inhibition of Notch signaling. Interestingly, Fgf10 overexpression for 3 days in vivo and in vitro increased the number of Mmp7/Muc2 double-positive cells, suggesting that goblet cells replace Paneth cells. Further studies are needed to determine the mechanism by which Fgf10 alters cell differentiation in the small intestine.

Published

2015

43. MYCN-dependent Expression of Sulfatase-2 Regulates Neuroblastoma Cell Survival

Author

Richard Sposto, Valeria Solari, Hiroyuki Shimada, Yves A. DeClerck, Lucia Borriello, Edwin A. Yates, Gianluca Turcatel, G. Esteban Fernandez, Shahab Asgharzadeh, and Jeremy E. Turnbull

Subjects

Cancer Research, Oncogene Proteins, Cell Survival, Biology, Malignancy, Article, Neuroblastoma, Mediator, Cell Line, Tumor, medicine, Tumor Microenvironment, Humans, Nuclear protein, neoplasms, Tumor microenvironment, N-Myc Proto-Oncogene Protein, Sulfatase, Nuclear Proteins, medicine.disease, Gene Expression Regulation, Neoplastic, Oncology, Cancer research, Signal transduction, Sulfatases, Sulfotransferases, Heparan Sulfate Proteoglycans, Signal Transduction

Abstract

Heparan sulfate proteoglycans (HSPG) play a critical role in the interaction of tumor cells and their microenvironment. HSPG activity is dictated by sulfation patterns controlled by sulfotransferases, which add sulfate groups, and sulfatases (Sulf), which remove 6-O-sulfates. Here, we report altered expression of these enzymes in human neuroblastoma cells with higher levels of Sulf-2 expression, a specific feature of MYCN-amplified cells (MYCN-A cells) that represent a particularly aggressive subclass. Sulf-2 overexpression in neuroblastoma cells lacking MYCN amplification (MYCN-NA cells) increased their in vitro survival. Mechanistic investigations revealed evidence of a link between Sulf-2 expression and MYCN pathogenicity in vitro and in vivo. Analysis of Sulf-2 protein expression in 65 human neuroblastoma tumors demonstrated a higher level of Sulf-2 expression in MYCN-A tumors than in MYCN-NA tumors. In two different patient cohorts, we confirmed the association in expression patterns of Sulf-2 and MYCN and determined that Sulf-2 overexpression predicted poor outcomes in a nonindependent manner with MYCN. Our findings define Sulf-2 as a novel positive regulator of neuroblastoma pathogenicity that contributes to MYCN oncogenicity. Cancer Res; 74(21); 5999–6009. ©2014 AACR.

Published

2014

44. ISDN2014_0387: Placode lineage contributes to enteric sensory neurons in response to endothelin signaling

Author

Monica Mendez, Takako Makita, and G. Esteban Fernandez

Subjects

Lineage (genetic), Developmental Neuroscience, Sensory system, Biology, Endothelin receptor, Developmental Biology, Cell biology

Published

2015

45. Laa1p, a conserved AP-1 accessory protein important for AP-1 localization in yeast

Author

G. Esteban Fernandez and Gregory S. Payne

Subjects

Saccharomyces cerevisiae Proteins, ADP ribosylation factor, Immunoprecipitation, Protein subunit, Saccharomyces cerevisiae, Adaptor Protein Complex 1, Genes, Fungal, Molecular Sequence Data, medicine.disease_cause, Clathrin, chemistry.chemical_compound, medicine, Amino Acid Sequence, Molecular Biology, Alleles, Adaptor Proteins, Signal Transducing, Mutation, Brefeldin A, biology, ADP-Ribosylation Factors, Cell Membrane, Clathrin-Coated Vesicles, Cell Biology, Articles, biology.organism_classification, Transport protein, Adaptor Proteins, Vesicular Transport, chemistry, Biochemistry, biology.protein, Carrier Proteins

Abstract

AP-1 and Gga adaptors participate in clathrin-mediated protein transport between the trans-Golgi network and endosomes. Both adaptors contain homologous domains that act to recruit accessory proteins involved in clathrin-coated vesicle formation, but the spectrum of known adaptor-binding partners is limited. This study describes an evolutionarily conserved protein of Saccharomyces cerevisiae, Laa1p (Yjl207cp), that interacts and functions specifically with AP-1. Deletion of LAA1, when combined with a conditional mutation in clathrin heavy chain or deletion of GGA genes, accentuated growth defects and increased disruption of clathrin-dependent α-factor maturation and transport of carboxypeptidase Y to the vacuole. In contrast, such genetic interactions were not observed between deletions of LAA1 and AP-1 subunit genes. Laa1p preferentially interacted with AP-1 compared with Gga proteins by glutathione S-transferase-fusion affinity binding and coimmunoprecipitations. Localization of AP-1 and Laa1p, but not Gga proteins, was highly sensitive to brefeldin A, an inhibitor of ADP-ribosylation factor (Arf) activation. Importantly, deletion of LAA1 caused mislocalization of AP-1, especially in cells at high density (postdiauxic shift), but it did not affect Gga protein distribution. Our results identify Laa1p as a new determinant of AP-1 localization, suggesting a model in which Laa1p and Arf cooperate to direct stable association of AP-1 with appropriate intracellular membranes.

Published

2006

46. Abstract 3963: MYCN-dependent expression of sulfatase2 regulates neuroblastoma cell survival

Author

Edwin A. Yates, G. Esteban Fernandez, Yves A. DeClerck, Hiroyuki Shimada, Lucia Borriello, Richard Sposto, Shahab Asgharzadeh, Valeria Solari, and Jeremy E. Turnbull

Subjects

Cancer Research, Tumor microenvironment, medicine.diagnostic_test, Cancer, Caspase 3, Biology, medicine.disease, Molecular biology, Oncology, Downregulation and upregulation, Western blot, Apoptosis, Neuroblastoma, medicine, Viability assay, neoplasms

Abstract

Despite the well-demonstrated role of MYCN in the pathogenesis of neuroblastoma, the mechanisms underlying its oncogenic function are not entirely understood and there is evidence that its function is in part dependent on the tumor microenvironment (TME). Heparan sulfate proteoglycans (HSPG) play a critical role in the interaction between tumor cells and the TME in great part because of their ability to retain cytokines, chemokines and growth factors and to control their bioavailability. This function of HSPG is dependent on the sulfation pattern that itself is controlled by sulfotransferases that add sulfate groups to the repeating disaccharide units and sulfatases (SULF) that selectively remove 6-O-sulfates. An unbiased analysis of the expression of 12 of these enzymes by RT-PCR in 8 human neuroblastoma cell lines revealed higher levels of expression of SULF2 in cell lines with amplification of the MYCN oncogene (MYCN-A), an observation that was confirmed at the protein level by Western blot analysis. We then demonstrated that the knock down (KD) of SULF2 in MYCN-A cells by siRNA resulted in a significant decrease in cell viability caused by a decrease in cell cycle entry and in apoptosis as documented by increase in caspase 3/7 activity, PARP cleavage and annexin-V expression. Evidence was provided that SULF2 is a downstream target of MYCN by demonstrating that overexpression of MYCN in CHLA-255 neuroblastoma cells increased SULF2 expression whereas downregulation of MYCN expression in SHEP-21N cells was followed by a downregulation of SULF2. Underlying the importance of SULF2 in neuroblastoma cell survival independently of MYCN, we demonstrated that overexpression of SULF2 in MYCN-NA cells increased cell viability without increasing MYCN expression. Finally, an analysis of SULF2 protein expression in 65 primary human neuroblastoma tumors indicated a statistically significant higher level of expression in MYCN-A tumors along with an almost complete absence of expression in MYCN-non amplified (NA) tumors, whether they were of favorable or unfavorable histology. The data thus identify SULF2 as a new downstream target of MYCN and a key contributor to its oncogenic function in human neuroblastoma. Citation Format: Valeria Solari, Lucia Borriello, G. Esteban Fernandez, Hiroyuki Shimada, Richard Sposto, Shahab Asgharzadeh, Edwin A. Yates, Jeremy E. Turnbull, Yves A. Declerck. MYCN-dependent expression of sulfatase2 regulates neuroblastoma cell survival. [abstract]. In: Proceedings of the 105th Annual Meeting of the American Association for Cancer Research; 2014 Apr 5-9; San Diego, CA. Philadelphia (PA): AACR; Cancer Res 2014;74(19 Suppl):Abstract nr 3963. doi:10.1158/1538-7445.AM2014-3963

Published

2014

47. Drosophila rab GDI mutants disrupt development but have normal Rab membrane extraction

Author

Philip D. Stahl, G. Esteban Fernandez, Gabriel Waksman, Christina Tsou, M. Alejandro Barbieri, John W. Verbsky, Cynthia S. Ricard, William M. Lewis, Janelle M. Jakubowski, Vinoy Prasad, Marion Vogel, and Clarissa M. Cheney

Subjects

Male, Mutant, Blotting, Western, Mutation, Missense, Embryonic Development, Pole cell formation, GTPase, Biology, In Vitro Techniques, Crystallography, X-Ray, Protein Structure, Secondary, Endocrinology, Genetics, Animals, Alleles, Conserved Sequence, Guanine Nucleotide Dissociation Inhibitors, fungi, Cell Membrane, Genetic Complementation Test, Homozygote, Cell Biology, Sequence Analysis, DNA, Phenotype, Cell biology, Vesicular transport protein, Complementation, Drosophila melanogaster, Biochemistry, Mutagenesis, Ethyl Methanesulfonate, Female, Genes, Lethal, Rab, Function (biology)

Abstract

Summary: Rab GTPases are essential for vesicular transport. Rab GDP dissociation inhibitor (GDI) binds to GDP-bound rabs, removes rabs from acceptor membranes and delivers rabs to donor membranes. We isolated lethal GDI mutations in Drosophila and analyzed their developmental phenotypes. To learn how these mutations affect GDI structure, the crystal structure of Drosophila GDI was determined by molecular replacement to a resolution of 3.0 A. Two hypomorphic, missense mutations are located in domain II of GDI at highly conserved positions, but not in previously identified sequence conserved regions. The mutant GDIs were tested for ability to extract rabs from membranes and showed wild-type levels of rab membrane extraction. The two missense alleles showed intragenic complementation, indicating that domain II of GDI may have two separable functions. This study indicates that GDI function is essential for development of a complex, multicellular organism and that puparium formation and pole cell formation are especially dependent on GDI function. genesis 31:17–29, 2001. © 2001 Wiley-Liss, Inc.

Published

2001