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1. Data from Macrophages Promote Circulating Tumor Cell–Mediated Local Recurrence following Radiotherapy in Immunosuppressed Patients

Author

Edward E. Graves, Amato J. Giaccia, Kathleen C. Horst, Allison W. Kurian, Melissa J. Jenkins, Anosheh Afghahi, Stavros Melemenidis, Yasaman Ahrari, Meghana A. Golla, Rie von Eyben, Luis A. Soto, Laura L. Bronsart, Marta Vilalta, Todd A. Aguilera, and Marjan Rafat

Abstract

Although radiotherapy (RT) decreases the incidence of locoregional recurrence in breast cancer, patients with triple-negative breast cancer (TNBC) have increased risk of local recurrence following breast-conserving therapy. The relationship between RT and local recurrence is unknown. Here, we tested the hypothesis that recurrence in some instances is due to the attraction of circulating tumor cells to irradiated tissues. To evaluate the effect of absolute lymphocyte count on local recurrence after RT in patients with TNBC, we analyzed radiation effects on tumor and immune cell recruitment to tissues in an orthotopic breast cancer model. Recurrent patients exhibited a prolonged low absolute lymphocyte count when compared with nonrecurrent patients following RT. Recruitment of tumor cells to irradiated normal tissues was enhanced in the absence of CD8+ T cells. Macrophages (CD11b+F480+) preceded tumor cell infiltration and were recruited to tissues following RT. Tumor cell recruitment was mitigated by inhibiting macrophage infiltration using maraviroc, an FDA-approved CCR5 receptor antagonist. Our work poses the intriguing possibility that excessive macrophage infiltration in the absence of lymphocytes promotes local recurrence after RT. This combination thus defines a high-risk group of patients with TNBC.Significance: This study establishes the importance of macrophages in driving tumor cell recruitment to sites of local radiation therapy and suggests that this mechanism contributes to local recurrence in women with TNBC that are also immunosuppressed.Graphical Abstract: http://cancerres.aacrjournals.org/content/canres/78/15/4241/F1.large.jpg. Cancer Res; 78(15); 4241–52. ©2018 AACR.

Published
2023

3. Data from Hypoxia in Models of Lung Cancer: Implications for Targeted Therapeutics

Author

Amato J. Giaccia, Quynh-Thu Le, Alejandro Sweet-Cordero, Leanne Sayles, Dean Felsher, Phuoc T. Tran, Janine T. Erler, Ivana K. Cecic, Marta Vilalta, and Edward E. Graves

Abstract

Purpose: To efficiently translate experimental methods from bench to bedside, it is imperative that laboratory models of cancer mimic human disease as closely as possible. In this study, we sought to compare patterns of hypoxia in several standard and emerging mouse models of lung cancer to establish the appropriateness of each for evaluating the role of oxygen in lung cancer progression and therapeutic response.Experimental Design: Subcutaneous and orthotopic human A549 lung carcinomas growing in nude mice as well as spontaneous K-ras or Myc-induced lung tumors grown in situ or subcutaneously were studied using fluorodeoxyglucose and fluoroazomycin arabinoside positron emission tomography, and postmortem by immunohistochemical observation of the hypoxia marker pimonidazole. The response of these models to the hypoxia-activated cytotoxin PR-104 was also quantified by the formation of γH2AX foci in vitro and in vivo. Finally, our findings were compared with oxygen electrode measurements of human lung cancers.Results: Minimal fluoroazomycin arabinoside and pimonidazole accumulation was seen in tumors growing within the lungs, whereas subcutaneous tumors showed substantial trapping of both hypoxia probes. These observations correlated with the response of these tumors to PR-104, and with the reduced incidence of hypoxia in human lung cancers relative to other solid tumor types.Conclusions: These findings suggest that in situ models of lung cancer in mice may be more reflective of the human disease, and encourage judicious selection of preclinical tumor models for the study of hypoxia imaging and antihypoxic cell therapies. Clin Cancer Res; 16(19); 4843–52. ©2010 AACR.

Published
2023

4. Table S1, Figures S1-S11 from Macrophages Promote Circulating Tumor Cell–Mediated Local Recurrence following Radiotherapy in Immunosuppressed Patients

Author

Edward E. Graves, Amato J. Giaccia, Kathleen C. Horst, Allison W. Kurian, Melissa J. Jenkins, Anosheh Afghahi, Stavros Melemenidis, Yasaman Ahrari, Meghana A. Golla, Rie von Eyben, Luis A. Soto, Laura L. Bronsart, Marta Vilalta, Todd A. Aguilera, and Marjan Rafat

Abstract

Table S1 summarizes the patient radiation and chemotherapy conditions. Figure S1 shows that viable tumor cells are recruited to the MFP following RT. Figure S2 shows that tumor cell recruitment is dose dependent. Figure S3 shows tumor growth curves and lung metastasis after RT. Figure S4 confirms CD4+ and CD8+ T cell depletion in BALB/c mice. Figure S5 presents overall mouse health following MFP RT. Figure S6 illustrates that irradiation of normal cells enhances in vitro cancer cell invasion. Figure S7 evaluates CD8+ T cell infiltration in irradiated normal tissues. Figure S8 shows immune cell infiltration following RT in Nu/Nu mice. Figure S9 shows immune cell infiltration kinetics in BALB/c mice. Figure S10 shows that secreted factors from macrophages influence tumor cell invasion and chemotaxis and that blocking these factors results in a decrease in tumor cell recruitment in vivo. Figure S11 evaluates systemic cytokines following RT.

Published
2023

5. Comparing radiolytic production of H

Author

Houda, Kacem, Serena, Psoroulas, Gael, Boivin, Michael, Folkerts, Veljko, Grilj, Tony, Lomax, Adrien, Martinotti, David, Meer, Jonathan, Ollivier, Benoit, Petit, Sairos, Safai, Ricky A, Sharma, Michele, Togno, Marta, Vilalta, Damien C, Weber, and Marie-Catherine, Vozenin

Subjects
Proton Therapy, Animals, Electrons, Radiotherapy Dosage, Hydrogen Peroxide, Protons, Zebrafish
Abstract

The physico-chemical and biological response to conventional and UHDR electron and proton beams was investigated, along with conventional photons. The temporal structure and nature of the beam affected both, with electron beam at ≥1400 Gy/s and proton beam at 0.1 and 1260 Gy/s found to be isoefficient at sparing zebrafish embryos.

Published
2022

6. Comparing radiolytic production of H2O2 and development of Zebrafish embryos after ultra high dose rate exposure with electron and transmission proton beams

Author

Houda Kacem, Serena Psoroulas, Gael Boivin, Michael Folkerts, Veljko Grilj, Tony Lomax, Adrien Martinotti, David Meer, Jonathan Ollivier, Benoit Petit, Sairos Safai, Ricky A. Sharma, Michele Togno, Marta Vilalta, Damien C. Weber, and Marie-Catherine Vozenin

Subjects
Oncology, 610 Medicine & health, Radiology, Nuclear Medicine and imaging, Hematology
Abstract

The physico-chemical and biological response to conventional and UHDR electron and proton beams was investigated, along with conventional photons. The temporal structure and nature of the beam affected both, with electron beam at ≥1400 Gy/s and proton beam at 0.1 and 1260 Gy/s found to be isoefficient at sparing zebrafish embryos.

Published
2022
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7. Abstract 1274: CCX559 is a potent orally-administered small molecule PD-L1 inhibitor that induces anti-tumor immunity

Author

Ton Dang, Ashton Easterday, Rajinder Singh, Kathleen Sullivan, Christopher I. Li, Yu Wang, Yibin Zeng, Penglie Zhang, Scamp Ryan J, Christopher S. Lange, Pingchen Fan, Thomas J. Schall, Niky Zhao, Darren Mcmurtrie, Shirley Liu, Ju Yang, Linda S. Ertl, Ryan Ong, Lui Rebecca M, Vicky Chhina, Marta Vilalta, Israel F. Charo, and Alice Kumamoto

Subjects
Cancer Research, biology, Chemistry, medicine.drug_class, T cell, T-cell receptor, Monoclonal antibody, Peripheral blood mononuclear cell, Immune system, medicine.anatomical_structure, Oncology, Cancer cell, biology.protein, medicine, Cancer research, Antibody, PD-L1 inhibitor
Abstract

Introduction: Cancer cells can escape tumor-specific T cell responses via engagement of inhibitory immune checkpoints. PD-L1/PD-1 interaction is one of the major checkpoints that limit effector T cell function against cancer cells, and monoclonal antibodies that block this interaction have been approved as therapies in multiple tumor indications. As a next generation therapy, small molecule inhibitors of PD-L1 potentially have advantageous properties compared to approved monoclonal antibodies, such as better penetration into solid tumors, reduced immunogenicity, lack of Fc-mediated side effects, convenience of oral administration, and lower cost of goods. We therefore embarked on an effort to identify and develop an orally available small molecule capable of targeting PD-L1/PD-1 interactions. Methods: Inhibition of the PD-L1/PD-1 interaction was measured using a binding assay, followed by a cell culture system assessing PD-1 inhibition of T cell receptor (TCR) activation. Human T cell responses were assessed in vitro using the mixed lymphocyte reaction (MLR) assay, and a human peripheral blood mononuclear cell (PBMC)-mediated tumor cell killing assay. For in vivo studies CCX559 was dosed orally in a syngeneic tumor model and in a human tumor cell/PBMC co-implantation model in immune deficient mice. Results: Using structural information and focused medicinal chemistry, we identified CCX559 as a potent inhibitor of PD-L1 interaction with PD-1. CCX559 prevented PD-L1/PD-1 inhibition of TCR signaling in a cell-based reporter assay, increased IFNγ secretion in allogeneic MLR assays, and increased tumor cell killing by human PBMCs. We demonstrated that CCX559 potentially employs multiple mechanisms to inhibit PD-L1, which are distinct from those published for human anti-PD-L1 antibodies. In murine tumor models, orally administered CCX559 reduced tumor growth similarly to a clinically-approved anti-human PD-L1 antibody. Summary: CCX559 is a highly potent, small molecule PD-L1 inhibitor that can be orally administered. CCX559 enhanced primary human T cell activity in vitro and demonstrated anti-tumor efficacy in two murine tumor models. Based on its unique mechanism of PD-L1 inhibition, strong anti-tumor activity, desirable drug properties, and good safety profile, we plan to advance CCX559 into clinical development in the first half of 2021. Citation Format: Chris Li, Marta Vilalta, Linda S. Ertl, Yu Wang, Yibin Zeng, Pingchen Fan, Christopher Lange, Darren McMurtrie, Ju Yang, Rebecca Lui, Ryan Scamp, Vicky Chhina, Alice Kumamoto, Ryan Ong, Ton Dang, Ashton Easterday, Niky Zhao, Shirley Liu, Rajinder Singh, Israel Charo, Kathleen Sullivan, Thomas J. Schall, Penglie Zhang. CCX559 is a potent orally-administered small molecule PD-L1 inhibitor that induces anti-tumor immunity [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1274.

Published
2021

8. Abstract 5693: Anti-tumor effect of orally available small molecule PD-L1 inhibitors in a murine model of colon adenocarcinoma

Author

Thomas J. Schall, Ashton Easterday, Christopher S. Lange, Pingchen Fan, Shirley Liu, Rajinder Singh, Penglie Zhang, Ton Dang, Yu Wang, Linda S. Ertl, Marta Vilalta, Yibin Zeng, Israel F. Charo, Simon Yau, Shijie 'Chris' Li, Alice Kumamoto, Ju Yang, Darren Mcmurtrie, Ryan Ong, Lui Rebecca M, and Vicky Chhina

Subjects
Cancer Research, Tumor microenvironment, biology, Chemistry, medicine.medical_treatment, Peripheral blood mononuclear cell, Immune checkpoint, Immune system, Oncology, Cancer immunotherapy, In vivo, PD-L1, biology.protein, Cancer research, medicine, Antibody
Abstract

Introduction: Antibody-based therapies targeting the Programmed cell Death-1/ Programmed Death-Ligand 1 (PD-1/PD-L1) immune checkpoint axis have achieved great success in cancer immunotherapy in recent years. As a next generation therapy, small molecule inhibitors of PD-1/PD-L1 offer the potential for increased tumor penetration, shorter half-life (to better manage immune related adverse events), and lower cost. We therefore embarked on an effort to identify and develop orally available small molecules capable of targeting PD-L1. Methods: We designed and optimized a number of small molecule PD-L1 inhibitors which potently disrupted the interaction of PD-1 with PD-L1. Active compounds were first profiled by an ELISA assay measuring inhibition of the PD-1/PD-L1 interaction, followed by a functional cell-based reporter assay, mixed lymphocyte reaction (MLR) assay, and human peripheral blood mononuclear cell (PBMC)-mediated tumor cell killing assay. Targeted medicinal chemistry efforts were employed to improve potency and oral bioavailability, and candidate compounds were then evaluated in murine tumor models. Due to the specific reactivity of these compounds to human PD-L1 (but not murine PD-L1), a syngeneic tumor model with murine MC-38 colon tumor cells expressing human PD-L1 (MC38-hPD-L1 tumor model) was used. Results: The optimized PD-L1 inhibitors were highly potent in cell-based reporter assay, the MLR assay and PBMC-mediated tumor cell killing assays. These compounds also possess high oral bioavailability and desirable safety profiles. In the MC38-hPD-L1 tumor model, Lead compounds potently reduced tumor growth similarly to an anti-human PD-L1 antibody, which was used as a positive control for the experiments. The tumor microenvironment analysis by flow cytometry demonstrated that these compounds almost completely occupied human PD-L1 on the tumor cells in vivo, and thus could potently block the interaction of PD-1/PD-L1 and enhance the immune responses against tumor. Summary: We have identified and advanced unique small molecule inhibitors of human PD-L1 by rational design and optimization. Molecules resulting from these efforts exhibited marked inhibition of the PD-1/PD-L1 interaction and signaling in vitro, and potent anti-tumor effects in an animal model. Citation Format: Shijie "Chris" Li, Marta Vilalta, Linda S. Ertl, Yu Wang, Yibin Zeng, Pingchen Fan, Christopher Lange, Darren McMurtrie, Ju Yang, Rebecca Lui, Ryan Ong, Vicky Chhina, Alice Kumamoto, Simon Yau, Ton Dang, Ashton Easterday, Shirley Liu, Rajinder Singh, Israel Charo, Thomas J. Schall, Penglie Zhang. Anti-tumor effect of orally available small molecule PD-L1 inhibitors in a murine model of colon adenocarcinoma [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 5693.

Published
2020

9. Patterns of Vasculature in Mouse Models of Lung Cancer Are Dependent on Location

Author

Nicholas P. Hughes, Amato J. Giaccia, Marta Vilalta, Rie von Eyben, and Edward E. Graves

Subjects
0301 basic medicine, Cancer Research, Pathology, Lung Neoplasms, Physiology, Angiogenesis, Mice, Subcutaneous Tissue, Computer-Assisted, 0302 clinical medicine, Vascularity, Tumor, Signal Processing, Computer-Assisted, Non-invasive imaging in animal models, Perfusion, Nuclear Medicine & Medical Imaging, medicine.anatomical_structure, Tumor microenvironment, Oncology, 030220 oncology & carcinogenesis, Vasculature, medicine.symptom, medicine.medical_specialty, Clinical Sciences, Article, Cell Line, Proto-Oncogene Proteins p21(ras), Xenograft models, 03 medical and health sciences, In vivo, Cell Line, Tumor, medicine, Animals, Radiology, Nuclear Medicine and imaging, Lung cancer, Lung, Animal, business.industry, Hypoxia (medical), medicine.disease, Disease Models, Animal, 030104 developmental biology, Disease Models, Signal Processing, business, Neoplasm Transplantation, Preclinical models of cancer
Abstract

PurposePreclinical studies of hypoxia are generally done using ectopic xenograft tumors, which behave differently from human tumors. Our previous findings have shown that subcutaneously implanted lung tumors exhibit more hypoxia than their orthotopic implanted or spontaneous K-ras-induced counterparts. We hypothesize that differences in hypoxia are due to site-specific differences in vascularity and perfusion.ProceduresTo compare the presence and functionality of vessels in these tumor models, we studied vascular perfusion in vivo in real time.ResultsOrthotopically implanted and spontaneous K-ras-induced lung tumors showed elevated perfusion, demonstrating vasculature functionality. Little contrast agent uptake was observed within the subcutaneously implanted tumors, indicating vascular dysfunction. These findings were corroborated at the microscopic level with Hoechst 33342 and Meca-32 staining.ConclusionsFrom these observations, we concluded that differences in hypoxia in experimental models is related to vessel perfusion. Thus, appropriate selection of preclinical lung tumor models is essential for the study of hypoxia, angiogenesis and therapies targeting these phenomena.

Published
2016

10. Induction of LIFR confers a dormancy phenotype in breast cancer cells disseminated to the bone marrow

Author

Rachelle W. Johnson, Joy Y. Wu, Marta Vilalta, Amato J. Giaccia, Monica M. Olcina, Elizabeth C. Finger, Joshua R. Johnson, Todd A. Aguilera, Julie A. Sterling, Alyssa R. Merkel, and Yu Miao

Subjects
0301 basic medicine, Cell signaling, Cancer, Leukemia inhibitory factor receptor, Cell Biology, Biology, medicine.disease, Metastatic breast cancer, Phenotype, Article, Metastasis, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Immunology, medicine, Dormancy, Bone marrow, skin and connective tissue diseases
Abstract

Breast cancer cells frequently home to the bone marrow, where they may enter a dormant state before forming a bone metastasis. Several members of the interleukin-6 (IL-6) cytokine family are implicated in breast cancer bone colonization, but the role for the IL-6 cytokine leukaemia inhibitory factor (LIF) in this process is unknown. We tested the hypothesis that LIF provides a pro-dormancy signal to breast cancer cells in the bone. In breast cancer patients, LIF receptor (LIFR) levels are lower with bone metastases and are significantly and inversely correlated with patient outcome and hypoxia gene activity. Hypoxia also reduces the LIFR:STAT3:SOCS3 signalling pathway in breast cancer cells. Loss of the LIFR or STAT3 enables otherwise dormant breast cancer cells to downregulate dormancy-, quiescence- and cancer stem cell-associated genes, and to proliferate in and specifically colonize the bone, suggesting that LIFR:STAT3 signalling confers a dormancy phenotype in breast cancer cells disseminated to bone.

Published
2016

11. Effects of radiation on metastasis and tumor cell migration

Author

Marjan Rafat, Edward E. Graves, and Marta Vilalta

Subjects
0301 basic medicine, Biochemistry & Molecular Biology, Pathology, medicine.medical_specialty, Epithelial-Mesenchymal Transition, Physiology, medicine.medical_treatment, Clinical Sciences, Article, Metastasis, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Circulating tumor cell, Cell Movement, Neoplasms, Animals, Humans, Medicine, Tumor Cell Migration, Neoplasm Metastasis, Cytokine, Molecular Biology, Migration, Cancer, Pharmacology, Radiotherapy, business.industry, Circulating tumor cells, Abscopal effect, Cell Biology, medicine.disease, Radiation therapy, 030104 developmental biology, 030220 oncology & carcinogenesis, Cancer research, Cytokines, Molecular Medicine, Biochemistry and Cell Biology, business, Radiation response
Abstract

It is well known that tumor cells migrate from the primary lesion to distant sites to form metastases and that these lesions limit patient outcome in a majority of cases. However, the extent to which radiation influences this process and to which migration in turn alters radiation response remains controversial. There are preclinical and clinical reports showing that focal radiotherapy can both increase the development of distant metastasis, as well as that it can induce the regression of established metastases through the abscopal effect. More recently, preclinical studies have suggested that radiation can attract migrating tumor cells and may, thereby, facilitate tumor recurrence. In this review, we summarize these phenomena and their potential mechanisms of action, and evaluate their significance for modern radiation therapy strategies.

Published
2016

12. Hypoxic induction of AKAP12 variant 2 shifts PKA-mediated protein phosphorylation to enhance migration and metastasis of melanoma cells

Author

Laura Castellini, Amato J. Giaccia, Marta Vilalta, Elizabeth C. Finger, Dadi Jiang, Erinn B. Rankin, Adam J. Krieg, Alice Banh, Wayne Zundel, and Marianne Broome Powell

Subjects
Proteomics, Scaffold protein, Cell signaling, Skin Neoplasms, Molecular Sequence Data, A Kinase Anchor Proteins, Cell Cycle Proteins, Biology, Mice, Cell Movement, Cell Line, Tumor, Animals, Humans, Neoplasm Invasiveness, Protein phosphorylation, Amino Acid Sequence, Neoplasm Metastasis, Phosphorylation, Protein kinase A, Melanoma, Tumor microenvironment, Multidisciplinary, Biological Sciences, AKAP12, Phosphoproteins, Cyclic AMP-Dependent Protein Kinases, Cell Hypoxia, Cell biology, Gene Expression Regulation, Neoplastic, Oxygen, Cancer research, Signal transduction, Neoplasm Transplantation, Signal Transduction
Abstract

Scaffold proteins are critical hubs within cells that have the ability to modulate upstream signaling molecules and their downstream effectors to fine-tune biological responses. Although they can serve as focal points for association of signaling molecules and downstream pathways that regulate tumorigenesis, little is known about how the tumor microenvironment affects the expression and activity of scaffold proteins. This study demonstrates that hypoxia, a common element of solid tumors harboring low oxygen levels, regulates expression of a specific variant of the scaffold protein AKAP12 (A-kinase anchor protein 12), AKAP12v2, in metastatic melanoma. In turn, through a kinome-wide phosphoproteomic and MS study, we demonstrate that this scaffolding protein regulates a shift in protein kinase A (PKA)-mediated phosphorylation events under hypoxia, causing alterations in tumor cell invasion and migration in vitro, as well as metastasis in an in vivo orthotopic model of melanoma. Mechanistically, the shift in AKAP12-dependent PKA-mediated phosphorylations under hypoxia is due to changes in AKAP12 localization vs. structural differences between its two variants. Importantly, our work defines a mechanism through which a scaffold protein can be regulated by the tumor microenvironment and further explains how a tumor cell can coordinate many critical signaling pathways that are essential for tumor growth through one individual scaffolding protein.

Published
2015

13. Abstract 1745: Inhibition of chemokine receptor 2 (CCR2) with a small molecule antagonist enhances the effectiveness of checkpoint inhibition by altering the tumor microenvironment in mouse colorectal tumors: Reducing tumor size and increasing long term survival

Author

Mcmahon Jeffrey P, Penglie Zhang, Ton Dang, Antoni Krasinski, Yibin Zheng, Shirley Liu, Mali Venkat Reddy, Xiaoping Zang, Christopher I. Li, Thomas J. Schall, James Campbell, Alice Kumamoto, Yu Wang, Rajinder Singh, Linda S. Ertl, Christine Janson, Simon Yao, Vicky Chhina, Zhenhua Miao, Lui Rebecca M, and Marta Vilalta

Subjects
Cancer Research, education.field_of_study, Tumor microenvironment, CCR2, business.industry, Population, Cancer, medicine.disease, Chemokine receptor, Oncology, Cancer research, Myeloid-derived Suppressor Cell, Medicine, Cytotoxic T cell, business, education, CD8
Abstract

Mouse CT26 colorectal tumors are heavily infiltrated by tumor-specific CD8 T cells, but nevertheless grow rapidly in Balb/c mice. These tumors are partially responsive to anti-PD-1 (α-PD-1) monoclonal antibody therapy, which suggests that an active suppression of the tumor-specific cytotoxic T cells exists in the untreated tumor. As chemokine receptor 2 (CCR2) is expressed by a potentially suppressive leukocyte subset within these tumors (monocytic myeloid derived suppressor cells aka M-MDSCs), we aimed to test whether CCR2 blockade could enhance the anti-tumor effects of α-PD-1. We have found that the therapeutic effects of α-PD-1 therapy are appreciably enhanced by specific blockade of CCR2 via a small molecule antagonist. This combined α-PD-1/CCR2i approach significantly decreases overall tumor size and increases the proportion of long-term survivors, with more than 50% of the mice (up to 73%) showing complete regression of a previously established tumor. The effects of this combined therapy are dependent on the presence of CD8+ T cells, as tumors do not respond to the therapy in CD8-depleted mice. The anti-CT26 tumor response is specific: long term survivors are resistant to re-inoculation with the CT26 tumor (even without further dosing of either drug) but are not resistant to the 4T1 breast tumor. CCR2 antagonism alters the tumor microenvironment by reducing the number of M-MDSC per gram of tumor (a CCR2hi population phenotypically defined as CD11b+/Ly6G-/Ly6Chi). Reduction in tumor size is inversely proportional to the ratio of CD8 T cells to M-MDSC. These data are consistent with a hypothesis that CCR2 antagonism enhances α-PD-1 therapy by preventing M-MDSC from accumulating within the tumor, thus reducing their suppressive effects on cytotoxic T cells. Citation Format: James J. Campbell, Christine Janson, Linda Ertl, Chris Li, Zhenhua Miao, Antoni Krasinski, Rebecca Lui, Venkat Mali, Jeffrey McMahon, Yibin Zheng, Yu Wang, Xiaoping Zang, Vicky Chhina, Marta Vilalta, Alice Kumamoto, Ton Dang, Shirley Liu, Simon Yao, Penglie Zhang, Thomas J. Schall, Rajinder Singh. Inhibition of chemokine receptor 2 (CCR2) with a small molecule antagonist enhances the effectiveness of checkpoint inhibition by altering the tumor microenvironment in mouse colorectal tumors: Reducing tumor size and increasing long term survival [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2018; 2018 Apr 14-18; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2018;78(13 Suppl):Abstract nr 1745.

Published
2018

14. Cyr61 silencing reduces vascularization and dissemination of osteosarcoma tumors

Author

O Fromigué, O Bawa, Marta Vilalta, P Opolon, Jerónimo Blanco, N Habel, Biomarqueurs prédictifs et nouvelles stratégies moléculaires en thérapeutique anticancéreuse (U981), Université Paris-Sud - Paris 11 (UP11)-Institut Gustave Roussy (IGR)-Institut National de la Santé et de la Recherche Médicale (INSERM), Consejo Superior de Investigaciones Científicas [Spain] (CSIC), Biomedical Research Networking Center in Bioengineering, Biomaterials and Nanomedicine (CIBER-BBN), Instituto de Salud Carlos III [Madrid] (ISC)-ministerio de ciencia e innovacion, and FROMIGUE, OLIVIA

Subjects
Cancer Research, Cell, Down-Regulation, Mice, Nude, Bone Neoplasms, Mice, Transgenic, [SDV.CAN]Life Sciences [q-bio]/Cancer, [SDV.BC]Life Sciences [q-bio]/Cellular Biology, Biology, Neovascularization, Mice, [SDV.CAN] Life Sciences [q-bio]/Cancer, RNA interference, Tumor Cells, Cultured, Genetics, medicine, Animals, Humans, Gene silencing, Neoplasm Invasiveness, Neoplasm Metastasis, [SDV.BC] Life Sciences [q-bio]/Cellular Biology, Molecular Biology, Cell Proliferation, Regulation of gene expression, Mice, Inbred BALB C, Osteosarcoma, Neovascularization, Pathologic, medicine.disease, Primary tumor, 3. Good health, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, CYR61, Immunology, Cancer research, RNA Interference, medicine.symptom, Cysteine-Rich Protein 61
Abstract

International audience; Osteosarcoma is the most prevalent primary pediatric cancer-related bone disease. These tumors frequently develop resistance to chemotherapy and are highly metastatic, leading to poor outcome. Thus, there is a need for new therapeutic strategies that can prevent cell dissemination. We previously showed that CYR61/CCN1 expression in osteosarcoma cells is correlated to aggressiveness both in vitro and in vivo in mouse models, as well as in patients. In this study, we found that CYR61 is a critical contributor to the vascularization of primary tumor. We demonstrate that silencing CYR61, using lentiviral transduction, leads to a significant reduction in expression level of pro-angiogenic markers such as VEGF, FGF2, PECAM and angiopoietins concomitantly to an increased expression of major anti-angiogenic markers such as thrombospondin-1 and SPARC. Matrix metalloproteinase-2 family member expression, a key pathway in osteosarcoma metastatic capacity was also downregulated when CYR61 was downregulated in osteosarcoma cells. Using a metastatic murine model, we show that CYR61 silencing in osteosarcoma cells results in reduced tumor vasculature and slows tumor growth compared with control. We also find that microvessel density correlates with lung metastasis occurrence and that CYR61 silencing in osteosarcoma cells limits the number of metastases. Taken together, our data indicate that CYR61 silencing can blunt the malignant behavior of osteosarcoma tumor cells by limiting primary tumor growth and dissemination process. INTRODUCTION Osteosarcoma is a highly vascular and extremely destructive bone malignancy that mainly affects children and young adults. It represents the most frequent pediatric cancer-related disease. Despite the introduction, during the 70 s, of aggressive multi-agent chemotherapy in addition to tumor ablation surgery, the long-term survival (45 years) increased from 10-60% for patients with localized primary tumors, but to o 30% for patients presenting metastases at initial diagnosis. Nowadays, knowledge of the mechanisms underlying osteosarcoma metastasis is quite limited. Thus, in order to improve the clinical outcomes for patients with poor prognosis and to manage primary osteosar-coma by preventing development of metastatic disease, it is imperative to find new approaches to block the metastasis process. Degradation of the extracellular matrix, facilitated by the action of matrix metalloproteinases (MMPs), is a prerequisite of tumor invasion and metastasis in a variety of cancers including osteosarcoma. MMP-2 and MMP-9 have been repetitively implicated in osteosarcoma cell invasion, 1-3 and increased expression of membrane type-1 MMP correlated with decreased overall survival. 4 A correlation was recently reported between the expression of the extracellular MMP inducer EMMPRIN (CD147) and vascular endothelial growth factor (VEGF) in osteosarcoma

Published
2014

15. Hypoxia in Models of Lung Cancer: Implications for Targeted Therapeutics

Author

Ivana K. Cecic, Alejandro Sweet-Cordero, Leanne C. Sayles, Marta Vilalta, Amato J. Giaccia, Phuoc T. Tran, Quynh-Thu Le, Janine T. Erler, Dean W. Felsher, and Edward E. Graves

Subjects
Male, Cancer Research, Pathology, medicine.medical_specialty, Lung Neoplasms, medicine.medical_treatment, Mice, Nude, Article, Targeted therapy, Histones, Proto-Oncogene Proteins c-myc, Mice, Carcinoma, Non-Small-Cell Lung, Cell Line, Tumor, medicine, Animals, Humans, Pimonidazole, Lung cancer, Electrodes, Cell Proliferation, Fluorodeoxyglucose, Lung, business.industry, Respiratory disease, Cancer, Neoplasms, Experimental, Hypoxia (medical), medicine.disease, Cell Hypoxia, Oxygen, Disease Models, Animal, medicine.anatomical_structure, Oncology, Nitroimidazoles, Positron-Emission Tomography, Nitrogen Mustard Compounds, ras Proteins, medicine.symptom, business, medicine.drug
Abstract

Purpose: To efficiently translate experimental methods from bench to bedside, it is imperative that laboratory models of cancer mimic human disease as closely as possible. In this study, we sought to compare patterns of hypoxia in several standard and emerging mouse models of lung cancer to establish the appropriateness of each for evaluating the role of oxygen in lung cancer progression and therapeutic response. Experimental Design: Subcutaneous and orthotopic human A549 lung carcinomas growing in nude mice as well as spontaneous K-ras or Myc-induced lung tumors grown in situ or subcutaneously were studied using fluorodeoxyglucose and fluoroazomycin arabinoside positron emission tomography, and postmortem by immunohistochemical observation of the hypoxia marker pimonidazole. The response of these models to the hypoxia-activated cytotoxin PR-104 was also quantified by the formation of γH2AX foci in vitro and in vivo. Finally, our findings were compared with oxygen electrode measurements of human lung cancers. Results: Minimal fluoroazomycin arabinoside and pimonidazole accumulation was seen in tumors growing within the lungs, whereas subcutaneous tumors showed substantial trapping of both hypoxia probes. These observations correlated with the response of these tumors to PR-104, and with the reduced incidence of hypoxia in human lung cancers relative to other solid tumor types. Conclusions: These findings suggest that in situ models of lung cancer in mice may be more reflective of the human disease, and encourage judicious selection of preclinical tumor models for the study of hypoxia imaging and antihypoxic cell therapies. Clin Cancer Res; 16(19); 4843–52. ©2010 AACR.

Published
2010

16. Exposure to cardiomyogenic stimuli fails to transdifferentiate human umbilical cord blood-derived mesenchymal stem cells

Author

Santiago Roura, Antoni Bayes-Genis, Carolina Gálvez-Montón, Leif Hove-Madsen, Carolina Soler-Botija, Jordi Farré, Cristina Prat-Vidal, and Marta Vilalta

Subjects
beta-Catenin, Physiology, Cell, Bone Morphogenetic Protein 2, Biology, Umbilical cord blood, Cardiac genes expression, Western blot, Physiology (medical), medicine, Animals, Humans, Myocyte, Dimethyl Sulfoxide, Myocytes, Cardiac, Insulin-Like Growth Factor I, Rats, Wistar, Cells, Cultured, Cardiomyocytes, Regulation of gene expression, Transdifferentiation, medicine.diagnostic_test, Stem Cells, Mesenchymal stem cell, Wnt signaling pathway, Cell Differentiation, Mesenchymal Stem Cells, Fetal Blood, Molecular biology, Coculture Techniques, Rats, Fibroblast Growth Factors, Wnt Proteins, medicine.anatomical_structure, Adipose Tissue, Azacitidine, Mesenchymal stem cells, Intercellular Signaling Peptides and Proteins, Tetradecanoylphorbol Acetate, Signal transduction, Lithium Chloride, Cardiology and Cardiovascular Medicine, Signal Transduction
Abstract

The ability of human umbilical cord blood-derived mesenchymal stem cells (UCBMSCs) to transdifferentiate towards cardiomyocytes remains unclear. The aim of this study was to direct UCBMSCs to the cardiac lineage by exposure to: (1) 5-azacytidine (AZ) or dimethyl sulfoxide (DMSO); (2) a combination of growth factors involved in early cardiomyogenesis (BMP-2 + bFGF + IGF-1); (3) the Wnt signaling activators lithium chloride (LiCl) and phorbol-12-myristate-13-acetate (PMA); and (4) direct contact with neonatal rat cardiomyocytes. Expression of cardiomyocyte-specific proteins and beta-catenin were assessed by quantitative RT-PCR, immunofluorescence and Western blot. Cocultures of human UCBMSCs with neonatal rat cardiomyocytes were also analyzed for the presence of calcium oscillations and changes in electrical potential using Fura Red and di-4-ANEPPS confocal imaging, respectively. Induction of cardiac-specific proteins was not detected in 5-AZ- or DMSO-treated cells. Following DMSO addition, beta-catenin cytoplasmic expression increased, but did not translocate into cell nuclei to promote cardiac gene activation. Likewise, neither co-stimulation with BMP-2 + bFGF + IGF-1, nor exposure to LiCl and PMA resulted in the acquisition of a cardiac phenotype by UCBMSCs. Direct contact with neonatal rat cardiomyocytes promoted neither the expression of cardiomyocyte-specific proteins, nor the presence of calcium rhythmic oscillations and potential-dependent fluorescence emission in UCBMSCs. The cardiomyogenic stimuli investigated in this study failed to transdifferentiate human UCBMSCs. Alternative strategies or regulatory factors and signaling pathways may be better suited to recruit UCBMSCs into cardiac cell lineage.

Published
2010

17. Dual luciferase labelling for non-invasive bioluminescence imaging of mesenchymal stromal cell chondrogenic differentiation in demineralized bone matrix scaffolds

Author

Jerónimo Blanco, José Becerra, Christian Jorgensen, Marta Vilalta, David Gould, Yuti Chernajovsky, José A. Andrades, Nuria Rubio, Danièle Noël, and Irene R. Dégano

Subjects
Diagnostic Imaging, Pathology, medicine.medical_specialty, Stromal cell, Cellular differentiation, Biophysics, Bone Marrow Cells, Bioengineering, Mice, SCID, 02 engineering and technology, Biology, Mesenchymal Stem Cell Transplantation, Cell Line, Biomaterials, Mice, 03 medical and health sciences, Chondrocytes, Genes, Reporter, Luciferases, Firefly, Osteogenesis, Transduction, Genetic, medicine, Animals, Humans, Bioluminescence imaging, Luciferase, Progenitor cell, Collagen Type II, Cell Proliferation, 030304 developmental biology, 0303 health sciences, Tissue Scaffolds, Demineralized bone matrix, Mesenchymal stem cell, Cell Differentiation, Mesenchymal Stem Cells, 021001 nanoscience & nanotechnology, Cell biology, Adipose Tissue, Gene Expression Regulation, Mechanics of Materials, Cell culture, Luminescent Measurements, Ceramics and Composites, Stromal Cells, 0210 nano-technology
Abstract

Non-invasive bioluminescence imaging (BLI) to monitor changes in gene expression of cells implanted in live animals should facilitate the development of biomaterial scaffolds for tissue regeneration. We show that, in vitro, induction of chondrogenic differentiation in mouse bone marrow stromal cell line (CL1) and human adipose tissue derived mesenchymal stromal cells (hAMSCs), permanently transduced with a procollagen II (COL2A1) promoter driving a firefly luciferase gene reporter (PLuc) (COL2A1p·PLuc), induces PLuc expression in correlation with increases in COL2A1 and Sox9 mRNA expression and acquisition of chondrocytic phenotype. To be able to simultaneously monitor in vivo cell differentiation and proliferation, COL2A1p·PLuc labelled cells were also genetically labelled with a renilla luciferase (RLuc) gene driven by a constitutively active cytomegalovirus promoter, and then seeded in demineralized bone matrix (DBM) subcutaneously implanted in SCID mice. Non-invasive BLI monitoring of the implanted mice showed that the PLuc/RLuc ratio reports on gene expression changes indicative of cell differentiation. Large (CL1) and moderated (hAMSCs) changes in the PLuc/RLuc ratio over a 6 week period, revealed different patterns of in vivo chondrogenic differentiation for the CL1 cell line and primary MSCs, in agreement with in vitro published data and our results from histological analysis of DBM sections. This double bioluminescence labelling strategy together with BLI imaging to analyze behaviour of cells implanted in live animals should facilitate the development of progenitor cell/scaffold combinations for tissue repair.

Published
2009

18. The effect of self-assembling peptide nanofiber scaffolds on mouse embryonic fibroblast implantation and proliferation

Author

Irene R. Dégano, Carlos E. Semino, Nuria Rubio, Jerónimo Blanco, Salvador Borrós, David Horna, Lluis Quintana, and Marta Vilalta

Subjects
Scaffold, Materials science, Light, Biophysics, Biocompatible Materials, Bioengineering, Matrix (biology), Mechanics, Hydrogel, Polyethylene Glycol Dimethacrylate, Prosthesis Implantation, Biomaterials, Mice, Tissue engineering, Cell Movement, Materials Testing, Animals, Bioluminescence imaging, Luciferases, Cell Proliferation, Mice, Inbred BALB C, Tissue Scaffolds, Cell growth, Fibroblasts, Embryo, Mammalian, Embryonic stem cell, Nanostructures, Cell biology, Mice, Inbred C57BL, Mechanics of Materials, Nanofiber, Luminescent Measurements, Ceramics and Composites, Rubber, Peptides, Self-assembling peptide, Biomedical engineering
Abstract

Development of new materials for tissue engineering can be facilitated by the capacity to efficiently monitor in vivo the survival, proliferation and differentiation behaviour of cells implanted in different target tissues. We present here the application of a previously developed platform that allows to monitor in real time the survival and proliferative behaviour of implanted cells in two anatomical sites: subcutaneous and intramuscular. Basically, the system is based on the use of a non-invasive bioluminescence imaging (BLI) technique to detect luciferase expressing C57BL/6 cells, mouse embryonic fibroblasts, seeded in two sets of scaffolds: 1, a RAD16-I self-assembling peptide nanofiber matrix and 2, a composite consisted of the same RAD16-I nanofibers contained into a microporous biorubber scaffold. Interestingly, our results indicated considerable differences in the behaviour of implanted cells in each scaffold type. We observed that the self-assembling peptide scaffold alone foster cell survival and promotes cell proliferation where the composite scaffold not. Since self-assembling peptide scaffolds presents value stiffness proximal to the implanted tissues it is suggestive to think that harder materials will provide a physical constriction for cells to proliferate as well as mechanical discontinuity. We therefore propose that it is important to close match the implantation environment with the cell/material constructs in order to obtain the best response of the cells, illustrating the convenience of this strategy for the development of new tissue engineering platforms.

Published
2009

19. Human adipose tissue-derived mesenchymal stromal cells as vehicles for tumor bystander effect: a model based on bioluminescence imaging

Author

Marta Vilalta, Jerónimo Blanco, Nuria Rubio, Elisabeth Aguilar, Sanjiv S. Gambhir, Juli R. Bagó, and Irene R. Dégano

Subjects
Male, Pathology, medicine.medical_specialty, noninvasive bioluminescence imaging, Stromal cell, Genetic enhancement, Genetic Vectors, Mice, Nude, Adipose tissue, Biology, Mesenchymal Stem Cell Transplantation, Mice, adipose tissue-derived mesenchymal stromal cells, thymidine kinase, Genetics, Bystander effect, medicine, Animals, Humans, Bioluminescence imaging, Ganciclovir, Molecular Biology, Cell Proliferation, Mice, Inbred BALB C, Cluster of differentiation, Lentivirus, Mesenchymal stem cell, Genes, Transgenic, Suicide, Prostatic Neoplasms, Cell Differentiation, Bystander Effect, Genetic Therapy, Xenograft Model Antitumor Assays, medicine.anatomical_structure, Adipose Tissue, bystander effect, Luminescent Measurements, Molecular Medicine, Bone marrow, tumor therapy
Abstract

Human adipose tissue mesenchymal stromal cells (AMSCs) share common traits, including similar differentiation potential and cell surface markers, with their bone marrow counterparts. Owing to their general availability, higher abundance and ease of isolation AMSCs may be convenient autologous delivery vehicles for localized tumor therapy. We demonstrate a model for tumor therapy development based on the use of AMSCs expressing renilla luciferase and thymidine kinase, as cellular vehicles for ganciclovir-mediated bystander killing of firefly luciferase expressing tumors, and noninvasive bioluminescence imaging to continuously monitor both, tumor cells and AMSCs. We show that the therapy delivering AMSCs survive long time within tumors, optimize the ratio of AMSCs to tumor cells for therapy, and asses the therapeutic effect in real time. Treatment of mice bearing prostate tumors plus therapeutic AMSCs with the prodrug ganciclovir induced bystander killing effect, reducing the number of tumor cells to 1.5 % that of control tumors. Thus, AMSCs could be useful vehicles to deliver localized therapy, with potential for clinical application in inoperable tumors and surgical borders after tumor resection. This approach, useful to evaluate efficiency of therapeutic models, should facilitate the selection of cell types, dosages, therapeutic agents and treatment protocols for cell-based therapies of specific tumors.

Published
2008

20. Biodistribution, Long-term Survival, and Safety of Human Adipose Tissue-derived Mesenchymal Stem Cells Transplanted in Nude Mice by High Sensitivity Non-invasive Bioluminescence Imaging

Author

Jerónimo Blanco, Ramon Ayats, Mariano García-Arranz, Carme Fuster, Damián García-Olmo, Marta Vilalta, Mònica Santos, Irene R. Dégano, Juli R. Bagó, Yuti Chernajovsky, David Gould, and Nuria Rubio

Subjects
Adult, Luminescence, Light, Cell Survival, Green Fluorescent Proteins, Population, Mice, Nude, Adipose tissue, Biology, Mesenchymal Stem Cell Transplantation, Cell therapy, Mice, Cell Movement, Transduction, Genetic, Animals, Humans, Bioluminescence imaging, Whole Body Imaging, Luciferases, education, Stem cell transplantation for articular cartilage repair, education.field_of_study, Genome, Muscles, Lentivirus, Mesenchymal stem cell, Mesenchymal Stem Cells, Cell Biology, Hematology, In vitro, Transplantation, Adipose Tissue, Immunology, Cancer research, Female, Developmental Biology
Abstract

Cultivated murine bone marrow mesenchymal stem cells (MSCs) frequently accumulate chromosome abnormalities, become oncogenically transformed, and generate sarcomas when transplanted in mice. Although human MSCs appear to be more resistant, oncogenic transformation has also been observed in MSCs cultivated past the senescence phase. Cell therapy for tissue regeneration using human autologous MSCs requires transplantation of cells previously expanded in vitro. Thus, an important concern is to determine if oncogenic transformation is a necessary outcome of the expansion procedures. We have analyzed the proliferation capacity, organ colonization, and oncogenicity of enhanced green fluorescent protein and luciferase-labeled human adipose tissue-derived mesenchymal stem cells (hAMSCs), implanted in immunocompromised mice during a prolonged time period (8 months) using a non-invasive bioluminescence imaging procedure. Our data indicates that the liver was the preferred target organ for colonization by intramuscular or intravenous implantation of hAMSCs. The implanted cells tended to maintain a steady state, population did not proliferate rapidly after implantation, and no detectable chromosomal abnormalities nor tumors formed during the 8 months of residence in the host's tissues. It would appear that hAMSCs, contrary to their murine correlatives, could be safe candidates for autologous cell therapy procedures since in our experiments they show undetectable predisposition to oncogenic transformation after cultivation in vitro and implantation in mice.

Published
2008

21. Bioluminescence imaging of calvarial bone repair using bone marrow and adipose tissue-derived mesenchymal stem cells

Author

Helen Dimitriou, Jeffrey A. Hubbell, Marta Vilalta, Irene R. Dégano, Annette M. Matthies, Juli R. Bagó, Jerónimo Blanco, Paolo Bianco, and Nuria Rubio

Subjects
Pathology, medicine.medical_specialty, Materials science, Biophysics, Gene Expression, Mice, Nude, Adipose tissue, Bone Marrow Cells, Bioengineering, Bone healing, scaffold, Metastases, Biomaterials, Mice, Cell Movement, Genes, Reporter, Osteogenesis, medicine, Animals, Humans, Regeneration, Bioluminescence imaging, Bone regeneration, Cells, Cultured, Cell Proliferation, Stem cell transplantation for articular cartilage repair, cell differentiation, enhanced green fluorescent protein (egfp), in vivo imaging, luciferase, Mice, Inbred BALB C, Skull, Mesenchymal stem cell, Mesenchymal Stem Cells, Hydrogels, enhanced green fluorescent protein (eGFP), medicine.anatomical_structure, Adipose Tissue, Mechanics of Materials, Differentiation, Luminescent Measurements, Adhesion, Ceramics and Composites, Bone marrow, Stem cell
Abstract

A combined strategy using bioluminescence imaging, bone densitometry and histology was used to analyze the bone regeneration capacity of human bone marrow (hBMSC) and adipose tissue (hAMSC) mesenchymal stem cells, seeded in an osteoconductive arginine-glycine-aspartate (RGD) crosslinked hydrogel scaffold, implanted in a mouse calvarial bone defect. We show that firefly luciferase labeled stem cells can be monitored in vivo through a prolonged 90 days period, during which hBMSCs survive better than hAMSCs and that the density of scaffold bearing defects increased significantly more than that of defects without scaffolds. (c) 2007 Elsevier Ltd. All rights reserved.

Published
2008

22. Analysis of progenitor cell–scaffold combinations by in vivo non-invasive photonic imaging

Author

Irene Román, Erella Livne, Annette M. Matthies, Jerónimo Blanco, Samer Srouji, Jeffrey A. Hubbell, Julio Rodriguez, Marta Vilalta, and Nuria Rubio

Subjects
Luminescence, Biophysics, Mice, Nude, Biocompatible Materials, Bioengineering, Biology, Fluorescence, Hydrogel, Polyethylene Glycol Dimethacrylate, Biomaterials, Mice, Imaging, Three-Dimensional, Tissue engineering, Cell Movement, In vivo, Enzyme Stability, Animals, Progenitor cell, Luciferases, Muscle, Skeletal, Embryonic Stem Cells, Cell Proliferation, Photons, Cell growth, Mesenchymal stem cell, Prostheses and Implants, Embryonic stem cell, Microspheres, Mechanics of Materials, Ceramics and Composites, Stem cell, Preclinical imaging, Biomedical engineering
Abstract

Recent developments in stem cell research have promoted a flourishing of new biomaterials and scaffolds for tissue repair. However, there is a scarcity of procedures to monitor the performance of scaffold-stem cell combinations implanted in live animals, avoiding the inherent artefacts associated with in vitro assay conditions. We report the implementation of a procedure based on the use of the luciferase gene as a cell proliferation tracer to monitor, by in vivo non-invasive imaging, the performance of stem cell-biomaterial combinations used for tissue regeneration. In a model system using immunodepressed mice we show preference of a mouse embryonic mesenchymal cell line (C3H/10T1/2) for specific implantation sites and biomaterials during a prolonged in vivo growth period (3 months). Moreover, we analyzed the safety of implanted cells using a sensitive luminometric procedure and showed that the implanted cells did not spread to other organs. Our results demonstrate the utility of this simple and resource-saving procedure in the development and screening of biomaterials for tissue engineering.

Published
2007

23. Abstract 5124: Tumor and immune cell infiltration are enhanced by irradiation of normal tissues in immunocompromised mice

Author

Edward E. Graves, Amato J. Giaccia, Marjan Rafat, Todd A. Aguilera, and Marta Vilalta

Subjects
Cancer Research, Pathology, medicine.medical_specialty, Stromal cell, medicine.diagnostic_test, medicine.medical_treatment, Cell, Cell migration, Biology, medicine.disease, Flow cytometry, Radiation therapy, medicine.anatomical_structure, Circulating tumor cell, Immune system, Oncology, medicine, Infiltration (medical)
Abstract

Breast cancer recurrence remains high in triple-negative cases despite aggressive surgical, radiological, and chemotherapeutic intervention. Recent studies suggest that circulating tumor cell re-seeding of primary tumors may facilitate recurrence. However, the tumor microenvironment's role in recurrence is not well understood. We hypothesize that the irradiated tumor stroma and microenvironment may influence tumor cell migration. In this study, we characterize the effects of normal tissue irradiation on tumor and immune cell migration to evaluate how tumor-stromal interactions modulate recurrence after therapy. This work represents the first step toward elucidating how stromal tissue radiation response contributes to tumor and immune cell recruitment. Mouse embryonic fibroblasts (MEF) were irradiated to 20 Gy with a cesium source. Supernatant was collected after 2 or 7 d incubation to be used as a chemoattractant in a transwell assay to investigate the induction of 4T1 murine or MDA-MB-231 human mammary carcinoma cell invasion. An orthotopic breast cancer model was used to evaluate the effect of radiation on tumor cell migration to normal tissues. Nude mice were inoculated with luciferase labeled 4T1 or MDA-MB-231 cells in the mammary fat pad (MFP), and BALB/c mice with depleted CD4 and CD8+ T cells were inoculated with 4T1 MFP tumors. The contralateral normal MFP was irradiated to a dose of 20 Gy with a 250 kVp cabinet x-ray machine when tumors were palpable. Cell migration was monitored with bioluminescence imaging (BLI) 10 d after irradiation. Irradiated and control tissues were evaluated using immunohistochemistry (IHC). Tissue sections were stained with F4/80 to determine the extent of macrophage infiltration. Flow cytometry was also performed on dissociated irradiated and control tissues to characterize immune cell populations. Of particular interest were CD11b+F4/80+ macrophages and CD11b+GR1+ myeloid-derived suppressor cells (MDSCs). Radiation enhanced tumor cell migration to normal tissues both in vitro and in vivo. 4T1 and MDA-MB-231 cells exhibited an increase in invasion (p This study establishes that normal tissue radiation response may play a role in modulating tumor and immune cell migration after radiation. The increase in macrophage and MDSC infiltration after irradiation indicates the immune contribution in tumor cell migration. These results suggest that the tumor stroma may facilitate tumor cell invasion and tumor regrowth following radiotherapy. Citation Format: Marjan Rafat, Marta Vilalta, Todd A. Aguilera, Amato J. Giaccia, Edward E. Graves. Tumor and immune cell infiltration are enhanced by irradiation of normal tissues in immunocompromised mice. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 5124.

Published
2016

24. Abstract 1645: Tumor-associated macrophages enhance DNA damage repair and improve survival of murine breast cancers after irradiation

Author

Marjan Rafat, Edward E. Graves, Luis A. Soto, Marta Vilalta Colomer, and Amato J. Giaccia

Subjects
Cancer Research, Angiogenesis, DNA damage, Cell, Macrophage polarization, Cancer, Biology, medicine.disease, medicine.anatomical_structure, Oncology, Tumor progression, Immunology, medicine, biology.protein, Cancer research, Macrophage, Antibody
Abstract

Tumor-associated macrophages (TAMs) are known to promote physiological processes that drive tumor progression and survival, including angiogenesis, immunosuppression, and invasion. While most studies on TAMs have focused on the molecular mechanisms by which TAMs drive these processes, less focus has been given to direct effects that TAMs may exert on tumor cells. It is known that monocytes are recruited to tumor sites after radiotherapy and support tumor regrowth. In this study we sought to determine if TAMs are able to exert a direct, protective effect on tumor cells against radiotherapy in vitro. We used murine 4T1 cells, a well-characterized animal model for breast cancer, and murine RAW264.7 macrophages to carry out co-culture experiments. Co-culture of 4T1 cells with RAW264.7 macrophages resulted in increased 4T1 cell survival rates post-irradiation compared to 4T1 cells cultured alone. We further determined that this effect is not contact-dependent but mediated through macrophage secreted factors. Next, we tested whether co-culturing RAW264.7 macrophages with 4T1 cells induced macrophage polarization to an M2/TAM phenotype. Using antibodies against M2 markers and FACS, we found that co-culture of RAW macrophages with 4T1 cells polarizes these macrophages toward an M2 phenotype. We hypothesized that the increased 4T1 cell survival rates were mediated by an enhanced DNA damage repair mechanism induced by TAMs. We tested this via a combination of immunofluorescence against phosphorylated histone H2AX and comet assays. We show that co-culture of 4T1 cells with TAMs after irradiation results in lower 4T1 cell levels of DNA damage and a faster decrease in DNA damage over time compared to 4T1 cells alone. Future work will focus on characterizing the molecular mechanism through which TAMs induce this enhanced DNA damage repair response in 4T1 cells after irradiation and we will test whether such response occurs in vivo after radiotherapy. In conclusion, we show that TAMs confer resistance against ionizing radiation to tumor cells in vitro and that this resistance is driven by an enhanced DNA damage repair mechanism in tumor cells induced by TAM secreted factors. Citation Format: Luis A. Soto, Marjan Rafat, Marta Vilalta Colomer, Amato Giaccia, Edward Graves. Tumor-associated macrophages enhance DNA damage repair and improve survival of murine breast cancers after irradiation. [abstract]. In: Proceedings of the 107th Annual Meeting of the American Association for Cancer Research; 2016 Apr 16-20; New Orleans, LA. Philadelphia (PA): AACR; Cancer Res 2016;76(14 Suppl):Abstract nr 1645.

Published
2016

25. Apuntes para el análisis del patrón de asentamiento en Tulum

Author

Patricia Santillán S., Marta Vilalta C., and Ernesto Vargas Pacheco

Subjects
Cultural Studies, Archeology, Anthropology
Abstract

Los sitios prehispánicos de la costa oriental de Quintana Roo han tenido siempre un lugar especial en la arqueología maya; se localizan a lo largo de la costa y en las cercanías de la misma; son tan abundantes que no dejan la menor duda que la región estuvo densamente poblada en tiempos prehispánicos (Andrews 1976: 10) (Fig. 1). Quintana Roo se puede dividir en tres provincias geográficas: la sur, cubierta por el bosque tropical y que se extiende un poco a la región central, la cual se caracteriza por el bosque tropical seco, y por ultimo la zona del norte que se localiza en la costa oriental y toda la parte norte.

Published
2013

27. Facilitating multimodal preclinical imaging studies in mice by using an immobilization bed

Author

Geoffrey S, Nelson, Jessica, Perez, Marta, Vilalta, Marta V, Colomer, Rehan, Ali, and Edward, Graves

Subjects
Immobilization, Mice, Sodium Radioisotopes, Neoplasms, Positron-Emission Tomography, Animals, Mice, Nude, Reproducibility of Results, Mouse Models, Tomography, X-Ray Computed, Multimodal Imaging
Abstract

We have designed an immobilization bed that accommodates mice of all ages and sizes, to improve image registration for multimodal scans and for longitudinal preclinical imaging studies. Stationary pegs were placed such that they effectively immobilized mice and reduced set-up time. (22)Na fiducial markers were placed into the pegs at unique depths to provide 3D references to facilitate image registration. Multiple users registered positron emission tomographic (PET) and CT data obtained with and without the bed to examine the effect of the bed on registration accuracy and interuser variability. The image registrations performed by different users were evaluated for their similarity by using the Entropy Correlation Coefficient as a metric. The immobilization bed significantly reduced variations in body movement and interuser variability. Average differences in quantification of tumor PET signal among users when registering images without versus with the fiduciary-marker bed fell from 9.1% to 0.8% for maximal percentage injected dose per gram (%ID/g), from 15.6% to 2.3% for mean %ID/g, and from 9.4% to 0.7% for the 90th percentile of the maximum %ID/g. The bed improves animal immobilization, greatly reduces interuser variability, and supports registration of image data acquired from different imaging sessions.

Published
2012

28. Abstract 1460: AKAP12 regulates melanoma tumor growth and metastasis

Author

Marta Vilalta, Elizabeth C. Finger, Erinn B. Rankin, Alice Banh, Amato J. Giaccia, Marianne Broome-Powell, and Adam J. Krieg

Subjects
Cancer Research, Pathology, medicine.medical_specialty, Kinase, business.industry, Melanoma, Cancer, medicine.disease, Primary tumor, Metastasis, Oncology, medicine, Cancer research, Skin cancer, Cell adhesion, business, Clonogenic assay
Abstract

Skin cancer, which accounts for at least half of all cancers in the United States, is predicted to affects 1 in 5 Americans in their lifetime. Melanoma, the most serious form of skin cancer, is also the leading cause of all skin cancer deaths. This study demonstrates that AKAP12 (SSeCKS, AKAP250, gravin), a hypoxia-inducible scaffold protein, is considerably increased at the protein and RNA level in melanoma cell lines. In addition, there is a significant increase in RNA expression in primary and metastatic tumors when compared to normal specimens, as well as patients with poor prognosis, as measured by diminished 5- year survival. AKAP12 functions to dock many kinases and signaling proteins that regulate cell adhesion, spreading and migration, including: PKC, Src and F-actin. Since these processes are critical for tumor cell metastasis, we hypothesize that AKAP12 could be a central regulator of cancer progression. Stable knockdown of AKAP12 in two melanoma cell lines demonstrate decreases in invasion, migration and clonogenic potential in vitro, as well reduced colony forming abilities in conditions requiring anchorage-independent growth in soft agar. In vivo studies in a metastatic model of melanoma demonstrate a statistically significant decrease in tumors within the lungs of the AKAP12 knockdown groups, highlighting the importance of AKAP12 in metastatic disease. An orthotopic model also demonstrates decreased primary tumor growth and metastatic potential in mice injected with AKAP12 knocked down cells. Additionally, changes in cell morphology characteristic of increased motility and invasiveness are seen in cells containing AKAP12 but not those in which it had been knocked down. While this scaffold protein has been found to act as a tumor suppressor in several tissue types (lung, colon, prostate), we have uncovered its novel oncogenic properties in metastatic melanoma. Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 102nd Annual Meeting of the American Association for Cancer Research; 2011 Apr 2-6; Orlando, FL. Philadelphia (PA): AACR; Cancer Res 2011;71(8 Suppl):Abstract nr 1460. doi:10.1158/1538-7445.AM2011-1460

Published
2011

29. TH-C-204B-04: Assessing the Potential of Cerenkov Radiation for in Vivo Imaging of Tumor Hypoxia

Author

Marta Vilalta, Edward E. Graves, Rehan Ali, and J Noll

Subjects
Biodistribution, Tumor hypoxia, business.industry, Tumor biology, Chemistry, medicine.medical_treatment, Intraperitoneal injection, General Medicine, Nuclear magnetic resonance, Medical imaging, medicine, Nuclear medicine, business, Human colon, Preclinical imaging, Cherenkov radiation
Abstract

Purpose: To assess whether in vivooptical imaging using Cerenkov radiation can (a) produce results that are comparable to those from microPET tumorimaging and (b) provide information that facilitates future dual‐tracer imaging experiments. Method and Materials: (a) Subcutaneous tumors were established by injecting HT‐29 human colon adenocarcinoma cells into the shoulders of 4 nude mice and were grown until they reached a volume of 1cm3. 200microCi of 18F‐EF5 was injected via intraperitoneal injection and 3 mice were imaged using microPET whilst the other was imaged in an IVIS Spectrum.Images were acquired immediately and 1 hour following injection on both machines using acquisition times of 10mins (PET) and 2mins (IVIS). (b) A mathematical model of the Cerenkov emission spectrum was developed and used to predict the ability of Cerenkov imaging to resolve signals from different tracers. Results: (a) In the initial PET and IVIS images the tracer signal was confined to the region of the gastrointestinal region and there was no accumulation in the tumor. After 1 hour both sets of images showed similar biodistribution throughout the body along with uptake in the tumor. (b) The model predicted that different radionuclides can be distinguished through an energy‐dependent red‐shift in their emission spectra leading to higher intensity signals in the optical spectrum.Conclusion: We have shown that 18F‐EF5 Cerenkov imaging of subcutaneous tumors can be performed optically. More specifically our results show that the biodistribution and tumor uptake observed using this technique is in agreement with the microPET data. Our modeling suggests that the spectral differences between radionuclides coupled with the differences in decay rates between tracers labeled with different radioisotopes could be used to develop techniques for separating signals from two tracers for surface‐level tumors thus potentially allowing multiple aspects of tumor biology to be imaged simultaneously.

Published
2010

30. SU-GG-J-131: Immobilization Bed for Multi-Modality Image Registration

Author

Magdalena Bazalova, J Perez, Edward E. Graves, Marta Vilalta, and G Nelson

Subjects
medicine.diagnostic_test, business.industry, Image registration, High throughput imaging, General Medicine, Multi modality, Optical imaging, Positron emission tomography, medicine, Medical imaging, Radiation treatment planning, Fiducial marker, business, Nuclear medicine
Abstract

Purpose: To construct an immobilization bed for mice that will allow for longitudinal multimodality imaging studies as well as conformai radiotherapy. The bed must be capable of both intra‐examination immobilization as well as inter‐examination positioning reproducibility. It must also accommodate mice of various sizes and facilitate image registration.Method and Materials: An immobilization bed was manufactured from clear acrylic to enable use with optical imaging modalities. Measurements of multiple mice of various ages and species were made in order to find the optimal size for the bed and for the restrainer pegs. The pegs were placed in stationary positions that effectively immobilize the majority of mice and enable high throughput imaging by avoiding adjustments for every mouse. The pegs were placed such that the front legs of the subject are each placed between two pegs as are the hind legs. An additional set of pegs were placed laterally and posteriorly to guide the hind legs in a reproducible direction. Na‐22 PET/CT fiducials were put into the pegs at unique depths to provide a three‐dimensional reference to allow fast and accurate image registration.Results: An average sized nude mouse without anesthesia (a worst case scenario test) was only capable of 3mm of movement vertically. Serial CT scans in‐between which the bed was moved showed no shifts in bony anatomy or external soft tissues. When PET and CT scans were registered without use of the fiducials, the heart was misplaced medially by ∼1mm and inferiorly by ∼1mm. The fiducials have allowed for accurate CT registration. Conclusion: The bed is effective in immobilization and image registration. The use of this bed will be enable the elucidation of minute changes in the PET scans and the use of molecular imaging data for radiation treatment planning and followup.

Published
2010

31. 72 poster: Molecular Imaging of Radiation Response in Preclinical Models Using a Novel Small Animal Radiotherapy System

Author

Magdalena Bazalova, Marta Vilalta, Edward E. Graves, Jessica R. Perez, Amato J. Giaccia, and G Nelson

Subjects
Radiation therapy, medicine.medical_specialty, Oncology, business.industry, Small animal, medicine.medical_treatment, Medicine, Radiology, Nuclear Medicine and imaging, Medical physics, Hematology, Molecular imaging, business, Radiation response
Published
2010

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