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4. Mrs. L.C. Hanna

Author

The Cleveland Museum of Art and The Cleveland Museum of Art

Published
1931

5. Development of Novel Patient-Derived Xenografts from Breast Cancer Brain Metastases

Author

María J. Contreras-Zárate, D. Ryan Ormond, Austin E. Gillen, Colton Hanna, Nicole L. Day, Natalie J. Serkova, Britta M. Jacobsen, Susan M. Edgerton, Ann D. Thor, Virginia F. Borges, Kevin O. Lillehei, Michael W. Graner, Peter Kabos, and Diana M. Cittelly

Subjects
patient-derived xenograft, brain metastases models, breast cancer, brain colonization, triple negative, HER2+, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282
Abstract

Brain metastases are an increasing burden among breast cancer patients, particularly for those with HER2+ and triple negative (TN) subtypes. Mechanistic insight into the pathophysiology of brain metastases and preclinical validation of therapies has relied almost exclusively on intracardiac injection of brain-homing cells derived from highly aggressive TN MDA-MB-231 and HER2+ BT474 breast cancer cell lines. Yet, these well characterized models are far from representing the tumor heterogeneity observed clinically and, due to their fast progression in vivo, their suitability to validate therapies for established brain metastasis remains limited. The goal of this study was to develop and characterize novel human brain metastasis breast cancer patient-derived xenografts (BM-PDXs) to study the biology of brain metastasis and to serve as tools for testing novel therapeutic approaches. We obtained freshly resected brain metastases from consenting donors with breast cancer. Tissue was immediately implanted in the mammary fat pad of female immunocompromised mice and expanded as BM-PDXs. Brain metastases from 3/4 (75%) TN, 1/1 (100%) estrogen receptor positive (ER+), and 5/9 (55.5%) HER2+ clinical subtypes were established as transplantable BM-PDXs. To facilitate tracking of metastatic dissemination using BM-PDXs, we labeled PDX-dissociated cells with EGFP-luciferase followed by reimplantation in mice, and generated a BM-derived cell line (F2-7). Immunohistologic analyses demonstrated that parental and labeled BM-PDXs retained expression of critical clinical markers such as ER, progesterone receptor, epidermal growth factor receptor, HER2, and the basal cell marker cytokeratin 5. Similarly, RNA sequencing analysis showed clustering of parental, labeled BM-PDXs and their corresponding cell line derivative. Intracardiac injection of dissociated cells from BM-E22-1, resulted in magnetic resonance imaging-detectable macrometastases in 4/8 (50%) and micrometastases (8/8) (100%) mice, suggesting that BM-PDXs remain capable of colonizing the brain at high frequencies. Brain metastases developed 8–12 weeks after ic injection, located to the brain parenchyma, grew around blood vessels, and elicited astroglia activation characteristic of breast cancer brain metastasis. These novel BM-PDXs represent heterogeneous and clinically relevant models to study mechanisms of brain metastatic colonization, with the added benefit of a slower progression rate that makes them suitable for preclinical testing of drugs in therapeutic settings.

Published
2017
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6. Estrogen promotes the brain metastatic colonization of triple negative breast cancer cells via an astrocyte-mediated paracrine mechanism

Author

Diana M. Cittelly, Colton Hanna, Patricia S. Steeg, Virginia F. Borges, Kendra M. Huber, Troy Schedin, Carol A. Sartorius, Peter Kabos, Hazel Cruz, Brunilde Gril, and Natalie J. Serkova

Subjects
0301 basic medicine, Cancer Research, TGF alpha, Stromal cell, medicine.drug_class, Mice, Nude, Triple Negative Breast Neoplasms, Biology, Article, 03 medical and health sciences, Paracrine signalling, Mice, 0302 clinical medicine, breast cancer, Cell Movement, Cell Line, Tumor, Paracrine Communication, Genetics, medicine, estrogen, Animals, Humans, brain metastasis, Neoplasm Invasiveness, Epidermal growth factor receptor, Molecular Biology, Triple-negative breast cancer, EGF, Estradiol, Brain Neoplasms, astrocytes, estrogen receptors, Estrogens, 3. Good health, ErbB Receptors, 030104 developmental biology, medicine.anatomical_structure, Cell Transformation, Neoplastic, Estrogen, 030220 oncology & carcinogenesis, Gene Knockdown Techniques, Immunology, Cancer research, biology.protein, Astrocyte
Abstract

Brain metastases (BM) are a devastating consequence of breast cancer. BM occur more frequently in patients with estrogen receptor-negative (ER-) breast cancer subtypes; HER2 overexpressing (HER2+) tumors and triple-negative (TN) (ER-, progesterone receptor-negative (PR-) and normal HER2) tumors. Young age is an independent risk factor for the development of BM, thus we speculated that higher circulating estrogens in young, pre-menopausal women could exert paracrine effects through the highly estrogen-responsive brain microenvironment. Using a TN experimental metastases model, we demonstrate that ovariectomy decreased the frequency of magnetic resonance imaging-detectable lesions by 56% as compared with estrogen supplementation, and that the combination of ovariectomy and letrozole further reduced the frequency of large lesions to 14.4% of the estrogen control. Human BM expressed 4.2-48.4% ER+ stromal area, particularly ER+ astrocytes. In vitro, E2-treated astrocytes increased proliferation, migration and invasion of 231BR-EGFP cells in an ER-dependent manner. E2 upregulated epidermal growth factor receptor (EGFR) ligands Egf, Ereg and Tgfa mRNA and protein levels in astrocytes, and activated EGFR in brain metastatic cells. Co-culture of 231BR-EGFP cells with E2-treated astrocytes led to the upregulation of the metastatic mediator S100 Calcium-binding protein A4 (S100A4) (1.78-fold, P

Published
2015

7. Development of Novel Patient-Derived Xenografts from Breast Cancer Brain Metastases

Author

D. Ryan Ormond, Virginia F. Borges, Ann D. Thor, Natalie J. Serkova, Maria J. Contreras-Zarate, Michael W. Graner, Susan M. Edgerton, Peter Kabos, Colton Hanna, Nicole L. Day, Diana M. Cittelly, Britta M. Jacobsen, Kevin O. Lillehei, and Austin E. Gillen

Subjects
0301 basic medicine, HER2+, Cancer Research, Pathology, medicine.medical_specialty, brain colonization, patient-derived xenograft, Estrogen receptor, lcsh:RC254-282, triple negative, 03 medical and health sciences, Cytokeratin, 0302 clinical medicine, Breast cancer, breast cancer, Progesterone receptor, Medicine, Epidermal growth factor receptor, Original Research, biology, business.industry, Cancer, Human brain, medicine.disease, lcsh:Neoplasms. Tumors. Oncology. Including cancer and carcinogens, 3. Good health, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, brain metastases models, biology.protein, business, Brain metastasis
Abstract

Brain metastases are an increasing burden among breast cancer patients, particularly for those with HER2+ and triple negative (TN) subtypes. Mechanistic insight into the pathophysiology of brain metastases and preclinical validation of therapies has relied almost exclusively on intracardiac injection of brain-homing cells derived from highly aggressive TN MDA-MB-231 and HER2+ BT474 breast cancer cell lines. Yet, these well characterized models are far from representing the tumor heterogeneity observed clinically and, due to their fast progression in vivo, their suitability to validate therapies for established brain metastasis remains limited. The goal of this study was to develop and characterize novel human brain metastasis breast cancer patient-derived xenografts (BM-PDXs) to study the biology of brain metastasis and to serve as tools for testing novel therapeutic approaches. We obtained freshly resected brain metastases from consenting donors with breast cancer. Tissue was immediately implanted in the mammary fat pad of female immunocompromised mice and expanded as BM-PDXs. Brain metastases from 3/4 (75%) TN, 1/1 (100%) estrogen receptor positive (ER+), and 5/9 (55.5%) HER2+ clinical subtypes were established as transplantable BM-PDXs. To facilitate tracking of metastatic dissemination using BM-PDXs, we labeled PDX-dissociated cells with EGFP-luciferase followed by reimplantation in mice, and generated a BM-derived cell line (F2-7). Immunohistologic analyses demonstrated that parental and labeled BM-PDXs retained expression of critical clinical markers such as ER, progesterone receptor, epidermal growth factor receptor, HER2, and the basal cell marker cytokeratin 5. Similarly, RNA sequencing analysis showed clustering of parental, labeled BM-PDXs and their corresponding cell line derivative. Intracardiac injection of dissociated cells from BM-E22-1, resulted in magnetic resonance imaging-detectable macrometastases in 4/8 (50%) and micrometastases (8/8) (100%) mice, suggesting that BM-PDXs remain capable of colonizing the brain at high frequencies. Brain metastases developed 8–12 weeks after ic injection, located to the brain parenchyma, grew around blood vessels, and elicited astroglia activation characteristic of breast cancer brain metastasis. These novel BM-PDXs represent heterogeneous and clinically relevant models to study mechanisms of brain metastatic colonization, with the added benefit of a slower progression rate that makes them suitable for preclinical testing of drugs in therapeutic settings.

Published
2017
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8. Labeling of Breast Cancer Patient-derived Xenografts with Traceable Reporters for Tumor Growth and Metastasis Studies

Author

Diana M. Cittelly, Letty Kwok, Colton Hanna, Jessica Finlay-Schultz, and Carol A. Sartorius

Subjects
0301 basic medicine, Genetically modified mouse, Pathology, medicine.medical_specialty, General Chemical Engineering, Transplantation, Heterologous, Heterologous, Breast Neoplasms, Article, General Biochemistry, Genetics and Molecular Biology, Metastasis, Mice, 03 medical and health sciences, Transduction (genetics), 0302 clinical medicine, Breast cancer, Transduction, Genetic, Animals, Humans, Medicine, Neoplasm Metastasis, General Immunology and Microbiology, business.industry, Gene Expression Profiling, General Neuroscience, Transfection, medicine.disease, Xenograft Model Antitumor Assays, Transplantation, Gene expression profiling, 030104 developmental biology, 030220 oncology & carcinogenesis, Luminescent Measurements, Heterografts, business
Abstract

The use of preclinical models to study tumor biology and response to treatment is central to cancer research. Long-established human cell lines, and many transgenic mouse models, often fail to recapitulate the key aspects of human malignancies. Thus, alternative models that better represent the heterogeneity of patients' tumors and their metastases are being developed. Patient-derived xenograft (PDX) models in which surgically resected tumor samples are engrafted into immunocompromised mice have become an attractive alternative as they can be transplanted through multiple generations,and more efficiently reflect tumor heterogeneity than xenografts derived from human cancer cell lines. A limitation to the use of PDXs is that they are difficult to transfect or transduce to introduce traceable reporters or to manipulate gene expression. The current protocol describes methods to transduce dissociated tumor cells from PDXs with high transduction efficiency, and the use of labeled PDXs for experimental models of breast cancer metastases. The protocol also demonstrates the use of labeled PDXs in experimental metastasis models to study the organ-colonization process of the metastatic cascade. Metastases to different organs can be easily visualized and quantified using bioluminescent imaging in live animals, or GFP expression during dissection and in excised organs. These methods provide a powerful tool to extend the use of multiple types of PDXs to metastasis research.

Published
2016
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9. Abstract A09: Development of novel breast cancer brain-metastases-derived xenografts and cell lines

Author

David Ormond, Virginia F. Borges, Carol A. Sartorius, Diana M. Cittelly, Britta M. Jacobsen, Michael W. Graner, Colton Hanna, Kevin O. Lillehei, and Peter Kabos

Subjects
Cancer Research, business.industry, Cell, Cancer, Human brain, medicine.disease, Metastatic breast cancer, medicine.anatomical_structure, Breast cancer, Oncology, Cell culture, Parenchyma, Cancer research, Medicine, business, Molecular Biology, Brain metastasis
Abstract

Symptomatic brain metastases develop in 10 to 16% of patients with metastatic breast cancer and the prognosis of these patients is dismal with a mortality rate of near 80% within 1 year of diagnosis. Understanding the mechanisms by which breast cancer cells adapt to the brain microenvironment is key to design therapies that could be used to prevent or treat brain metastases. To date, the field has relied almost exclusively on intracardiac (ic) injection of brain-homing cells derived from highly aggressive triple negative (TN) MDA-MB-231 and HER2+ BT474 (BT474BR) cell lines to study these interactions. Although these are well characterized models, these are far from representing the heterogeneity observed in breast tumors and their metastases. Purpose: The goal of this study was to develop and characterize novel human brain metastases patient-derived xenografts (BM-PDX) to study the biology of brain metastases and to serve as tools for testing novel therapeutic approaches. We have also developed a labeling method to tag these PDXs with traceable markers for in vivo studies. Experimental procedures: Metastatic tissue was removed from brain parenchyma during surgery (n=5) or from cerebral spinal fluid (CSF) via catheter (n=1) from consenting donors harboring TN (n=3) or HER2+ (n=3) metastatic breast cancer. Tissue was immediately implanted in the mammary fat pad of NOD/SCID/GAMMA female mice and tumor expanded as solid tumors (BM-PDX). Upon reaching a volume of >200 mm3, partitioned pieces were transplanted into new recipient mice and growth kinetics measured. In order to track metastatic spread using PDXs, we developed a protocol to label PDX-dissociated cells with GFP-luciferin followed by re-implantation in mice. Tumor sections before and after labeling were immunostained for hormone receptors (estrogen, progesterone and androgen receptors –ER, PR, AR), HER2, and the basal cell marker cytokeratin 5 (CK5). These were scored by a pathologist. Dissociated cells from an established BM-PDX were cultured under different conditions in vitro, to generate a BM-derived cell line. Gene expression profiling was performed in some PDX before and after GFP-luciferase labeling, and in derived cell lines. Dissociated cells from BM-PDXs (E22-1) were injected intracardially (n=5) to measure their ability to colonize the brain in an experimental model of brain metastasis. Summary: Three of 3 TN brain metastases were successfully established as transplantable PDXs, while 0 of 3 HER2+ tumors grew in mice. Immunohistochemical analyses demonstrated that BM-PDXs retain morphology and markers comparable to those of donor samples. Labeled tumors grew in the mammary fat pad without spontaneous metastatic spread as measured via in vivo imaging (IVIS). Intracardiac injection of dissociated cells from BM-PDX E22-1 resulted in micro or macrometastases in 5/5 (100%) injected mice, indicating that BM-PDXs remain capable of colonizing the organ of origin. Metastases developed in brain parenchyma, surrounding vessels, with associated microglia and astroglia activation, similar to what is observed in human brain metastases. BM-PDX dissociated cells were cultured under different conditions to derive BM-cell lines. Two cell lines have been derived from a TN BM-PDX (F2-6) after in vitro culture using brain-like media or primary cell media. RNAseq analyses to fully characterize the genetic makeup of BM-PDX and cell line derivatives are currently in progress. Conclusions: We have developed novel PDXs derived from breast cancer brain metastases, which retain their ability to colonize the brain when disseminated in circulation. These novel GFP-luciferase labeled xenografts and cell lines, represent unique tools to study brain metastasis biology and to test novel therapeutic treatments for brain metastasis in clinically relevant models. Citation Format: Colton Hanna, Britta M. Jacobsen, Carol A. Sartorius, Peter Kabos, Kevin Lillehei, David R. Ormond, Michael Graner, Virginia F. Borges, Diana M. Cittelly. Development of novel breast cancer brain-metastases-derived xenografts and cell lines. [abstract]. In: Proceedings of the AACR Special Conference on Advances in Breast Cancer Research; Oct 17-20, 2015; Bellevue, WA. Philadelphia (PA): AACR; Mol Cancer Res 2016;14(2_Suppl):Abstract nr A09.

Published
2016
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10. The Picassos in the 1901 Vollard Exhibition and Their History.

Author

Mallen, Enrique

Subjects
CATALOGS, EXHIBITIONS, YOUNG artists, CAREER changes, ART museums, CUBAN Missile Crisis, 1962
Abstract

This article describes Picasso's first visit to the French capital in 1900, and the events that led to his first major exhibition at the acclaimed Galerie Ambroise Vollard in Paris in 1901. The first section provides a narrative of his early experiences abroad as a young unknown artist, his influences, and the contacts he established with friends, artists and dealers during this important period of his career; the second section traces the histories of the sixty-five artworks that were exhibited, identifying the collections those items went through after they were exhibited, their current locations, as well as the exhibitions in which they have been featured since Vollard first displayed them in his gallery. The last section elaborates on some of the immediate repercussions of the exhibition. The reported findings are the result of extensive research on hundreds of books and catalogs published on Pablo Picasso from 1901 to the present. The new facts we have uncovered are published here for the first time. Readers of the article will learn that the works included in Picasso's first exhibition in France have been part of the most prestigious art collections, such as those of Justin K. Thannhauser, Gertrude Stein, Chester Dale, Paul Guillaume, Walter P. Chrysler, Jr., Paul Mellon, Helena Rubinstein, Alfred Flechtheim, Walter C. Arensberg, among others. The works have also been featured in such important overviews of his career as "Picasso, 75th Anniversary" 1957–1958, and "Picasso: An American Tribute", 1962. Thus, while Vollard claimed that the exhibition at his gallery had no major impact, the facts show that it not only played an important role in Picasso's acceptance as a groundbreaking newcomer, but also left a significant mark on the rest of his career, as evidenced by the works' inclusion in the retrospectives held in Paris and Zürich in 1932, and New York in 1980. [ABSTRACT FROM AUTHOR]

Published
2023
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18. Cleveland's Millionaires' Row

Author

Alan F. Dutka and Alan F. Dutka

Subjects
Historic buildings--Ohio--Cleveland--Pictorial works, Millionaires--Ohio--Cleveland--Pictorial works, Mansions--Ohio--Cleveland--History--Pictorial works
Abstract

The incredible affluence and extravagance of Euclid Avenue's Millionaires'Row have fascinated Clevelanders for more than a century. Within these stately mansions, US presidents enjoyed dinners and discussions with powerful politicians and influential industrial and banking leaders. Through photographs and meticulously researched captions, Cleveland's Millionaires'Row provides authoritative visual and written answers to the most often-asked questions regarding the famous avenue: where were these mansions located, how did their occupants acquire such enormous wealth, what caused the street's demise, and what replaced the famous old homes? The book also reveals the progress in remaking Euclid Avenue's four-mile stretch from Public Square to University Circle. Cleveland's Millionaires'Row vividly illustrates the birth, glamor, decline, and renaissance of the grand old avenue.

Published
2019

19. The Letters of Cole Porter

Author

Cole Porter, Cliff Eisen, Dominic McHugh, Cole Porter, Cliff Eisen, and Dominic McHugh

Subjects
Composers--United States--Correspondence
Abstract

The first comprehensive collection of the letters of one of the most successful American songwriters of the twentieth century From Anything Goes to Kiss Me, Kate, Cole Porter left a lasting legacy of iconic songs including'You're the Top,''Love For Sale,'and'Night and Day.'Yet, alongside his professional success, Porter led an eclectic personal life which featured exuberant parties, scandalous affairs, and chronic health problems. This extensive collection of letters (most of which are published here for the first time) dates from the first decade of the twentieth century to the early 1960s and features correspondence with stars such as Irving Berlin, Ethel Merman, and Orson Welles, as well as his friends and lovers. Cliff Eisen and Dominic McHugh complement these letters with lively commentaries that draw together the loose threads of Porter's life and highlight the distinctions between Porter's public and private existence. This book reveals surprising insights into his attitudes toward Hollywood and Broadway, and toward money, love, and dazzling success.

Published
2019

20. Pablo Picasso : The Interaction Between Collectors and Exhibitions, 1899-1939

Author

Dr Enrique Mallen and Dr Enrique Mallen

Subjects
Art--Economic aspects--History--20th century, Art--Collectors and collecting--History--20th century
Abstract

This book explores the interaction between collectors, dealers and exhibitions in Pablo Picassos entire career. The former two often played a determining role in which artworks were included in expositions as well as their availability and value in the art market. The term collector/dealer must often be used in combination since the distinction between both is often unclear; Heinz Berggruen, for instance, identified himself primarily as a collector, although he also sold quite a few Picassos through his Paris gallery. On the whole, however, dealers bought more often than collectors; and they bought works by artists they were already involved with. While some dealers were above all professional gallery owners; most were mainly collectors who sporadically sold items from their collection. Picassos first known dealer was Pere Manyach, whom he met as he travelled to Paris in 1900 when he was only 19 years old. As his representative, Manyach went about setting up exhibitions of his works at galleries in the French capital, such as Bethe Weills and Ambroise Vollards. Picassos first major exhibition took place in 1901 at Vollards. Daniel-Henry Kahnweiler and Leonce Rosenberg came in after Vollard lost interest during the Cubist period, as they had a manifest preference for the new style. Like Vollard, later dealers often preferred the more conventional Neoclassical phase in Picasso. This was the case with Leonces brother, Paul Rosenberg. The book is organized chronologically and discusses the interaction between Picassos collectors, dealers and exhibitions as they take place. Once collectors acquired an artwork, their willingness to lend them to exhibitions or their necessity to submit them to auction had a direct impact on Picassos prominence in the art world.

Published
2018

21. Cleveland in the Gilded Age : A Stroll Down Millionaires' Row

Author

Dan Ruminski, Alan Dutka, Dan Ruminski, and Alan Dutka

Subjects
Millionaires--Ohio--Cleveland--Biography, Millionaires--Homes and haunts--Ohio--Clevel, Historic buildings--Ohio--Cleveland, Mansions--History.--Ohio--Cleveland
Abstract

Cleveland storyteller Dan Ruminski discovered that the 6 acres under his home were originally part of a 1,400-acre grand estate known as the Circle W Farm.The impressive estate was created by Walter White, founding brother of the White Motor Company. Drawn in by the fascinating history, Ruminski's investigation soon embraced the full legacy of Cleveland's industrial history and the indomitable characters who created the city's Gilded Age. John D. Rockefeller, Samuel Mather and more giants of industry built Cleveland's Millionaires'Row. Come peek inside the once-grand mansions these millionaires called home and hear the delightful stories that bring the past to life. Join Ruminski and Alan Dutka on a return to this section of Euclid Avenue, which wasn't merely the most stunning show of wealth in Cleveland but also in the entire country.

Published
2012

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