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148 results on '"James E. Fitzpatrick"'

1. Loren Golitz

Author

James E. Fitzpatrick, Whitney A. High, Lori Prok, and Joshua Wisell

Subjects
business.industry, Medicine, Dermatology, Obituary, Theology, business
Published
2021
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2. Beyond Theory and Degrees : The Alley Smarts of Educational Leadership

Author

James E. Fitzpatrick and James E. Fitzpatrick

Subjects
Educational leadership--United States, School management and organization--United State, School districts--Administration--United State
Abstract

This book is a must read for anyone who has a passion for leadership. Fitzpatrick's style and story presentation could be a blueprint for any leader in any profession. His insights into building a culture of leaders, through mentoring and distributing responsibility in growing the capacity of an organization while celebrating and affirming people are the tenants of his approach to authentic accountability, where people when feeling valued become invested and perform at a high level! In the book Fitzpatrick shares the POCDICE theory, the seven key processes of Leadership that every aspiring and seasoned leaders must become good at, while never becoming complacent in improving in their roles. They are: planning, organization, communication, decision-making, influence, coordination, and evaluation.School Leadership and Governance in American schools is at a crossroads. Fewer candidates are entering this noble and honorable profession. We need great leaders for our schools and districts to flourish. This book is designed to inspire candidates to consider school and district leadership while giving insight into school governance from the principalship, superintendency, and Board of Education levels.

Published
2020

3. Contextual role of E2F1 in suppression of melanoma cell motility and invasiveness

Author

Addanki P. Kumar, Rita Ghosh, Roble Bedolla, Peng Meng, James E. Fitzpatrick, and Huiyoung Yun

Subjects
0301 basic medicine, MAPK/ERK pathway, Proto-Oncogene Proteins B-raf, endocrine system, Cancer Research, Myosin light-chain kinase, Skin Neoplasms, MAP Kinase Signaling System, Biology, 03 medical and health sciences, 0302 clinical medicine, Cell Movement, Cell Line, Tumor, medicine, E2F1, Humans, Neoplasm Invasiveness, Phosphorylation, neoplasms, Molecular Biology, Melanoma, Kinase, MYLK, medicine.disease, 030104 developmental biology, Drug Resistance, Neoplasm, 030220 oncology & carcinogenesis, Lymphatic Metastasis, Cancer cell, Mutation, Cancer research, biological phenomena, cell phenomena, and immunity, V600E, E2F1 Transcription Factor
Abstract

The general transcription factor E2F1 reportedly functions in a protumorigenic manner in several cancer models. We show that the genetic context of cancer cells influence E2F1's role to impede the protumorigenic role. Thirty to fifty percent of melanoma patients carry mutant BRAF with about 90% of mutant BRAF melanomas being V600E mutation. Tissue microarrays from melanoma patients were used to establish an association between E2F1 and BRAFV600E . We show for the first time that low E2F1 levels in BRAFV600E melanomas are associated with lymph node metastasis. Genetic manipulation of E2F1 in BRAFV600E and BRAFwt cells were used to determine its role in malignant melanoma progression by examining effects on migration and invasion. E2F1-mediated negative regulation of myosin light chain kinase (MYLK) increased migration and invasion in BRAFV600E cells by phosphorylating myosin light chain and increased stress fiber formation. We show that E2F1 inhibits extracellular signal-regulated kinase (ERK) activation in BRAFV600E cells and provide evidence for a negative feedback loop between E2F1 and ERK in these cells. This study shows for the first time that E2F1 has a cancer protective role in oncogenic BRAF-activated melanoma cells and that loss of E2F1 can allow disease progression through a novel mechanism of E2F1-mediated MYLK regulation. This study has implications for oncogenic BRAF-activated tumors and resistance to targeted oncogenic BRAF therapy.

Published
2018

4. Urgent Care Dermatology: Symptom-Based Diagnosis E-Book : Urgent Care Dermatology: Symptom-Based Diagnosis E-Book

Author

James E. Fitzpatrick, Whitney A. High, James E. Fitzpatrick, and Whitney A. High

Subjects
Skin--Diseases--Diagnosis
Abstract

Urgent Care Dermatology: Symptom-Based Diagnosis, by Drs. James E. Fitzpatrick, Whitney A. High, and Lamar Kyle, helps you quickly identify skin conditions and provide necessary treatment at the point of care. Concise, to-the-point text is highlighted by more than 1,000 high-quality photographs – all conveniently organized by lesion appearance – making this resource ideal for first-line clinicians to quickly identify and treat dermatologic conditions. - Appearance-based format designed for non-specialists who diagnose and treat skin conditions, such as family practice physicians, urgent care providers, nurse practitioners, and physician assistants - Organized by presentation (scaly lesions, blisters, etc.), with a full chapter on treatment pearls that offers expert advice pertaining to diagnosis and treatment - Richly illustrated with more than 1,000 full-color clinical examples of lesions you're likely to see - Each topic is covered in a two-page spread for quick reference – text on the left and images on the right - Up-to-date coverage of morbilliform eruptions, scaly papular lesions, dermatitis (eczematoid reactions), and abscesses, as well as a timely chapter on cutaneous diseases of travelers organized by global region - Expert Consult eBook version included with purchase. This enhanced eBook experience allows you to search all of the text, figures, images, videos (including video updates), glossary, and references from the book on a variety of devices - Appearance-based format designed for non-specialists who diagnose and treat skin conditions, such as family practice physicians, urgent care providers, nurse practitioners, and physician assistants. - Organized by presentation (scaly lesions, blisters, etc.), with a full chapter on treatment pearls that offers expert advice pertaining to diagnosis and treatment. - Richly illustrated with more than 1,000 full-color clinical examples of lesions you're likely to see. - Each topic is covered in a two-page spread for quick reference – text on the left and images on the right. - Up-to-date coverage of morbilliform eruptions, scaly papular lesions, dermatitis (eczematoid reactions), and abscesses, as well as a timely chapter on cutaneous diseases of travelers organized by global region. - Expert Consult eBook version included with purchase. This enhanced eBook experience allows you to search all of the text, figures, images, videos (including video updates), glossary, and references from the book on a variety of devices.

Published
2018

8. List of Contributors

Author

Anthony Abdullah, Michael Abrouk, Tashmeeta Ahad, Imtiaz Ahmed, Anwar Al Hammadi, Caroline Allen, Amer Ali Almohssen, Wisam Alwan, Mahreen Ameen, Sadegh Amini, Bryan E. Anderson, Grant J. Anhalt, Donald J. Baker, Harini Rajgopal Bala, Julia Baltz, David Banach, Cedric C. Banfield, Robert Baran, Ajoy Bardhan, Melissa C. Barkham, Ysabel M. Bello, Emma Benton, Wilma F. Bergfeld, Eric Berkowitz, Brian Berman, Jeffrey D. Bernhard, Daniel Bernstein, John Berth-Jones, Chinmoy Bhate, Bhavnit K. Bhatia, Jonathan E. Blume, Nevianna Bordet, Catherine Borysiewicz, Gary J. Brauner, Robert T. Brodell, Marc D. Brown, Robert M. Burd, Anne E. Burdick, Niraj Butala, Jeffrey P. Callen, Ivan D. Camacho, Helena Camasmie, Daniel Caplivski, Mitchell S. Cappell, Genevieve A. Casey, Lawrence S. Chan, Loi-Yuen Chan, Jennifer K. Chen, Chen 'Mary' Chen, Nicole Yi Zhen Chiang, Anthony J. Chiaravalloti, Fiona J. Child, Anthony C. Chu, Timothy H. Clayton, Steven R. Cohen, Elizabeth A. Cooper, Susan M. Cooper, Nick Collier, Christina M. Correnti, Ian H. Coulson, M. Laurin Council, Shawn E. Cowper, Nicholas M. Craven, Daniel Creamer, Ponciano D. Cruz, Carrie Ann R. Cusack, Adam Daunton, Mark D.P. Davis, Robert S. Dawe, David P. D’Cruz, David de Berker, Danielle M. DeHoratius, Min Deng, Seemal R. Desai, Georgina Devlin, John J. DiGiovanna, Alexander Doctoroff, Roni P. Dodiuk-Gad, Dawn Z. Eichenfield, Lawrence F. Eichenfield, Drore Eisen, Ure Eke, Dirk M. Elston, Patrick O.M. Emanuel, Clinton W. Enos, Shaheen H. Ensanyat, Anna F. Falabella, Aaron S. Farberg, Lawrence S. Feigenbaum, Kristen Heins Fernandez, Nicole Fett, Andrew Y. Finlay, Bahar F. Firoz, Elnaz F. Firoz, James E. Fitzpatrick, Amy E. Flischel, Kelly A. Foley, Derek Freedman, Georgina A. Fremlin, Richard Fried, Philip Friedlander, Adam Friedman, Amy K. Forrestel, Brian S. Fuchs, Joanna E. Gach, Anjela Galan, Jaya Ganesh, Amit Garg, Lauren Geller, Carlo M. Gelmetti, Elizabeth Ghazi, Sneha Ghunawat, Leonard H. Goldberg, Mark J.D. Goodfield, Marsha L. Gordon, Asha Gowda, Daniel A. Grabell, Matthew Grant, Clive E.H. Grattan, Malcolm W. Greaves, Justin J. Green, Christopher E.M. Griffiths, Charles A. Gropper, Anna L. Grossberg, Aditya K. Gupta, Ali S. Hadi, Suhail M. Hadi, Iris A. Hagans, Bethany R. Hairston, Analisa Vincent Halpern, Caroline Halverstam, Natasha Harper, Matthew J. Harries, John Harris, Shannon Harrison, Michael M. Hatch, Adrian H.M. Heagerty, Adelaide A. Hebert, Stephen E. Helms, Camile L. Hexsel, Doris M. Hexsel, Warren R. Heymann, Elisabeth M. Higgins, Claire L. Higgins, Whitney A. High, Herbert Hönigsmann, Marcelo G. Horenstein, George J. Hruza, Andrea Hui, Ran Huo, Sally H. Ibbotson, Sherrif F. Ibrahim, Andrew Ilchyshyn, Dina Ismail, Stefania Jablonska, Heidi T. Jacobe, William D. James, Aysha Javed, Gregor B.E. Jemec, Graham A. Johnston, Stephen K. Jones, Jacqueline M. Junkins-Hopkins, Jessica Kaffenberger, Kelly R. Kane, Antonios Kanelleas, Ayşe Serap Karadağ, Laura Karas, Ruwani P. Katugampola, Bruce E. Katz, Roselyn Kellen, Murtaza Khan, Hooman Khorasani, Ellen J. Kim, Hee J. Kim, Brian Kirby, Joslyn S. Kirby, Rachel S. Klein, Kate Kleydman, Dimitra Koch, John J. Kohorst, John Y.M. Koo, Sandra A. Kopp, Neil J. Korman, Carrie Kovarik, Kenneth H. Kraemer, Bernice R. Krafchik, Karthik Krishnamurthy, Knut Kvernebo, Charlene Lam, Peter C. Lambert, James A.A. Langtry, Amir A. Larian, Cecilia A. Larocca, E. Frances Lawlor, Clifford M. Lawrence, Mark G. Lebwohl, Oscar Lebwohl, Julia S. Lehman, Tabi A. Leslie, Stuart R. Lessin, Jacob O. Levitt, Fiona M. Lewis, Maryam Liaqat, Kristina J. Liu, Michael P. Loosemore, Thomas A. Luger, Omar Lupi, Boris D. Lushniak, Calum C. Lyon, Andrea D. Maderal, Bassel H. Mahmoud, Slawomir Majewski, Richard B. Mallett, Steven M. Manders, Ranon Mann, Yasaman Mansouri, David J. Margolis, Orit Markowitz, Alexander Marsland, Agustin Martin-Clavijo, Daniela Martinez, Catalina Matiz, Marcus Maurer, Kevin McKerrow, Nekma Meah, Giuseppe Micali, Robert G. Micheletti, Leslie G. Millard, James E. Miller, Jillian W. Wong Millsop, Daniel Mimouni, Ginat W. Mirowski, Sultan A. Mirza, Sonja Molin, Adisbeth Morales-Burgos, Warwick L. Morison, Cato Mørk, Colin A. Morton, Richard J. Motley, Megan Mowbray, Eavan G. Muldoon, Anna E. Muncaster, George J. Murakawa, Jenny E. Murase, Michele E. Murdoch, Adam S. Nabatian, Mio Nakamura, Rajani Nalluri, Zeena Y. Nawas, Glen R. Needham, Glenn C. Newell, Julia Newton-Bishop, Adam V. Nguyen, Rosemary L. Nixon, Jack C. O’Brien, Stephanie Ogden, Suzanne M. Olbricht, Sally Jane O’Shea, Cindy E. Owen, Michael Pan, Lisa Pappas-Taffer, Jennifer L. Parish, Lawrence Charles Parish, Michael Payette, Gary L. Peck, Sandra Pena, Jarad Peranteau, Frederick A. Pereira, William Perkins, Clifford S. Perlis, Robert G. Phelps, Tania J. Phillips, Maureen B. Poh-Fitzpatrick, Miriam Keltz Pomeranz, Samantha R. Pop, Pierluigi Porcu, James B. Powell, Lori D. Prok, Tia M. Pyle, Surod Qazaz, Vikram Rajkomar, Rabia S. Rashid, Mehdi Rashighi, Ravi Ratnavel, Christie G. Regula, Michael Renzi, Jean Revuz, Rachel V. Reynolds, Elisabeth Richard, Gabriele Richard, Darrell S. Rigel, Wanda Sonia Robles, Megan Rogge, Alain H. Rook, Jamie R. Manning, Ted Rosen, Misha Rosenbach, David Rosenfeld, Christopher Rowland Payne, Adam I. Rubin, Courtney Rubin, Malcolm H.A. Rustin, Thomas Ruzicka, Sara Samimi, Lawrence A. Schachner, Noah Scheinfeld, Bethanee J. Schlosser, Rhonda E. Schnur, Robert A. Schwartz, Matthew J. Scorer, Bryan A. Selkin, Jamie Seymour, Christine M. Shaver, Christopher R. Shea, Neil H. Shear, Tang Ngee Shim, Hiroshi Shimizu, Julia Siegel, Elisha Singer, Maral Kibarian Skelsey, Chris Sladden, Michael Sladden, Janellen Smith, Joanne E. Smucker, Najwa Somani, Lacy L. Sommer, Mary Sommerlad, Christine Soon, Jennifer A. Sopkovich, Nicholas A. Soter, James M. Spencer, Richard C.D. Staughton, Jane C. Sterling, Cord Sunderkötter, Saleem M. Taibjee, Deborah Tamura, Eunice Tan, William Y-M. Tang, Lynsey Taylor, Bruce H. Thiers, Lucy J. Thomas, Cody R. Thornton, Anne-Marie Tobin, Rochelle R. Torgerson, Antonella Tosti, Fragkiski Tsatsou, Yukiko Tsuji-Abe, William F.G. Tucker, Stephen K. Tyring, Jeremy Udkoff, Robin H. Unger, Walter P. Unger, Sarah Utz, Martha C. Valbuena, Peter van de Kerkhof, Abby S. Van Voorhees, Ramya Vangipuram, David Veitch, Vanessa Venning, Sarah G. Versteeg, Martha Viera, Carmela C. Vittorio, Ruth Ann Vleugels, Gorav N. Wali, Joanna Wallengren, Joy Wan, Karolyn A. Wanat, Gabriele Weichert, Anja K. Weidmann, Jeffrey M. Weinberg, Victoria P. Werth, Lucile E. White, Adam H. Wiener, Jonathan K. Wilkin, Nathaniel K. Wilkin, Jason Williams, Niall Wilson, Karen Wiss, Joseph A. Witkowski, Lauren E. Wiznia, Henry K. Wong, Junie Li Chun Wong, Andrew L. Wright, Cooper C. Wriston, Benedict C. Wu, Adam Wulkan, Andrea L. Zaenglein, Irshad Zaki, Joshua A. Zeichner, Tian Hao Zhu, John J. Zone, Christos C. Zouboulis, and Torstein Zuberbeir

Published
2018
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12. Tumors With Scale

Author

W. Lamar Kyle, James E. Fitzpatrick, and Whitney A. High

Subjects
Scale (ratio), business.industry, Climatology, Medicine, business
Published
2018
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16. Blisters and Vesicles

Author

Whitney A. High, James E. Fitzpatrick, and W. Lamar Kyle

Subjects
business.industry, Vesicle, medicine, Blisters, medicine.symptom, business
Published
2018
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27. Cysts and Sinuses

Author

Whitney A. High, James E. Fitzpatrick, and W. Lamar Kyle

Subjects
business.industry, Medicine, business
Published
2018
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33. Diffuse or Reticulated Erythema

Author

James E. Fitzpatrick, W. Lamar Kyle, and Whitney A. High

Subjects
medicine.medical_specialty, Erythema, business.industry, Medicine, medicine.symptom, business, Dermatology
Published
2018
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34. Topical Treatment Pearls

Author

Whitney A. High, W. Lamar Kyle, and James E. Fitzpatrick

Subjects
medicine.medical_specialty, business.industry, Medicine, Topical treatment, business, Dermatology
Published
2018
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41. Desmosomal defects in acantholytic squamous cell carcinomas

Author

Peter Koch, Charlene O'Shea, and James E. Fitzpatrick

Subjects
Pathology, medicine.medical_specialty, Histology, biology, Desmoplakin, Chemistry, Acantholysis, Cell, Dermatology, Adhesion, medicine.disease, Desmoglein, Pathology and Forensic Medicine, Adherens junction, stomatognathic diseases, medicine.anatomical_structure, biology.protein, medicine, Desmocollin, Cell adhesion
Abstract

Background Acantholytic squamous cell carcinoma (Acantholytic SCC) are epithelial tumors characterized by a loss of cell adhesion between neoplastic keratinocytes. The mechanism underlying loss of cell-cell adhesion in these tumors is not understood. Methods A retrospective analysis of acantholytic SCC (n = 17) and conventional SCC (n = 16, controls not showing acantholysis) was conducted using a set of desmosomal and adherens junction protein antibodies. Immunofluorescence microscopy was used to identify tumors with loss of adhesion protein expression. Results The vast majority of acantholytic SCC (89%) showed focal loss of at least one desmosomal cell adhesion protein. Most interestingly, 65% of these tumors lost expression of two or more desmosomal proteins. Conclusions Loss of cell adhesion in acantholytic SCC is most likely linked to the focal loss of desmosomal protein expression, thus providing potential mechanistic insight into the patho-mechanism underlying this malignancy.

Published
2014
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42. Dermatology Secrets Plus E-Book : Dermatology Secrets Plus E-Book

Author

James E. Fitzpatrick, Joseph G. Morelli, James E. Fitzpatrick, and Joseph G. Morelli

Subjects
Skin--Diseases, Dermatology--Miscellanea
Abstract

For 30 years, the highly regarded Secrets Series® has provided students and practitioners in all areas of health care with concise, focused, and engaging resources for quick reference and exam review. Dermatology Secrets Plus, 5th Edition, by Drs. James E. Fitzpatrick and Joseph G. Morelli, features the Secrets'popular question-and-answer format that also includes lists, tables, and an informal tone – making reference and review quick, easy, and enjoyable. - Top 100 Secrets and Key Points boxes provide a fast overview of the secrets you must know for success in practice. - The proven Secrets® format gives you the most return for your study time – concise, easy to read, engaging, and highly effective. - Larger page size provides the visual detail necessary to understand and diagnose skin disorders, yet is still easy to carry with you for quick reference or review. - NEW: Expert Consult eBook features online and mobile access. - Thorough updates throughout, including new chapters on disorders of the male genitalia and disorders of the oral mucosa.

Published
2015

43. Recent Observations on the Heterogeneity of Human Effector Memory T Cells and Novel Cytokines Implicated in Cutaneous Inflammation and Psoriasis

Author

Karen R. Jonscher, Michelle G. Pedler, Diana Fulan Yang, Carl K. Edwards, Mayumi Fujita, James E. Fitzpatrick, and David A. Norris

Subjects
Effector, General Arts and Humanities, Psoriasis, Immunology, medicine, Cutaneous inflammation, Biology, medicine.disease
Abstract

Psoriasis is a chronic inflammatory skin disease that affects 2.2% of Americans and is a substantial detriment on the quality of life. Psoriasis is a complex interaction between numerous immune cells and has been considered largely a T-helper type 1 (Th1) T-cell-mediated response. Although numerous cytokines, including tumor necrosis factor-αβ, interleukin 1β, and interferon-γ, have been identified with distinct roles in skin inflammation and psoriasis, proinflammatory functions of newly identified cytokines have been linked recently to the alternative T-cell subsets Th17 and Th22 that are distinct in their functions and cytokine profiles. This review summarizes the basic research, translational applications, and new therapeutic developments contributing to the understanding of the diversity of human effector CD4+ Th1, Th17, and Th22 T cells, as well as the proinflammatory cytokines associated with these subsets in psoriasis.

Published
2012
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44. A visible response to an invisible tattoo

Author

James E. Fitzpatrick, Lori Prok, Katrina Bassett, Whitney A. High, Amanda F. Marsch, and Matthew Tsang

Subjects
medicine.medical_specialty, Histology, Fluorescent light, business.industry, medicine, Dermatology, Granulomatous Dermatitis, business, Pathology and Forensic Medicine
Abstract

Invisible (or blacklight) tattoos are fast becoming the trend in the world of tattoo art, and with their rise comes the onset of associated complications. Though there have been many reports of cutaneous reactions to traditional tattoo pigments, literature regarding reactions to invisible tattoos is scarce. We report the case of a 28-year-old man who presented with an inflammatory eruption of 2 months' duration confined to the area of a recently placed invisible tattoo; the eruption was diagnosed as granulomatous dermatitis to a foreign material. Under fluorescent light, a refractile foreign material was identified in the biopsy specimen, which we believe to be melamine, one of the invisible tattoo's five ingredients. Previous cases of cutaneous reactions to invisible tattoos were attributed to polymethylmethacrylate, not a component of the tattoo in this case. To our knowledge, this is the first case implicating melamine as the cause of a granulomatous tattoo reaction. Given the rising popularity of invisible tattoos, we present this case to raise awareness of the risks associated with this alternative tattoo trend.

Published
2012
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45. A Mediator of Rho-dependent Invasion Moonlights as a Methionine Salvage Enzyme

Author

Yukihito Kabuyama, Kirsi Polvinen, Paul D. Templeton, Natalie G. Ahn, Eric S. Witze, James E. Fitzpatrick, Elizabeth S. Litman, Stephen J. Langer, Sandra I. Metzner, Gretchen M. Argast, Daniel Chan, Marcelo C. Sousa, Katheryn A. Resing, Yiqun G. Shellman, and John B. Shabb

Subjects
Proteomics, S-Adenosylmethionine, RHOA, Molecular Sequence Data, Transplantation, Heterologous, Cell, Mice, Nude, Biology, Biochemistry, Analytical Chemistry, Focal adhesion, Mice, 03 medical and health sciences, chemistry.chemical_compound, Methionine, 0302 clinical medicine, Cell Line, Tumor, medicine, Animals, Humans, Neoplasm Invasiveness, Amino Acid Sequence, Neoplasm Metastasis, Melanoma, Molecular Biology, Aldose-Ketose Isomerases, Actin, 030304 developmental biology, 0303 health sciences, Molecular Structure, Research, Tyrosine phosphorylation, Cell biology, Enzyme Activation, medicine.anatomical_structure, chemistry, Cell culture, Cytoplasm, 030220 oncology & carcinogenesis, biology.protein, Female, RNA Interference, Signal transduction, rhoA GTP-Binding Protein, Signal Transduction
Abstract

RhoA controls changes in cell morphology and invasion associated with cancer phenotypes. Cell lines derived from melanoma tumors at varying stages revealed that RhoA is selectively activated in cells of metastatic origin. We describe a functional proteomics strategy to identify proteins regulated by RhoA and report a previously uncharacterized human protein, named “mediator of RhoA-dependent invasion (MRDI),” that is induced in metastatic cells by constitutive RhoA activation and promotes cell invasion. In human melanomas, MRDI localization correlated with stage, showing nuclear localization in nevi and early stage tumors and cytoplasmic localization with plasma membrane accentuation in late stage tumors. Consistent with its role in promoting cell invasion, MRDI localized to cell protrusions and leading edge membranes in cultured cells and was required for cell motility, tyrosine phosphorylation of focal adhesion kinase, and modulation of actin stress fibers. Unexpectedly MRDI had enzymatic function as an isomerase that converts the S-adenosylmethionine catabolite 5-methylribose 1-phosphate into 5-methylribulose 1-phosphate. The enzymatic function of MRDI was required for methionine salvage from S-adenosylmethionine but distinct from its function in cell invasion. Thus, mechanisms used by signal transduction pathways to control cell movement have evolved from proteins with ancient function in amino acid metabolism.

Published
2009
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46. A Genetic Variant of Aurora Kinase A Promotes Genomic Instability Leading to Highly Malignant Skin Tumors

Author

James E. Fitzpatrick, Hiroshi Katayama, Dennis R. Roop, Subrata Sen, Yiyun Chen, Enrique C. Torchia, Carlos Caulin, Hong Sheng, and William R. Brinkley

Subjects
Adult, Keratinocytes, Cancer Research, Programmed cell death, Skin Neoplasms, 9,10-Dimethyl-1,2-benzanthracene, Cell, Mice, Transgenic, Human skin, Spindle Apparatus, macromolecular substances, Protein Serine-Threonine Kinases, Biology, medicine.disease_cause, Article, Genomic Instability, Mice, Aurora kinase, Aurora Kinases, medicine, Animals, Humans, Aurora Kinase A, Cell Death, Papilloma, Malignant Conversion, Cancer, medicine.disease, Molecular biology, enzymes and coenzymes (carbohydrates), Cell Transformation, Neoplastic, medicine.anatomical_structure, Oncology, embryonic structures, Carcinoma, Squamous Cell, biological phenomena, cell phenomena, and immunity, Carcinogenesis
Abstract

Aurora kinase A (Aurora-A) belongs to a highly conserved family of mitotis-regulating serine/threonine kinases implicated in epithelial cancers. Initially we examined Aurora-A expression levels at different stages of human skin cancer. Nuclear Aurora-A was detected in benign lesions and became more diffused but broadly expressed in well and poorly differentiated squamous cell carcinomas (SCC), indicating that Aurora-A deregulation may contribute to SCC development. To mimic the overexpression of Aurora-A observed in human skin cancers, we established a gene-switch mouse model in which the human variant of Aurora-A (Phe31Ile) was expressed in the epidermis upon topical application of the inducer RU486 (Aurora-AGS). Overexpression of Aurora-A alone or in combination with the tumor promoter 12-O-tetradecanoylphorbol 13-acetate (TPA), did not result in SCC formation in Aurora-AGS mice. Moreover, Aurora-A overexpression in naive keratinocytes resulted in spindle defects in vitro and marked cell death in vivo, suggesting that the failure of Aurora-A to initiate tumorigenesis was due to induction of catastrophic cell death. However, Aurora-A overexpression combined with exposure to TPA and the mutagen 7,12-dimethylbenz(a)anthracene accelerated SCC development with greater metastastic activity than control mice, indicating that Aurora-A cannot initiate skin carcinogenesis but rather promotes the malignant conversion of skin papillomas. Further characterization of SCCs revealed centrosome amplification and genomic alterations by array CGH analysis, indicating that Aurora-A overexpression induces a high level of genomic instability that favors the development of aggressive and metastatic tumors. Our findings strongly implicate Aurora-A overexpression in the malignant progression of skin tumors and suggest that Aurora-A may be an important therapeutic target. [Cancer Res 2009;69(18):7207–15]

Published
2009
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47. Gastrointestinal Melanoma or Clear Cell Sarcoma? Molecular Evaluation of 7 Cases Previously Diagnosed as Malignant Melanoma

Author

Pamela L Lyle, Carol M. Amato, William A. Robinson, and James E. Fitzpatrick

Subjects
Adult, Male, Pathology, medicine.medical_specialty, Biology, Pathology and Forensic Medicine, Metastasis, medicine, Humans, Melanoma, In Situ Hybridization, Fluorescence, Gastrointestinal Neoplasms, medicine.diagnostic_test, Reverse Transcriptase Polymerase Chain Reaction, fungi, Middle Aged, medicine.disease, Fusion transcript, Pleomorphism (cytology), Cutaneous melanoma, Female, Surgery, Sarcoma, Clear Cell, Sarcoma, Clear-cell sarcoma, Anatomy, Fluorescence in situ hybridization
Abstract

Clear cell sarcoma (CCS) is a rare tumor classically associated with the tendons and aponeuroses of distal extremities of young adults. CCS and malignant melanoma (MM) share immunohistochemical profiles and ultrastructural features, but classic CCS has characteristic morphology with low mitotic activity and minimal pleomorphism. Occasional cases show pleomorphism, high mitotic index, and/or melanin pigmentation, making CCS indistinguishable from MM based on morphology. However, CCS is genetically distinct owing to its consistent association with a t(12;22)(q13;q12) chromosomal translocation, leading to the formation of the EWS/ATF1 fusion transcript. This translocation has never been documented in cutaneous melanoma, and thus is regarded as specific for CCS. Recent evidence suggests that primary "malignant melanomas" in unusual anatomic sites, most notably the gastrointestinal (GI) tract, may be CCS. This is supported by 11 cases of primary GI CCS with the t(12;22) translocation. We used reverse-transcription polymerase chain reaction and fluorescence in situ hybridization to examine whether a proportion of cases diagnosed as MM of the GI tract in patients without a history of cutaneous MM actually represent primary GI CCS. In total, we examined 7 cases: Four with no prior history of MM, 2 with histories of cutaneous MM, and 1 with an anal MM. All 4 cases for which there was no history of cutaneous/mucosal MM harbored the EWS/ATF1 fusion transcript. We report the largest series of GI CCS and have shown that molecular studies may be warranted in cases that otherwise seem to represent MM of unusual primary locations.

Published
2008
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48. Tattoo Pigment Interpreted as Lymph Node Metastasis in a Case of Subungual Melanoma

Author

Steven L. Peterson, Lela A. Lee, James E. Fitzpatrick, and Kagan Ozer

Subjects
Pathology, medicine.medical_specialty, business.industry, Melanoma, Lymph node metastasis, Sentinel node, medicine.disease, Article, Metastasis, Medicine, Orthopedics and Sports Medicine, Surgery, Axillary Dissection, Lymph, Tattoo pigment, Subungual melanoma, business
Abstract

We present a patient with subungual melanoma of the thumb who, during radioisotope-guided selective sentinel lymphadenectomy, was found to have black, hard lymph nodes at multiple axillary node levels. This finding was interpreted intraoperatively as clinical evidence of metastasis and a formal axillary dissection was carried out. Pathological examination of excised nodes failed to demonstrate metastasis but instead showed collections of tattoo pigment.

Published
2008
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49. Basaloid Follicular Hamartoma: A Cautionary Tale and Review of the Literature

Author

Michael D. Shapiro, Aradhna Saxena, J. Ramsey Mellette, James E. Fitzpatrick, and David A. Kasper

Subjects
Adult, Pathology, medicine.medical_specialty, Skin Neoplasms, Hamartoma, medicine.medical_treatment, Dermatology, Diagnosis, Differential, medicine, Mohs surgery, Humans, business.industry, Dermabrasion, Skin Transplantation, General Medicine, Mohs Surgery, medicine.disease, Hair follicle, Skin transplantation, Basaloid follicular hamartoma, medicine.anatomical_structure, Carcinoma, Basal Cell, Female, Surgery, Differential diagnosis, business, Hair Follicle
Published
2007
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50. Pustulo-ovoid bodies of Milian in granular cell tumors

Author

Loren E. Golitz, Edgar Hunt, Darin S. Epstein, James E. Fitzpatrick, and Shayesteh Pashaei

Subjects
Adult, Inclusion Bodies, Male, Pathology, medicine.medical_specialty, Mucous Membrane, Skin Neoplasms, Histology, Adolescent, H&E stain, Dermatology, Middle Aged, Biology, Immunohistochemistry, Pathology and Forensic Medicine, Cytoplasmic granules, Granular cell, Granular Cell Tumor, Child, Preschool, medicine, Humans, Ovoid, Female, Child, Aged
Abstract

Background: Granular cell tumors (GCTs) are benign neural tumors with a distinct histologic appearance on light microscopy, characterized by eosinophilic cytoplasmic granules. Pustulo-ovoid bodies of Milian (POB) are larger granules surrounded by a clear halo. There have been no histologic studies to document their prevalence in GCT. Methods: We examined the sections of 47 cases of GCT stained with hematoxylin and eosin to determine the frequency of POB within this tumor. POB were measured per 10 high-power fields (HPFs) and were divided into the following categories: less than 10 POB per 10 HPFs, 10–30 per 10 HPFs, 30–50 per 10 HPFs and greater than 50 per 10 HPFs. Results: POB were present in 100% of the specimens examined. Eleven cases (23%) had between 1 and 9 POBs per 10 HPFs, twelve cases (26%) had between 10 and 29 POBs per HPFs, five cases (11%) had between 30 and 50 POBs per HPFs and nineteen cases (40%) had greater than 50 POBs per HPFs. When grouped according to clinical characteristics, there was an even distribution of POB by age, sex and site of the tumor. Conclusions: In our series, POB were present in varying numbers in all the tumors studied. They appear to represent the heterogeneity of the lysosomes, giving the appearance of large granules that have partially detached from the adjacent cytoplasm. POB are an easily recognizable component of GCTs.

Published
2007
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