Bone Marrow-Derived Progenitors
Bone Marrow-Derived Progenitors

Author: Katalin Kauser

Publisher: Springer Science & Business Media

Published: 2007-06-07

Total Pages: 293

ISBN-13: 3540689761

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The ambitious goal of this volume is to provide – in chapters written by accomplished scientists and experts in their field – a comprehensive overview of the currently available information related to the therapeutic utility of adult bone marrow-derived cells. With excitement generated almost daily about the possible uses of stem cells to treat human disease, but the controversy surrounding their use still raging, adult bone-marrow derived cells are more readily available, and have a staggering range of uses.

In Vitro Processing of Human Bone Marrow Derived Mesenchymal Stem Cells to Enhance Delivery in Liver Disease
In Vitro Processing of Human Bone Marrow Derived Mesenchymal Stem Cells to Enhance Delivery in Liver Disease

Author: Abhilok Garg

Publisher:

Published: 2013

Total Pages:

ISBN-13:

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Currently the only effective treatment for end stage liver disease is transplantation together with immune-modulating drugs. Human bone marrow derived mesenchymal stem cells (MSC) have been shown to suppress inflammation, potentiate regeneration and act as vectors for gene therapy. Thus, MSC infusions offer an attractive potential therapy for treating liver disease. However a number of obstacles exist in MSC delivery before they can be used therapeutically. Although MSC can migrate to sites of injury after in vivo administration, their engraftment within the liver is often poor, potentially limiting their therapeutic action. I have shown that detaching MSC from culture using non-enzymatic methods is superior in retaining surface chemokine receptor expression. Furthermore, I have shown that these receptors are functional in migration and attachment assays both in vitro and in vivo in carbon-tetrachloride induced liver injury. TGF[beta]1 stimulated MSC were able to further enhance engraftment via up-regulation of surface CXCR3. Additionally the potent immunosuppressive properties of MSC, mediated via Prostaglandin E2, were enhanced after TGF[beta]1 stimulation. Thus my studies demonstrate that manipulation of MSC through careful choice of detachment methods and exogenous cytokine stimulation can improve their engraftment in injured liver and their immunosuppressive properties with implications for improving the efficacy of MSC therapy.

Establishing a Relationship Between Bone Marrow Cells and Liver Progenitor Cells by Expression Profiling and Cell Tracing Studies
Establishing a Relationship Between Bone Marrow Cells and Liver Progenitor Cells by Expression Profiling and Cell Tracing Studies

Author: Joanne Tonkin

Publisher:

Published: 2011

Total Pages: 95

ISBN-13:

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[Truncated abstract] There is great interest in the field of liver progenitor (oval) cells which are a bipotential compartment of cells responding to chronic liver damage. Oval cells have enormous potential to treat patients with liver disease by a cell therapy approach but their use is limited by their scarcity and number of donor livers from which they can be derived. Knowledge is lacking in the origin of oval cells as well as the mechanisms which drive their activation, proliferation and differentiation which is required for their therapeutic potential to be realised. Bone marrow may be a suitable source of liver progenitor cells which could circumvent both disadvantages of using liver-derived material. Derivation of oval cells from bone marrow has been examined in rodents using hepatotoxins and partial hepatectomy to create liver damage. These protocols induce oval cell proliferation however they do not mimic the disease conditions that occur in humans. The first aim of this thesis was therefore to evaluate the contribution of bone marrow cells to oval cells in conditions that more closely mimic human liver disease pathophysiology using a choline-deficient, ethionine-supplemented (CDE) diet which causes fatty liver and virus-induced hepatitis. To determine the contribution of bone marrow cells to CDE and viral-hepatitis injury, lacZ transgenic bone marrow cells were transplanted into congenic mice, liver injury was induced and the movement of bone marrow cells to the liver monitored. Cells originating from donor BM were identified by x-gal staining and their phenotype was determined by immunohistochemical staining with cell type specific markers. Bone marrow-derived oval cells were observed in response to the CDE diet and viral injury but represented a minor fraction (0-1.6%) of the oval cell compartment. The combination of the CDE diet and viral infection produced more severe liver damage with larger numbers of proliferating oval cells; however the proportion of oval cells generated from BM did not increase. In all situations only rare, individual BM-derived oval cells were observed. We hypothesized that the BM cells may replenish oval cells that are expended by protracted liver injury and regeneration, however experiments involving a subsequent episode of chronic liver injury failed to induce proliferation of the BM-derived oval cells which appeared as a result of the first episode. BM-derived hepatocytes were also observed in all injury models and controls in numbers unrelated to that of oval cells. We conclude that during chronic liver disease induced by agents also responsible for human disease the contribution of BM cells to hepatocytes either via oval cell or by independent mechanisms is minimal and that the majority of oval cells responding to this injury are sourced from the liver. The second aim of this thesis was to advance knowledge of the mechanisms which govern oval cell behaviour. The transcriptional profile of oval cells freshly isolated from CDE-fed mice was analysed by microarray to obtain evidence of their relationship to hematopoietic cells and to establish changes in pattern of gene expression following their differentiation into hepatocytes...

Fibrosis Research
Fibrosis Research

Author: John Varga

Publisher: Springer Science & Business Media

Published: 2008-02-02

Total Pages: 393

ISBN-13: 1592599400

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Leading investigators review the highlights of current fibrosis research and the experimental methodologies used uncover the mechanisms that drive it. In their discussion of research methodologies utilizing cultured cells to model various aspects of the fibrotic response in vitro, the authors describe the isolation, characterization, and propagation of mesenchymal cells, and highlight the similarities and differences between methods that are appropriate for different types of fibroblasts. Approaches for studying collagen gene regulation and TGF-b production are also discussed, along with experimental methodologies utilizing animal models to study the pathogenesis of fibrosis. The protocols follow the successful Methods in Molecular MedicineTM series format, each offering step-by-step laboratory instructions, an introduction outlining the principles behind the technique, lists of the necessary equipment and reagents, and tips on troubleshooting and avoiding known pitfalls.

Hepatocyte Transplantation
Hepatocyte Transplantation

Author: S. Gupta

Publisher: Springer Science & Business Media

Published: 2002-09-30

Total Pages: 386

ISBN-13: 9780792387763

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In recent years there has been an increasing need for transplantation, but the number of donor livers available has increased only slightly, despite intensive public relations activities. New concepts in the field of transplantation, for instance the transplantation of living donor organs or the splitting of organs, are urgently required, to safeguard the treatment of patients with severe liver disease. The development and clinical application of cell therapy for patients with liver disease could soon present a significant enhancement of the therapeutic options. The aim of such cell therapy is to repair or improve the biological function of the chronically and acutely damaged liver. Even though systematic trials are not available, individual case reports and small series already show promising clinical results. Present concepts of cell therapy for liver diseases based on the use of primary hepatocytes have recently been considerably extended through new data on the biology of stem cells. The adult haematopoetic stem cell as a pool for hepatocyte grafts - what would be the perspectives for the clinical application? This book is the proceedings of the Falk Symposium No. 126 on `Hepatocyte Transplantation' (Progress in Gastroenterology and Hepatology Part III) held in Hannover, Germany, October 2-3, 2001, and is a forum for basic research, but also for questions concerning clinical applications in the field of hepatocyte transplantation.

Hematopoietic Stem Cell Development
Hematopoietic Stem Cell Development

Author: Isabelle Godin

Publisher: Springer Science & Business Media

Published: 2010-05-27

Total Pages: 188

ISBN-13: 0387335358

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This book collects articles on the biology of hematopoietic stem cells during embryonic development, reporting on fly, fish, avian and mammalian models. The text invites a comparative overview of hematopoietic stem cell generation in the different classes, emphasizing conserved trends in development. The book reviews current knowledge on human hematopoietic development and discusses recent breakthroughs of relevance to both researchers and clinicians.

Cooperation of Liver Cells in Health and Disease
Cooperation of Liver Cells in Health and Disease

Author: Z. Kmiec

Publisher: Springer Science & Business Media

Published: 2013-06-29

Total Pages: 154

ISBN-13: 3642565530

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It is only during the last decade that the functions of sinusoidal endothelial cells, Kupffer cells, hepatic stellate cells, pit cells and other intrahepatic lymphocytes have been better understood. The development of methods for isolation and co-culturing various types of liver cells has established that they communicate and cooperate via secretion of various intercellular mediators. This monograph summarizes multiple data that suggest the important role of cellular cross-talk for the functions of both normal and diseased liver. Special features of the book include concise presentation of the majority of detailed data in 19 tables. Original schemes allow for the clear illustration of complicated intercellular relationships. This is the first ever presentation of the newly emerging field of liver biology, which is important for hepatic function in health and disease and opens new avenues for therapeutic interventions.

Adipose-Derived Stem Cells
Adipose-Derived Stem Cells

Author: Jeffrey M. Gimble

Publisher: Humana Press

Published: 2011-08-24

Total Pages: 474

ISBN-13: 9781617379611

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During the past decade, a wide range of scientific disciplines have adopted the use of adipose-derived stem/stromal cells (ASCs) as an important tool for research and discovery. In Adipose-Derived Stem Cells: Methods and Protocols, experts from the field, including members of the esteemed International Federation of Adipose Therapeutics and Science (IFATS), provide defined and established protocols in order to further codify the utilization of these powerful and accessible cells. With chapters organized around approaches spanning the discovery, pre-clinical, and clinical processes, much of the emphasis is placed on human ASC, while additional techniques involving small and large animal species are included. As a volume in the highly successful Methods in Molecular BiologyTM series, the detailed contributions include introductions to their respective topics, lists of the necessary materials and reagents, step-by-step, readily reproducible laboratory protocols, and notes on troubleshooting and avoiding known pitfalls. Comprehensive and cutting-edge, Adipose-Derived Stem Cells: Methods and Protocols serves as a vital reference text for experienced researchers as well as new students on the path to further exploring the incredible potential of ASCs.

Innovative Medicine
Innovative Medicine

Author: Kazuwa Nakao

Publisher: Springer

Published: 2015-10-13

Total Pages: 330

ISBN-13: 4431556516

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This book is devoted to innovative medicine, comprising the proceedings of the Uehara Memorial Foundation Symposium 2014. It remains extremely rare for the findings of basic research to be developed into clinical applications, and it takes a long time for the process to be achieved. The task of advancing the development of basic research into clinical reality lies with translational science, yet the field seems to struggle to find a way to move forward. To create innovative medical technology, many steps need to be taken: development and analysis of optimal animal models of human diseases, elucidation of genomic and epidemiological data, and establishment of “proof of concept”. There is also considerable demand for progress in drug research, new surgical procedures, and new clinical devices and equipment. While the original research target may be rare diseases, it is also important to apply those findings more broadly to common diseases. The book covers a wide range of topics and is organized into three complementary parts. The first part is basic research for innovative medicine, the second is translational research for innovative medicine, and the third is new technology for innovative medicine. This book helps to understand innovative medicine and to make progress in its realization.