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(Ebook) Retinal Degenerative Diseases XIX: Mechanisms and Experimental Therapy (Advances in Experimental Medicine and Biology, 1415) by John D. Ash (editor), Eric Pierce (editor), Robert E. Anderson (editor), Catherine Bowes Rickman (editor), Joe G. Hollyfield (editor), Christian Grimm (editor) ISBN 9783031276804, 3031276809

  • SKU: EBN-50883036
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Instant download (eBook) Retinal Degenerative Diseases XIX: Mechanisms and Experimental Therapy (Advances in Experimental Medicine and Biology, 1415) after payment.
Authors:John D. Ash (editor), Eric Pierce (editor), Robert E. Anderson (editor), Catherine Bowes Rickman (editor), Joe G. Hollyfield (editor), Christian Grimm (editor)
Pages:607 pages.
Year:2023
Editon:1st ed. 2023
Publisher:Springer
Language:english
File Size:82.04 MB
Format:epub
ISBNS:9783031276804, 3031276809
Categories: Ebooks

Product desciption

(Ebook) Retinal Degenerative Diseases XIX: Mechanisms and Experimental Therapy (Advances in Experimental Medicine and Biology, 1415) by John D. Ash (editor), Eric Pierce (editor), Robert E. Anderson (editor), Catherine Bowes Rickman (editor), Joe G. Hollyfield (editor), Christian Grimm (editor) ISBN 9783031276804, 3031276809

This book contains the proceedings of the XVIII International Symposium on Retinal Degeneration (RD2018). A majority of those who spoke  and presented posters at the meeting contributed to this volume. The blinding diseases of inherited retinal degenerations have no treatments, and age-related macular degeneration has no cures, despite the fact that it is an epidemic among the elderly, with 1 in 3-4 affected by the age of 70. The RD Symposium focused on the exciting new developments aimed at understanding these diseases and providing therapies for them. Since most major scientists in the field of retinal degenerations attend the biennial RD Symposia, they are known by most as the “best” and “most important” meetings in the field.The volume presents representative state-of-the-art research in almost all areas of retinal degenerations, ranging from cytopathologic, physiologic, diagnostic and clinical aspects; animal models; mechanisms of cell death; candidate genes, cloning, mapping and other aspects of molecular genetics; and developing potential therapeutic measures such as gene therapy and neuroprotective agents for potential pharmaceutical therapy. While advances in these areas of retinal degenerations were described, there will be many new topics that either are in their infancy or did not exist at the time of the last RD Symposium. These include the role of inflammation and immunity, as well as other basic mechanisms, in age-related macular degeneration, several new aspects of gene therapy, and revolutionary new imaging and functional testing that will have a huge impact on the diagnosis and following the course of retinal degenerations, as well as to provide new quantitative endpoints for clinical trials. The retina is an approachable part of the central nervous system (CNS), and there is a major interest in neuroprotective and gene therapy for CNS diseases and neurodegenerations, in general. It should be noted that with successful and exciting initial clinical trials in neuroprotective and gene therapy, including the restoration of sight in blind children, the retinal degeneration therapies are leading the way towards new therapeutic measures for neurodegenerations of the CNS. Many of the successes recently reported in these areas of retinal degeneration sprang from collaborations established at previous RD Symposia, and many of those were reported at the RD2016 meeting and included in the current volume. We anticipate the excitement of those working in the field and those afflicted with retinal degenerations is reflected in the volume.
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