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Iron Chelation Therapy 1st Edition Nancy C Andrews Auth Chaim Hershko Eds

  • SKU: BELL-4495766
Iron Chelation Therapy 1st Edition Nancy C Andrews Auth Chaim Hershko Eds
$ 31.00 $ 45.00 (-31%)

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Iron Chelation Therapy 1st Edition Nancy C Andrews Auth Chaim Hershko Eds instant download after payment.

Publisher: Springer US
File Extension: PDF
File size: 10.41 MB
Pages: 277
Author: Nancy C. Andrews (auth.), Chaim Hershko (eds.)
ISBN: 9780306467851, 9781461505938, 0306467852, 1461505933
Language: English
Year: 2002
Edition: 1

Product desciption

Iron Chelation Therapy 1st Edition Nancy C Andrews Auth Chaim Hershko Eds by Nancy C. Andrews (auth.), Chaim Hershko (eds.) 9780306467851, 9781461505938, 0306467852, 1461505933 instant download after payment.

Within the last few years, iron research has yielded exciting new insights into the under­ standing of normal iron homeostasis. However, normal iron physiology offers little protec­ tion from the toxic effects of pathological iron accumulation, because nature did not equip us with effective mechanisms of iron excretion. Excess iron may be effectively removed by phlebotomy in hereditary hemochromatosis, but this method cannot be applied to chronic anemias associated with iron overload. In these diseases, iron chelating therapy is the only method available for preventing early death caused mainly by myocardial and hepatic iron toxicity. Iron chelating therapy has changed the quality of life and life expectancy of thalassemic patients. However, the high cost and rigorous requirements of deferoxamine therapy, and the significant toxicity of deferiprone underline the need for the continued development of new and improved orally effective iron chelators. Such development, and the evolution of improved strategies of iron chelating therapy require better understanding of the pathophysiology of iron toxicity and the mechanism of action of iron chelating drugs. The timeliness of the present volume is underlined by several significant develop­ ments in recent years. New insights have been gained into the molecular basis of aberrant iron handling in hereditary disorders and the pathophysiology of iron overload (Chapters 1-5).

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