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Titlebook: Gene Therapy for Acute and Acquired Diseases; Phillip Factor Book 2001 Kluwer Academic Publishers 2001 HIV.Trauma.gene therapy.gene transf

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978-1-4613-5668-4Kluwer Academic Publishers 2001
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ired disorders. It is expected that human gene therapytrials for these conditions will be forthcoming in the near future,leading to previously unimaginable therapies. Thus, this first-everbook about gene therapy for acute and acquired diseases is intended toserve as a glimpse into the future.978-1-4613-5668-4978-1-4615-1667-5
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Class, Capital and Social Policyite the institution of standard therapy aimed at the underlying process, many patients die secondary to the deleterious effects of the exaggerated systemic inflammatory response and end-organ damage seen in these disease states.
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Time, Myth and Power: , (2012),l advantages of giving therapeutic genes rather than giving proteins: 1) transfer of genes encoding intracellular proteins produces higher levels of therapeutic proteins within the cell, 2) gene transfer could be cell specific with modified vectors, 3) gene transfer may have less risk of antigenicit
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https://doi.org/10.1007/978-3-030-16222-1 of alveolar proteolysis, cell proliferation, apoptosis, angiogenesis, matrix synthesis and epithelial cell re-population provide ample and complementary biological pathways for targeting gene therapy (.–.). This chapter will review the alveolar architectural and biochemical abnormalities that occur
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Matthias Bernhard,Christian Wesselskynimal and azotemia is rapidly reversible by restoration of renal blood flow and glomerular filtration rate. Therefore, correction of renal perfusion is generally decisive in resolving pre-renal azotemia. Post-renal ARF occurs as a result of urinary tract obstruction, removal or bypass the obstructio
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