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Proliferation Organ perfusates

Interleukin-2 Human recombinant lL-2 aldesleukin, proleukin des-alanyl-1, serine-125 human lL-2) differs from native lL-2 in that it is not glycosylated, has no amino terminal Ala, and has an Ser substituted for the Cys at amino acid 125. The potency of the preparation is represented in International Units in a lymphocyte proliferation assay such that 1.1 mg of recombinant lL-2 protein equals 18 million International Units. Aldesleukin has the following in vitro biologic activities of native lL-2 enhancement of lymphocyte proliferation and growth of lL-2-dependent cell lines enhancement of lymphocyte-mediated cytotoxicity and killer cell activity and induction of interferon-7 activity. In vivo administration of aldesleukin in animals produces multiple immunologic effects in a dose-dependent manner. Cellular immunity is profoundly activated with lymphocytosis, eosinophilia, thrombocytopenia, and release of multiple cytokines e.g., TNF-a, lL-1, interferon-7). Aldesleukin is indicated for the treatment of adults with metastatic renal cell carcinoma and melanoma. Administration of aldesleukin has been associated with serious cardiovascular toxicity resulting from capillary leak syndrome, which involves loss of vascular tone and leak of plasma proteins and fluid into the extravascular space. Hypotension, reduced organ perfusion, and death may occur. An increased risk of disseminated infection due to impaired neutrophil function also has been associated with aldesleukin treatment. [Pg.921]

Other potential uses for iron chelators are reducing post-ischaemic perfusion injury [23], organ transplantation [24] and graft versus host disease [25], as anticancer agents through their effect on cell proliferation [26], mobilizing iron from the reticuloendothelial cells in the anaemia of chronic disease [27], and selective metalloenzyme inhibitors of lipoxygenase and ribonucleotide reductase. [Pg.195]


See other pages where Proliferation Organ perfusates is mentioned: [Pg.246]    [Pg.121]    [Pg.184]    [Pg.74]    [Pg.343]    [Pg.1938]    [Pg.2615]    [Pg.1167]    [Pg.90]    [Pg.466]    [Pg.689]    [Pg.402]    [Pg.74]    [Pg.1231]    [Pg.1452]   
See also in sourсe #XX -- [ Pg.147 ]




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Organ perfusion

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