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Literature DB >> 22352729

Dexrazoxane for the prevention of cardiac toxicity and treatment of extravasation injury from the anthracycline antibiotics.

Abstract

The cumulative cardiac toxicity of the anthracycline antibiotics and their propensity to produce severe tissue injury following extravasation from a peripheral vein during intravenous administration remain significant problems in clinical oncologic practice. Understanding of the free radical metabolism of these drugs and their interactions with iron proteins led to the development of dexrazoxane, an analogue of EDTA with intrinsic antineoplastic activity as well as strong iron binding properties, as both a prospective cardioprotective therapy for patients receiving anthracyclines and as an effective treatment for anthracycline extravasations. In this review, the molecular mechanisms by which the anthracyclines generate reactive oxygen species and interact with intracellular iron are examined to understand the cardioprotective mechanism of action of dexrazoxane and its ability to protect the subcutaneous tissues from anthracycline-induced tissue necrosis.

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Year: 2012 PMID： 22352729 PMCID： PMC7366388 DOI： 10.2174/138920112802273245

Source DB: PubMed Journal: Curr Pharm Biotechnol ISSN： 1389-2010 Impact factor: 2.837

107 in total

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Authors: Rui A Carvalho; Rui P B Sousa; Virgilio J J Cadete; Gary D Lopaschuk; Carlos M M Palmeira; James A Bjork; Kendall B Wallace
Journal: Toxicology Date: 2010-02-01 Impact factor: 4.221

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Journal: FASEB J Date: 1999-02 Impact factor: 5.191

Review 8. The use of dexrazoxane for the prevention of anthracycline extravasation injury.

Authors: Brian B Hasinoff
Journal: Expert Opin Investig Drugs Date: 2008-02 Impact factor: 6.206

9. Protective effect of the bispiperazinedione ICRF-187 against doxorubicin-induced cardiac toxicity in women with advanced breast cancer.

Authors: J L Speyer; M D Green; E Kramer; M Rey; J Sanger; C Ward; N Dubin; V Ferrans; P Stecy; A Zeleniuch-Jacquotte
Journal: N Engl J Med Date: 1988-09-22 Impact factor: 91.245

Dexrazoxane for the prevention of cardiac toxicity and treatment of extravasation injury from the anthracycline antibiotics.

1. ICRF-187 permits longer treatment with doxorubicin in women with breast cancer.

2. NADPH- and adriamycin-dependent microsomal release of iron and lipid peroxidation.

3. Mitochondrial NADH dehydrogenase-catalyzed oxygen radical production by adriamycin, and the relative inactivity of 5-iminodaunorubicin.

4. Histologic changes induced in skin by extravasation of doxorubicin (adriamycin).

5. Metabolic remodeling associated with subchronic doxorubicin cardiomyopathy.

6. Suppression of doxorubicin cardiotoxicity by overexpression of catalase in the heart of transgenic mice.

Review 7. Role of iron in anthracycline cardiotoxicity: new tunes for an old song?

Review 8. The use of dexrazoxane for the prevention of anthracycline extravasation injury.

9. Protective effect of the bispiperazinedione ICRF-187 against doxorubicin-induced cardiac toxicity in women with advanced breast cancer.

10. Inhibition of nitric oxide synthase by antineoplastic anthracyclines.

Review 1. Can Some Anticancer Treatments Preserve the Ovarian Reserve?

2. Twisting and ironing: doxorubicin cardiotoxicity by mitochondrial DNA damage.

3. Dexrazoxane Diminishes Doxorubicin-Induced Acute Ovarian Damage and Preserves Ovarian Function and Fecundity in Mice.

4. Dexrazoxane Protects Cardiomyocyte from Doxorubicin-Induced Apoptosis by Modulating miR-17-5p.

5. Control of doxorubicin-induced, reactive oxygen-related apoptosis by glutathione peroxidase 1 in cardiac fibroblasts.

6. Effect of Anticancer Quinones on Reactive Oxygen Production by Adult Rat Heart Myocytes.