Safety Experience with Trisenox® (Arsenic Trioxide) Injection.

Holman, Joan; Kirkhart, Barbara; Maxon, M. Scot; Oliva, Cristina; Earhart, Robert H.

doi:10.1182/blood.v104.11.4521.4521

Cited by 2 publications

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“…The adverse events noted in postmarketing use of As 2 O 3 are generally similar to those observed in clinical trials, and no deaths due to As 2 O 3 related cardiac arrhythmia have been reported. This experience appears to confirm that As 2 O 3 is generally well tolerated and that the observed adverse effects are manageable and reversible [28] . However, when 7 patients with refractory or relapsed APL were treated with As 2 O 3 , 6 noted water retention (shown by weight gain, pleural and pericardial exudates); 2 of 3 patients on As 2 O 3 maintenance therapy showed polyneuropathy related to chronic arsenic poisoning, and 1 of those 2 patients suffered myoatrophy of a limb end [29] .…”

Section: Toxicity and Side Effectssupporting

confidence: 57%

On arsenic trioxide in the clinical treatment of acute promyelocytic leukemia

Zhang

2017

Leukemia Research Reports

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Arsenic is generally considered hypertoxic. However, it has been used in traditional Chinese medicine since ancient times, to treat serious illnesses. Recently, a single dose of arsenic trioxide (As2O3) has been found especially effective in treating acute promyelocytic leukemia (APL). Generally speaking, As2O3 is a more effective treatment of APL than other, newer medications and has less severe adverse reactions and greater safety.

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Section: Toxicity and Side Effectssupporting

confidence: 57%

On arsenic trioxide in the clinical treatment of acute promyelocytic leukemia

Zhang

2017

Leukemia Research Reports

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“…However, because of its adverse effects and the emergence of new treatments, its use in treating these diseases has been avoided. Nonetheless, arsenic trioxide remains relevant, as in 2000, the FDA approved [61] this compound for use in the treatment of acute promyelocytic leukemia [34,62]. Paul Ehrlich, who is the "father of chemotherapy", having introduced the concepts of specific targets when developing new drugs, introduced Salvarsan in 1910 as an effective treatment for syphilis [35].…”

Section: Historical Timeline Of Anticancer Drugs: Casiopeínas ®mentioning

confidence: 99%

The Importance of Being Casiopeina as Polypharmacologycal Profile (Mixed Chelate–Copper (II) Complexes and Their In Vitro and In Vivo Activities)

Aguilar-Jiménez,

Espinoza-Guillén,

Resendiz-Acevedo

et al. 2023

Inorganics

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In this review, we present a timeline that shows the origin of mixed chelate copper (II) complexes, registered as Mark Title Casiopeínas®, as the first copper (II) compounds proposed as anticancer drugs in 1988 and 1992. In the late twentieth century, the use of essential metals as anticancer agents was not even considered, except for their antifungal or antibacterial effects; also, copper, as gold salts, was used for arthritis problems. The use of essential metals as anticancer drugs to diminish the secondary toxic effects of Cisplatin was our driving force: to find less toxic and even more economical compounds under the rational design of metal chelate complexes. Due to their chemical properties, copper compounds were the choice to continue anticancer drug development. In this order of ideas, the rational designs of mixed chelate–copper (II) complexes (Casiopeínas, (Cas) homoleptic or heteroleptic, depending on the nature of the secondary ligand) were synthesized and fully characterized. In the search for new, more effective, and less toxic drugs, Casiopeína® (Cas) emerged as a family of approximately 100 compounds synthesized from coordinated Cu(II) complexes with proven antineoplastic potential through cytotoxic action. The Cas have the general formula [Cu(N–N)(N–O)]NO3 and [Cu(N–N)(O–O)]NO3, where N–N is an aromatic substituted diimine (1,10-phenanthroline or 2,2′-bipyridine), and the oxygen donor (O–O) is acetylacetonate or salicylaldehyde. Lately, some similar compounds have been developed by other research groups considering a similar hypothesis after Casiopeína’s discoveries had been published, as described herein. As an example of translational medicine criteria, we have covered each step of the established normative process for drug development, and consequently, one of the molecules (Casiopeína III ia (CasIIIia)) has reached the clinical phase I. For these copper compounds, other activities, such as antibacterial, antiparasitic and antiviral, have been discovered.

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Safety Experience with Trisenox® (Arsenic Trioxide) Injection.

Cited by 2 publications

References 0 publications

On arsenic trioxide in the clinical treatment of acute promyelocytic leukemia

On arsenic trioxide in the clinical treatment of acute promyelocytic leukemia

The Importance of Being Casiopeina as Polypharmacologycal Profile (Mixed Chelate–Copper (II) Complexes and Their In Vitro and In Vivo Activities)

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