Category

Archives

Preclinical pharmacologic evaluation of geldanamycin as an antitumor agent

The plasma pharmacokinetics of the anti-tumor antibiotic geldanamycin (GM: NSC 122750), a naturally occurring benzoquinoid ansamycin, was characterized in mice and a beagle dog. Concentrations of GM well above 0.1 microgram/ml, which was typically effective against neoplastic cell lines responsive to the drug in vitro, were achieved in the plasma of the mice and the dog treated by i.v. injection. However, the systemic duration of the drug was relatively short. Plasma levels decayed below 0.1 microgram/ml within 3-4 h after administration of the apparent maximum tolerated doses, which were approximately 20 mg/kg for the mice and 4 mg/kg for the dog. The drug exhibited linear pharmacokinetic behavior within the dose ranges studied. However, there were significant interspecies differences in its disposition. Whereas the mean biological half-life of GM was slightly longer in the mice (77.7 min) than in the dog (57.9 min), its mean residence time in the dog (46.6 min) was more than twofold greater than that observed in the mice (20.7 min). Nevertheless, the drug was cleared from plasma much faster by the dog (49.4 ml/min per kg) than by the mice (30.5 ml/min per kg). These apparent anomalies were principally associated with differences in the relative significance of the terminal phase upon overall drug disposition. The liver appeared to be the principal target organ of acute drug toxicity in the dog. Doses of 2.0 and 4.2 mg/kg both produced elevations in serum levels of the transaminases and other indicators of liver function characteristic of acute hepatic necrosis. Additional effects included symptoms of minor gastrointestinal toxicity and alterations in serum chemistry parameters consistent with less severe nephrotoxicity. Drug-related toxicity appeared to be reversible. In consideration of the potential for acute hepatotoxic reactions to GM, as well as to the other benzoquinoid ansamycins based upon structural analogy, additional pharmacological and therapeutic information is required to ascertain whether these compounds are viable candidates for clinical development.

 

Comments:

The passage describes the pharmacokinetics of the anti-tumor antibiotic geldanamycin (GM) in mice and a beagle dog. The drug achieved plasma concentrations well above the minimum effective concentration for neoplastic cell lines in vitro, but the systemic duration of the drug was relatively short, with plasma levels declining below the minimum effective concentration within 3-4 hours after administration of the maximum tolerated doses. The drug exhibited linear pharmacokinetic behavior within the dose ranges studied, but there were significant interspecies differences in its disposition, with the liver being the principal target organ of acute drug toxicity in the dog.

The study indicates that more pharmacological and therapeutic information is needed to determine whether GM and other benzoquinoid ansamycins based on structural analogy are viable candidates for clinical development due to their potential for acute hepatotoxic reactions.

 

Related Products

Cat.No. Product Name Information
S2713 Geldanamycin Geldanamycin is a natural existing HSP90 inhibitor with Kd of 1.2 μM, specifically disrupts glucocorticoid receptor (GR)/HSP association. Geldanamycin attenuates virus infection-induced ALI (acute lung injury)/ARDS (acute respiratory distress syndrome) by reducing the host's inflammatory responses.

Related Targets

Autophagy HSP (HSP90) Antiviral Antineoplastic and Immunosuppressive Antibiotics