Literature DB >> 9816201

Tissue and tumor distribution of C-penclomedine in rats.

S O'Reilly1, N R Hartman, S A Grossman, J M Strong, R F Struck, S Eller, G J Lesser, R C Donehower, E K Rowinsky.   

Abstract

Penclomedine, a lipophilic alpha-picoline derivative, is undergoing clinical development presently because of its pronounced antitumor activity against intracerebral (i.c.) tumor xenografts. Penclomedine may be metabolized in vivo to a more potent compound. Although it may be useful in the treatment of brain tumors, the drug has caused significant neurotoxicity in early clinical trials. The possibility that antitumor activity and neurotoxicity may be mediated by different mechanisms prompted a study assessing the differential distribution of penclomedine and penclomedine metabolites to brain and i.c.-implanted tumors in rats. In the present study, quantitative autoradiographic analysis demonstrated a homogenous distribution of 14C-penclomedine in all organs within 1 h of administration. Levels of 14C-penclomedine in both i.c. and s.c. tumors were three times higher than in normal brain tissue. High-performance liquid chromatography combined with gas chromatography and mass spectrophotometry demonstrated that two metabolites, O-demethyl penclomedine and penclomic acid, were responsible for most of the plasma radioactivity. Penclomic acid was also the most common urinary metabolite of penclomedine. In liver samples, although a large number of metabolite peaks were detected, no parent compound could be identified. However, in tumors and all other tissues, penclomedine was the main compound detected. The finding of penclomedine in normal brain tissue indicates not only that this drug may be useful in tumors with normal blood-brain barrier function, but also that it may be directly neurotoxic.

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Year:  1996        PMID: 9816201

Source DB:  PubMed          Journal:  Clin Cancer Res        ISSN: 1078-0432            Impact factor:   12.531


  2 in total

1.  The alkylating agent penclomedine induces degeneration of purkinje cells in the rat cerebellum.

Authors:  Seamus O'Reilly; Elizabeth O'Hearn; Robert F Struck; Eric K Rowinsky; Mark E Molliver
Journal:  Invest New Drugs       Date:  2003-08       Impact factor: 3.850

2.  Carbonate and carbamate derivatives of 4-demethylpenclomedine as novel anticancer agents.

Authors:  Lee Roy Morgan; Robert F Struck; William R Waud; Blaise LeBlanc; Andrew H Rodgers; Branko S Jursic
Journal:  Cancer Chemother Pharmacol       Date:  2009-03-03       Impact factor: 3.333

  2 in total

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