1. Phase 1 trial of dichloroacetate (DCA) in adults with recurrent malignant brain tumors.
- Author
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Dunbar, E., Coats, B., Shroads, A., Langaee, T., Lew, A., Forder, J., Shuster, J., Wagner, D., and Stacpoole, P.
- Subjects
THERAPEUTIC use of biochemical markers ,INVESTIGATIONAL drugs ,ACADEMIC medical centers ,ANTINEOPLASTIC agents ,BLOOD testing ,BRAIN tumors ,CLINICAL trials ,GENES ,METASTASIS ,PHARMACEUTICAL arithmetic ,RESEARCH funding ,SAFETY ,URINALYSIS ,DISEASE relapse ,GENOMICS ,PHARMACODYNAMICS ,THERAPEUTICS - Abstract
Background Recurrent malignant brain tumors (RMBTs) carry a poor prognosis. Dichloroacetate (DCA) activates mitochondrial oxidative metabolism and has shown activity against several human cancers. Design We conducted an open-label study of oral DCA in 15 adults with recurrent WHO grade III - IV gliomas or metastases from a primary cancer outside the central nervous system. The primary objective was detection of a dose limiting toxicity for RMBTs at 4 weeks of treatment, defined as any grade 4 or 5 toxicity, or grade 3 toxicity directly attributable to DCA, based on the National Cancer Institute's Common Toxicity Criteria for Adverse Events, version 4.0. Secondary objectives involved safety, tolerability and hypothesis-generating data on disease status. Dosing was based on haplotype variation in glutathione transferase zeta 1/maleylacetoacetate isomerase (GSTZ1/MAAI), which participates in DCA and tyrosine catabolism. Results Eight patients completed at least 1 four week cycle. During this time, no dose-limiting toxicities occurred. No patient withdrew because of lack of tolerance to DCA, although 2 subjects experienced grade 0-1 distal parasthesias that led to elective withdrawal and/or dose-adjustment. All subjects completing at least 1 four week cycle remained clinically stable during this time and remained on DCA for an average of 75.5 days (range 26-312). Conclusions Chronic, oral DCA is feasible and well-tolerated in patients with recurrent malignant gliomas and other tumors metastatic to the brain using the dose range established for metabolic diseases. The importance of genetic-based dosing is confirmed and should be incorporated into future trials of chronic DCA administration. [ABSTRACT FROM AUTHOR]
- Published
- 2014
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