• Wiley Online Library will be disrupted on 26 May from 10:00-12:00 BST (05:00-07:00 EDT) for essential maintenance

Research Article

Biodistribution of [35S]-cysteine and cysteine prodrugs: potential impact on chemoprotection strategies

  1. Jeanette C. Roberts*,
  2. Holly L. Phaneuf,
  3. Pamela K. Dominick,
  4. Britta H. Wilmore,
  5. Pamela B. Cassidy

Article first published online: 9 JUL 1999

DOI: 10.1002/(SICI)1099-1344(199905)42:5<485::AID-JLCR209>3.0.CO;2-L

Issue

Journal of Labelled Compounds and Radiopharmaceuticals

Journal of Labelled Compounds and Radiopharmaceuticals

Volume 42, Issue 5, pages 485–495, May 1999

Additional Information

How to Cite

Roberts, J. C., Phaneuf, H. L., Dominick, P. K., Wilmore, B. H. and Cassidy, P. B. (1999), Biodistribution of [35S]-cysteine and cysteine prodrugs: potential impact on chemoprotection strategies. J Label Compd Radiopharm, 42: 485–495. doi: 10.1002/(SICI)1099-1344(199905)42:5<485::AID-JLCR209>3.0.CO;2-L

Author Information

  1. Department of Medicinal Chemistry, 295 BPRB, University of Utah, Salt Lake City, UT 84112, USA

*Department of Medicinal Chemistry, 295 BPRB, University of Utah, Salt Lake City, UT 84112, USA.

Publication History

  1. Issue published online: 9 JUL 1999
  2. Article first published online: 9 JUL 1999
  3. Manuscript Accepted: 25 NOV 1998
  4. Manuscript Revised: 24 NOV 1998
  5. Manuscript Received: 17 AUG 1998

SEARCH

SEARCH BY CITATION

ARTICLE TOOLS

Get PDF (394K)

Keywords:

  • L-cysteine prodrugs;
  • thiazolidines;
  • chemoprotection;
  • carbohydrate targeting

Abstract

Thiazolidine prodrugs of L-cysteine constructed with aldose monosaccharides as the carbonyl donor offer powerful protection against acetaminophen (APAP)-induced hepato-toxicity, but require large doses to be effective. Using disaccharides in prodrug synthesis produces a thiazolidine ring form with a cyclic sugar moiety present. This structural motif may allow the delivery of the prodrug to specific carbohydrate receptors, such as the asialoglycoprotein receptor (ASGPR) of hepatocytes, thus reducing the required dose of prodrug and enhancing the effectiveness of cytoprotection. The bio-distribution of [35S]-labeled prodrugs was investigated in Swiss-Webster mice, both in the presence and absence of APAP, and compared to labeled L-cysteine itself. Accumulation of radioactivity in liver appeared to be stimulated by the presence of APAP in some cases, but organ levels after prodrug administration were much lower than after the administration of L-cysteine itself. These studies identified differences in the biodistribution of L-cysteine prodrugs of different structural types, as well as effects of the hepatotoxin on localization, but the occurrence of targeted delivery to hepatocytes remains speculative. Copyright © 1999 John Wiley & Sons, Ltd.

Get PDF (394K)