Cancer Res. 2004 Feb 1;64(3):1114-21.

Cullin 3 promotes proteasomal degradation of the topoisomerase I-DNA covalent complex.

Zhang HF, Tomida A, Koshimizu R, Ogiso Y, Lei S, Tsuruo T.

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Institute of Molecular and Cellular Biosciences, The University of Tokyo, Tokyo, Japan.

Abstract

DNA topoisomerase I (TOP1)-DNA covalent complexes are the initial lesions produced by antitumor camptothecins (CPTs). The TOP1-directed drugs stimulate degradation of TOP1 via the ubiquitin-proteasome pathway. We found that proteasome inhibition prevents degradation of DNA-bound TOP1 and sustains high levels of covalent complexes, thus enhancing CPT-induced cell death. Consistent with this, increased degradation of TOP1-DNA covalent complexes was seen in acquired CPT-resistant cells. We found that the resistant cells showed elevated expressions of Cul3, a member of the cullin family of E3 ubiquitin ligases. The reduction in Cul3 expression by small interfering RNA decreased degradation of TOP1-DNA covalent complexes. Conversely, Cul3 overexpression by stable transfection promoted covalent complex degradation and reduced CPT-induced cell death without affecting basal TOP1 expression levels. These results indicate that Cul3, by promoting proteasomal degradation of TOP1-DNA covalent complexes, becomes an important regulator for cellular CPT sensitivity.

PMID:: 14871846; [PubMed - indexed for MEDLINE]

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