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The purpose of this page is to explain a semisynthetic derivative of podophyllotoxin [[Image:PODO.png|thumb|right|50 px|Chemical structure of podophyllotoxin]] (etoposide) that demonstrates antitumor activity by inhibiting DNA topoisomerase II, thereby inhibiting DNA re-ligation which lead to apoptosis of the cancer cell and also, to describe the mechanisms of resistance of etoposide.
The purpose of this page is to explain a semisynthetic derivative of podophyllotoxin [[Image:PODO.png|thumb|right|50 px|Chemical structure of podophyllotoxin]] (etoposide) that demonstrates antitumor activity by inhibiting DNA topoisomerase II, thereby inhibiting DNA re-ligation which lead to apoptosis of the cancer cell and also, to describe the mechanisms of resistance of etoposide.
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[http://www.en.wikipedia.org/wiki/Podophyllotoxin/ptp]
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[http://en.wikipedia.org/wiki/Podophyllotoxin-pop]
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==INTRODUCTION ==
==INTRODUCTION ==

Revision as of 18:50, 25 November 2012

Human topoisomerase IIbeta in complex with DNA and etoposide

Structure of the human topoisomeraseIIbcore-DNA cleavage complex stabilized by the anticancer drug etoposide. (PDB entry 3QX3)

Drag the structure with the mouse to rotate


References

  1. Wu CC, Li TK, Farh L, Lin LY, Lin TS, Yu YJ, Yen TJ, Chiang CW, Chan NL. Structural basis of type II topoisomerase inhibition by the anticancer drug etoposide. Science. 2011 Jul 22;333(6041):459-62. PMID:21778401 doi:10.1126/science.1204117
  2. Kathryn L. Gilroy, Chrysoula Leontiou, Kay Padget, Jeremy H. Lakey and Caroline A. Austin* "mAMSA resistant human topoisomerase IIβ mutation G465D has reduced ATP hydrolysis activity” Oxford JournalsLife Sciences Nucleic Acids Research Volume 34, Issue 5Pp. 1597-1607. DOI: 10.1093/nar/gkl057
  3. Wu CC, Li TK, Farh L, Lin LY, Lin TS, Yu YJ, Yen TJ, Chiang CW, Chan NL. Structural basis of type II topoisomerase inhibition by the anticancer drug etoposide. Science. 2011 Jul 22;333(6041):459-62. PMID:21778401 doi:10.1126/science.1204117
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