A comprehensive study of Sansalvamide A derivatives: the structure-activity relationships of 78 derivatives in 2 pancreatic cancer cell lines

A comprehensive study of Sansalvamide A derivatives: the structure-activity relationships of 78 derivatives in 2 pancreatic cancer cell lines

We report an extensive structure-activity relationship (SAR) of seventy-eight compounds active against two pancreatic cancer cell lines. Our comprehensive evaluation of these compounds utilizes SAR that allow us to evaluate which features of potent compounds play a key role in their cytotoxicity. Th...

Full description

Saved in:
Bibliographic Details
Published in:Bioorganic & medicinal chemistry Vol. 17; no. 16; pp. 5806 - 5825
Main Authors: Pan, Po-Shen, Vasko, Robert C., Lapera, Stephanie A., Johnson, Victoria A., Sellers, Robert P., Lin, Chun-Chieh, Pan, Chung-Mao, Davis, Melinda R., Ardi, Veronica C., McAlpine, Shelli R.
Format: Journal Article
Language:English
Published: 15-07-2009
Online Access:Get full text
Tags: Add Tag
No Tags, Be the first to tag this record!
Description
Summary:We report an extensive structure-activity relationship (SAR) of seventy-eight compounds active against two pancreatic cancer cell lines. Our comprehensive evaluation of these compounds utilizes SAR that allow us to evaluate which features of potent compounds play a key role in their cytotoxicity. This is the first report of 19 new second-generation structures, where these new compounds were designed from the first generation of 59 compounds. These 78 structures were tested for their cytotoxicity and this is the first report of their activity against 2 pancreatic cancer cell lines. Our results show that out of 78 compounds, three compounds are worth pursuing as leads, as they show potency of ≥55% in both cancer cell lines. These three compounds all have a common structural motif, 2 consecutive D-amino acids and an N-methyl moiety. Further, of these three compounds, two are second-generation structures, indicating that we can incorporate and utilize data from the first generation to design potency into the second generation. Finally, one analog is in the mid nanomolar range, and has the lowest IC 50 of any reported San A derivative. These analogs share no structural homology to current pancreatic cancer drugs, and are cytotoxic at levels on par with existing drugs treating other cancers. Thus, we have established Sansalvamide A as an excellent lead for killing multiple pancreatic cancer cell lines.
ISSN:0968-0896
1464-3391
DOI:10.1016/j.bmc.2009.07.017