Synthesis and Cytotoxicity of 2,4-Disubstituted and 2,3,4-Trisubstituted Brominated Pyrroles in Murine and Human Cultured Tumor Cells

“…These compounds represent an emerging class of agents with potential activity against a variety of human tumors with activity expressed at nM or µM concentrations in human tumor cell lines [18,19], but having advantages over natural products in terms of drug design and development. In particular, we have been exploring a series of brominated pyrroles whose structure suggests that they might interfere with tubulin function.…”

“…In particular, we have been exploring a series of brominated pyrroles whose structure suggests that they might interfere with tubulin function. One member of this series (JG-03-14, 3,5-dibromo-4-(3,4-dimethoxyphenyl)-1H-pyrrole-2-carboxylic acid ethyl ester), for which NCI tumor panel activity had been obtained [19], was suggested by COMPARE [16] to have an activity profile similar to colchicine. Cellular studies with JG-03-14 further support the contention that these compounds function as microtubule poisons [18].…”

“…In addition, JG-03-14 was found to have the capacity to promote both autophagic and apoptotic cell death, albeit in different cell lines, while retaining activity in tumor cells expressing the multidrug resistant pump P-glycoprotein [18,24]. Because the development of additional synthetic or semi-synthetic pyrrole derivatives in this class is facilitated with their relatively facile syntheses, including modification of the molecule by adding and removing functional groups [19], we have both a rather extensive collection of molecules in-hand (Scheme 1) for building predictive molecular models and the potential for rational design and synthesis of many others.…”

“…Results from a number of assays have previously appeared regarding the antiproliferative and cytotoxic activities of the lead compound JG-03-14 [18,19,24]. However, most of the compounds in this series have not been examined in detail.…”

“…The synthetic methods used to prepare the highly functionalized pyrroles and related derivatives depicted in Scheme I can be found in previously reported work [19][20][21][22][23].…”

Docking and hydropathic scoring of polysubstituted pyrrole compounds with antitubulin activity

“…These compounds represent an emerging class of agents with potential activity against a variety of human tumors with activity expressed at nM or µM concentrations in human tumor cell lines [18,19], but having advantages over natural products in terms of drug design and development. In particular, we have been exploring a series of brominated pyrroles whose structure suggests that they might interfere with tubulin function.…”

“…In particular, we have been exploring a series of brominated pyrroles whose structure suggests that they might interfere with tubulin function. One member of this series (JG-03-14, 3,5-dibromo-4-(3,4-dimethoxyphenyl)-1H-pyrrole-2-carboxylic acid ethyl ester), for which NCI tumor panel activity had been obtained [19], was suggested by COMPARE [16] to have an activity profile similar to colchicine. Cellular studies with JG-03-14 further support the contention that these compounds function as microtubule poisons [18].…”

“…In addition, JG-03-14 was found to have the capacity to promote both autophagic and apoptotic cell death, albeit in different cell lines, while retaining activity in tumor cells expressing the multidrug resistant pump P-glycoprotein [18,24]. Because the development of additional synthetic or semi-synthetic pyrrole derivatives in this class is facilitated with their relatively facile syntheses, including modification of the molecule by adding and removing functional groups [19], we have both a rather extensive collection of molecules in-hand (Scheme 1) for building predictive molecular models and the potential for rational design and synthesis of many others.…”

“…Results from a number of assays have previously appeared regarding the antiproliferative and cytotoxic activities of the lead compound JG-03-14 [18,19,24]. However, most of the compounds in this series have not been examined in detail.…”

“…The synthetic methods used to prepare the highly functionalized pyrroles and related derivatives depicted in Scheme I can be found in previously reported work [19][20][21][22][23].…”

Docking and hydropathic scoring of polysubstituted pyrrole compounds with antitubulin activity

Synthesis and Cytotoxicity of Substituted Ethyl 2‐Phenacyl‐3‐phenylpyrrole‐4‐carboxylates

Pyrrole Natural Products with Antitumor Properties