Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors

Developing safer and/ or more effective chemotherapeutics has been a long-standing challenge in the drug discovery field. To address these shortcomings, the designed-multiple ligand (DML) and targeted approaches were used to design novel series of histone deacetylase inhibitors (HDACi). Under the DM...

Full description

Bibliographic Details
Main Author: Raji, Idris
Other Authors: Oyelere, Adegboyega K., Finn, M. G., France, Stefan, Bommarius, Andreas, Bellamkonda, Ravi, Chemistry and Biochemistry
Format: Doctoral or Postdoctoral Thesis
Language:English
Published: Georgia Institute of Technology 2018
Subjects:
Histone deacetylase
HDACi
Cyclooxygenase
Macrolide
Clarithromycin
Melanoma
Designed-multiple ligand
Lung cancer
Prostate cancer
Liposome
PGE2
NF-kB
Celecoxib
Indomethacin
Benzamides
Androgen receptor
DML
Online Access:http://hdl.handle.net/1853/59152
id ftgeorgiatech:oai:repository.gatech.edu:1853/59152
record_format openpolar
spelling ftgeorgiatech:oai:repository.gatech.edu:1853/59152 2024-06-02T08:05:48+00:00 Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors Raji, Idris Oyelere, Adegboyega K. Finn, M. G. France, Stefan Bommarius, Andreas Bellamkonda, Ravi Chemistry and Biochemistry 2018-01-22T21:04:10Z application/pdf http://hdl.handle.net/1853/59152 en_US eng Georgia Institute of Technology http://hdl.handle.net/1853/59152 Histone deacetylase HDACi Cyclooxygenase Macrolide Clarithromycin Melanoma Designed-multiple ligand Lung cancer Prostate cancer Liposome PGE2 NF-kB Celecoxib Indomethacin Benzamides Androgen receptor Text Dissertation 2018 ftgeorgiatech 2024-05-06T11:44:58Z Developing safer and/ or more effective chemotherapeutics has been a long-standing challenge in the drug discovery field. To address these shortcomings, the designed-multiple ligand (DML) and targeted approaches were used to design novel series of histone deacetylase inhibitors (HDACi). Under the DML approach, bifunctional compounds capable of binding to both histone deacetylase and cyclooxygenase enzymes were made. A subset of the bifunctional compounds was significantly less toxic towards healthy cells compared to the US Food Drug and Administration (FDA) approved HDACi, vorinostat, despite their impressive anticancer profiles. On the other hand, the targeted approach was conceptualized to address the lack of efficacy in solid tumors seen with clinically approved HDACi. Two different series of compounds are reported herein as potential interventions in lung cancer and melanoma. In one of the series, clarithromycin- known for its preferential accumulation in lung tissues, was incorporated into the structures of HDACi to generate clarithromycin-targeted HDACi. With the eventual goal of achieving compounds that will preferentially localize in lung cancer tissues, the clarithromycin-targeted HDACi showed very good anticancer profiles in in vitro studies. The second series of compounds generated using the targeted approach are aimed as potential intervention in melanoma. In this approach, a template, known as benzamide, with high affinity for melanin, was incorporated into the design of HDACi. The benzamide compounds obtained showed some promise in melanoma cell lines, and warrant further studies to optimize for potency. Ph.D. Doctoral or Postdoctoral Thesis DML Georgia Institute of Technology: SMARTech - Scholarly Materials and Research at Georgia Tech
institution Open Polar
collection Georgia Institute of Technology: SMARTech - Scholarly Materials and Research at Georgia Tech
op_collection_id ftgeorgiatech
language English
topic Histone deacetylase
HDACi
Cyclooxygenase
Macrolide
Clarithromycin
Melanoma
Designed-multiple ligand
Lung cancer
Prostate cancer
Liposome
PGE2
NF-kB
Celecoxib
Indomethacin
Benzamides
Androgen receptor
spellingShingle Histone deacetylase
HDACi
Cyclooxygenase
Macrolide
Clarithromycin
Melanoma
Designed-multiple ligand
Lung cancer
Prostate cancer
Liposome
PGE2
NF-kB
Celecoxib
Indomethacin
Benzamides
Androgen receptor
Raji, Idris
Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
topic_facet Histone deacetylase
HDACi
Cyclooxygenase
Macrolide
Clarithromycin
Melanoma
Designed-multiple ligand
Lung cancer
Prostate cancer
Liposome
PGE2
NF-kB
Celecoxib
Indomethacin
Benzamides
Androgen receptor
description Developing safer and/ or more effective chemotherapeutics has been a long-standing challenge in the drug discovery field. To address these shortcomings, the designed-multiple ligand (DML) and targeted approaches were used to design novel series of histone deacetylase inhibitors (HDACi). Under the DML approach, bifunctional compounds capable of binding to both histone deacetylase and cyclooxygenase enzymes were made. A subset of the bifunctional compounds was significantly less toxic towards healthy cells compared to the US Food Drug and Administration (FDA) approved HDACi, vorinostat, despite their impressive anticancer profiles. On the other hand, the targeted approach was conceptualized to address the lack of efficacy in solid tumors seen with clinically approved HDACi. Two different series of compounds are reported herein as potential interventions in lung cancer and melanoma. In one of the series, clarithromycin- known for its preferential accumulation in lung tissues, was incorporated into the structures of HDACi to generate clarithromycin-targeted HDACi. With the eventual goal of achieving compounds that will preferentially localize in lung cancer tissues, the clarithromycin-targeted HDACi showed very good anticancer profiles in in vitro studies. The second series of compounds generated using the targeted approach are aimed as potential intervention in melanoma. In this approach, a template, known as benzamide, with high affinity for melanin, was incorporated into the design of HDACi. The benzamide compounds obtained showed some promise in melanoma cell lines, and warrant further studies to optimize for potency. Ph.D.
author2 Oyelere, Adegboyega K.
Finn, M. G.
France, Stefan
Bommarius, Andreas
Bellamkonda, Ravi
Chemistry and Biochemistry
format Doctoral or Postdoctoral Thesis
author Raji, Idris
author_facet Raji, Idris
author_sort Raji, Idris
title Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
title_short Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
title_full Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
title_fullStr Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
title_full_unstemmed Novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
title_sort novel approaches towards the discovery of tumor-selective histone deacetylase inhibitors
publisher Georgia Institute of Technology
publishDate 2018
url http://hdl.handle.net/1853/59152
genre DML
genre_facet DML
op_relation http://hdl.handle.net/1853/59152
_version_ 1800750687135465472

Similar Items