Small Molecules as Modulators of Different Targets Involved in Tumor Progression

Tumor is a lesion that may be formed by an abnormal growth of neoplastic cells. Many factors increase the risk of cancer and different targets are involved in tumor progression. Within this thesis, we have addressed two different biological targets, independently connected with tumor formation, e.g....

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Main Author: Ferroni, Claudia <1980>
Other Authors: Bisi, Alessandra
Format: Doctoral Thesis
Language:en
Published: Alma Mater Studiorum - Università di Bologna 2012
Subjects:
Online Access:http://amsdottorato.unibo.it/4680/
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spelling ndltd-unibo.it-oai-amsdottorato.cib.unibo.it-46802014-11-18T04:51:25Z Small Molecules as Modulators of Different Targets Involved in Tumor Progression Ferroni, Claudia <1980> CHIM/08 Chimica farmaceutica Tumor is a lesion that may be formed by an abnormal growth of neoplastic cells. Many factors increase the risk of cancer and different targets are involved in tumor progression. Within this thesis, we have addressed two different biological targets, independently connected with tumor formation, e.g. Hsp90 and androgen receptor. The ATP-dependent chaperone Hsp90 is responsible for the conformational maturation and the renaturation of proteins. “Client” proteins are associated with the cancer hallmarks, as cell proliferation and tumor progression. Consequently, Hsp90 has evolved into promising anticancer target. Over the past decade, radicicol has been identified as potential anticancer agent targeting Hsp90, but it is not active in vivo. With that aim of obtaining radicicol-related derivatives, we developed the design and synthesis of new chalcones analogs. Chalcones, which are abundant in edible plants, own a diverse array of pharmacological activities and are considered a versatile scaffold for drug design. Antiproliferative assays and western blot analysis on the new compounds showed that some of those display an interesting cytotoxic effect and the ability to modulate Hsp90 client proteins expression. Androgen Receptor (AR) hypersensitivity plays crucial role in prostate cancer, which progression is stimulated by androgens. The therapy consists in a combination of surgical or chemical castration, along with antiandrogens treatment. Casodex® (bicalutamide), is the most widespread antiandrogen used in clinic. However, hormonal therapy is time-limited since many patients develop resistance. Commercially available antiandrogens show a common scaffold, e.g. two substituted aromatic rings linked by a linear or a cyclic spacer. With the aim of obtaining novel pure AR antagonists, we developed a new synthetic methodology, which allowed us to introduce, as linker between two suitably chosen aromatic rings, a triazole moiety. Preliminary data suggest that the herein reported new molecules generally decrease PSA expression, thus confirming their potential AR antagonistic activity. Alma Mater Studiorum - Università di Bologna Bisi, Alessandra 2012-04-20 Doctoral Thesis PeerReviewed application/pdf en http://amsdottorato.unibo.it/4680/ info:eu-repo/semantics/openAccess
collection NDLTD
language en
format Doctoral Thesis
sources NDLTD
topic CHIM/08 Chimica farmaceutica
spellingShingle CHIM/08 Chimica farmaceutica
Ferroni, Claudia <1980>
Small Molecules as Modulators of Different Targets Involved in Tumor Progression
description Tumor is a lesion that may be formed by an abnormal growth of neoplastic cells. Many factors increase the risk of cancer and different targets are involved in tumor progression. Within this thesis, we have addressed two different biological targets, independently connected with tumor formation, e.g. Hsp90 and androgen receptor. The ATP-dependent chaperone Hsp90 is responsible for the conformational maturation and the renaturation of proteins. “Client” proteins are associated with the cancer hallmarks, as cell proliferation and tumor progression. Consequently, Hsp90 has evolved into promising anticancer target. Over the past decade, radicicol has been identified as potential anticancer agent targeting Hsp90, but it is not active in vivo. With that aim of obtaining radicicol-related derivatives, we developed the design and synthesis of new chalcones analogs. Chalcones, which are abundant in edible plants, own a diverse array of pharmacological activities and are considered a versatile scaffold for drug design. Antiproliferative assays and western blot analysis on the new compounds showed that some of those display an interesting cytotoxic effect and the ability to modulate Hsp90 client proteins expression. Androgen Receptor (AR) hypersensitivity plays crucial role in prostate cancer, which progression is stimulated by androgens. The therapy consists in a combination of surgical or chemical castration, along with antiandrogens treatment. Casodex® (bicalutamide), is the most widespread antiandrogen used in clinic. However, hormonal therapy is time-limited since many patients develop resistance. Commercially available antiandrogens show a common scaffold, e.g. two substituted aromatic rings linked by a linear or a cyclic spacer. With the aim of obtaining novel pure AR antagonists, we developed a new synthetic methodology, which allowed us to introduce, as linker between two suitably chosen aromatic rings, a triazole moiety. Preliminary data suggest that the herein reported new molecules generally decrease PSA expression, thus confirming their potential AR antagonistic activity.
author2 Bisi, Alessandra
author_facet Bisi, Alessandra
Ferroni, Claudia <1980>
author Ferroni, Claudia <1980>
author_sort Ferroni, Claudia <1980>
title Small Molecules as Modulators of Different Targets Involved in Tumor Progression
title_short Small Molecules as Modulators of Different Targets Involved in Tumor Progression
title_full Small Molecules as Modulators of Different Targets Involved in Tumor Progression
title_fullStr Small Molecules as Modulators of Different Targets Involved in Tumor Progression
title_full_unstemmed Small Molecules as Modulators of Different Targets Involved in Tumor Progression
title_sort small molecules as modulators of different targets involved in tumor progression
publisher Alma Mater Studiorum - Università di Bologna
publishDate 2012
url http://amsdottorato.unibo.it/4680/
work_keys_str_mv AT ferroniclaudia1980 smallmoleculesasmodulatorsofdifferenttargetsinvolvedintumorprogression
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