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Comprehensive Account on the Synthesis of (-)-Balanol and its Analogues
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Background:
A variety of diseases have been associated with hyperactivation of
protein kinase C (PKC) enzymes such as cancer, diabetes, asthma, cardiovascular and central
nervous system disorders. There is a dire need to selectively inhibit these enzymes by
synthesizing new potent inhibitors. Balanol, a fungal metabolite belonging to the PKC inhibitor
family, is especially included in this aspect. Tremendous effort has been put towards the
synthesis of balanol by different research groups.
Objective:
The aim of this review is to provide a detailed description of synthetic approaches
adopted for the synthesis of key fragments of balanol (azepane and benzophenone). All the
factors that resulted in excellent yield and high enantioselectivity have also been mentioned.
Conclusion:
It has been shown throughout this review that the synthesis of hexahydroazepine
and benzophenone cores of balanol was achieved by employing a variety of important key steps
with commercially available starting precursors, which make this total synthesis more valuable.
Moreover, this article provides ideas to the synthetic as well as pharmaceutical chemists for the
synthesis of (-)-balanol and its analogues.
Bentham Science Publishers Ltd.
Title: Comprehensive Account on the Synthesis of (-)-Balanol and its Analogues
Description:
Background:
A variety of diseases have been associated with hyperactivation of
protein kinase C (PKC) enzymes such as cancer, diabetes, asthma, cardiovascular and central
nervous system disorders.
There is a dire need to selectively inhibit these enzymes by
synthesizing new potent inhibitors.
Balanol, a fungal metabolite belonging to the PKC inhibitor
family, is especially included in this aspect.
Tremendous effort has been put towards the
synthesis of balanol by different research groups.
Objective:
The aim of this review is to provide a detailed description of synthetic approaches
adopted for the synthesis of key fragments of balanol (azepane and benzophenone).
All the
factors that resulted in excellent yield and high enantioselectivity have also been mentioned.
Conclusion:
It has been shown throughout this review that the synthesis of hexahydroazepine
and benzophenone cores of balanol was achieved by employing a variety of important key steps
with commercially available starting precursors, which make this total synthesis more valuable.
Moreover, this article provides ideas to the synthetic as well as pharmaceutical chemists for the
synthesis of (-)-balanol and its analogues.
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