Structure–Activity Relationships for Development of Neurokinin-3 Receptor Antagonists

Reducing Environmental Impact

Specificaties
Gebonden, blz. | Engels
Springer Nature Singapore | e druk, 2020
ISBN13: 9789811529641
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Juridisch :
Springer Nature Singapore e druk, 2020 9789811529641
Onderdeel van serie Springer Theses
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This book explores the possible development of neurokinin-3 receptor (NK3R) antagonists with reduced environmental impact. Pharmaceuticals are used to cure diseases and to alleviate symptoms in humans and animals. However, the stable, bioactive substances excreted by patients have unfavorable effects on non-target species. To overcome these disadvantages of these highly stable, potent substances, drug design to turn off bioactivity after release into the environment is needed. The book describes the development of eco-friendly NK3R antagonists by introducing a labile functional moiety and substituting a scaffold. This resulted in a novel NK3R antagonist that oxidized into its inactive form when exposed to air. Further, the book presents an efficient and easily achievable synthetic method of creating triazolopiperazine scaffolds, as well as a structure–activity relationship study involving scaffold hopping for decomposable motifs, which led to a novel photodegradable NK3R antagonist. Demonstrating that it is possible to develop compounds that convert into their inactive forms under environmental conditions, this book is useful for anyone interested in therapeutic agents with reduced environmental impact.

Specificaties

ISBN13:9789811529641
Taal:Engels
Bindwijze:gebonden
Uitgever:Springer Nature Singapore

Inhoudsopgave

1. Introduction.- 2. Development of NK3R Antagonists with a Labile Functional Group in the Natural Environment.- 3. Development of NK3R Antagonists with a Degradable Scaffold in the Natural Environment: Synthesis and Application of Fused Piperazine Derivatives for Investigation of Degradable Core Motifs.- 4. Development of NK3R Antagonists with a Degradable Scaffold in the Natural Environment: Identification of NK3R Antagonists with a Decomposable Core Structure by Scaffold Hopping.- 5. Conclusion.

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        Structure–Activity Relationships for Development of Neurokinin-3 Receptor Antagonists