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Monosaccharide-based beta turn mimetics for the somatostatin and neurokinin-1 receptors.
紀錄類型:
書目-電子資源 : Monograph/item
正題名/作者:
Monosaccharide-based beta turn mimetics for the somatostatin and neurokinin-1 receptors.
作者:
McVaugh, Cheryl T.
面頁冊數:
349 p.
附註:
Source: Dissertation Abstracts International, Volume: 64-04, Section: B, page: 1735.
附註:
Supervisors: Ralph Hirschmann; Amos B. Smith, III.
Contained By:
Dissertation Abstracts International64-04B.
標題:
Chemistry, Organic.
電子資源:
http://pqdd.sinica.edu.tw/twdaoapp/servlet/advanced?query=3087434
ISBN:
0496352040
Monosaccharide-based beta turn mimetics for the somatostatin and neurokinin-1 receptors.
McVaugh, Cheryl T.
Monosaccharide-based beta turn mimetics for the somatostatin and neurokinin-1 receptors.
[electronic resource] - 349 p.
Source: Dissertation Abstracts International, Volume: 64-04, Section: B, page: 1735.
Thesis (Ph.D.)--University of Pennsylvania, 2003.
*Please refer to dissertation for diagrams.
ISBN: 0496352040Subjects--Topical Terms:
193634
Chemistry, Organic.
Monosaccharide-based beta turn mimetics for the somatostatin and neurokinin-1 receptors.
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Supervisors: Ralph Hirschmann; Amos B. Smith, III.
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*Please refer to dissertation for diagrams.
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In Chapter 1, the application of mono saccharide-based peptidomimetics at the human somatostatin subtype-4 (hSST4) receptor is discussed. Incorporation of heterocyclic substituents, such as pyridin-3-ylmethyl, pyrazin-2-ylmethyl and 2-fluoropyridin-3-ylmethyl (typified by (+)-1--2), at the C4 position of the glucose scaffold afforded an unexpected affinity enhancement. Evidence suggests that a hydrogen bond between the substituent and the hSST4 receptor is responsible for this affinity enhancement. Additionally, incorporation of an imidazole substituent at the C2 position afforded (-)-1--28, a 53 nM hSST4 ligand. Preparation of (-)-1--29 to explore this affinity-enhancement revealed that imidazole by itself is not enough to enhance affinity in this series, but the presence of pyridin-3-ylmethyl is required. This resulted is explained by conformational analysis wherein the exocyclic C-O bond is eclipsed.*
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In Chapter 2, the affinity of (+)-0--1 for the neurokinin-1 receptor (hNK-1) is attempted to be explained through structural correlation with other classes of NK-1 receptor ligands. In Chapter 3 describes how optimization of the affinity of (+)-0--1 at the NK-1 receptor was accomplished by placing the side chains at different contiguous positions on the glucose scaffold; elucidation of the SAR of (-)-3--4 led to the discovery of 8 nM hNK-1 receptor ligand (-)-3--12. Finally, the radial symmetry inherent to the glucose scaffold is postulated to be a major contributing factor for the established usefulness of former in lead discovery.*
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This dissertation describes the design and synthesis of mono saccharide-based peptidomimetics for the somatostatin and neurokinin-1 receptors. The introductory chapter gives a brief overview of the use of carbohydrates as peptidomimetic scaffolds, with examples from the Hirschmann-Smith laboratories, as well as the laboratories of others.
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