Your search keyword '"allotopic"' showing total 5 results

1. Studies toward bivalent κ opioids derived from salvinorin A: heteromethylation of the furan ring reduces affinity

Author

Thomas A. Munro, Wei Xu, Douglas M. Ho, Lee-Yuan Liu-Chen, and Bruce M. Cohen

Subjects

allotopic, bivalent ligand, designed multiple ligand, JDTic, κ-opioid receptor, natural products, Salvinorin A, Science, Organic chemistry, QD241-441

Abstract

The recent crystal structure of the κ-opioid receptor (κ-OR) revealed, unexpectedly, that the antagonist JDTic is a bivalent ligand: in addition to the orthosteric pocket occupied by morphinans, JDTic also occupies a distinct (allotopic) pocket. Mutagenesis data suggest that salvinorin A (1) also binds to this allotopic pocket, adjacent to the aspartate residue that anchors the basic nitrogen atom of classical opiates (Asp138). It has been suggested that an H-bond donor appended to 1 might interact with Asp138, increasing affinity. Such a bivalent ligand might also possess altered functional selectivity. Based on modeling and known N-furanylmethyl opioid antagonists, we appended H-bond donors to the furan ring of 1. (Dimethylamino)methyl groups at C-15 or C-16 abolished affinity for κ-OR. Hydroxymethylation at C-16 was tolerated, but 15,16-bis-hydroxymethylation was not. Since allosteric modulators may go undetected in binding assays, we also tested these and other low-affinity derivatives of 1 for allosteric modulation of dynorphin A in the [35S]GTPγS assay. No modulation was detected. As an alternative attachment point for bivalent derivatives, we prepared the 2-(hydroxyethoxy)methyl ether, which retained high affinity for κ-OR. We discuss alternative design strategies for linked, fused or merged bivalent derivatives of 1.

Published

2013

2. Settlement and possible competition for space between the invasive violet tunicate Botrylloides violaceus and the native star tunicate Botryllus schlosseri in The Netherlands.

Author

Gittenberger, Adriaan and Moons, Jean Jacques Simeon

Subjects

SEA squirts, BOTRYLLOIDES violaceus, COMPETITION (Biology), SPECIES, TUNICATA

Abstract

Settlement and competition for space of two colonial sea squirts, the non-native violet tunicate Botrylloides violaceus and the native golden star tunicate Botryllus schlosseri, were compared in The Netherlands. In each year, from March 2006 to March 2010, 125-150 grey, 14 × 14 cm, PVC plates were deployed along the Dutch coast at 13 localities, at a depth of 1 m, and checked for species after three and six months. New plates were deployed every three months. While comparing plates with only one species represented to plates with both species represented, it appeared that Botrylloides violaceus outcompeted Botryllus schlosseri for space. Botryllus schlosseri is nevertheless expected to remain abundant along the Dutch coast because it can inhabit places with low or fluctuating salinities where Botrylloides violaceus is at a disadvantage. Settlement and the interactions between these species in The Netherlands resembled the situation in North America where both of them are considered non-native. The interactions between the two species seemed to be independent of their being native or introduced in a particular area. [ABSTRACT FROM AUTHOR]

Published

2011

3. Studies toward bivalent κ opioids derived from salvinorin A: heteromethylation of the furan ring reduces affinity

Author

Bruce M. Cohen, Thomas A. Munro, Wei Xu, Lee-Yuan Liu-Chen, and Douglas M. Ho

Subjects

natural products, Stereochemistry, Organic Chemistry, Allosteric regulation, Dynorphin A, Ether, JDTic, Salvinorin A, Morphinans, Full Research Paper, Bivalent (genetics), lcsh:QD241-441, Chemistry, chemistry.chemical_compound, lcsh:Organic chemistry, chemistry, designed multiple ligand, Functional selectivity, bivalent ligand, lcsh:Q, allotopic, κ-opioid receptor, lcsh:Science

Abstract

The recent crystal structure of the κ-opioid receptor (κ-OR) revealed, unexpectedly, that the antagonist JDTic is a bivalent ligand: in addition to the orthosteric pocket occupied by morphinans, JDTic also occupies a distinct (allotopic) pocket. Mutagenesis data suggest that salvinorin A (1) also binds to this allotopic pocket, adjacent to the aspartate residue that anchors the basic nitrogen atom of classical opiates (Asp138). It has been suggested that an H-bond donor appended to 1 might interact with Asp138, increasing affinity. Such a bivalent ligand might also possess altered functional selectivity. Based on modeling and known N-furanylmethyl opioid antagonists, we appended H-bond donors to the furan ring of 1. (Dimethylamino)methyl groups at C-15 or C-16 abolished affinity for κ-OR. Hydroxymethylation at C-16 was tolerated, but 15,16-bis-hydroxymethylation was not. Since allosteric modulators may go undetected in binding assays, we also tested these and other low-affinity derivatives of 1 for allosteric modulation of dynorphin A in the [35S]GTPγS assay. No modulation was detected. As an alternative attachment point for bivalent derivatives, we prepared the 2-(hydroxyethoxy)methyl ether, which retained high affinity for κ-OR. We discuss alternative design strategies for linked, fused or merged bivalent derivatives of 1.

Published

2013

4. Studies toward bivalent κ opioids derived from Salvinorin A: heteromethylation of the furan ring reduces affinity

Author

Munro, Thomas A, Xu, Wei, Ho, Douglas M, Liu-Chen, Lee-Yuan, Cohen, Bruce M, Munro, Thomas A, Xu, Wei, Ho, Douglas M, Liu-Chen, Lee-Yuan, and Cohen, Bruce M

Published

2013

5. Studies toward bivalent κ opioids derived from salvinorin A: heteromethylation of the furan ring reduces affinity.

Author

Munro TA, Xu W, Ho DM, Liu-Chen LY, and Cohen BM

Abstract

The recent crystal structure of the κ-opioid receptor (κ-OR) revealed, unexpectedly, that the antagonist JDTic is a bivalent ligand: in addition to the orthosteric pocket occupied by morphinans, JDTic also occupies a distinct (allotopic) pocket. Mutagenesis data suggest that salvinorin A (1) also binds to this allotopic pocket, adjacent to the aspartate residue that anchors the basic nitrogen atom of classical opiates (Asp138). It has been suggested that an H-bond donor appended to 1 might interact with Asp138, increasing affinity. Such a bivalent ligand might also possess altered functional selectivity. Based on modeling and known N-furanylmethyl opioid antagonists, we appended H-bond donors to the furan ring of 1. (Dimethylamino)methyl groups at C-15 or C-16 abolished affinity for κ-OR. Hydroxymethylation at C-16 was tolerated, but 15,16-bis-hydroxymethylation was not. Since allosteric modulators may go undetected in binding assays, we also tested these and other low-affinity derivatives of 1 for allosteric modulation of dynorphin A in the [(35)S]GTPγS assay. No modulation was detected. As an alternative attachment point for bivalent derivatives, we prepared the 2-(hydroxyethoxy)methyl ether, which retained high affinity for κ-OR. We discuss alternative design strategies for linked, fused or merged bivalent derivatives of 1.

Published

2013