Muscarinic thioligands with cyclopentane nucleus

Alessandro Piergentili; Maria Pigini; Wilma Quaglia; Seyed K. Tayebati; Francesco Amenta; Maurizio Sabbatini; Mario Giannella

doi:10.1016/S0968-0896(96)00231-3

Muscarinic thioligands with cyclopentane nucleus

Alessandro Piergentili, Maria Pigini, Wilma Quaglia, Seyed K. Tayebati, Francesco Amenta, Maurizio Sabbatini, Mario Giannella

Risultato della ricerca: Contributo su rivista › Articolo in rivista › peer review

Abstract

Some thio- and the benzoyl-derivatives of deoxamuscarine were synthesized and tested as muscarinic agonists using radioligand binding assays and functional tests. In comparison with deoxamuscarine, used as reference compound, no dimensional distance modification is tolerated for correct lipophilic pocket recognition. The substitution of the ammonium group with a sulphonium group significantly decreased muscarinic potency. The so-called 'muscarinic sub-site' accepts relatively bulky functions as long as it is bound to the cyclopentane carrier by an oxygen bridge. Esterification of this moiety increases the M₂ subtype selectivity, while etherification heightens that of M₃.

Lingua originale	Inglese
pagine (da-a)	2193-2199
Numero di pagine	7
Rivista	Bioorganic and Medicinal Chemistry
Volume	4
Numero di pubblicazione	12
DOI	https://doi.org/10.1016/S0968-0896(96)00231-3
Stato di pubblicazione	Pubblicato - dic 1996
Pubblicato esternamente	Sì

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10.1016/S0968-0896(96)00231-3

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@article{477214d7b87544fbaba4426dddfc2cae,

title = "Muscarinic thioligands with cyclopentane nucleus",

abstract = "Some thio- and the benzoyl-derivatives of deoxamuscarine were synthesized and tested as muscarinic agonists using radioligand binding assays and functional tests. In comparison with deoxamuscarine, used as reference compound, no dimensional distance modification is tolerated for correct lipophilic pocket recognition. The substitution of the ammonium group with a sulphonium group significantly decreased muscarinic potency. The so-called 'muscarinic sub-site' accepts relatively bulky functions as long as it is bound to the cyclopentane carrier by an oxygen bridge. Esterification of this moiety increases the M2 subtype selectivity, while etherification heightens that of M3.",

keywords = "Deoxymuscarine thioderivatives, M/M selectivity, Muscarinic binding affinity, Muscarinic thioligands",

author = "Alessandro Piergentili and Maria Pigini and Wilma Quaglia and Tayebati, {Seyed K.} and Francesco Amenta and Maurizio Sabbatini and Mario Giannella",

note = "Funding Information: This work was supportedin part by grantsf rom the CamerinoU niversitya nd the Italian ResearchC ouncil (C.N.R., Rome).",

year = "1996",

month = dec,

doi = "10.1016/S0968-0896(96)00231-3",

language = "English",

volume = "4",

pages = "2193--2199",

journal = "Bioorganic and Medicinal Chemistry",

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TY - JOUR

T1 - Muscarinic thioligands with cyclopentane nucleus

AU - Piergentili, Alessandro

AU - Pigini, Maria

AU - Quaglia, Wilma

AU - Tayebati, Seyed K.

AU - Amenta, Francesco

AU - Sabbatini, Maurizio

AU - Giannella, Mario

N1 - Funding Information: This work was supportedin part by grantsf rom the CamerinoU niversitya nd the Italian ResearchC ouncil (C.N.R., Rome).

PY - 1996/12

Y1 - 1996/12

N2 - Some thio- and the benzoyl-derivatives of deoxamuscarine were synthesized and tested as muscarinic agonists using radioligand binding assays and functional tests. In comparison with deoxamuscarine, used as reference compound, no dimensional distance modification is tolerated for correct lipophilic pocket recognition. The substitution of the ammonium group with a sulphonium group significantly decreased muscarinic potency. The so-called 'muscarinic sub-site' accepts relatively bulky functions as long as it is bound to the cyclopentane carrier by an oxygen bridge. Esterification of this moiety increases the M2 subtype selectivity, while etherification heightens that of M3.

AB - Some thio- and the benzoyl-derivatives of deoxamuscarine were synthesized and tested as muscarinic agonists using radioligand binding assays and functional tests. In comparison with deoxamuscarine, used as reference compound, no dimensional distance modification is tolerated for correct lipophilic pocket recognition. The substitution of the ammonium group with a sulphonium group significantly decreased muscarinic potency. The so-called 'muscarinic sub-site' accepts relatively bulky functions as long as it is bound to the cyclopentane carrier by an oxygen bridge. Esterification of this moiety increases the M2 subtype selectivity, while etherification heightens that of M3.

KW - Deoxymuscarine thioderivatives

KW - M/M selectivity

KW - Muscarinic binding affinity

KW - Muscarinic thioligands

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U2 - 10.1016/S0968-0896(96)00231-3

DO - 10.1016/S0968-0896(96)00231-3

M3 - Article

SN - 0968-0896

VL - 4

SP - 2193

EP - 2199

JO - Bioorganic and Medicinal Chemistry

JF - Bioorganic and Medicinal Chemistry

IS - 12

ER -

Muscarinic thioligands with cyclopentane nucleus

Abstract

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