| Author | dc.contributor.author | Gómez Jeria, Juan | |
| Author | dc.contributor.author | Lagos Arancibia, Luis | es_CL |
| Author | dc.contributor.author | Sobarzo Sánchez, Eduardo | es_CL |
| Admission date | dc.date.accessioned | 2012-06-08T19:56:18Z | |
| Available date | dc.date.available | 2012-06-08T19:56:18Z | |
| Publication date | dc.date.issued | 2002-12-02 | |
| Cita de ítem | dc.identifier.citation | J. Chil. Chem. Soc., 48, 061-066, 2003. | es_CL |
| Identifier | dc.identifier.issn | 0717-9324 | |
| Identifier | dc.identifier.uri | https://repositorio.uchile.cl/handle/2250/119425 | |
| Abstract | dc.description.abstract | AZINDO/1 quantum-chemical structure-affinity relationship study
is presented for the interaction of a group of 7-arylidenenaltrexones
with !l, Kand O opioid receptors. From this work it is concluded tha!:
1. The internal occupied molecular orbitals are extremely important
to regulate receptor affinity and, in the case of the drug-receptor
interaction, they seem to play a fundamental role in receptor
affinity and selectivity.
2. Receptor selectivity seems to be regulated by subtle electronic
differences, sometimes at the same atomic center.
3. In 7-arylidenenaltrexones, phenyl ring D is important for the
interaction with all three receptors. Here, atoms 4 and/or 17 are
possible targets for modifying receptor selectivity and/or affinity.
4. Reactivity indices of a given atom are affected by substituents
placed on atoms that may be very far from it. It is suggested that
this may be one of the main reasons to treat the drug-receptor
interaction quantum-mechanically. | es_CL |
| Lenguage | dc.language.iso | en | es_CL |
| Publisher | dc.publisher | Sociedad Chilena de Química | es_CL |
| Keywords | dc.subject | ZINDO/l | es_CL |
| Título | dc.title | THEORETICAL STUDY OF THE OPIOID RECEPTOR SELECTIVITY OF SOME 7-ARYLIDENENALTREXONES | es_CL |
| Document type | dc.type | Artículo de revista | |
