Supramolekulska struktura novog fenaciloksimskog derivata piridoksal oksima

Cetina, Mario; Gašo-Sokač, Dajana; Bušić, Valentina

Pregled bibliografske jedinice broj: 997195

Supramolekulska struktura novog fenaciloksimskog derivata piridoksal oksima

Cetina, Mario; Gašo-Sokač, Dajana; Bušić, Valentina

Supramolekulska struktura novog fenaciloksimskog derivata piridoksal oksima // Knjiga sažetaka / Galić, N. ; Rogošić, M. (ur.).
Zagreb: Hrvatsko društvo kemijskih inženjera i tehnologa (HDKI), 2019. str. 119-119 (poster, domaća recenzija, sažetak, znanstveni)

CROSBI ID: 997195 Za ispravke kontaktirajte CROSBI podršku putem web obrasca

Naslov
Supramolekulska struktura novog fenaciloksimskog derivata piridoksal oksima
(Supramolecular structure of new phenacyloxime derivative of piridoxal oxime)

Autori
Cetina, Mario ; Gašo-Sokač, Dajana ; Bušić, Valentina

Vrsta, podvrsta i kategorija rada
Sažeci sa skupova, sažetak, znanstveni

Izvornik
Knjiga sažetaka / Galić, N. ; Rogošić, M. - Zagreb : Hrvatsko društvo kemijskih inženjera i tehnologa (HDKI), 2019, 119-119

ISBN
978-953-6894-67-3

Skup
26. hrvatski skup kemičara i kemijskih inženjera (26HSKIKI) ; 4. simpozij Vladimir Prelog

Mjesto i datum
Šibenik, Hrvatska, 09.04.2019. - 12.04.2019

Vrsta sudjelovanja
Poster

Vrsta recenzije
Domaća recenzija

Ključne riječi
piridoxal oxime, supramolecular structure

Sažetak
In the past few decades, a whole series of aliphatic, aromatic and heterocyclic oximes have been synthesized and tested as antidotes in poisoning with organophosphorus compounds (OPC). Among them only mono‐ and bis‐pyridinium compounds possessing an oxime group in position 2 and 4 (PAM‐2, TMB‐4, HI‐6) have been used in human therapy. Reactivating action of these compounds is due to the quaternary nitrogen of the pyridine ring and to the oxime groups which make possible the rupture of the phosphorylated enzyme and its reactivation. Compounds that possess quaternary pyridinium nitrogen and an oxime group, but in the aliphatic part of the molecule, are also synthesized. Malatesta et al. have synthesized 1‐phenacyloxime quinoline chloride, which proved to be a better in vitro reactivator of cholinestrase inhibited by sarin then PAM‐2. Binenfeld et al. synthesized derivatives of 1‐phenacyloxime quinoline chloride and showed that the replacement of the pyridine ring by quinoline analogue produces an enhancement of its inhibitory effect on ChE and also makes it possible to reactivate ChE inhibited by sarin 1. Hankonyi et al. prepared 1‐phenacyloxime‐pyridinium chloride and 2‐ methyl and 4‐methylpyridinium derivatives 2. In this work we present supramolecular structure of new dioxime, 3‐hydroxy‐1‐((2‐ (hydroxyimino)‐2‐phenylethyl)‐4‐ (hydroxyiminomethyl)‐5‐(hydroxymethyl)‐2‐ methylpyridin‐ 1‐ium bromide (1), prepared by quaternisation of pyridoxaloxime with phenacyloxime bromide (Figure 1a). It will be shown that cations and anions in 1 form a complex network of hydrogen bonds and a three‐dimensional network (Figure 1b).

Izvorni jezik
Engleski

Znanstvena područja
Kemija

POVEZANOST RADA

Ustanove:
Prehrambeno-tehnološki fakultet, Osijek,
Tekstilno-tehnološki fakultet, Zagreb

Profili:

Dajana Gašo-Sokač (autor)

Mario Cetina (autor)

Valentina Bušić (autor)

CROSBI Hrvatska znanstvena bibliografija

Pregled bibliografske jedinice broj: 997195

Supramolekulska struktura novog fenaciloksimskog derivata piridoksal oksima

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Pregled bibliografske jedinice broj: 997195

Supramolekulska struktura novog fenaciloksimskog derivata piridoksal oksima

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