Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system

Chloramphenicol eye drops are commonly prescribed in concentrations of 0.5-1% in the treatment of infectious conjunctivitis. In terms of ophthalmic solution preparation, the major disadvantage of chloramphenicol consists in its low solubility in water. The solubility is increased by substances that...

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Main Authors: Todoran Nicoleta, Ciurba Adriana, Rédai Emőke, Ion V., Lazăr Luminița, Sipos Emese
Format: Article
Language:English
Published: Sciendo 2014-12-01
Series:Acta Medica Marisiensis
Subjects:
Online Access:https://doi.org/10.1515/amma-2015-0007
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spelling doaj-3011a767f16b43e78423efdda3394f352021-09-06T19:39:50ZengSciendoActa Medica Marisiensis2247-61132014-12-0160626927410.1515/amma-2015-0007amma-2015-0007Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax systemTodoran Nicoleta0Ciurba Adriana1Rédai Emőke2Ion V.3Lazăr Luminița4Sipos Emese5University of Medicine and Pharmacy of Tirgu MuresUniversity of Medicine and Pharmacy of Tirgu MuresUniversity of Medicine and Pharmacy of Tirgu MuresUniversity of Medicine and Pharmacy of Tirgu MuresUniversity of Medicine and Pharmacy of Tirgu MuresUniversity of Medicine and Pharmacy of Tirgu MuresChloramphenicol eye drops are commonly prescribed in concentrations of 0.5-1% in the treatment of infectious conjunctivitis. In terms of ophthalmic solution preparation, the major disadvantage of chloramphenicol consists in its low solubility in water. The solubility is increased by substances that form chloramphenicol-complexes, for example: boric acid/borax or cyclodextrins. Objective: Experimental studies aimed to evaluate the potential advantages of enhancing the solubility and stability of chloramphenicol (API) by molecular encapsulation in b-cyclodextrin (CD), in formulation of ophthalmic solutions buffered with boric acid/borax system. Methods and Results: We prepared four APIb- CD complexes, using two methods (kneading and co-precipitation) and two molar ratio of API/b-cyclodextrin (1:1 and 1:2). The formation of complexes was proved by differential scanning calorimetry (DSC) and the in vitro dissolution tests. Using these compounds, we prepared eight ophthalmic solutions, formulated in two variants of chloramphenicol concentrations (0.4% and 0.5%). Each solution was analyzed, by the official methods, at preparation and periodically during three months of storing in different temperature conditions (4°C, 20°C and 30°C). Conclusions: Inclusion of chloramphenicol in b-cyclodextrin only partially solves the difficulties due to the low solubility of chloramphenicol. The protection of chloramphenicol molecules is not completely ensured when the ophthalmic solutions are buffered with the boric acid/borax system.https://doi.org/10.1515/amma-2015-0007chloramphenicolb-cyclodextrin complexesophthalmic solutionsboric acid/borax system
collection DOAJ
language English
format Article
sources DOAJ
author Todoran Nicoleta
Ciurba Adriana
Rédai Emőke
Ion V.
Lazăr Luminița
Sipos Emese
spellingShingle Todoran Nicoleta
Ciurba Adriana
Rédai Emőke
Ion V.
Lazăr Luminița
Sipos Emese
Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
Acta Medica Marisiensis
chloramphenicol
b-cyclodextrin complexes
ophthalmic solutions
boric acid/borax system
author_facet Todoran Nicoleta
Ciurba Adriana
Rédai Emőke
Ion V.
Lazăr Luminița
Sipos Emese
author_sort Todoran Nicoleta
title Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
title_short Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
title_full Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
title_fullStr Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
title_full_unstemmed Limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
title_sort limitations when use chloramphenicol-bcyclodextrins complexes in ophtalmic solutions buffered with boric acid/borax system
publisher Sciendo
series Acta Medica Marisiensis
issn 2247-6113
publishDate 2014-12-01
description Chloramphenicol eye drops are commonly prescribed in concentrations of 0.5-1% in the treatment of infectious conjunctivitis. In terms of ophthalmic solution preparation, the major disadvantage of chloramphenicol consists in its low solubility in water. The solubility is increased by substances that form chloramphenicol-complexes, for example: boric acid/borax or cyclodextrins. Objective: Experimental studies aimed to evaluate the potential advantages of enhancing the solubility and stability of chloramphenicol (API) by molecular encapsulation in b-cyclodextrin (CD), in formulation of ophthalmic solutions buffered with boric acid/borax system. Methods and Results: We prepared four APIb- CD complexes, using two methods (kneading and co-precipitation) and two molar ratio of API/b-cyclodextrin (1:1 and 1:2). The formation of complexes was proved by differential scanning calorimetry (DSC) and the in vitro dissolution tests. Using these compounds, we prepared eight ophthalmic solutions, formulated in two variants of chloramphenicol concentrations (0.4% and 0.5%). Each solution was analyzed, by the official methods, at preparation and periodically during three months of storing in different temperature conditions (4°C, 20°C and 30°C). Conclusions: Inclusion of chloramphenicol in b-cyclodextrin only partially solves the difficulties due to the low solubility of chloramphenicol. The protection of chloramphenicol molecules is not completely ensured when the ophthalmic solutions are buffered with the boric acid/borax system.
topic chloramphenicol
b-cyclodextrin complexes
ophthalmic solutions
boric acid/borax system
url https://doi.org/10.1515/amma-2015-0007
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