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Pregled bibliografske jedinice broj: 885095

Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system

Ukrainczyk, Marko; Štajner, Lara; Brkljača, Zlatko; Stepić, Robert; Smith, David Matthew; Smith, Ana-Sunčana; Gredičak, Matija; Jerić, Ivanka; Jakas, Andreja; Kralj, Damir
Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system // The 10th Joint Meeting on Medicinal Chemistry : Book of Abstracts / Basarić, Nikola ; Namjesnik, Danijel ; Perković, Ivana ; Stepanić Višnja (ur.).
Zagreb: Hrvatsko kemijsko društvo, 2017. str. 145-145 (poster, nije recenziran, sažetak, znanstveni)

CROSBI ID: 885095 Za ispravke kontaktirajte CROSBI podršku putem web obrasca

Naslov
Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system

Autori
Ukrainczyk, Marko ; Štajner, Lara ; Brkljača, Zlatko ; Stepić, Robert ; Smith, David Matthew ; Smith, Ana-Sunčana ; Gredičak, Matija ; Jerić, Ivanka ; Jakas, Andreja ; Kralj, Damir

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

Izvornik
The 10th Joint Meeting on Medicinal Chemistry : Book of Abstracts / Basarić, Nikola ; Namjesnik, Danijel ; Perković, Ivana ; Stepanić Višnja - Zagreb : Hrvatsko kemijsko društvo, 2017, 145-145

Skup
Joint Meeting on Medicinal Chemistry (10 ; 2017)

Mjesto i datum
Dubrovnik, Hrvatska, 25.06.2017. - 28.06.2017

Vrsta sudjelovanja
Poster

Vrsta recenzije
Nije recenziran

Ključne riječi
calcite, salicylic acid, drug delivery

Sažetak
Targeted or sustained drug delivery is a promising strategy for improving the therapeutic efficiency of existing active pharmaceutical molecules. Typically, liposomal, micellar or biodegradable polymeric matrices are used for encapsulation of model drug molecules and/or design of new drug delivery systems. Recently, however, porous inorganic materials have been proposed as suitable carriers. Calcium carbonate is a rather common mineral, which has been considered as a mineral drug carrier due to recognized biocompatibility, nontoxicity and biodegradability. Indeed, it has been suggested that CaCO3 may significantly improve drug stability and bioavailability, as well as to control the release of active compounds by influencing their desorption and/or dissolution rates. However, the understanding of the basic molecular interactions of model pharmaceutical compounds with mineral surfaces is a critical step in the development of efficient CaCO3 based hybrid materials that could be used as biocompatible carriers in drug delivery systems. Previously, we studied the molecular interactions between well defined calcite surfaces and salicylic acid (Sal), as well as its derivatives, which were selected as a simple models of anti-inflammatory drug substances. The inspiration for derivatization of salicylic acid molecules with glutamic acid (Glu) or aspartic acid (Asp) is taken from the process of biomineralization, in which organic- inorganic hybrid materials are composed of CaCO3 polymorphs (calcite or aragonite) and Asp-rich acidic glycoproteins. The synthesized amino acid adducts with Sal exerted significantly enhanced binding to specific calcite surfaces, in comparison to free Sal. The aim of this study is to design new salicylic acid adducts, which should be biocompatible and water-soluble. The adducts should also enable stronger Sal binding by means of multiple carboxylic groups, while the linkers should be easily cleaved after binding to CaCO3 surface. Thus, we designed and synthesized 6 tripeptides (L-Asp-L-Asp-L-Asp ; D-Asp-D-Asp-D-Asp ; L-Asp-D-Asp-L-Asp ; L-Asp- Gly-L-Asp ; L-Asp--Ala-L-Asp and L-Asp-Gly-D- Asp), as well as the respective adducts with salicylic acid (Sal-Gly-L-Asp-D-Asp-L-Asp ; Sal- L-Asp-D-Asp-L-Asp ; Sal-Gly-L-Asp-L-Asp-L-Asp and Sal-L-Asp-L-Asp-L-Asp) in order to test the efficiency of their binding with rhombohedral calcite crystals bounded by the stable {; ; 1 0 4}; ; faces. The efficiency has been correlated with the number of carboxylic groups, their orientation in space, charge separation effect and chirality of α-carbon atom. The qualitative compliance of the results of molecular dynamics calculations (MD) of binding energies (Eb = -755 kJ mol-1) and the Langmuir adsorption constants (Kad = 0.56 dm3 mol-1), determined from the crystal growth kinetics of calcite crystals in the presence of respective adducts, indicated the strongest interactions of L-Asp- D-Asp-L-Asp. Similarly, the MD and the crystal growth kinetic data showed the strongest surface interactions of Sal-Gly-L-Asp-D-Asp-L- Asp (Kad = 1.58 dm3 mol-1). The obtained results and proposed systematic approach (MD and crystal growth kinetics) can contribute to a better understanding of molecular interactions between model drug derivatives containing carboxylic functional groups with mineral surfaces, thus being the basis for the design of efficient mineral drug delivery systems.

Izvorni jezik
Engleski

Znanstvena područja
Fizika, Kemija



POVEZANOST RADA

Ustanove:
Institut "Ruđer Bošković", Zagreb

Profili:

Avatar Url Lara Jurković (autor)

Avatar Url Matija Gredičak (autor)

Avatar Url Marko Ukrainczyk (autor)

Avatar Url Ana Sunčana Smith (autor)

Avatar Url Ivanka Jerić (autor)

Avatar Url Andreja Jakas (autor)

Avatar Url Damir Kralj (autor)

Avatar Url David Matthew Smith (autor)

Citiraj ovu publikaciju:

Ukrainczyk, Marko; Štajner, Lara; Brkljača, Zlatko; Stepić, Robert; Smith, David Matthew; Smith, Ana-Sunčana; Gredičak, Matija; Jerić, Ivanka; Jakas, Andreja; Kralj, Damir
Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system // The 10th Joint Meeting on Medicinal Chemistry : Book of Abstracts / Basarić, Nikola ; Namjesnik, Danijel ; Perković, Ivana ; Stepanić Višnja (ur.).
Zagreb: Hrvatsko kemijsko društvo, 2017. str. 145-145 (poster, nije recenziran, sažetak, znanstveni)
Ukrainczyk, M., Štajner, L., Brkljača, Z., Stepić, R., Smith, D., Smith, A., Gredičak, M., Jerić, I., Jakas, A. & Kralj, D. (2017) Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system. U: Basarić, N., Namjesnik, D., Perković, I. & Stepanić Višnja (ur.)The 10th Joint Meeting on Medicinal Chemistry : Book of Abstracts.
@article{article, author = {Ukrainczyk, Marko and \v{S}tajner, Lara and Brklja\v{c}a, Zlatko and Stepi\'{c}, Robert and Smith, David Matthew and Smith, Ana-Sun\v{c}ana and Gredi\v{c}ak, Matija and Jeri\'{c}, Ivanka and Jakas, Andreja and Kralj, Damir}, year = {2017}, pages = {145-145}, keywords = {calcite, salicylic acid, drug delivery}, title = {Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system}, keyword = {calcite, salicylic acid, drug delivery}, publisher = {Hrvatsko kemijsko dru\v{s}tvo}, publisherplace = {Dubrovnik, Hrvatska} }
@article{article, author = {Ukrainczyk, Marko and \v{S}tajner, Lara and Brklja\v{c}a, Zlatko and Stepi\'{c}, Robert and Smith, David Matthew and Smith, Ana-Sun\v{c}ana and Gredi\v{c}ak, Matija and Jeri\'{c}, Ivanka and Jakas, Andreja and Kralj, Damir}, year = {2017}, pages = {145-145}, keywords = {calcite, salicylic acid, drug delivery}, title = {Surface interactions between oligopeptide derivatives of salicylic acid and calcite as a model of an inorganic drug delivery system}, keyword = {calcite, salicylic acid, drug delivery}, publisher = {Hrvatsko kemijsko dru\v{s}tvo}, publisherplace = {Dubrovnik, Hrvatska} }

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