Light Scattering Studies of Hydration and Structural Transformations of Lysozyme

Szymańska, Agnieszka; Ślósarek, G.

doi:10.12693/aphyspola.121.694

Cited by 9 publications

(7 citation statements)

References 28 publications

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“…With the increase in the ethanol concentration, up to about 30% (v/v), the specific volume increases up to the value of 0.726 cm 3 · g -1 . These data are in a good correlation with our observations of the changes of lysozyme hydrodynamic radius, R H (Szymańska & Ślósarek, 2012). According to the data from dynamic light scattering R H remains constant and equals (1.856±0.023) nm when the ethanol concentration increases up to about 4.3% (v/v) and then starts to increase with a growing amount of alcohol.…”

Section: Resultssupporting

confidence: 90%

Denaturation and aggregation of lysozyme in water-ethanol solution.

Szymańska

Hornowski²,

Ślósarek³

2012

Acta Biochim Pol

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We have applied rheological methods for the analysis of ethanol-lysozyme interaction during the process of denaturation and aggregation of the protein. At low concentration of ethanol a destruction of the hydration shell of lysozyme is observed. With the increase in the ethanol concentration a structural transformation takes place. It leads to the formation of a protein aggregate with an elongated structure. The rheological characteristics of lysozyme-water-ethanol solution changes from Newtonian to pseudoplastic.

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Section: Resultssupporting

confidence: 90%

Denaturation and aggregation of lysozyme in water-ethanol solution.

Szymańska

Hornowski²,

Ślósarek³

2012

Acta Biochim Pol

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“…R h of Lyz was determined to be 23 Å. This is larger than 18–19 Å often reported in the literature . These values are almost always reported at pH 4.5 in solutions containing at least 0.1 M salt.…”

Section: Resultsmentioning

confidence: 48%

“…This is larger than 18-19Å often reported in the literature. 67,68 These values are almost always reported at pH 4.5 in solutions containing at least 0.1 M salt. Esposito et al 69 found that R h was only 6Å at pH 3 in the presence of 4 mM NaCl.…”

Section: Size and Protein-protein Interactionsmentioning

confidence: 79%

The Effect of Protein PEGylation on Physical Stability in Liquid Formulation

Holm

McUmber

Rasmussen

et al. 2014

Journal of Pharmaceutical Sciences

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“…* MZ, NAD, KETO and BSA formulations were also prepared with 1 % of PEG6000 and 0.3 % of trehalose for freeze-drying. (Avdeef, et al 2000;Sheng, et al 2006;Singhai, et al 1996;Zhou, et al 2005) NAD* 309 8.3 (25 °C), 8.3 (pH 7) 9.28 + 1.7 (Avdeef and Berger 2001;Zhou, et al 2005) MZ* 171 10.5 (25 °C), 10.5 (pH 7) 2.38 ø 2 (Kim, et al 2012;Wu and Fassihi 2005;Zhou, et al 2005) BSA* 6.65x10 4 40 4.6 -4.8 -~ 7 1 (Sigma-Aldrich; Yohannes, et al 2010) LZ 1.47x10 4 >10 11.1 + ~ 3.7 0.5 (Fritz, et al 1995;Szymańska and Ślósarek 2012) FITC-DEX 4000 50 ø ~ 2.8 1 (Sigma-Aldrich) † 40.7 mg/ml solubility at pH 7 was used for the calculation of diffusion coefficients of KETO with the Hiquchi equation. Excess KETO remained in the crystalline form in the hydrogel at 3.4%, and therefore in practice initial drug concentration ˃ drug solubility.…”

Section: Preparation Of the Anfc Hydrogel Formulationsmentioning

confidence: 99%

Nanofibrillar cellulose hydrogels and reconstructed hydrogels as matrices for controlled drug release

Paukkonen

Kunnari

Laurén

et al. 2017

International Journal of Pharmaceutics

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Concentrated 3% and 6.5% anionic nanofibrillar cellulose (ANFC) hydrogels were introduced as matrix reservoirs for controlled delivery applications of small molecules and proteins. A further aim was to study how the freeze-drying and subsequent rehydration of ANFC hydrogel affects the rheological properties and drug release of selected model compounds from the reconstructed hydrogels. It was demonstrated that the 3% and 6.5% ANFC hydrogels can be freeze-dried with suitable excipients into highly porous aerogel structures and redispersed back into the hydrogel form without significant change in the rheological properties. Freeze-drying did not affect the drug release properties from redispersed ANFC hydrogels, indicating that these systems could be stored in the dry form and only redispersed when needed. For large molecules, the diffusion coefficients were significantly smaller when higher ANFC fiber content was used, indicating that the amount of ANFC fibers in the hydrogel can be used to control the release rate. The release of small molecules was controlled with the ANFC fiber content only to a moderate extent. The results indicate that ANFC hydrogel can be used for controlled delivery of several types of molecules and that the hydrogel can be successfully freeze-dried and redispersed.

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Light Scattering Studies of Hydration and Structural Transformations of Lysozyme

Cited by 9 publications

References 28 publications

Denaturation and aggregation of lysozyme in water-ethanol solution.

Denaturation and aggregation of lysozyme in water-ethanol solution.

The Effect of Protein PEGylation on Physical Stability in Liquid Formulation

Nanofibrillar cellulose hydrogels and reconstructed hydrogels as matrices for controlled drug release

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