Controlled Hydrogel Formation in the Internal Compartment of Giant Unilamellar Vesicles

Jesorka, Aldo; Markström, Martin; Karlsson, Mattias; Orwar, Owe

doi:10.1021/jp052162t

Cited by 40 publications

(36 citation statements)

References 16 publications

(25 reference statements)

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“…Fluctuation of crosslinking density, known to influence hydrogel particle morphology, may also account for the lack of defined shape. 13 Non spherical particles have also been reported with other nanogels prepared using vesicles. 17,37 Particle swelling was estimated directly and the swelling ratio (Q) was 10, i.e., particles absorb only 10 times their mass in water.…”

Section: Particle Characterizationmentioning

confidence: 79%

“…Larger nanogels (about 450 nm) are obtained from encapsulation of 20% dextran hydroyethylmethacrylate solution ( -Mn= 19000) inside vesicles obtained by phospholipids film hydration, followed by extru- sion. 37 Poly(ethylenedioxythiophene)/poly(styrenesulfonate) 13 and poly(N-isopropylacrylamide) 12,16 microgels, in conjunction with lipid bilayers, are obtained by injecting a polymer solution inside GUVs, followed by freeze-thaw cycles and electroporation. The vesicle diameters, in these latter cases, vary from 5 to 100 µm.…”

Section: Particle Characterizationmentioning

confidence: 99%

“…9 Alternatively, nanogels can be prepared by inclusion in reverse micelles of pre-formed polymers, followed by crosslinking. 10 Vesicles also can be used to obtain hydrogels nanoparticles, by monomer encapsulation followed by polymerization 11 or gelation of encapsulated polymers, generally induced by sol-gel temperature transitions 12 or ionic crosslinking, 13 typically without removal of the lipid bilayer. 14 These gel-like vesicles work as cell models, since they have elastic modulus comparable to that of cell cytoplasm 14 and are considered artificial cytoskeletons.…”

Section: Introductionmentioning

confidence: 99%

See 2 more Smart Citations

Preparation of PVP hydrogel nanoparticles using lecithin vesicles

Bueno¹,

Catalani²,

Perez³

et al. 2010

Quím. Nova

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Recebido em 21/6/10; aceito em 20/8/10; publicado na web em 15/10/10 Hydrogels micro, sub-micro and nanoparticles are of great interest for drug encapsulation and delivery or as embolotherapic agents. In this work it is described the preparation of nano and sub-microparticles of pre-formed, high molecular weight and monomer free poly(N-vinyl-2-pyrrolidone) encapsulated inside the core of lecithin vesicles. The hydrogel particles are formed with a very narrow diameter distribution, of about 800 nm, and a moderate swelling ratio, of approximately 10.

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Section: Particle Characterizationmentioning

confidence: 79%

Section: Particle Characterizationmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

See 1 more Smart Citation

Preparation of PVP hydrogel nanoparticles using lecithin vesicles

Bueno¹,

Catalani²,

Perez³

et al. 2010

Quím. Nova

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“…The internal and external solution composition as well as different lipid compositions (which can also include membrane proteins) can be used to tailor a reactor. Furthermore, polymers can be included to create crowded environments (32,33). Network topology can be controlled, too, and it is possible to use either static-or dynamic-shell networks (where the network geometry is changed during the course of a reaction).…”

Section: Chemical Reactions In Biomimetic Networkmentioning

confidence: 99%

Chemical Analysis in Nanoscale Surfactant Networks

Karlsson¹,

Ewing²,

Dommersnes³

et al. 2006

Anal. Chem.

Self Cite

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A lthough the "hard matter" physical sciences (e.g., microelectronics) and the "soft matter" biological sciences (e.g. cell biology and molecular biology) are two distinct areas of research, they are now progressively being combined to create new systems and devices with applications in analytical chemistry. Miniaturization is one of the important factors here: A major goal is to create devices that can operate with high sensitivity and resolution on length scales and time frames relevant to single-molecule studies. Using top-down strategies to fabricate ultrasmall structures is technologically challenging. Therefore, new bottom-up methods of nanoscale fabrication based on self-assembly and self-organization of biological or biomimetic materials are constantly being developed (1-6). The type of nanoscale engineering described in this article has, at least partly, been derived from our growing understanding of living cells, where many nanomechanical and chemical operations are based on controlled shape transitions in surfactant bilayer membranes that also carry proteins to support important functions. Biological cells have a staggering ability to parallel-process multiple chemical reactions and physical (e.g., transport) processes in nanometer-sized systems and to perform a great number of tasks based on single-molecule processes. Thus, nature has solved many engineering problems on small length scales and achieved truly nanoscale, complex chemical devices that can be used for computational, biophysical, synthetic, and analytical applications (7-11). The philosophy behind the work reviewed here is to produce human-made, biomimetic systems that imitate some key features of small biological systems with the overall goal of providing micro-and nanoscale devices that can perform complex chemical operations.

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“…On the contrary, performing inorganic synthesis reactions in GUVs should be expected to shed light on cell-based nanoparticle synthesis and the corresponding mechanism, since GUVs have dimensions in the cell-size scale (micrometer). Until now, the investigations on various biological activities using GUVs as prototypes of cells have been widely performed covering many aspects: preparation (Angelova et al, 1986;Larsen et al, 2003;Takakura et al, 2003;Mohanty et al, 2003;Pautot et al, 2003), membrane related processes like fusion, fission, budding (Walde et al, 2010;Wang et al, 2010;Hanczyc et al, 2004), cellular processes and mechanisms like adhesion, communication, endocytosis, exocytosis (Marrink et al, 2003;Haque et al, 2001;Chen et al, 2005;Rustom et al, 2004;Menger et al, 1992Menger et al, , 1997Menger et al, and 2002Hanczyc et al, 2003;Espinoza et al, 1999;Ichikawa et al, 2004;Davidson et al, 2003), structure and shape transformation (Suezaki, 2002;Sasaki et al, 2004;Boon et al, 2002;Lee et al, 2005;Hamada et al, 2005;Tomšiè et al, 2005;Brückner et al, 2001), drug release Barragan et al, 2001;Park et al, 2000;Sun et al, 2003;Vandenburg et al, 2002), micromanipulation (Karlsson et al, 2001;Marmottant et al, 2003), compartmentation (Jesorka et al, 2005;Bucher et al, 1998;) and microreactors (Vriezema et ...…”

Section: Introductionmentioning

confidence: 99%