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1.
ACS Appl Mater Interfaces ; 4(12): 6835-41, 2012 Dec.
Artigo em Inglês | MEDLINE | ID: mdl-23163608

RESUMO

Indium zinc oxide thin-film transistors are fabricated via a precursor in solution route on silicon substrates with silicon dioxide gate dielectric. It is found that the extracted mobility rises, peaks, and then decreases with increasing precursor concentration instead of rising and saturating. Investigation with scanning probe techniques reveals full thickness variations within the film which are assumed to adversely affect charge transport. Additional layers are coated, and the extracted mobility is observed to increase up to 19.7 cm(2) V(-1) s(-1). The reasons for this are examined in detail by direct imaging with scanning tunneling microscopy and extracting electron density profiles from X-ray reflection measurements. It is found that the optimal concentration for single layer films is suboptimal when coating multiple layers and in fact using many layers of very low concentrations of precursor in the solution, leading to a dense, defect and void free film, affording the highest mobilities. A consistent qualitative model of layer formation is developed explaining how the morphology of the film develops as the concentration of precursor in the initial solution is varied.

2.
Chem Commun (Camb) ; (20): 2358-9, 2004 Oct 21.
Artigo em Inglês | MEDLINE | ID: mdl-15490019

RESUMO

Stepwise, irreversible self-assembly of porphyrinphosphonates by zirconium(IV) produces cones of 20 nm height and similar widths. Side-on growth cannot be prevented. Reversible fiber growth without metal ions gave micrometer long fibers on mica of 2 nm width, because charge repulsion allowed only for end-on growth.

3.
Angew Chem Int Ed Engl ; 41(11): 1828-52, 2002 Jun 03.
Artigo em Inglês | MEDLINE | ID: mdl-19750613

RESUMO

Amphiphilic lipids associate in water spontaneously to form micelles, vesicles, monolayers, or biological membranes. These aggregates are soft and their shape can be changed easily. They behave like complex fluids because they are merely held together by weak, nondirected forces. The most important characteristic of these monolayers is their ability to dissolve hydrophobic molecules in the form of freely movable monomers. The fluid molecular layers are not suitable to anchor the components of chain reactions. However, if the alkyl chains are replaced by rigid skeletons or if the head groups are connected through intermolecular interactions, the aggregates become rigid and their fluid solvent character is lost. The construction of chiral surfaces by synkinesis (synthesis of noncovalent compounds) and of enzyme-type surface clefts of defined size can now be carried out by using rigid lipid membranes. Monolayers and nanometer pores on solid substrates attain sharp edges, and upright nanometer columns on smooth surfaces no longer dissipate. Five examples illustrate the advantages of using rigid molecular assemblies: 1) Cationic domains of rigid edge amphiphiles in fluid membranes act as manipulable ion channels. 2) Spherical micelles, micellar helical fibers, and vesicular tubes can be dried and stored as stable material. Molecular landscapes form on smooth surfaces. 3) alpha,omega-Diamide bolaamphiphiles form rigid nanometer-thick walls on smooth surfaces and these barriers cannot be penetrated by amines. Around steroids and porphyrins, they form rigid nanometer clefts whose walls and water-filled centers can be functionalized. 4) The structure of rigid oligophenylene- and quinone monolayers on electrodes can be changed drastically and reversibly by changing the potential. 5) 10(10) Porphyrin cones on a 1-cm2 gold electrode can be controlled individually by AFM- and STM-tips and investigated by electrochemical, photochemical, and mechanical means. In summary, rigid monolayers and bilayers allow the formation of a great variety of membrane structures that cannot be obtained from classical fluid alkyl amphiphiles.


Assuntos
Bicamadas Lipídicas/química , Nanoestruturas/química , Coloides/química , Micelas , Nanoestruturas/ultraestrutura , Porfirinas/química , Lipossomas Unilamelares/química
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