First surface modification

Chemical surface modifications The first surface modification for the purpose of eliminating EOF and protein adsorption was recommended by Hjerten.28 The attachment of vinyl silanes allowed the polymerization of a variety of molecules to the surface. Most of the chemical modifications used for preparing capillaries for electrophoresis originated from the experience acquired over the years preparing GC and LC stationary phases. Chemical modification should conform to certain requirements, including the prevention of adsorption, the provision of stable and constant EOF over a wide pH range, chemical stability, ease of preparation, and reproduciblity of preparation. The effects of silanization of the inner surface of capillaries on electrophoretic separations have been extensively studied.26-29... 

Preparation of polyfethylene oxide) (PEO) and poly(arylene ether) based hydrophilic-hydrophobic block copolymer is of special interest because PEO has been proven to be particularly reliable and versatile for the surface modification of biomaterials. The first poly(ediylene oxide)-/ /oc/c-polysulfonc (PEO-fc-PSF) copolymers were reported by Aksenov et al.217 They employed diisocyanate chemistry to link hydroxy-terminated sulfone oligomers and polyfethylene... 

In order to improve the tribological properties of molecular films, molecular surface modification is the first choice to make an approach. A Diblock polymer polystyrene-poly(ethylene)oxide (PS-PEO) thin-films were studied in our previous research because of its interesting structure (one... 

The improvement of its activity and stability has been approach by the use of GE tools (see Refs. [398] and [399], respectively). A process drawback is the fact that the oxidation of hydrophobic compounds in an organic solvent becomes limited by substrate partition between the active site of the enzyme and the bulk solvent [398], To provide the biocatalyst soluble with a hydrophobic active site access, keeping its solubility in organic solvents, a double chemical modification on horse heart cytochrome c has been performed [400,401], First, to increase the active-site hydrophobicity, a methyl esterification on the heme propionates was performed. Then, polyethylene glycol (PEG) was used for a surface modification of the protein, yielding a protein-polymer conjugates that are soluble in organic solvents. 

Fig. 8 Immobilization of urokinase on the surfaces of islet cells, (a) Surface modification (/) chemical structure of ssDNA-PEG-lipid, and (2) ssDNA-PEG-lipid anchoring to the cell membrane. (b) Introduction of a complementary ssDNA onto urokinase, which was first modified with a madeimide group by a cross-linker, EMCS. (c) Urokinase-immobilization through DNA...

Medieval brass), although the problems of electrochemical surface modification due to corrosion are minimized if the first few turns of the drilling are discarded and only bright metal turnings are used. 

In order to overcome this drawback, there are two main approaches for the surface modification of carbon nanostructures that reoccur in the literature. The first one is covalent functionalization, mainly by chemical bonding of functional groups and the second one is noncovalent functionalization, mainly by physical interactions with other molecules or particles. Both strategies have been used to provide different physical and chemical properties to the carbon nanostructures. Those that will be presented here are only a few examples of the modifications that can be achieved in carbon nanostructure surfaces and composite fabrication. 

The first report on living carbocationic surface-initiated polymerization (LCSIP) using a defined surface modification is by Vidal and Kennedy [268-270]. They prepared poly(isobutene) (PIB) brushes from silica surfaces using a silane functionalized benzylchloride activated by a Lewis acid. 

Classic solid phase substrates used in biotesting, such as microtiter plates, membrane filters or microscope slides, have been the first supports used for NA immobilization in array fabrication [27]. Desired attributes of any DNA array substrate include (i) chemical homogeneity (ii) thermal and chemical stability (iii) ability to control surface chemical properties such as polarity or hydrophobicity (iv) ability to be activated with a wide range of chemical functionalities (v) reproducibihty of the surface modification processes involved (vi) inert with respect to enzymatic activity especially ones involved in DNA manipulation and (vii) ultra-low intrinsic fluorescence. 

Therefore, surface modification strategies for the formation of direct silicon-carbon bonds require, first, a special pre-treatment of the silicon surface to prevent oxidation and, second, an activation of the silicon surface for subsequent reaction with organic moieties. This has been achieved by treatment of the silicon surface with hydrofluoric acid to generate a hydrogen-terminated Si(lll) surface, which can further react with unsaturated co-functionahzed alkenes in the presence of UV irradiation or by thermal activation [27,44,45]. Using this method, carboxylic acid modified silicon substrates have been successfully generated and coupled to thiol modified ONDs via a polylysine/sulfosuccinimidyl 4-(M-maleimidomethyl)-cyclohexane-l-carboxylate couphng (Fig. 12). 

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