Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning

Holger Schönherr; Gyula J. Vancso; Geerten H. Degenhart; Günter Reiter; K. Albrecht; B. Dordi; C.L. Feng; D.I. Rozkiewicz; A. Shovsky

doi:10.1007/12_014

Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning

Holger Schönherr, Gyula J. Vancso (Editor), Geerten H. Degenhart, Günter Reiter (Editor), K. Albrecht (Editor), B. Dordi, C.L. Feng, D.I. Rozkiewicz, A. Shovsky

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

In this contribution we review our recent progress in studies that aim at the understanding of the relationship between structure and surface reactivity of organic thin films on the one hand, and at the micro- and nanofabrication of bioreactive or biocompatible platforms on the other hand. Self-assembled monolayers (SAMs) of n,n′-dithiobis(N-hydroxysuccinimidyl-n-alkanoate) exposing NHS reactive ester groups were studied as model systems for immobilization reactions of DNA, proteins, and receptors. Reaction kinetics and activation energies were determined quantitatively at length scales ranging from millimeters down to nanometers using, for example, surface infrared spectroscopy and in situ inverted chemical force microscopy (iCFM), respectively. The increase in conformational order with increasing alkane segment length was found to result in reduced reactivity due to steric crowding. This drawback of highly organized monolayer architectures and the inherently limited loading can be circumvented by utilizing well-defined macromolecular thin films. Using amine-terminated polyamidoamine (PAMAM) dendrimers immobilized via soft lithography, as well as scanning probe lithography (SPL) approaches (dip-pen nanolithography, DPN) on NHS ester surfaces, robust micrometer and submicrometer patterned (bio)reactive surfaces, which allow one to achieve high molecular loading in coupling reactions for chip-based assays and sensor surfaces, were fabricated. Covalent coupling afforded the required robustness of the patterned assemblies. Finally, we address micro- and nanopatterned bilayer-based systems. SPL was applied in order to fabricate nanoscale biocompatible supramolecular architectures on solid supports. The adsorption of vesicles onto lipid bilayers was spatially controlled and directed in situ with nanometer-scale precision using SPL. This methodology, which provides a platform for research on proteins incorporated in the lipid bilayers comprising the vesicles, does not require that the vesicles are chemically labeled in order to guide their deposition.

Original language	Undefined
Pages (from-to)	169-208
Number of pages	40
Journal	Advances in polymer science
Volume	200
DOIs	https://doi.org/10.1007/12_014
Publication status	Published - 2006

Keywords

METIS-230350
IR-74159

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10.1007/12_014

Cite this

Schönherr, H., Vancso, G. J. (Ed.), Degenhart, G. H., Reiter, G. (Ed.), Albrecht, K. (Ed.), Dordi, B., Feng, C. L., Rozkiewicz, D. I., & Shovsky, A. (2006). Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning. Advances in polymer science, 200, 169-208. https://doi.org/10.1007/12_014

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title = "Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning",

abstract = "In this contribution we review our recent progress in studies that aim at the understanding of the relationship between structure and surface reactivity of organic thin films on the one hand, and at the micro- and nanofabrication of bioreactive or biocompatible platforms on the other hand. Self-assembled monolayers (SAMs) of n,n′-dithiobis(N-hydroxysuccinimidyl-n-alkanoate) exposing NHS reactive ester groups were studied as model systems for immobilization reactions of DNA, proteins, and receptors. Reaction kinetics and activation energies were determined quantitatively at length scales ranging from millimeters down to nanometers using, for example, surface infrared spectroscopy and in situ inverted chemical force microscopy (iCFM), respectively. The increase in conformational order with increasing alkane segment length was found to result in reduced reactivity due to steric crowding. This drawback of highly organized monolayer architectures and the inherently limited loading can be circumvented by utilizing well-defined macromolecular thin films. Using amine-terminated polyamidoamine (PAMAM) dendrimers immobilized via soft lithography, as well as scanning probe lithography (SPL) approaches (dip-pen nanolithography, DPN) on NHS ester surfaces, robust micrometer and submicrometer patterned (bio)reactive surfaces, which allow one to achieve high molecular loading in coupling reactions for chip-based assays and sensor surfaces, were fabricated. Covalent coupling afforded the required robustness of the patterned assemblies. Finally, we address micro- and nanopatterned bilayer-based systems. SPL was applied in order to fabricate nanoscale biocompatible supramolecular architectures on solid supports. The adsorption of vesicles onto lipid bilayers was spatially controlled and directed in situ with nanometer-scale precision using SPL. This methodology, which provides a platform for research on proteins incorporated in the lipid bilayers comprising the vesicles, does not require that the vesicles are chemically labeled in order to guide their deposition.",

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author = "Holger Sch{\"o}nherr and Vancso, {Gyula J.} and Degenhart, {Geerten H.} and G{\"u}nter Reiter and K. Albrecht and B. Dordi and C.L. Feng and D.I. Rozkiewicz and A. Shovsky",

year = "2006",

doi = "10.1007/12_014",

language = "Undefined",

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Schönherr, H, Vancso, GJ (ed.), Degenhart, GH, Reiter, G (ed.), Albrecht, K (ed.), Dordi, B, Feng, CL, Rozkiewicz, DI & Shovsky, A 2006, 'Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning', Advances in polymer science, vol. 200, pp. 169-208. https://doi.org/10.1007/12_014

Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning. / Schönherr, Holger; Vancso, Gyula J. (Editor); Degenhart, Geerten H. et al.
In: Advances in polymer science, Vol. 200, 2006, p. 169-208.

Research output: Contribution to journal › Article › Academic › peer-review

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T1 - Organic and Macromolecular Films and Assemblies as (Bio)reactive Platforms: From Model Studies on Structure-Reactivity Relationships to Submicrometer Patterning

AU - Schönherr, Holger

AU - Degenhart, Geerten H.

AU - Dordi, B.

AU - Feng, C.L.

AU - Rozkiewicz, D.I.

AU - Shovsky, A.

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A2 - Reiter, Günter

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N2 - In this contribution we review our recent progress in studies that aim at the understanding of the relationship between structure and surface reactivity of organic thin films on the one hand, and at the micro- and nanofabrication of bioreactive or biocompatible platforms on the other hand. Self-assembled monolayers (SAMs) of n,n′-dithiobis(N-hydroxysuccinimidyl-n-alkanoate) exposing NHS reactive ester groups were studied as model systems for immobilization reactions of DNA, proteins, and receptors. Reaction kinetics and activation energies were determined quantitatively at length scales ranging from millimeters down to nanometers using, for example, surface infrared spectroscopy and in situ inverted chemical force microscopy (iCFM), respectively. The increase in conformational order with increasing alkane segment length was found to result in reduced reactivity due to steric crowding. This drawback of highly organized monolayer architectures and the inherently limited loading can be circumvented by utilizing well-defined macromolecular thin films. Using amine-terminated polyamidoamine (PAMAM) dendrimers immobilized via soft lithography, as well as scanning probe lithography (SPL) approaches (dip-pen nanolithography, DPN) on NHS ester surfaces, robust micrometer and submicrometer patterned (bio)reactive surfaces, which allow one to achieve high molecular loading in coupling reactions for chip-based assays and sensor surfaces, were fabricated. Covalent coupling afforded the required robustness of the patterned assemblies. Finally, we address micro- and nanopatterned bilayer-based systems. SPL was applied in order to fabricate nanoscale biocompatible supramolecular architectures on solid supports. The adsorption of vesicles onto lipid bilayers was spatially controlled and directed in situ with nanometer-scale precision using SPL. This methodology, which provides a platform for research on proteins incorporated in the lipid bilayers comprising the vesicles, does not require that the vesicles are chemically labeled in order to guide their deposition.

AB - In this contribution we review our recent progress in studies that aim at the understanding of the relationship between structure and surface reactivity of organic thin films on the one hand, and at the micro- and nanofabrication of bioreactive or biocompatible platforms on the other hand. Self-assembled monolayers (SAMs) of n,n′-dithiobis(N-hydroxysuccinimidyl-n-alkanoate) exposing NHS reactive ester groups were studied as model systems for immobilization reactions of DNA, proteins, and receptors. Reaction kinetics and activation energies were determined quantitatively at length scales ranging from millimeters down to nanometers using, for example, surface infrared spectroscopy and in situ inverted chemical force microscopy (iCFM), respectively. The increase in conformational order with increasing alkane segment length was found to result in reduced reactivity due to steric crowding. This drawback of highly organized monolayer architectures and the inherently limited loading can be circumvented by utilizing well-defined macromolecular thin films. Using amine-terminated polyamidoamine (PAMAM) dendrimers immobilized via soft lithography, as well as scanning probe lithography (SPL) approaches (dip-pen nanolithography, DPN) on NHS ester surfaces, robust micrometer and submicrometer patterned (bio)reactive surfaces, which allow one to achieve high molecular loading in coupling reactions for chip-based assays and sensor surfaces, were fabricated. Covalent coupling afforded the required robustness of the patterned assemblies. Finally, we address micro- and nanopatterned bilayer-based systems. SPL was applied in order to fabricate nanoscale biocompatible supramolecular architectures on solid supports. The adsorption of vesicles onto lipid bilayers was spatially controlled and directed in situ with nanometer-scale precision using SPL. This methodology, which provides a platform for research on proteins incorporated in the lipid bilayers comprising the vesicles, does not require that the vesicles are chemically labeled in order to guide their deposition.

KW - METIS-230350

KW - IR-74159

U2 - 10.1007/12_014

DO - 10.1007/12_014

M3 - Article

SN - 0065-3195

VL - 200

SP - 169

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JO - Advances in polymer science

JF - Advances in polymer science

ER -