Design of atto-vial based recombinant antibody arrays combined with a planar wave-guide detection system

Ghatnekar-Nilsson, Sara; Dexlin Mellby, Linda; Wingren, Christer; Montelius, Lars; Borrebaeck, Carl

Design of atto-vial based recombinant antibody arrays combined with a planar wave-guide detection system

Mark

Ghatnekar-Nilsson, Sara ^LU ; Dexlin Mellby, Linda ^LU ; Wingren, Christer ^LU ; Montelius, Lars ^LU and Borrebaeck, Carl ^LU (2007) In Proteomics 7(4). p.540-547

Abstract: Antibody microarray is a rapidly emerging, powerful approach with great promise within high-throughput proteomics. However, before a truly proteome-wide analysis can be performed, the antibody array format needs to be miniaturized even further in order to enable ultradense arrays to be fabricated. To this end, we have designed and generated proof-of-concept for the first generation of an atto-vial based recombinant antibody array platform. Briefly, we have designed a novel nanostructured substrate using electron beam lithography. Vials, ranging in volume/size from 6 (200 nm in diameter) to 4000 aL (5 mu m in diameter), were fabricated. Human recombinant single-chain Fv antibody fragments, microarray adopted by design, were used as probes.... (More); Antibody microarray is a rapidly emerging, powerful approach with great promise within high-throughput proteomics. However, before a truly proteome-wide analysis can be performed, the antibody array format needs to be miniaturized even further in order to enable ultradense arrays to be fabricated. To this end, we have designed and generated proof-of-concept for the first generation of an atto-vial based recombinant antibody array platform. Briefly, we have designed a novel nanostructured substrate using electron beam lithography. Vials, ranging in volume/size from 6 (200 nm in diameter) to 4000 aL (5 mu m in diameter), were fabricated. Human recombinant single-chain Fv antibody fragments, microarray adopted by design, were used as probes. The set-up was interfaced with planar wave-guide technology for evanescant field fluorescence detection. The results showed that protein analytes could be specifically detected in the subzeptomole range for pure systems, using vials down to 57 aL. Further, low-abundant (pg/mL) protein analytes could be detected in directly labeled complex proteomes, such as human whole serum, using 157 aL-vials. Taken together, these results outline the potential of the atto-vial array set-up for miniaturized affinity proteomics-based approaches. (Less)

Please use this url to cite or link to this publication: https://lup.lub.lu.se/record/670385

author

Ghatnekar-Nilsson, Sara ^LU ; Dexlin Mellby, Linda ^LU ; Wingren, Christer ^LU ; Montelius, Lars ^LU and Borrebaeck, Carl ^LU

organization

publishing date

2007

type

Contribution to journal

publication status

published

subject

keywords

microarray, antibody, atto-vial, recombinant

in

Proteomics

volume

7

issue

4

pages

540 - 547

publisher

John Wiley & Sons Inc.

external identifiers

wos:000244807500007
scopus:33847683875

ISSN

1615-9861

DOI

10.1002/pmic.200600485

language

English

LU publication?

yes

id

eab74b16-12c2-4983-8165-12ecf9f4afcc (old id 670385)

date added to LUP

2016-04-01 11:56:28

date last changed

2022-01-26 20:27:20

@article{eab74b16-12c2-4983-8165-12ecf9f4afcc,
  abstract     = {{Antibody microarray is a rapidly emerging, powerful approach with great promise within high-throughput proteomics. However, before a truly proteome-wide analysis can be performed, the antibody array format needs to be miniaturized even further in order to enable ultradense arrays to be fabricated. To this end, we have designed and generated proof-of-concept for the first generation of an atto-vial based recombinant antibody array platform. Briefly, we have designed a novel nanostructured substrate using electron beam lithography. Vials, ranging in volume/size from 6 (200 nm in diameter) to 4000 aL (5 mu m in diameter), were fabricated. Human recombinant single-chain Fv antibody fragments, microarray adopted by design, were used as probes. The set-up was interfaced with planar wave-guide technology for evanescant field fluorescence detection. The results showed that protein analytes could be specifically detected in the subzeptomole range for pure systems, using vials down to 57 aL. Further, low-abundant (pg/mL) protein analytes could be detected in directly labeled complex proteomes, such as human whole serum, using 157 aL-vials. Taken together, these results outline the potential of the atto-vial array set-up for miniaturized affinity proteomics-based approaches.}},
  author       = {{Ghatnekar-Nilsson, Sara and Dexlin Mellby, Linda and Wingren, Christer and Montelius, Lars and Borrebaeck, Carl}},
  issn         = {{1615-9861}},
  keywords     = {{microarray; antibody; atto-vial; recombinant}},
  language     = {{eng}},
  number       = {{4}},
  pages        = {{540--547}},
  publisher    = {{John Wiley & Sons Inc.}},
  series       = {{Proteomics}},
  title        = {{Design of atto-vial based recombinant antibody arrays combined with a planar wave-guide detection system}},
  url          = {{http://dx.doi.org/10.1002/pmic.200600485}},
  doi          = {{10.1002/pmic.200600485}},
  volume       = {{7}},
  year         = {{2007}},
}

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Design of atto-vial based recombinant antibody arrays combined with a planar wave-guide detection system