Reverse-phase versus sandwich antibody microarray, technical comparison from a clinical perspective Journal Article


Authors: Järås, K.; Ressine, A.; Nilsson, E.; Malm, J.; Marko-Varga, G.; Lilja, H.; Laurell, T.
Article Title: Reverse-phase versus sandwich antibody microarray, technical comparison from a clinical perspective
Abstract: Protein microarrays are powerful tools to quantify and characterize proteins in multiplex assays. They have great potential within clinical diagnostics and prognostics, as they minimize consumption of both analyte and biological sample. Assays that do not require labeling of the biological specimen, henceforth called label-free, are vital for ease of clinical sample processing. Here, we evaluate two label-free techniques, reverse-phase and sandwich antibody assays, using microarrays on high-performance porous silicon surfaces and fluorescence detection. In view of increasing interest in reverse microarrays, this paper focuses on analytical sensitivity of the reverse assays compared to the more complex but highly sensitive sandwich assay. Sensitivity, linear range, and reproducibility of the two assays were compared using prostate-specific antigen (PSA) in buffer. The sandwich assay displayed 5 orders of magnitude lower detection limit (0.7 ng/mL) compared to the reverse assay (70 μg/mL). PSA at 50 nM (1.5 μg/mL) in cell lysates was detected by the sandwich assay but not by the reverse assay, demonstrating again a far lower detection limit for sandwich microarrays. In independent assay runs of PSA spiked in female serum, the sandwich assay had good linearity (R2 > 0.99) and reproducibility (coefficient of variation ≤15%), and the detection limit could be improved to 0.14 ng/mL. Without further signal amplification, the sandwich assay would be our choice for PSA analysis of clinical samples using a microarray technology platform. © 2007 American Chemical Society.
Keywords: protein array analysis; sensitivity and specificity; reproducibility; prostate specific antigen; reproducibility of results; fluorescence; prostate-specific antigen; antibodies, monoclonal; microarray analysis; diagnosis; intermethod comparison; fluorescence microscopy; immunoassay; antibodies; porosity; protein microarray; technology; cell extracts; porous silicon; silicon; cell lysate; medical applications; microarrays; buffer; analytical sensitivity; biological specimen; prostate-specific antigen (psa); signal amplification
Journal Title: Analytical Chemistry
Volume: 79
Issue: 15
ISSN: 0003-2700
Publisher: American Chemical Society  
Date Published: 2007-08-01
Start Page: 5817
End Page: 5825
Language: English
DOI: 10.1021/ac0709955
PUBMED: 17605470
PROVIDER: scopus
DOI/URL:
Notes: --- - "Cited By (since 1996): 15" - "Export Date: 17 November 2011" - "CODEN: ANCHA" - "Source: Scopus"
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  1. Hans Gosta Lilja
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