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  4. Microfluidics-based immunofluorescence for fast staining of ALK in lung adenocarcinoma
 
research article

Microfluidics-based immunofluorescence for fast staining of ALK in lung adenocarcinoma

Brajkovic, Saska  
•
Pelz, Benjamin  
•
Procopio, Maria-Giuseppina
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October 16, 2018
Diagnostic Pathology

BackgroundAnaplastic lymphoma kinase (ALK) is a key oncogenic driver in lung adenocarcinoma patients and its fusion proteins are routinely assessed. The microfluidic tissue processor (MTP) device is based on a chip-confined low-volume technology allowing for rapid immunohistochemistry/immunofluorescence (IHC/IF) stainings of formalin-fixed paraffin-embedded (FFPE) or frozen tissue samples.MethodsA novel ALK IF protocol was developed for the MTP device using the primary mouse anti-human ALK antibody clone 5A4. FFPE tumor whole sections from 14 resected lung adenocarcinoma patients documented to be ALK positive (ALK+) by automated chromogenic IHC and/or FISH were used. MTP-derived IF immunoreactivity was measured by computerized analysis of digitalized images on individual frames of tumor epithelia and surrounding stroma, using an ImageJ plug-in.ResultsThe 5A4 antibody yielded saturated immunoreactivity at an incubation time of 4min on a titration curve ranging from 2 to 32min. Total staining time on the MTP device was 18min including secondary IgG Alexa Fluor 647. MTP-based ALK IF confirmed all 12 cases; with epithelial signal above stromal staining based on computerized pixel-based measurement. MTP-IF (mean intensity levels 458 to 1301) and chromogenic IHC (H-score 120 to 300) showed an equal range of variation of 2.8 and 2.5 folds, respectively, and a trend for direct correlation (p-value 0.051).ConclusionThe newly developed protocol for immunofluorescent detection of ALK protein with the MTP device confirms chromogenic IHC results on FFPE lung adenocarcinoma specimens. MTP-based IF is fast and reliable. We foresee this study to be a first step opening the road for further realization of microfluidic-based assays for rapid simultaneous detection of targetable oncogenic and immune-system related markers in their topographical context to investigate tumour heterogeneity and micro-environmental interactions.

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Type
research article
DOI
10.1186/s13000-018-0757-1
Web of Science ID

WOS:000447655000001

Author(s)
Brajkovic, Saska  
Pelz, Benjamin  
Procopio, Maria-Giuseppina
Leblond, Anne-Laure
Repond, Gregoire
Schaub-Clerigue, Ariane
Dupouy, Diego G.  
Soltermann, Alex
Date Issued

2018-10-16

Publisher

BMC

Published in
Diagnostic Pathology
Volume

13

Start page

79

Subjects

Pathology

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microfluidic tissue processor

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immunofluorescence

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anaplastic lymphoma kinase

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lung adenocarcinoma

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platform lungscape project

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cancer

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immunohistochemistry

Editorial or Peer reviewed

REVIEWED

Written at

EPFL

EPFL units
LMIS2  
Available on Infoscience
December 13, 2018
Use this identifier to reference this record
https://infoscience.epfl.ch/handle/20.500.14299/152087
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