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High-resolution dose-response screening using droplet-based microfluidics.


ABSTRACT: A critical early step in drug discovery is the screening of a chemical library. Typically, promising compounds are identified in a primary screen and then more fully characterized in a dose-response analysis with 7-10 data points per compound. Here, we describe a robust microfluidic approach that increases the number of data points to approximately 10,000 per compound. The system exploits Taylor-Aris dispersion to create concentration gradients, which are then segmented into picoliter microreactors by droplet-based microfluidics. The large number of data points results in IC(50) values that are highly precise (± 2.40% at 95% confidence) and highly reproducible (CV = 2.45%, n = 16). In addition, the high resolution of the data reveals complex dose-response relationships unambiguously. We used this system to screen a chemical library of 704 compounds against protein tyrosine phosphatase 1B, a diabetes, obesity, and cancer target. We identified a number of novel inhibitors, the most potent being sodium cefsulodine, which has an IC(50) of 27 ± 0.83 ?M.

SUBMITTER: Miller OJ 

PROVIDER: S-EPMC3258639 | biostudies-literature | 2012 Jan

REPOSITORIES: biostudies-literature

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High-resolution dose-response screening using droplet-based microfluidics.

Miller Oliver J OJ   El Harrak Abdeslam A   Mangeat Thomas T   Baret Jean-Christophe JC   Frenz Lucas L   El Debs Bachir B   Mayot Estelle E   Samuels Michael L ML   Rooney Eamonn K EK   Dieu Pierre P   Galvan Martin M   Link Darren R DR   Griffiths Andrew D AD  

Proceedings of the National Academy of Sciences of the United States of America 20111227 2


A critical early step in drug discovery is the screening of a chemical library. Typically, promising compounds are identified in a primary screen and then more fully characterized in a dose-response analysis with 7-10 data points per compound. Here, we describe a robust microfluidic approach that increases the number of data points to approximately 10,000 per compound. The system exploits Taylor-Aris dispersion to create concentration gradients, which are then segmented into picoliter microreact  ...[more]

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