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Grouped-seq for integrated phenotypic and transcriptomic screening of patient-derived tumor organoids.


ABSTRACT: Patient-derived tumor organoids (PDOs) have emerged as a reliable in vitro model for drug discovery. However, RNA sequencing-based analysis of PDOs treated with drugs has not been realized in a high-throughput format due to the limited quantity of organoids. Here, we translated a newly developed pooled RNA-seq methodology onto a superhydrophobic microwell array chip to realize an assay of genome-wide RNA output unified with phenotypic data (Grouped-seq). Over 10-fold reduction of sample and reagent consumption together with a new ligation-based barcode synthesis method lowers the cost to ∼$2 per RNA-seq sample. Patient-derived colorectal cancer (CRC) organoids with a number of 10 organoids per microwell were treated with four anti-CRC drugs across eight doses and analyzed by the Grouped-seq. Using a phenotype-assisted pathway enrichment analysis (PAPEA) method, the mechanism of actions of the drugs were correctly derived, illustrating the great potential of Grouped-seq for pharmacological screening with tumor organoids.

SUBMITTER: Wu Y 

PROVIDER: S-EPMC8934649 | biostudies-literature | 2022 Mar

REPOSITORIES: biostudies-literature

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Grouped-seq for integrated phenotypic and transcriptomic screening of patient-derived tumor organoids.

Wu Yushuai Y   Li Kaiyi K   Li Yaqian Y   Sun Tao T   Liu Chang C   Dong Chunhui C   Zhao Tian T   Tang Decong D   Chen Xiaojie X   Chen Xiaofang X   Liu Peng P  

Nucleic acids research 20220301 5


Patient-derived tumor organoids (PDOs) have emerged as a reliable in vitro model for drug discovery. However, RNA sequencing-based analysis of PDOs treated with drugs has not been realized in a high-throughput format due to the limited quantity of organoids. Here, we translated a newly developed pooled RNA-seq methodology onto a superhydrophobic microwell array chip to realize an assay of genome-wide RNA output unified with phenotypic data (Grouped-seq). Over 10-fold reduction of sample and reag  ...[more]

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