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Pitfalls of mapping high-throughput sequencing data to repetitive sequences: Piwi's genomic targets still not identified.


ABSTRACT: Huang et al. (2013) recently reported that chromatin immunoprecipitation sequencing (ChIP-seq) reveals the genome-wide sites of occupancy by Piwi, a piRNA-guided Argonaute protein central to transposon silencing in Drosophila. Their study also reported that loss of Piwi causes widespread rewiring of transcriptional patterns, as evidenced by changes in RNA polymerase II occupancy across the genome. Here we reanalyze their data and report that the underlying deep-sequencing dataset does not support the authors' genome-wide conclusions.

SUBMITTER: Marinov GK 

PROVIDER: S-EPMC4494788 | biostudies-literature | 2015 Mar

REPOSITORIES: biostudies-literature

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Pitfalls of mapping high-throughput sequencing data to repetitive sequences: Piwi's genomic targets still not identified.

Marinov Georgi K GK   Wang Jie J   Handler Dominik D   Wold Barbara J BJ   Weng Zhiping Z   Hannon Gregory J GJ   Aravin Alexei A AA   Zamore Phillip D PD   Brennecke Julius J   Toth Katalin Fejes KF  

Developmental cell 20150301 6


Huang et al. (2013) recently reported that chromatin immunoprecipitation sequencing (ChIP-seq) reveals the genome-wide sites of occupancy by Piwi, a piRNA-guided Argonaute protein central to transposon silencing in Drosophila. Their study also reported that loss of Piwi causes widespread rewiring of transcriptional patterns, as evidenced by changes in RNA polymerase II occupancy across the genome. Here we reanalyze their data and report that the underlying deep-sequencing dataset does not suppor  ...[more]

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