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A database built with INDRA combining content from numerous readers and databases. This page allows you to curate the loaded statements. For more information please see the manual.

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INDRA is developed by indralabs, a part of the Harvard Medical School Laboratory of Systems Pharmacology.

This project, indra_db, is also developed by the indralab team. For more information on how we procure our sources, you can go here. This work was funded by ARO grant W911NF‐15‐1‐0544 under the DARPA Communicating with Computers program.

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AKT phosphorylates USP35 on S613. 3 / 3

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"Collectively, our data indicate that USP35-S613 phosphorylation by AKT is required, but not sufficient, for USP35 enhancement of ERα target gene expression."

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"In addition, Akt phosphorylating Ser613 in USP35 is critical for USP35 nuclear translocation and enhancing ERα transcriptional activity (Fig. xref )."

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"Furthermore, phosphorylation of Ser613 in USP35 by AKT, an effector of PI3K, is critical for USP35 nuclear translocation and promoting ERα transcriptional activity and the growth of ER+ breast cancer cells."

34131114

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AKT phosphorylates USP35 on S613. 3 / 3

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