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Direct interaction between the PRDM3 and PRDM16 tumor suppressors and the NuRD chromatin remodeling complex.

Nucleic Acids Res. 2019; 
Ivanochko D,,, Halabelian L, Henderson E, Savitsky P, Jain H, Marcon E,, Duan S, Hutchinson A, Seitova A, Barsyte-Lovejoy D, Filippakopoulos P, Greenblatt J,, Lima-Fernandes E,,, Arrowsmith CH,,.
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Peptide Synthesis 2 molar ratio with synthetic hu- man PRDM3 or PRDM16 peptide (1–12; Genscript) at 4◦C. Get A Quote

摘要

Aberrant isoform expression of chromatin-associated proteins can induce epigenetic programs related to disease. The MDS1 and EVI1 complex locus (MECOM) encodes PRDM3, a protein with an N-terminal PR-SET domain, as well as a shorter isoform, EVI1, lacking the N-terminus containing the PR-SET domain (ΔPR). Imbalanced expression of MECOM isoforms is observed in multiple malignancies, implicating EVI1 as an oncogene, while PRDM3 has been suggested to function as a tumor suppressor through an unknown mechanism. To elucidate functional characteristics of these N-terminal residues, we compared the protein interactomes of the full-length and ΔPR isoforms of PRDM3 and its closely related paralog, PRDM16. Unlike the Δ... More

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