[No authors listed]
The calcium ion (Ca(2+)) is a ubiquitous second messenger that is crucial for the regulation of a wide variety of cellular processes. The diverse transient signals transduced by Ca(2+) are mediated by intracellular Ca(2+)-binding proteins, also known as Ca(2+) sensors. A key obstacle to studying many Ca(2+)-sensing proteins is the difficulty in identifying the numerous downstream target interactions that respond to Ca(2+)-induced conformational changes. Among a number of Ca(2+) sensors in the eukaryotic cell, calmodulin (CaM) is the most widespread and the best studied. Employing the mRNA display technique, we have scanned the human proteome for CaM-binding proteins and have identified and characterized a large number of both known and previously uncharacterized proteins that interact with CaM in a Ca(2+)-dependent manner. The interactions of several identified proteins with Ca(2+)/CaM were confirmed by using pull-down assays and coimmunoprecipitation. Many of the CaM-binding proteins identified belong to protein families such as the DEAD/H box proteins, ribosomal proteins, proteasome 26S subunits, and deubiquitinating enzymes, suggesting the possible involvement of Ca(2+)/CaM in different signaling pathways. The selection method described herein could be used to identify the binding partners of other calcium sensors on the proteome-wide scale.
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Akt1, Rad23b, Cdc5l, HUWE1, PDCD7, OPTN, STAG1, TRDN, USP16, MORF4L1, METAP2, IMMT, LACTB, CKMT1B, SCLT1, DOCK11, DDX5, DMXL1, DOCK3, AKT1, FKBP3, NT5C2, MYCBP2, KIF1B, SYNE2, DNAJC13, SF3B1, RPL13A, DDAH1, LY96, PPIL2, FBXO9, GNAS, GTF2I, ACADM, ITGA6, LMO7, NBR1, MYBPC1, NEB, YBX1, SCAPER, PRDX1, PAM, UCHL5, NOL7, MBIP, BRWD1, DCUN1D1, POLR2B, ATRX, ARMC1, CDC37L1, LUC7L, SLF2, PSMD2, PSMD12, STIM2, SNX6, RAD23B, RANBP2, RDX, RPL22, RPS4Y1, RPS8, RPS14, RPS15A, CLIP1, S100B, SET, SRSF5, CCDC14, PHACTR4, SNRPB2, DST, SRP14, TPT1, XRCC4, SLTM, CALM1, KDM5C, EIF3C, SQSTM1, HERC2, NEXN, DDX21, OPALIN, AKAP6, STX8, CLINT1, MATR3, ZBTB24, CDC5L, PUM3, CASP8AP2
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