[No authors listed]
During protein synthesis, it is often necessary for the ribosome to form a complex with a membrane-bound channel, the SecY/Sec61 complex, in order to translocate nascent proteins across a cellular membrane. Structural data on the ribosome-channel complex are currently limited to low-resolution cryo-electron microscopy maps, including one showing a bacterial ribosome bound to a monomeric SecY complex. Using that map along with available atomic-level models of the ribosome and SecY, we have determined, through molecular dynamics flexible fitting (MDFF), an atomic-resolution model of the ribosome-channel complex. We characterized computationally the sites of ribosome-SecY interaction within the complex and determined the effect of ribosome binding on the SecY channel. We also constructed a model of a ribosome in complex with a SecY dimer by adding a second copy of SecY to the MDFF-derived model. The study involved 2.7-million-atom simulations over altogether nearly 50 ns.
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rpsT, ftsQ, rplT, rpmA, rplY, rpmF, rpmG, rpmI, rpmB, rplS, rpsP, rpsU, rpsO, rplQ, rpsM, rpsK, rpsD, rpsE, rpmD, rplO, secY, rplE, rpsN, rpsH, rplF, rplR, rpmJ, rplP, rpmC, rpsQ, rplN, rplX, rpsS, rplV, rpsC, rpsJ, rplC, rplD, rplW, rplB, rplM, rpsL, rpsG, rpsB, rpmH, rpmE, rplA, rplK, secE, rplL, rplJ, rplI, rpsR, rpsF, rpsI, rplU
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