Translocon

Translocon: don't pass me by ranslocon proteins are intimately involved with the proteins they import into the ER—including transmembrane portions of the incoming proteins, based on results from Import of membrane proteins into the ER requires a joint effort between the T ribosome and the translocon to ensure that each domain of the translocating protein is targeted correctly to either the lumenal or cytoplasmic face of the ER. Transmem-brane domains present an additional problem—the hydrophobic portion must move laterally past the trans-locon into the lipid bilayer. Current models suggest that membrane-spanning domains Transmembrane domains make prolonged contacts with the translocon. ometimes a step back is needed before going forward.) find that uniquely specialized serine proteases evolved in two steps: an ancestor protease first became more promiscuous and despecial-ized before its duplicated progeny were then respecialized. Serine proteases found in vertebrates today come in various flavors: trypsin-like enzymes cleave after basic residues, but nontrypsin-like proteases favor S Evolution of a wider binding pocket entrance created a despecialized serine protease. nonbasic residues. Husain's group used phylogenetic inference to predict the structure of ancient serine proteases. They find that, although the most ancient proteases were specialized with trypsin-like qualities, the increased diversity that later spawned nontrypsin-like qualities was achieved by recreating a less specialized intermediate. An in vitro–produced enzyme based on the predicted sequence of this less specialized ancestor did indeed have broad substrate specificities—a feature not found in its descendants. This promiscuity seems to be due to a wider Evolution steps back entrance to the substrate pocket that would allow diverse side chains to bind in the cleavage site. The despecialized intermediate could be mutated in its substrate-binding pocket so that its substrate preference more closely resembled modern proteases. In the modern proteases, attempts to change binding specificities to that of other classes only kill the enzyme. So the intermediate was uniquely able to tolerate mutations that might lead to diversification. The intermediate is an ancestor of serine proteases that are important in immune defense responses. According to Husain, " respecialization in duplicated daughter genes would have allowed the evolutionary narrowing of specificities. .. thereby increasing the repertoire of efficient armaments necessary for efficient host defense. " Husain hopes to determine the structural basis of respecial-ization using crystallography. " The answers gained would not only have evolutionary significance, " he says, " but could also allow us to predict and make designer …