Download MendeleyThe ClpS adaptor mediates staged delivery of N-end rule substrates to the AAA+ ClpAP protease.
Roman-Hernandez, G., Hou, J.Y., Grant, R.A., Sauer, R.T., Baker, T.A.(2011) Mol Cell 43: 217-228
- PubMed: 21777811
- DOI: https://doi.org/10.1016/j.molcel.2011.06.009
- Primary Citation of Related Structures:
3O1F, 3O2B, 3O2H, 3O2O - PubMed Abstract:
The ClpS adaptor delivers N-end rule substrates to ClpAP, an energy-dependent AAA+ protease, for degradation. How ClpS binds specific N-end residues is known in atomic detail and clarified here, but the delivery mechanism is poorly understood. We show that substrate binding is enhanced when ClpS binds hexameric ClpA. Reciprocally, N-end rule substrates increase ClpS affinity for ClpA(6). Enhanced binding requires the N-end residue and a peptide bond of the substrate, as well as multiple aspects of ClpS, including a side chain that contacts the substrate α-amino group and the flexible N-terminal extension (NTE). Finally, enhancement also needs the N domain and AAA+ rings of ClpA, connected by a long linker. The NTE can be engaged by the ClpA translocation pore, but ClpS resists unfolding/degradation. We propose a staged-delivery model that illustrates how intimate contacts between the substrate, adaptor, and protease reprogram specificity and coordinate handoff from the adaptor to the protease.
Organizational Affiliation:
Department of Biology, Massachusetts Institute of Technology, Cambridge, MA 02139, USA.
