Database of articles cited by EMDB/PDB/SASBDB data

Keywords
Structure methods	All X-ray diffraction NMR electron microscopy small angle scattering neutron diffraction fiber diffraction powder diffraction infrared spectroscopy EPR fluorescence transfer theoretical model Hybrid
Author
Journal
IF	>30 >20 >10 >5 all

Title	Mechanism of allosteric activation in human mitochondrial ClpP protease.
Journal, issue, pages	Proc Natl Acad Sci U S A, Vol. 122, Issue 16, Page e2419881122, Year 2025
Publish date	Apr 22, 2025
Authors	Monica M Goncalves / Adwaith B Uday / Taylor J B Forrester / S Quinn W Currie / Angelina S Kim / Yue Feng / Yulia Jitkova / Algirdas Velyvis / Robert W Harkness / Matthew S Kimber / Aaron D Schimmer / Natalie Zeytuni / Siavash Vahidi /
PubMed Abstract	Human ClpP protease contributes to mitochondrial protein quality control by degrading misfolded proteins. ClpP is overexpressed in cancers such as acute myeloid leukemia (AML), where its inhibition ...Human ClpP protease contributes to mitochondrial protein quality control by degrading misfolded proteins. ClpP is overexpressed in cancers such as acute myeloid leukemia (AML), where its inhibition leads to the accumulation of damaged respiratory chain subunits and cell death. Conversely, hyperactivating ClpP with small-molecule activators, such as the recently discovered ONC201, disrupts mitochondrial protein degradation and impairs respiration in cancer cells. Despite its critical role in human health, the mechanism underlying the structural and functional properties of human ClpP remains elusive. Notably, human ClpP is paradoxically activated by active-site inhibitors. All available structures of human ClpP published to date are in the inactive compact or compressed states, surprisingly even when ClpP is bound to an activator molecule such as ONC201. Here, we present structures of human mitochondrial ClpP in the active extended state, including a pair of structures where ClpP is bound to an active-site inhibitor. We demonstrate that amino acid substitutions in the handle region (A192E and E196R) recreate a conserved salt bridge found in bacterial ClpP, stabilizing the extended active state and significantly enhancing ClpP activity. We elucidate the ClpP activation mechanism, highlighting a hormetic effect where substoichiometric inhibitor binding triggers an allosteric transition that drives ClpP into its active extended state. Our findings link the conformational dynamics of ClpP to its catalytic function and provide high-resolution structures for the rational design of potent and specific ClpP inhibitors, with implications for targeting AML and other disorders with ClpP involvement.
External links	Proc Natl Acad Sci U S A / PubMed:40232800 / PubMed Central
Methods	EM (single particle) / X-ray diffraction
Resolution	2.49 - 3.2 Å
Structure data	46970 9dkv EMDB-46970, PDB-9dkv: Human mitochondrial ClpP in Apo state Method: EM (single particle) / Resolution: 2.81 Å 46971 9dkw EMDB-46971, PDB-9dkw: Human mitochondrial ClpP in complex with Bortezomib Method: EM (single particle) / Resolution: 2.49 Å PDB-9dqk: human ClpP - Apo - A192E / E196R Method: X-RAY DIFFRACTION / Resolution: 2.75 Å PDB-9dql: human ClpP - Bortezomib - A192E / E196R Method: X-RAY DIFFRACTION / Resolution: 3.2 Å
Chemicals	ChemComp-HOH: WATER ChemComp-BO2: N-[(1R)-1-(DIHYDROXYBORYL)-3-METHYLBUTYL]-N-(PYRAZIN-2-YLCARBONYL)-L-PHENYLALANINAMIDE / medication, anticancerYM ChemComp-CL*: Unknown entry
Source	homo sapiens (human)
Keywords	HYDROLASE / Protease / Proteolysis / Endopeptidase / Extended / Mutant / Inhibitor