Knockout Mouse Studies Show That Mitochondrial CLPP Peptidase and CLPX Unfoldase Act in Matrix Condensates near IMM, as Fast Stress Response in Protein Assemblies for Transcript Processing, Translation, and Heme Production

被引:0
作者
Key, Jana [1 ]
Gispert, Suzana [1 ]
Auburger, Georg [1 ]
机构
[1] Goethe Univ Frankfurt, Univ Hosp, Clin Neurol, Expt Neurol, Heinrich Hoffmann Str 7, D-60590 Frankfurt, Germany
关键词
Perrault syndrome type 3 (PRLTS3); iron toxicity; pyridoxal-5 '-phosphate; VWA8; GFM1; PNPT1; RNA-G4; ISC; ALAS; OAT; TRANSFER-RNA SYNTHETASE; SENSORINEURAL HEARING-LOSS; CAUSE PERRAULT SYNDROME; DOUBLE-STRANDED-RNA; POLYNUCLEOTIDE PHOSPHORYLASE; MISSENSE MUTATION; PROTOPORPHYRIN IX; GENE-EXPRESSION; RECESSIVE MUTATIONS; OVARIAN DYSGENESIS;
D O I
10.3390/genes15060694
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
LONP1 is the principal AAA+ unfoldase and bulk protease in the mitochondrial matrix, so its deletion causes embryonic lethality. The AAA+ unfoldase CLPX and the peptidase CLPP also act in the matrix, especially during stress periods, but their substrates are poorly defined. Mammalian CLPP deletion triggers infertility, deafness, growth retardation, and cGAS-STING-activated cytosolic innate immunity. CLPX mutations impair heme biosynthesis and heavy metal homeostasis. CLPP and CLPX are conserved from bacteria to humans, despite their secondary role in proteolysis. Based on recent proteomic-metabolomic evidence from knockout mice and patient cells, we propose that CLPP acts on phase-separated ribonucleoprotein granules and CLPX on multi-enzyme condensates as first-aid systems near the inner mitochondrial membrane. Trimming within assemblies, CLPP rescues stalled processes in mitoribosomes, mitochondrial RNA granules and nucleoids, and the D-foci-mediated degradation of toxic double-stranded mtRNA/mtDNA. Unfolding multi-enzyme condensates, CLPX maximizes PLP-dependent delta-transamination and rescues malformed nascent peptides. Overall, their actions occur in granules with multivalent or hydrophobic interactions, separated from the aqueous phase. Thus, the role of CLPXP in the matrix is compartment-selective, as other mitochondrial peptidases: MPPs at precursor import pores, m-AAA and i-AAA at either IMM face, PARL within the IMM, and OMA1/HTRA2 in the intermembrane space.
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