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A structure and function relationship study to identify the impact of the R721G mutation in the human mitochondrial lon protease

Arch Biochem Biophys. 2021-07; 
Zhou Sha, Monica M Montano, Kristy Rochon, Jason A Mears, Daniel Deredge, Patrick Wintrode, Luke Szweda, Natalie Mikita, Irene Lee
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Proteins, Expression, Isolation and Analysis … Synthetic peptides used in this study were custom synthesized by Genscript. Radioactive 32 P-gamma ATP was purchased from PerkinElmer. Chemicals used to prepare buffers, Western blot transfer, protein purification were purchased from Sigma-Aldrich and Thermo Fisher … Get A Quote

摘要

Lon is an ATP-dependent protease belonging to the "ATPase associated with diverse cellular activities" (AAA+) protein family. In humans, Lon is translated as a precursor and imported into the mitochondria matrix through deletion of the first 114 amino acid residues. In mice, embryonic knockout of lon is lethal. In humans, some dysfunctional lon mutations are tolerated but they cause a developmental disorder known as the CODAS syndrome. To gain a better understanding on the enzymology of human mitochondrial Lon, this study compares the structure-function relationship of the WT versus one of the CODAS mutants R721G to identify the mechanistic features in Lon catalysis that are affected. To this end, steady-state ... More

關鍵詞

CODAS, Hydrogen-deuterium exchange, Lon protease, Nucleotide induced conformational changes, Steady-state kinetics
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