Metabolomics Workbench : NIH Data Repository

Compare metabolites in 2 of these studies:

List of Studies ( Metabolite:Ile-Lys-Pro)

Study_id	Analysis_id	Study_title	Source	Species	Disease	Institute	Analysis Type
ST004291	AN007135	Metabolomics analysis of Plasmodium falciparum asexual-stage parasites treated with plasmepsin V peptidomimetics - 16 hour treatment	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST004290	AN007133	Metabolomics characterisation of Plasmodium falciparum response to plasmepsin V peptidomimetic inhibitors - 5 hour treatment	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST004194	AN006966	PfK13-associated artemisinin resistance slows drug activation and enhances antioxidant defence, which can be overcome with sulforaphane	Cultured cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003778	AN006205	Human to mouse microbiota transfer model demonstrates disease-modifying effects of the short-chain fatty acid biotherapy modified microbiota	Feces	Mouse	Diabetes	University of Queensland	LC-MS
ST003565	AN005857	Metaboloomics analysis of the antimalarial compound WEHI-1888504 (aka compound 59) in Plasmodium falciparum (3D7) infected red blood cells	Cultured cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003521	AN005782	Metabolic Profiling Unveils Enhanced Antibacterial Synergy of Polymyxin B and Teixobactin against Multi-Drug Resistant Acinetobacter baumannii	Bacterial cells	Acinetobacter baumannii	Bacterial infection	Monash University	LC-MS
ST003179	AN005221	Property and Activity Refinement of Dihydroquinazolinone-3-carboxamides as Orally Efficacious Antimalarials that Target PfATP4	Plasmodium cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003144	AN005159	On-target, dual aminopeptidase inhibition provides cross-species antimalarial activity	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003036	AN004977	Identifying and mathematically modeling the time-course of extracellular metabolic markers associated with resistance to ceftolozane/tazobactam in Pseudomonas aeruginosa - Part 2	Bacterial cells	Pseudomonas aeruginosa	Bacterial infection	Monash Institute of Pharmaceutical Sciences	LC-MS
ST003024	AN004958	Identifying and mathematically modeling the time-course of extracellular metabolic markers associated with resistance to ceftolozane/tazobactam in Pseudomonas aeruginosa - Part 1	Bacterial cells	Pseudomonas aeruginosa		Monash Institute of Pharmaceutical Sciences	LC-MS
ST002926	AN004798	Multi-“omics” analysis reveals the orphan P. falciparum protein kinase PfPK8 regulates multi-gene family expression	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST002792	AN004542	Chemoproteomics validates selective targeting of Plasmodium M1 alanyl aminopeptidase as a cross-species strategy to treat malaria	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST002698	AN004372	Systemic host inflammation induces stage-specific transcriptomic modification and slower maturation in malaria parasites	Infected Red Blood Cells	Plasmodium berghei	Malaria	Peter Doherty Institute for Infection and Immunity	LC-MS
ST002412	AN003931	Metabolic effects of the protein kinase R	Macrophages	Mouse		Hudson Institute of Medical Research	LC-MS
ST002309	AN003771	Targeting malaria parasites with novel derivatives of azithromycin	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST002106	AN003444	Genetic and chemical validation of Plasmodium falciparum aminopeptidase PfA-M17 as a drug target in the hemoglobin digestion pathway (Part 1)	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST002104	AN003439	Chemoresistant Cancer Cell Lines are Characterized by Migratory, Amino Acid Metabolism, Protein Catabolism and IFN1 Signalling Perturbations	Cultured cells	Human	Cancer	Future Industries Institute	LC-MS
ST002010	AN003276	Chemoresistant Ovarian Cancer Global Metabolomics	Cultured cells	Human	Cancer	University of South Australia	LC-MS
ST001549	AN002580	β-Adrenergic regulation of metabolism in macrophages (part-III)	Macrophages	Human		Monash University	LC-MS
ST001547	AN002576	β-Adrenergic regulation of metabolism in macrophages	Macrophages	Human		Monash University	LC-MS
ST001315	AN002189	Retargeting azithromycin-like compounds as antimalarials with dual modality	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST001304	AN002172	Multi-omics analysis delineates the distinct functions of sub-cellular acetyl-CoA pools in Toxoplasma gondii	Fibroblast cells	Toxoplasma gondii	Parasitic infection	Monash University	LC-MS
ST001201	AN001998	Peroxide antimalarial treatment timecourse on trophozoite-stage P. falciparum parasites	Cultured cells	Human	Malaria	Monash University	LC-MS
ST001201	AN001998	Peroxide antimalarial treatment timecourse on trophozoite-stage P. falciparum parasites	Cultured cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST001175	AN001950	Multi-omics analysis demonstrates unique mode of action of a potent new antimalarial compound, JPC-3210, against Plasmodium falciparum	Plasmodium cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST001033	AN001694	Determination of mode of action of anti-malalrial drugs using untargeted metabolomics	Cultured cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST000546	AN000832	Multi-omics based identification of specific biochemical changes associated with PfKelch13-mutant artemisinin resistant Plasmodium	Cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST000414	AN000655	Metabolomics-based screening of the Malaria Box reveals both novel and established mechanisms of action	Cells	Plasmodium falciparum	Malaria	Monash Institute of Pharmaceutical Sciences	LC-MS