Metabolomics Workbench : NIH Data Repository

Compare metabolites in 2 of these studies:

List of Studies ( Metabolite:N-Nitrosoproline)

Study_id	Analysis_id	Study_title	Source	Species	Disease	Institute	Analysis Type
ST004291	AN007136	Metabolomics analysis of Plasmodium falciparum asexual-stage parasites treated with plasmepsin V peptidomimetics - 16 hour treatment	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003565	AN005858	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
ST003340	AN005474	Effect of feeding and the mTORC1 activity on metabolism in Caenorhabditis elegans	Worms	C. elegans		Hiroshima University	LC-MS
ST003179	AN005222	Property and Activity Refinement of Dihydroquinazolinone-3-carboxamides as Orally Efficacious Antimalarials that Target PfATP4	Plasmodium cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003160	AN005185	New class of heterospirocyclic compounds present strong and rapid activity against artemisinin- and multidrug-resistant P. falciparum parasites	Plasmodium cells	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST003085	AN005044	Metabolome changes in embryonic CSF (Part 7)	Cerebrospinal fluid	Mouse	Autism	Boston Children's Hospital, Harvard Medical School	LC-MS
ST003065	AN005021	Investigative needle core biopsies for multi-omics in Glioblastoma	Brain	Human	Cancer	Brigham and Women's Hospital	MALDI-MS
ST003053	AN005007	Providing insight into the mechanism of action of Cationic Lipidated Oligomers (CLOs) using metabolomics	Bacterial cells	Staphylococcus aureus	Bacterial infection	Monash University	LC-MS
ST002108	AN003449	Genetic and chemical validation of Plasmodium falciparum aminopeptidase PfA-M17 as a drug target in the hemoglobin digestion pathway (Part 3)	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST002107	AN003447	Genetic and chemical validation of Plasmodium falciparum aminopeptidase PfA-M17 as a drug target in the hemoglobin digestion pathway (Part 2)	Blood	Plasmodium falciparum	Malaria	Monash University	LC-MS
ST002104	AN003440	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
ST002094	AN003420	Commensal intestinal microbiota regulates host luminal proteolytic activity and intestinal barrier integrity through β-glucuronidase activity (Part 1)	Feces	Human	Irritable bowel syndrome	Mayo Clinic	LC-MS
ST002094	AN003422	Commensal intestinal microbiota regulates host luminal proteolytic activity and intestinal barrier integrity through β-glucuronidase activity (Part 1)	Feces	Human	Irritable bowel syndrome	Mayo Clinic	LC-MS
ST002010	AN003276	Chemoresistant Ovarian Cancer Global Metabolomics	Cultured cells	Human	Cancer	University of South Australia	LC-MS
ST001304	AN002173	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
ST001175	AN001951	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
ST000291	AN000464	LC-MS Based Approaches to Investigate Metabolomic Differences in the Urine of Young Women after Drinking Cranberry Juice or Apple Juice	Urine	Human		University of Florida	LC-MS