InAADR: Drug-Protein-ADRs database

Drug Name:	Cephaloridine (50-59-9)
PubChem ID:	5773
SMILES:	C1C(=C(N2[C@H](S1)[C@@H](C2=O)NC(=O)CC3=CC=CS3)C(=O)[O-])C[N+]4=CC=CC=C4
InchiKey:	CZTQZXZIADLWOZ-CRAIPNDOSA-N
Therapeutic Category:	Anti-Bacterial Agents, Anti-Infective Agents

This panel provides information on interacting drugs and their ADRs along with references

Interacting drug	Toxicity	Interaction Type	Mechanism	Reference
Furosemide (54-31-9)	Nephrotoxicity	Antagonistic	Cefaloridine is nephrotoxic, but why this should be increased by furosemide is not understood. It may possibly be related to a reduction in its clearance	Enhancement by potent diuretics of renal tubular necrosis induced by cephaloridine
Probenecid (57-66-9)	Nephrotoxicity	Antagonistic	Probenecid inhibits the excretion of most cephalosporins by the kidney tubules by successfully competing for the excretory mechanisms. Thus the cephalosporin is retained in the body and its serum levels rise. The extent of the rise cannot always be fully accounted for by this mechanism alone and it is suggested that some change in tissue distribution may sometimes have a part to play.	Probenecid: an unexplained effect on cephalosporin pharmacology

This panel provides drug-protein interaction and their ADRs along with references

Toxicity	Interacting Protein	Mechanism	Reference
Impair Antioxidant Status	Glutathione peroxidase 1 (P07203)	Selenium deficiency impaired antioxidant status and enhanced cephaloridine-induced injury [ ADR Type 3 ]	Cephaloridine nephrotoxicity is potentiated by selenium deficiency but not copper deficiency in rats
Nephrotoxicity	Glutathione peroxidase 1 (P07203)	Selenium deficiency potentiated cephaloridine nephrotoxicity [ ADR Type 3 ]	Cephaloridine nephrotoxicity is potentiated by selenium deficiency but not copper deficiency in rats

This panel provides drug-food interactions and their ADRs along with references

Food	Toxicity	Reference

This panel provides information on metabolites and their ADRs along with references

Metabolite	Toxicity	Place of Metabolism	Mechanism	Reference

This panel provides information on drug category

Toxicity	Source
Acute Kidney Injury	MetaADEDB
Anuria	MetaADEDB
Basal Ganglia Diseases	MetaADEDB
Brain Diseases	MetaADEDB
Drug Hypersensitivity	MetaADEDB
Drug-Induced Liver Injury	MetaADEDB
Exanthema	MetaADEDB
Glycosuria	MetaADEDB
Kidney Diseases	MetaADEDB
Kidney Tubular Necrosis Acute	MetaADEDB
Necrosis	MetaADEDB
Nephritis Interstitial	MetaADEDB
Parkinsonian Disorders	MetaADEDB
Polyuria	MetaADEDB
Proteinuria	MetaADEDB
Renal Insufficiency	MetaADEDB
Seizures	MetaADEDB
Unconsciousness	MetaADEDB
Uremia	MetaADEDB

Molecular Weight (dalton)	:	415.496
LogP	:	-0.3178
Ring Count	:	2
Hydrogen Bond Acceptor Count	:	6
Hydrogen Bond Donor Count	:	1
Total Polar Surface Area	:	93.42