SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4285605422> ?p ?o ?g. }

Showing items 1 to 100 of ±146 with 100 items per page.

W4285605422 endingPage "120801" @default.
W4285605422 startingPage "120801" @default.
W4285605422 abstract "Drug-induced nephrotoxicity is frequently reported. However, the mechanisms underlying nephrotoxic medications and their overlapping molecular events, which might have therapeutic value, are unclear. We performed a genome-wide analysis of gene expression and a gene set enrichment analysis to identify common and unique pathways associated with the toxicity of colistin, ifosfamide, indomethacin, and puromycin. Rats were randomly allocated into the treatment or control group. The treatment group received a toxic dose once daily of each investigated drug for 1 week. Differentially expressed genes were found in the drug-treated kidney and liver compared to the control, except for colistin in the liver. Upregulated pathways were mainly related to cell death, cell cycle, protein synthesis, and immune response modulation in the kidney. Cell cycle was upregulated by all drugs. Downregulated pathways were associated with carbon metabolism, amino acid metabolism, and fatty acid metabolism. Indomethacin, colistin, and puromycin shared the most altered pathways in the kidney. Ifosfamide and indomethacin affected molecular processes greatly in the liver. Our findings provide insight into the mechanisms underlying the renal and hepatic adverse effects of the four drugs. Further investigation should explore the combinatory drug therapies that attenuate the toxic effects and maximize the effectiveness of nephrotoxic drugs." @default.
W4285605422 created "2022-07-16" @default.
W4285605422 creator A5002251529 @default.
W4285605422 creator A5020448496 @default.
W4285605422 creator A5023891207 @default.
W4285605422 creator A5026101027 @default.
W4285605422 creator A5035112064 @default.
W4285605422 creator A5035147466 @default.
W4285605422 creator A5059760054 @default.
W4285605422 creator A5062320913 @default.
W4285605422 creator A5068092189 @default.
W4285605422 creator A5086975371 @default.
W4285605422 date "2022-10-01" @default.
W4285605422 modified "2023-09-24" @default.
W4285605422 title "Genome-wide gene expression analysis reveals molecular insights into the drug-induced toxicity of nephrotoxic agents" @default.
W4285605422 cites W1518814346 @default.
W4285605422 cites W1565605888 @default.
W4285605422 cites W1939174480 @default.
W4285605422 cites W1953460679 @default.
W4285605422 cites W1965388408 @default.
W4285605422 cites W1970737887 @default.
W4285605422 cites W1995454475 @default.
W4285605422 cites W2002200686 @default.
W4285605422 cites W2008887283 @default.
W4285605422 cites W2011678217 @default.
W4285605422 cites W2020503360 @default.
W4285605422 cites W2021560851 @default.
W4285605422 cites W2024302689 @default.
W4285605422 cites W2039107480 @default.
W4285605422 cites W2068335053 @default.
W4285605422 cites W2076781542 @default.
W4285605422 cites W2087664337 @default.
W4285605422 cites W2087826013 @default.
W4285605422 cites W2089801438 @default.
W4285605422 cites W2111239148 @default.
W4285605422 cites W2130410032 @default.
W4285605422 cites W2146512944 @default.
W4285605422 cites W2147294934 @default.
W4285605422 cites W2151685719 @default.
W4285605422 cites W2159482845 @default.
W4285605422 cites W2159683231 @default.
W4285605422 cites W2167578561 @default.
W4285605422 cites W2228153896 @default.
W4285605422 cites W2245932016 @default.
W4285605422 cites W2264921308 @default.
W4285605422 cites W2289921214 @default.
W4285605422 cites W2548410084 @default.
W4285605422 cites W2604619953 @default.
W4285605422 cites W2781977913 @default.
W4285605422 cites W2888131251 @default.
W4285605422 cites W2910111050 @default.
W4285605422 cites W2928591174 @default.
W4285605422 cites W2930009663 @default.
W4285605422 cites W2935024989 @default.
W4285605422 cites W2962821542 @default.
W4285605422 cites W3036366704 @default.
W4285605422 cites W3146216614 @default.
W4285605422 cites W3171646083 @default.
W4285605422 cites W3197716339 @default.
W4285605422 cites W3211558043 @default.
W4285605422 cites W4206908401 @default.
W4285605422 cites W4212782342 @default.
W4285605422 cites W4213231519 @default.
W4285605422 cites W4256409604 @default.
W4285605422 doi "https://doi.org/10.1016/j.lfs.2022.120801" @default.
W4285605422 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/35850247" @default.
W4285605422 hasPublicationYear "2022" @default.
W4285605422 type Work @default.
W4285605422 citedByCount "1" @default.
W4285605422 countsByYear W42856054222023 @default.
W4285605422 crossrefType "journal-article" @default.
W4285605422 hasAuthorship W4285605422A5002251529 @default.
W4285605422 hasAuthorship W4285605422A5020448496 @default.
W4285605422 hasAuthorship W4285605422A5023891207 @default.
W4285605422 hasAuthorship W4285605422A5026101027 @default.
W4285605422 hasAuthorship W4285605422A5035112064 @default.
W4285605422 hasAuthorship W4285605422A5035147466 @default.
W4285605422 hasAuthorship W4285605422A5059760054 @default.
W4285605422 hasAuthorship W4285605422A5062320913 @default.
W4285605422 hasAuthorship W4285605422A5068092189 @default.
W4285605422 hasAuthorship W4285605422A5086975371 @default.
W4285605422 hasConcept C104317684 @default.
W4285605422 hasConcept C126189478 @default.
W4285605422 hasConcept C126322002 @default.
W4285605422 hasConcept C134018914 @default.
W4285605422 hasConcept C150194340 @default.
W4285605422 hasConcept C2776637226 @default.
W4285605422 hasConcept C2776694085 @default.
W4285605422 hasConcept C2777506904 @default.
W4285605422 hasConcept C2778239845 @default.
W4285605422 hasConcept C2779259085 @default.
W4285605422 hasConcept C2780035454 @default.
W4285605422 hasConcept C2780091579 @default.
W4285605422 hasConcept C29730261 @default.
W4285605422 hasConcept C501593827 @default.
W4285605422 hasConcept C54355233 @default.
W4285605422 hasConcept C55493867 @default.
W4285605422 hasConcept C71924100 @default.