FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2971302725> ?p ?o ?g. }

• W2971302725 endingPage "12347" @default.
• W2971302725 startingPage "12334" @default.
• W2971302725 abstract "Lysosomal cysteine peptidase cathepsin B (catB) is an important tumor-promoting factor involved in tumor progression and metastasis representing a relevant target for the development of new antitumor agents. In the present study, we synthesized 11 ruthenium compounds bearing either the clinical agent nitroxoline that was previously identified as potent selective reversible inhibitor of catB activity or its derivatives. We demonstrated that organoruthenation is a viable strategy for obtaining highly effective and specific inhibitors of catB endo- and exopeptidase activity, as shown using enzyme kinetics and microscale thermophoresis. Furthermore, we showed that the novel metallodrugs by catB inhibition significantly impair processes of tumor progression in in vitro cell based functional assays at low noncytotoxic concentrations. Generally, by using metallodrugs we observed an improvement in catB inhibition, a reduction of extracellular matrix degradation and tumor cell invasion in comparison to free ligands, and a correlation with the reactivity of the monodentate halide leaving ligand." @default.
• W2971302725 created "2019-09-05" @default.
• W2971302725 creator A5022113201 @default.
• W2971302725 creator A5025878524 @default.
• W2971302725 creator A5048326409 @default.
• W2971302725 creator A5051865871 @default.
• W2971302725 creator A5059184386 @default.
• W2971302725 creator A5059675124 @default.
• W2971302725 creator A5071460704 @default.
• W2971302725 date "2019-08-29" @default.
• W2971302725 modified "2023-10-14" @default.
• W2971302725 title "Organoruthenated Nitroxoline Derivatives Impair Tumor Cell Invasion through Inhibition of Cathepsin B Activity" @default.
• W2971302725 cites W1607080847 @default.
• W2971302725 cites W1826848231 @default.
• W2971302725 cites W1845792010 @default.
• W2971302725 cites W1964901114 @default.
• W2971302725 cites W1966245361 @default.
• W2971302725 cites W1975883081 @default.
• W2971302725 cites W1980251832 @default.
• W2971302725 cites W1982592578 @default.
• W2971302725 cites W1990932054 @default.
• W2971302725 cites W1993992129 @default.
• W2971302725 cites W1994462959 @default.
• W2971302725 cites W2002906868 @default.
• W2971302725 cites W2003835776 @default.
• W2971302725 cites W2021423882 @default.
• W2971302725 cites W2023185574 @default.
• W2971302725 cites W2023653247 @default.
• W2971302725 cites W2036243377 @default.
• W2971302725 cites W2039150265 @default.
• W2971302725 cites W2042170565 @default.
• W2971302725 cites W2045464802 @default.
• W2971302725 cites W2058160302 @default.
• W2971302725 cites W2059205366 @default.
• W2971302725 cites W2068341079 @default.
• W2971302725 cites W2070460611 @default.
• W2971302725 cites W2070625765 @default.
• W2971302725 cites W2072747325 @default.
• W2971302725 cites W2085957556 @default.
• W2971302725 cites W2086201428 @default.
• W2971302725 cites W2089627958 @default.
• W2971302725 cites W2090985686 @default.
• W2971302725 cites W2107488926 @default.
• W2971302725 cites W2112253518 @default.
• W2971302725 cites W2114160655 @default.
• W2971302725 cites W2128410748 @default.
• W2971302725 cites W2128581376 @default.
• W2971302725 cites W2130440034 @default.
• W2971302725 cites W2132454074 @default.
• W2971302725 cites W2133693793 @default.
• W2971302725 cites W2144131403 @default.
• W2971302725 cites W2149451102 @default.
• W2971302725 cites W2165097920 @default.
• W2971302725 cites W2167872699 @default.
• W2971302725 cites W2171744625 @default.
• W2971302725 cites W2173889361 @default.
• W2971302725 cites W2313711272 @default.
• W2971302725 cites W2331558215 @default.
• W2971302725 cites W2419256959 @default.
• W2971302725 cites W2420879890 @default.
• W2971302725 cites W2479845289 @default.
• W2971302725 cites W2519868710 @default.
• W2971302725 cites W2592604348 @default.
• W2971302725 cites W2595920893 @default.
• W2971302725 cites W2624177752 @default.
• W2971302725 cites W2739679837 @default.
• W2971302725 cites W2765171483 @default.
• W2971302725 cites W2765362780 @default.
• W2971302725 cites W2765463682 @default.
• W2971302725 cites W2783125373 @default.
• W2971302725 cites W2794043274 @default.
• W2971302725 cites W2803313138 @default.
• W2971302725 cites W2888713522 @default.
• W2971302725 cites W2895186407 @default.
• W2971302725 cites W2896152740 @default.
• W2971302725 cites W2905045357 @default.
• W2971302725 cites W2913365458 @default.
• W2971302725 cites W2965821985 @default.
• W2971302725 cites W4236220604 @default.
• W2971302725 doi "https://doi.org/10.1021/acs.inorgchem.9b01882" @default.
• W2971302725 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6751773" @default.
• W2971302725 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31464130" @default.
• W2971302725 hasPublicationYear "2019" @default.
• W2971302725 type Work @default.
• W2971302725 sameAs 2971302725 @default.
• W2971302725 citedByCount "24" @default.
• W2971302725 countsByYear W29713027252020 @default.
• W2971302725 countsByYear W29713027252021 @default.
• W2971302725 countsByYear W29713027252022 @default.
• W2971302725 countsByYear W29713027252023 @default.
• W2971302725 crossrefType "journal-article" @default.
• W2971302725 hasAuthorship W2971302725A5022113201 @default.
• W2971302725 hasAuthorship W2971302725A5025878524 @default.
• W2971302725 hasAuthorship W2971302725A5048326409 @default.
• W2971302725 hasAuthorship W2971302725A5051865871 @default.
• W2971302725 hasAuthorship W2971302725A5059184386 @default.
• W2971302725 hasAuthorship W2971302725A5059675124 @default.
• W2971302725 hasAuthorship W2971302725A5071460704 @default.

• next