FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4280568762> ?p ?o ?g. }

• W4280568762 endingPage "1113" @default.
• W4280568762 startingPage "1113" @default.
• W4280568762 abstract "Pancreatic cancer (PCa), one of the most malignant solid tumors, has a high mortality rate. Although there have been many trials of chemotherapeutic drugs such as gemcitabine, the mortality rates remain significantly higher than for other types of cancer. Therefore, more effective ways of improving conventional therapy for PCa are needed. Cancer cells take up large amounts of glutamine to drive their rapid proliferation. Recent studies show that the amino acid transporter SLC6A14 is upregulated in some cancers alongside glutamine metabolism. Alloferon, a peptide isolated from the insect immune system, exerts anti-viral and anti-inflammatory effects via its immunomodulatory function. In addition, it has anti-tumoral effects, although the underlying mechanisms are largely unknown. Therefore, we investigated the effects of alloferon on the PCa cell lines Panc-1 and AsPC-1. Exposure of these cells to alloferon for 3 weeks led to the downregulation of SLC6A14 expression and decreased glutamine uptake. Given that SLC6A14 plays a role in tumor progression and survival by promoting glutamine uptake into cancer cells, alloferon could be a potential adjuvant for the chemotherapeutic drug gemcitabine." @default.
• W4280568762 created "2022-05-22" @default.
• W4280568762 creator A5007122170 @default.
• W4280568762 creator A5024660659 @default.
• W4280568762 creator A5025050406 @default.
• W4280568762 creator A5037701924 @default.
• W4280568762 creator A5039429164 @default.
• W4280568762 creator A5048132059 @default.
• W4280568762 creator A5069015546 @default.
• W4280568762 creator A5075620151 @default.
• W4280568762 creator A5080390580 @default.
• W4280568762 creator A5086930411 @default.
• W4280568762 date "2022-05-11" @default.
• W4280568762 modified "2023-09-26" @default.
• W4280568762 title "Alloferon Affects the Chemosensitivity of Pancreatic Cancer by Regulating the Expression of SLC6A14" @default.
• W4280568762 cites W1490655572 @default.
• W4280568762 cites W1494546891 @default.
• W4280568762 cites W1558737388 @default.
• W4280568762 cites W1970779614 @default.
• W4280568762 cites W1972504016 @default.
• W4280568762 cites W2006547875 @default.
• W4280568762 cites W2007026131 @default.
• W4280568762 cites W2014621333 @default.
• W4280568762 cites W2030186434 @default.
• W4280568762 cites W2033228549 @default.
• W4280568762 cites W2039759902 @default.
• W4280568762 cites W2051648135 @default.
• W4280568762 cites W2060592426 @default.
• W4280568762 cites W2064476588 @default.
• W4280568762 cites W2090265589 @default.
• W4280568762 cites W2090406819 @default.
• W4280568762 cites W2105535255 @default.
• W4280568762 cites W2113108127 @default.
• W4280568762 cites W2125590861 @default.
• W4280568762 cites W2140662194 @default.
• W4280568762 cites W2141856080 @default.
• W4280568762 cites W2142682640 @default.
• W4280568762 cites W2151101871 @default.
• W4280568762 cites W2155319744 @default.
• W4280568762 cites W2162862905 @default.
• W4280568762 cites W2169903226 @default.
• W4280568762 cites W2200217449 @default.
• W4280568762 cites W2211215064 @default.
• W4280568762 cites W2219161659 @default.
• W4280568762 cites W2503851771 @default.
• W4280568762 cites W2528445830 @default.
• W4280568762 cites W2533930104 @default.
• W4280568762 cites W2534904302 @default.
• W4280568762 cites W2588856093 @default.
• W4280568762 cites W2599846384 @default.
• W4280568762 cites W2744034133 @default.
• W4280568762 cites W2767768509 @default.
• W4280568762 cites W2774400393 @default.
• W4280568762 cites W2789412699 @default.
• W4280568762 cites W2791860635 @default.
• W4280568762 cites W2794284698 @default.
• W4280568762 cites W2891670030 @default.
• W4280568762 cites W2909836981 @default.
• W4280568762 cites W2917919815 @default.
• W4280568762 cites W2920167237 @default.
• W4280568762 cites W2948707395 @default.
• W4280568762 cites W2960128031 @default.
• W4280568762 cites W2975456977 @default.
• W4280568762 cites W3013194607 @default.
• W4280568762 cites W3018093016 @default.
• W4280568762 cites W3018608736 @default.
• W4280568762 cites W3022650582 @default.
• W4280568762 cites W3116521081 @default.
• W4280568762 cites W3197559541 @default.
• W4280568762 cites W3216747254 @default.
• W4280568762 doi "https://doi.org/10.3390/biomedicines10051113" @default.
• W4280568762 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/35625849" @default.
• W4280568762 hasPublicationYear "2022" @default.
• W4280568762 type Work @default.
• W4280568762 citedByCount "2" @default.
• W4280568762 countsByYear W42805687622022 @default.
• W4280568762 crossrefType "journal-article" @default.
• W4280568762 hasAuthorship W4280568762A5007122170 @default.
• W4280568762 hasAuthorship W4280568762A5024660659 @default.
• W4280568762 hasAuthorship W4280568762A5025050406 @default.
• W4280568762 hasAuthorship W4280568762A5037701924 @default.
• W4280568762 hasAuthorship W4280568762A5039429164 @default.
• W4280568762 hasAuthorship W4280568762A5048132059 @default.
• W4280568762 hasAuthorship W4280568762A5069015546 @default.
• W4280568762 hasAuthorship W4280568762A5075620151 @default.
• W4280568762 hasAuthorship W4280568762A5080390580 @default.
• W4280568762 hasAuthorship W4280568762A5086930411 @default.
• W4280568762 hasBestOaLocation W42805687621 @default.
• W4280568762 hasConcept C104317684 @default.
• W4280568762 hasConcept C121608353 @default.
• W4280568762 hasConcept C126322002 @default.
• W4280568762 hasConcept C127561419 @default.
• W4280568762 hasConcept C185592680 @default.
• W4280568762 hasConcept C203014093 @default.
• W4280568762 hasConcept C2777863537 @default.
• W4280568762 hasConcept C2779349466 @default.
• W4280568762 hasConcept C2780210213 @default.
• W4280568762 hasConcept C2780258809 @default.

• next