1996
DOI: 10.1016/0009-2797(96)03698-8
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Signal transduction mechanism in response to aflatoxin B1 exposure: protein kinase C activity

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Cited by 12 publications
(8 citation statements)
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“…To further test the hypothesis that aflatoxins can activate PKC activity, we utilized a Förster resonance energy transfer (FRET)-based PKC construct, CKAR 48 49 . Because AFs activate PKC in a variety of cell types 29 30 31 50 , we hypothesized that the mechanism of activation was not cell-type dependent. As primary sinonasal ALIs are very difficult to transfect, even with viral systems, CKAR was transfected into A549 cells, a commonly used lung epithelial cell line.…”
Section: Resultsmentioning
confidence: 99%
See 1 more Smart Citation
“…To further test the hypothesis that aflatoxins can activate PKC activity, we utilized a Förster resonance energy transfer (FRET)-based PKC construct, CKAR 48 49 . Because AFs activate PKC in a variety of cell types 29 30 31 50 , we hypothesized that the mechanism of activation was not cell-type dependent. As primary sinonasal ALIs are very difficult to transfect, even with viral systems, CKAR was transfected into A549 cells, a commonly used lung epithelial cell line.…”
Section: Resultsmentioning
confidence: 99%
“…There is some evidence that airway cells can activate aflatoxins in vitro 4 25 and in vivo 26 27 28 , though the link between aflatoxin exposure and human lung cancer is unclear. However, aflatoxins can increase protein kinase C (PKC) activity in some cell lines in vitro 29 30 31 . Because PKC can decrease CBF 32 33 through phosphorylation of ciliary proteins 32 33 , we hypothesized that aflatoxins may have acute effects on MCC that contribute to A. flavus pathogenesis.…”
mentioning
confidence: 99%
“…Previous studies demonstrated that protein biosynthesis is weakened due to the formation of AFB 1 -DNA adducts. In addition, AFB 1 could change the activity of enzymes such as cyclic nucleotide phosphodiesterase, protein kinase, and Ca 2+ -ATPase, alter hepatic protein phosphorylation ( Mistry et al, 1996 ; Ricordy et al, 2002 ), and causes p53 mutation which may develop carcinogenesis in experimental animals ( Aguilar et al, 1994 ). Similarly, our data showed that Nrf2 mRNA and protein expression level significantly down-regulated in AFB 1 -fed group.…”
Section: Discussionmentioning
confidence: 99%
“…FB1 induces protein kinase C translocation via direct interaction with diacylglycerol site that also binds phorbol esters. Because phorbol esters are well-known tumor promoters, it is a more plausible cellular mechanism to explain the carcinogenicity of FB1 [46,47]. Other studies suggested that the concept that FB1-induced mitogenesis might be the mechanism of carcinogenesis and that the primary target organs are the kidney and liver [48].…”
Section: The Mechanism Of Mycotoxic Carcinogenesismentioning
confidence: 99%