2005
DOI: 10.1242/jeb.01897
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Actin cytoskeleton of rabbit intestinal cells is a target for potent marine phycotoxins

Abstract: Biotoxins produced by harmful marine microalgae (phycotoxins) can be accumulated into seafood, representing a great risk for public health. Some of these phycotoxins are responsible for a variety of gastrointestinal disturbances; however, the relationship between their mechanism of action and toxicity in intestinal cells is still unknown. The actin cytoskeleton is an important and highly complicated structure in intestinal cells, and on that basis our aim has been to investigate the effect of representative ph… Show more

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Cited by 70 publications
(51 citation statements)
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“…Pectenotoxins disrupt actin in the cytoskeleton, and may cause cell cycle arrest and cell death (Spector et al, 1999;Ares et al, 2005;Anonymous, 2009). Thus, accumulation of both toxin groups is undesirable at best.…”
Section: Accumulationmentioning
confidence: 99%
“…Pectenotoxins disrupt actin in the cytoskeleton, and may cause cell cycle arrest and cell death (Spector et al, 1999;Ares et al, 2005;Anonymous, 2009). Thus, accumulation of both toxin groups is undesirable at best.…”
Section: Accumulationmentioning
confidence: 99%
“…Hepatic-enteric cell models are particularly useful in studying the effect of hepatotoxins and DSP-related toxins (Louzao et al, 2003;Ares et al, 2005;. At this cellular level, primary cultured cells isolated from rodents' liver are common in vitro models; also immortalized hepatocytes offer a renewable source of hepatocytes.…”
Section: Introductionmentioning
confidence: 99%
“…Studying the effect of this toxin on hepatic cells is thus fundamental to a better understanding of the pharmacokinetics and pharmacodynamics of MeOk (Gomez-Lechon et al, 2004). In addition, hepatic cells have some characteristics very appropriate to our study, such as glucose uptake and the marked actin cytoskeletal structure (Oda et al, 2008).Hepatic-enteric cell models are particularly useful in studying the effect of hepatotoxins and DSP-related toxins (Louzao et al, 2003;Ares et al, 2005;. At this cellular level, primary cultured cells isolated from rodents' liver are common in vitro models; also immortalized hepatocytes offer a renewable source of hepatocytes.…”
mentioning
confidence: 99%
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“…In culture, cancerous and undifferentiated mammalian cells have weaker actin cytoskeletons than normal cells [38,39]. Cellular F-actin and monomeric G-actin (depolymerized F-actin) levels have been used as biomarkers of bladder cancer risk, breast cancer, prostate adenocarcinoma and cholestasis [37,[40][41][42], hepatotoxicity caused by pectenotoxins [43][44][45][46], and nanoparticle-induced toxicity [47]. Moreover, actin remodeling has been contemplated as a potential target for cancer drug development [48].…”
Section: Toxicant-induced Actin Cytosketal Modulation In Embryosmentioning
confidence: 99%