Molecular mechanisms underlying the interaction of motuporin and microcystins with type-1 and type-2A protein phosphatases

Craig, Marcia; Luu, Hue Anh; McCready, Tara; Williams, David E.; Andersen, Raymond J.; Holmes, Charles F.B.

doi:10.1139/o96-061

Cited by 152 publications

(132 citation statements)

References 30 publications

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“…Although motuporin contains valine instead of the arginine in nodularin, these compounds are equipotent inhibitors of PP1 and PP2A (Craig et al 1996). The results are consistent with the report that the arginine residue in microcystin-LR does not significantly contribute to biological activity, based on a comparison of enzyme inhibition and receptor binding activity ).…”

Section: Nodularinsupporting

confidence: 90%

See 1 more Smart Citation

Developmental Biology of Neoplastic Growth

Macieira‐Coelho¹

2005

Progress in Molecular and Subcellular Biology

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Section: Nodularinsupporting

confidence: 90%

“…Sponges of the order Haplosclerida often contain 3-alkylpyridinium salts (Andersen et al 1996;Sep i 2000), some of which were reported to be toxic to mammals. The first example of this class is halitoxin (29) isolated from Haliclona spp.…”

Section: Polyalkylpyridiniumsmentioning

confidence: 99%

Developmental Biology of Neoplastic Growth

Macieira‐Coelho¹

2005

Progress in Molecular and Subcellular Biology

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“…Second, part of the MC-LR may covalently bind with protein phosphatases in liver and then released gradually over time. Covalent binding of MCs with protein phosphatases reduces extractability of microcystins (Craig et al 1996), which could result in an underestimation of the amount of toxin really present into the liver (Malbrouck et al 2004). Although the mechanism of sustainedrelease behavior of MC-LR is not well studied so far, the binding form and subsequent release may account for the fluctuation of MC-LR detected in the rat liver during the experimental process.…”

Section: Fig 2 Esi Lc/ms/ms Analysis Of Mc-lr and Its Two Metabolitementioning

confidence: 99%

Quantitatively evaluating detoxification of the hepatotoxic microcystin-LR through the glutathione (GSH) pathway in SD rats

Guo

Chen

et al. 2015

Environ Sci Pollut Res

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Glutathione (GSH) plays crucial roles in antioxidant defense and detoxification metabolism of microcystin-LR (MC-LR). However, the detoxification process of MC-LR in mammals remains largely unknown. This paper, for the first time, quantitatively analyzes MC-LR and its GSH pathway metabolites (MC-LR-GSH and MC-LR-Cys) in the liver of Sprague-Dawley (SD) rat after MC-LR exposure. Rats received intraperitoneal (i.p.) injection of 0.25 and 0.5 lethal dose 50 (LD 50 ) of MC-LR with or without pretreatment of buthionine-(S,R)-sulfoximine (BSO), an inhibitor of GSH synthesis. The contents of MC-LR-GSH were relatively low during the experiment; however, the ratio of MC-LR-Cys to MC-LR reached as high as 6.65 in 0.5 LD 50 group. These results demonstrated that MC-LR-GSH could be converted to MC-LR-Cys efficiently, and this metabolic rule was in agreement with the data of aquatic animals previously reported. MC-LR contents were much higher in BSO+MC-LRtreated groups than in the single MC-LR-treated groups. Moreover, the ratio of MC-LR-Cys to MC-LR decreased significantly after BSO pretreatment, suggesting that the depletion of GSH induced by BSO reduced the detoxification of MCs. Moreover, MC-LR remarkably induced liver damage, and the effects were more pronounced in BSO pretreatment groups. In conclusion, this study verifies the role of GSH in the detoxification of MC-LR and furthers our understanding of the biochemical mechanism for SD rats to counteract toxic cyanobacteria.

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“…Indeed, MCs can covalently bind to various proteins (Craig et al, 1996;Gehringer et al, 2004). However, our investigation of the accumulation of MCs in these two gastropods used ELISA methods, which detects only free forms of MCs (Hastie et al, 2005;Maynes et al, 2006).…”

Section: Potential Risk To Human Healthmentioning

confidence: 99%