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P-glycoprotein expression in Perna viridis after exposure to Prorocentrum lima, a dinoflagellate producing DSP toxins

机译:暴露于利罗氏原鞭毛虫(一种鞭毛产生DSP毒素的利马原虫)后,Perna viridis中的P糖蛋白表达

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Bivalves naturally exposed to toxic algae have mechanisms to prevent from harmful effects of diarrhetic shellfish poisoning (DSP) toxins. However, quite few studies have examined the mechanisms associated, and the information currently available is still insufficient. Multixenobiotic resistance (MXR) is ubiquitous in aquatic invertebrates and plays an important role in defense against xenobiotics. Here, to explore the roles of P-glycoprotein (P-gp) in the DSP toxins resistance in shellfish, complete cDNA of P-gp gene in the mussel Perna viridis was cloned and analyzed. The accumulation of okadaic acid (OA), a main component of DSP toxins, MXR activity and expression of P-gp in gills of P. viridis were detected after exposure to Prorocentrum lima, a dinoflagellate producing DSP toxins in the presence or absence of P-gp inhibitors PGP-4008, verapamil (VER) and cyclosporin A (CsA). The mussel P. viridis P-gp closely matches MDR/P-gp/ABCB protein from various organisms, having a typical sequence organization as full transporters from the ABCB family. After exposure to P. lima, OA accumulation, MXR activity and P-gp expression significantly increased in gills of P. viridis. The addition of P-gp-specific inhibitors PGP-4008 and VER decreased MXR activity induced by P. lima, but had no effect on the OA accumulation in gills of P. viridis. However, CsA, a broad-spectrum inhibitor of ABC transporter not only decreased MXR activity, but also increased OA accumulation in gills of P. viridis. Together with the ubiquitous presence of other ABC transporters such as MRP/ABCC in bivalves and potential compensatory mechanism in P-gp and MRP-mediated resistance, we speculated that besides P-gp, other ABC transporters, especially MRP might be involved in the resistance mechanisms to DSP toxins
机译:天然暴露于有毒藻类的双壳类动物具有防止腹泻性贝类中毒(DSP)毒素的有害影响的机制。但是,很少有研究检查了相关的机制,并且目前可用的信息仍然不足。多异生物抗性(MXR)在水生无脊椎动物中普遍存在,并且在防御异生物的过程中起着重要作用。在这里,为探讨P-糖蛋白(P-gp)在贝类DSP毒素抗性中的作用,克隆并分析了贻贝贻贝中P-gp基因的完整cDNA。冈田酸(OA)的积累,DSP毒素的主要成分,MXR活性和P.gp在绿色假单胞菌g中的暴露在暴露于利罗菌原(Prorocentrum lima)后即被检出,后者是在P的存在或不存在下会产生DSP的鞭毛的毒素。 -gp抑制剂PGP-4008,维拉帕米(VER)和环孢菌素A(CsA)。贻贝贻贝P-gp与来自各种生物体的MDR / P-gp / ABCB蛋白紧密匹配,具有典型的序列组织作为ABCB家族的完整转运蛋白。暴露于利马假单胞菌后,绿色假单胞菌g中的OA积累,MXR活性和P-gp表达显着增加。 P-gp特异性抑制剂PGP-4008和VER的添加降低了利马毕赤酵母诱导的MXR活性,但对绿色假单胞菌g中的OA积累没有影响。然而,CsA,一种广谱的ABC转运蛋白抑制剂,不仅降低了MXR活性,而且还增加了绿色假单胞菌g中的OA积累。结合其他ABC转运蛋白(如MRP / ABCC)在双壳类动物中的普遍存在以及P-gp和MRP介导的抗药性的潜在补偿机制,我们推测除P-gp外,其他ABC转运蛋白,尤其是MRP可能参与了抗药性DSP毒素的机制

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