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天然响尾蛇毒素在脂质体中的包封:一种生产抗蛇毒血清和针对巴西矛头蝮蛇毒液进行疫苗接种的安全方法。

Encapsulation of native crotoxin in liposomes: a safe approach for the production of antivenom and vaccination against Crotalus durissus terrificus venom.

作者信息

Freitas T V, Frézard F

机构信息

Centro de Pesquisa e Desenvolvimento, Fundaçào Ezequiel Dias (FUNED), Belo Horizonte, Minas Gerais, Brazil.

出版信息

Toxicon. 1997 Jan;35(1):91-100. doi: 10.1016/s0041-0101(96)00061-x.

Abstract

Crotoxin, the neurotoxic component of Crotalus durissus terrificus (Cdt) venom that displays phospholipase A2 activity, was successfully encapsulated into dehydration-rehydration vesicles (DRV/crotoxin) and reverse-phase evaporation vesicles (REV/crotoxin) made from sphingomyelin and cholesterol. The encapsulation efficiency of native crotoxin was higher in DRV/crotoxin than in REV/crotoxin. DRV/crotoxin was not toxic when i.v. inoculated in mice at a dose of crotoxin as high as 91 times its L.D50 or when s.c. inoculated at 42 times its LD50. On the other hand, crotoxin released from DRV/crotoxin retained its original toxicity. REV/crotoxin was found to be at least 1.9 times more toxic than DRV/crotoxin. The fact that DRV/crotoxin retained crotoxin more efficiently than REV/crotoxin may account for the difference in acute toxicity between the two preparations. DRV/crotoxin, when s.c. inoculated in mice, induced anti-crotoxin antibodies that protected animals against the lethal effect of Cdt venom. Following immunization with three doses of DRV/crotoxin (3 x 20 micrograms of crotoxin/mouse) and challenge with 8 x LD50 of Cdt venom, 75% of mice were protected. The DRV/crotoxin preparation was compared to crotoxin emulsified in Freund's adjuvant (FCA/crotoxin). DRV/crotoxin was found to be less toxic than FCA/crotoxin, and to induce lower levels of anti-crotoxin antibodies but similar levels of protection when inoculated at high doses (20 or 70 micrograms crotoxin/mouse). When DRV/crotoxin was adsorbed to alum at the time of immunization, it induced antibody and protection levels comparable to those produced by FCA/crotoxin.

摘要

响尾蛇毒素是南美巨蝮(Cdt)毒液中的神经毒性成分,具有磷脂酶A2活性,已成功包封于由鞘磷脂和胆固醇制成的脱水-复水囊泡(DRV/响尾蛇毒素)和反相蒸发囊泡(REV/响尾蛇毒素)中。天然响尾蛇毒素在DRV/响尾蛇毒素中的包封效率高于REV/响尾蛇毒素。当以高达其半数致死剂量(LD50)91倍的响尾蛇毒素剂量静脉注射给小鼠时,DRV/响尾蛇毒素无毒;当以其LD50的42倍剂量皮下注射时,同样无毒。另一方面,从DRV/响尾蛇毒素中释放的响尾蛇毒素保留了其原始毒性。发现REV/响尾蛇毒素的毒性至少比DRV/响尾蛇毒素高1.9倍。DRV/响尾蛇毒素比REV/响尾蛇毒素更有效地保留响尾蛇毒素这一事实,可能解释了这两种制剂在急性毒性上的差异。当皮下注射给小鼠时,DRV/响尾蛇毒素诱导产生抗响尾蛇毒素抗体,可保护动物免受Cdt毒液的致死作用。用三剂DRV/响尾蛇毒素(每只小鼠3×20微克响尾蛇毒素)免疫并以8×LD50的Cdt毒液攻击后,75%的小鼠受到保护。将DRV/响尾蛇毒素制剂与弗氏佐剂乳化的响尾蛇毒素(FCA/响尾蛇毒素)进行比较。发现DRV/响尾蛇毒素的毒性低于FCA/响尾蛇毒素,诱导产生的抗响尾蛇毒素抗体水平较低,但在高剂量(每只小鼠20或70微克响尾蛇毒素)接种时,保护水平相似。当在免疫时将DRV/响尾蛇毒素吸附到明矾上时,它诱导产生的抗体和保护水平与FCA/响尾蛇毒素产生的相当。

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