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Novel System for the Stabilization and Delivery of Proteins to the Insect Hemocoel through Conjugation with Aliphatic Polyethylene Glycol.

机译:通过与脂肪族聚乙二醇共轭,将蛋白质稳定化并传递至昆虫血丝的新型系统。

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摘要

Despite the numerous insecticidal proteins identified, there are few commercially-successful protein insecticides. Oral delivery of proteins is difficult due to their degradation by digestive endo- and exo-peptidases and their limited movement across the gut epithelium. PEGylation, the process of covalently attaching polyethylene glycol (PEG) polymer chains to another molecule, has been used in the pharmaceutical industry for decades to deliver proteins across the digestive system of humans. In this study, two PEGylated insulins and a PEGylated insecticidal decapeptide, Trypsin Modulating Oostatic Factor (TMOF), were created to determine if PEGylation could reduce the rate of degradation and enhance the accumulation of the parent compounds from the diet or cuticle in the insect hemocoel. The chemistry for the synthesis of monodispersed aliphatic TMOF-K-PEG7P, polydispersed aliphatic PEG350-insulin and monodispersed aliphatic PEG333-insulin are described herein. The PEGylation of insulin yields a 6.7 and 7.3 fold increase in appearance of insulin species in the hemolymph of Heliothis virescens larvae after feeding for the PEG350 and PEG333 chemistries, respectively. When insulin is topically applied to the dorsum of H. virescens, no insulin is found in the hemolymph. However, after topical application of the PEGylated insulins, insulin species were detected in the hemolymph. After injections of insulin into the hemocoel of 4th stadium H. virescens, insulin is completely cleared from the hemolymph in 120 minutes. In comparison, when PEG350-insulin and PEG333-insulin are injected into the hemocoel, insulin species were still present in the hemolymph 300 and 240 minutes after injection, respectively, translating to a 3.3 and 2.7 fold increases in the length of time insulin remains in the hemolymph after injection. Conjugation of TMOF to polyethylene glycol increased its insecticidal effects against several insect species. For example, the addition of lysine to TMOF reduced its per os activity relative to the parent TMOF, but conjugation of TMOF-K with methyl(ethyleneglycol)7-O-propionyl increased it toxicity 5.8 and 10.1 fold above that of TMOF and TMOF-K for Aedes aegypti. However, unlike the PEGylated insulin species, no TMOF, TMOF-K, or PEGylated TMOF-K was detected in the hemolymph after topical application to the cuticle.
机译:尽管已鉴定出许多杀虫蛋白,但很少有商业上成功的杀虫蛋白。由于蛋白质被消化内肽酶和外肽酶降解,并且它们在肠道上皮细胞中的运动受到限制,因此很难口服蛋白质。聚乙二醇化是将聚乙二醇(PEG)聚合物链共价连接到另一个分子的过程,几十年来一直用于制药行业,以在整个人体的消化系统中传递蛋白质。在这项研究中,创建了两种聚乙二醇化的胰岛素和一个聚乙二醇化的杀虫十肽,胰蛋白酶调节静息因子(TMOF),以确定聚乙二醇化是否可以降低降解速率并增强昆虫血中饮食或表皮中母体化合物的积累。 。本文描述了用于合成单分散的脂族TMOF-K-PEG 7 P,多分散的脂族PEG350-胰岛素和单分散的脂族PEG333-胰岛素的化学。分别饲喂PEG350和PEG333化学物质后, Heliothis virescens 幼虫的血淋巴中,胰岛素的PEG化作用使胰岛素种类的出现分别增加了6.7和7.3倍。将胰岛素局部应用于 H的背部时。病毒,在血淋巴中未发现胰岛素。然而,在局部应用聚乙二醇化胰岛素后,在血淋巴中检测到胰岛素种类。向第四体育场H的血细胞注射胰岛素后。在120分钟内,胰岛素将从静脉血淋巴中完全清除。相比之下,当将PEG350胰岛素和PEG333胰岛素注射到血细胞中时,注射后300和240分钟,血淋巴中仍分别存在胰岛素,这意味着胰岛素在体内的停留时间增加了3.3倍和2.7倍。注射后的血淋巴。 TMOF与聚乙二醇的缀合增加了其对几种昆虫的杀虫作用。例如,相对于母体TMOF,向TMOF中添加赖氨酸会降低其 per os 活性,但TMOF-K与甲基(乙二醇) 7 -O-丙酰的缀合将其对埃及伊蚊的毒性提高到TMOF和TMOF-K的5.8和10.1倍。但是,与PEG化的胰岛素种类不同,在其中未检测到TMOF,TMOF-K或PEG化的TMOF-K。局部应用到角质层后有血淋巴。

著录项

  • 作者

    Jeffers, Laura Ann.;

  • 作者单位

    North Carolina State University.;

  • 授予单位 North Carolina State University.;
  • 学科 Biology Entomology.;Biology Physiology.;Chemistry Biochemistry.
  • 学位 Ph.D.
  • 年度 2012
  • 页码 152 p.
  • 总页数 152
  • 原文格式 PDF
  • 正文语种 eng
  • 中图分类
  • 关键词

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