Li Jianxu, Wu Hongbing, Hong Jing, Xu Xueqing, Yang Hailong, Wu Bingxian, Wang Yipeng, Zhu Jianhua, Lai Ren, Jiang Xinguo, Lin Donghai, Prescott Mark C, Rees Huw H
Biotoxin Units of Key Laboratory of Animal Models and Human Disease Mechanisms, Kunming Institute of Zoology, Chinese Academy of Sciences, Kunming Yunnan, China.
PLoS One. 2008 Jun 11;3(6):e2381. doi: 10.1371/journal.pone.0002381.
Lectins are sugar-binding proteins that specifically recognize sugar complexes. Based on the specificity of protein-sugar interactions, different lectins could be used as carrier molecules to target drugs specifically to different cells which express different glycan arrays. In spite of lectin's interesting biological potential for drug targeting and delivery, a potential disadvantage of natural lectins may be large size molecules that results in immunogenicity and toxicity. Smaller peptides which can mimic the function of lectins are promising candidates for drug targeting.
Small peptide with lectin-like behavior was screened from amphibian skin secretions and its structure and function were studied by NMR, NMR-titration, SPR and mutant analysis. A lectin-like peptide named odorranalectin was identified from skin secretions of Odorrana grahami. It was composed of 17 aa with a sequence of YASPKCFRYPNGVLACT. L-fucose could specifically inhibit the haemagglutination induced by odorranalectin. (125)I-odorranalectin was stable in mice plasma. In experimental mouse models, odorranalectin was proved to mainly conjugate to liver, spleen and lung after i.v. administration. Odorranalectin showed extremely low toxicity and immunogenicity in mice. The small size and single disulfide bridge of odorranalectin make it easy to manipulate for developing as a drug targeting system. The cyclic peptide of odorranalectin disclosed by solution NMR study adopts a beta-turn conformation stabilized by one intramolecular disulfide bond between Cys6-Cys16 and three hydrogen bonds between Phe7-Ala15, Tyr9-Val13, Tyr9-Gly12. Residues K5, C6, F7, C16 and T17 consist of the binding site of L-fucose on odorranalectin determined by NMR titration and mutant analysis. The structure of odorranalectin in bound form is more stable than in free form.
These findings identify the smallest lectin so far, and show the application potential of odorranalectin for drug delivery and targeting. It also disclosed a new strategy of amphibian anti-infection.
凝集素是一类能特异性识别糖复合物的糖结合蛋白。基于蛋白质 - 糖相互作用的特异性,不同的凝集素可作为载体分子,将药物特异性地靶向到表达不同聚糖阵列的不同细胞。尽管凝集素在药物靶向和递送方面具有有趣的生物学潜力,但天然凝集素的一个潜在缺点可能是其大分子尺寸导致免疫原性和毒性。能够模拟凝集素功能的较小肽段是药物靶向的有前景的候选物。
从两栖动物皮肤分泌物中筛选出具有凝集素样行为的小肽,并通过核磁共振(NMR)、NMR滴定、表面等离子体共振(SPR)和突变分析研究了其结构和功能。从滇蛙皮肤分泌物中鉴定出一种名为滇蛙凝集素的凝集素样肽。它由17个氨基酸组成,序列为YASPKCFRYPNGVLACT。L - 岩藻糖能特异性抑制滇蛙凝集素诱导的血细胞凝集。碘 - 125标记的滇蛙凝集素在小鼠血浆中稳定。在实验小鼠模型中,静脉注射后,滇蛙凝集素被证明主要与肝脏、脾脏和肺结合。滇蛙凝集素在小鼠中显示出极低的毒性和免疫原性。滇蛙凝集素的小尺寸和单个二硫键使其易于操作,可用于开发药物靶向系统。溶液NMR研究揭示的滇蛙凝集素环肽采用β - 转角构象,由Cys6 - Cys16之间的一个分子内二硫键以及Phe7 - Ala15、Tyr9 - Val13、Tyr9 - Gly12之间的三个氢键稳定。通过NMR滴定和突变分析确定,残基K5、C6、F7、C16和T17构成滇蛙凝集素上L - 岩藻糖的结合位点。结合形式的滇蛙凝集素结构比游离形式更稳定。
这些发现确定了迄今为止最小的凝集素,并展示了滇蛙凝集素在药物递送和靶向方面的应用潜力。它还揭示了两栖动物抗感染的新策略。
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