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茄病镰刀菌主要变应原肽IV-1可结合IgE,但不释放组胺。

Fusarium solani major allergen peptide IV-1 binds IgE but does not release histamine.

作者信息

Verma J, Sridhara S, Singh B P, Pasha S, Gangal S V, Arora N

机构信息

Allergy & Immunology Section, Centre for Biochemical Technology, Mall Road, Delhi, India.

出版信息

Clin Exp Allergy. 2001 Jun;31(6):920-7. doi: 10.1046/j.1365-2222.2001.01080.x.

Abstract

BACKGROUND

Fusarium solani (FS) is an important allergen source afflicting 4% of the nasobronchial allergy patients. Fus s I3596*, a 65 kDa major glycoprotein allergen of FS reacts with 95% fungus sensitive patients.

OBJECTIVES

To purify and characterize a potent peptide from Fus s I3596* which may be useful for therapeutic purposes.

METHODS

The 65 kDa protein was sequentially cleaved with trypsin and cyanogen bromide (CNBr). The cleaved products were purified on reverse phase high performance liquid chromatography (rpHPLC) column and functionally characterized by in vitro and in vivo methods for its IgE binding and histamine release.

RESULTS

The protein on cleavage showed 11 peaks (I to XI). Of these, peaks I, III, IV and V were highly allergenic as determined by IgE ELISA. These peaks were further purified and peptide IV-1 was most potent in comparison to other peptides by ELISA-inhibition. This peptide showed IgE binding but could not evoke intradermal response in Fusarium-sensitive patients. Heparinized blood challenged with peptide IV-1 does not release histamine. Preincubation of heparinized blood with peptide IV-1 and challenging with crude extract blocked histamine release in a dose dependent manner.

CONCLUSION

Peptide IV-1 binds to IgE but does not release histamine, demonstrating its potential use in therapy of Fusarium-allergic patients.

摘要

背景

茄病镰刀菌(FS)是一种重要的过敏原来源,折磨着4%的鼻支气管过敏患者。Fus s I3596*是FS的一种65 kDa主要糖蛋白过敏原,与95%的真菌敏感患者发生反应。

目的

从Fus s I3596*中纯化并鉴定一种可能用于治疗目的的有效肽。

方法

用胰蛋白酶和溴化氰(CNBr)依次切割65 kDa蛋白。切割产物在反相高效液相色谱(rpHPLC)柱上纯化,并通过体外和体内方法对其IgE结合和组胺释放进行功能鉴定。

结果

切割后的蛋白显示出11个峰(I至XI)。其中,通过IgE ELISA测定,峰I、III、IV和V具有高度致敏性。这些峰进一步纯化,与其他肽相比,肽IV-1通过ELISA抑制法最为有效。该肽显示出IgE结合,但在镰刀菌敏感患者中不能引起皮内反应。用肽IV-1攻击肝素化血液不会释放组胺。将肝素化血液与肽IV-1预孵育,然后用粗提取物攻击,可剂量依赖性地阻断组胺释放。

结论

肽IV-1与IgE结合但不释放组胺,证明其在治疗镰刀菌过敏患者中的潜在用途。

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