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一种工程合成杀伤性抗独特型抗体片段对实验性黏膜和全身性念珠菌病的治疗活性

Therapeutic activity of an engineered synthetic killer antiidiotypic antibody fragment against experimental mucosal and systemic candidiasis.

作者信息

Polonelli Luciano, Magliani Walter, Conti Stefania, Bracci Luisa, Lozzi Luisa, Neri Paolo, Adriani Daniela, De Bernardis Flavia, Cassone Antonio

机构信息

Sezione di Microbiologia, Dipartimento di Patologia e Medicina di Laboratorio, Università degli Studi di Parma, Parma, Italy.

出版信息

Infect Immun. 2003 Nov;71(11):6205-12. doi: 10.1128/IAI.71.11.6205-6212.2003.

Abstract

Peptides derived from the sequence of a single-chain, recombinant, antiidiotypic antibody (IdAb; KT-scFv) acting as a functional internal image of a microbicidal, wide-spectrum yeast killer toxin (KT) were synthesized and studied for their antimicrobial activity by using the KT-susceptible Candida albicans as model organism. A decapeptide containing the first three amino acids (SAS) of the light chain CDR1 was selected and optimized by alanine replacement of a single residue. This peptide exerted a strong candidacidal activity in vitro, with a 50% inhibitory concentration of 0.056 microM, and was therefore designated killer peptide (KP). Its activity was neutralized by laminarin, a beta1-3 glucan molecule, but not by pustulan, a beta1-6 glucan molecule. KP also competed with the binding of a KT-like monoclonal IdAb to germinating cells of the fungus. In a rat model of vaginal candidiasis, local, postchallenge administration of KP was efficacious in rapidly abating infections caused by fluconazole-susceptible or -resistant C. albicans strains. In systemic infection of BALB/c or SCID mice preinfected intravenously with a lethal fungal load, KP caused a highly significant prolongation of the median survival time, with >80% of the animals still surviving after >60 days, whereas >90% of control mice died within 3 to 5 days. KP is therefore the first engineered peptide derived from a recombinant IdAb retaining KT microbicidal activity, probably through the interaction with the beta-glucan KT receptor on target microbial cells.

摘要

合成了源自单链重组抗独特型抗体(IdAb;KT-scFv)序列的肽段,该抗体作为一种杀微生物的广谱酵母杀伤毒素(KT)的功能性内影像,并以对KT敏感的白色念珠菌为模式生物研究了它们的抗菌活性。选择了包含轻链互补决定区1(CDR1)前三个氨基酸(SAS)的十肽,并通过丙氨酸取代单个残基进行优化。该肽在体外具有很强的杀念珠菌活性,50%抑制浓度为0.056微摩尔,因此被命名为杀伤肽(KP)。其活性被β1-3葡聚糖分子海带多糖中和,但未被β1-6葡聚糖分子 pustulan 中和。KP 还与一种类似 KT 的单克隆 IdAb 与真菌萌发细胞的结合竞争。在阴道念珠菌病大鼠模型中,攻击后局部给予 KP 可有效快速减轻由氟康唑敏感或耐药的白色念珠菌菌株引起的感染。在静脉内预先感染致死性真菌负荷的 BALB/c 或 SCID 小鼠的全身感染中,KP 导致中位生存时间显著延长,超过80%的动物在60多天后仍存活,而超过90%的对照小鼠在3至5天内死亡。因此,KP 是第一个源自重组 IdAb 的工程肽,可能通过与靶微生物细胞上的β-葡聚糖 KT 受体相互作用而保留 KT 杀微生物活性。

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