蛋白酶稳定的DARPins作为有前途的口服治疗药物。

IF 2.6 4区 生物学 Q3 BIOCHEMISTRY & MOLECULAR BIOLOGY Protein Engineering Design & Selection Pub Date : 2021-02-15 DOI:10.1093/protein/gzab028
Rudo A Simeon, Yu Zeng, Vikas Chonira, Andrea Martinez Aguirre, Mauricio Lasagna, Marko Baloh, Joseph A Sorg, Cecilia Tommos, Zhilei Chen
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引用次数: 0

摘要

艰难梭菌是一种肠道细菌,其外毒素TcdA和TcdB使宿主细胞内的小gtp酶失活,导致血性腹泻。在之前的工作中,我们的团队设计了一组有效的tcb中和设计的锚蛋白重复蛋白(DARPin)作为口服治疗艰难梭菌感染的药物。然而,所有这些darpin都很容易被肠道蛋白酶消化,如胰蛋白酶和凝乳胰蛋白酶。对蛋白质序列的密切评估显示,在DARPin支架中有大量带正电荷和芳香残基。在本研究中,我们通过蛋白工程显著提高了其中一种DARPins 1.4E的蛋白酶稳定性。与1.4E不同,在胰蛋白酶(1 mg/ml)或凝乳胰蛋白酶(0.5 mg/ml)孵育1小时后,其抗tcdb EC50增加了83倍,而最佳子代t10 -2和t10b在PBS中表现出与亲本相似的抗tcdb效力,无论蛋白酶处理如何。T10-2和T10b具有优异的蛋白酶稳定性,这是由于除直接参与目标结合的残基外,几乎去除了所有带正电的残基和芳香残基。此外,我们发现T10-2在离体盲肠液中仍具有明显的毒素中和能力,并且在口服给药的小鼠粪便样本中很容易检测到T10-2。T10-2和T10b都具有很高的热稳定性和化学稳定性,并且可以在大肠杆菌中非常有效地表达(摇瓶中100 mg/l)。我们相信,T10-2和T10b除了作为口服治疗艰难梭菌感染的潜力外,还可以作为具有优越蛋白酶稳定性的新一代DARPin支架。
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Protease-stable DARPins as promising oral therapeutics.

Clostridioides difficile is an enteric bacterium whose exotoxins, TcdA and TcdB, inactivate small GTPases within the host cells, leading to bloody diarrhea. In prior work, our group engineered a panel of potent TcdB-neutralizing designed ankyrin repeat proteins (DARPin) as oral therapeutics against C. difficile infection. However, all these DARPins are highly susceptible to digestion by gut-resident proteases, i.e. trypsin and chymotrypsin. Close evaluation of the protein sequence revealed a large abundance of positively charged and aromatic residues in the DARPin scaffold. In this study, we significantly improved the protease stability of one of the DARPins, 1.4E, via protein engineering. Unlike 1.4E, whose anti-TcdB EC50 increased >83-fold after 1-hour incubation with trypsin (1 mg/ml) or chymotrypsin (0.5 mg/ml), the best progenies-T10-2 and T10b-exhibit similar anti-TcdB potency as their parent in PBS regardless of protease treatment. The superior protease stability of T10-2 and T10b is attributed to the removal of nearly all positively charged and aromatic residues except those directly engaged in target binding. Furthermore, T10-2 was found to retain significant toxin-neutralization ability in ex vivo cecum fluid and can be easily detected in mouse fecal samples upon oral administration. Both T10-2 and T10b enjoy a high thermo- and chemo-stability and can be expressed very efficiently in Escherichia coli (>100 mg/l in shaker flasks). We believe that, in additional to their potential as oral therapeutics against C. difficile infection, T10-2 and T10b can also serve as a new generation DARPin scaffold with superior protease stability.

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来源期刊
Protein Engineering Design & Selection
Protein Engineering Design & Selection 生物-生化与分子生物学
CiteScore
3.30
自引率
4.20%
发文量
14
审稿时长
6-12 weeks
期刊介绍: Protein Engineering, Design and Selection (PEDS) publishes high-quality research papers and review articles relevant to the engineering, design and selection of proteins for use in biotechnology and therapy, and for understanding the fundamental link between protein sequence, structure, dynamics, function, and evolution.
期刊最新文献
Optimized single-cell gates for yeast display screening. TIMED-Design: flexible and accessible protein sequence design with convolutional neural networks. Correction to: De novo design of a polycarbonate hydrolase. Interactive computational and experimental approaches improve the sensitivity of periplasmic binding protein-based nicotine biosensors for measurements in biofluids. Design of functional intrinsically disordered proteins.
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