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乳酸乳球菌 NZ9000 诱导的生物活性单链胰岛素类似物的尼辛诱导分泌。

Nisin-inducible secretion of a biologically active single-chain insulin analog by Lactococcus lactis NZ9000.

机构信息

Department of Bioengineering, University of Pennsylvania, Philadelphia, Pennsylvania 19104-6321, USA.

出版信息

Biotechnol Bioeng. 2011 Aug;108(8):1987-96. doi: 10.1002/bit.23130. Epub 2011 Mar 29.

Abstract

Oral delivery of insulin to diabetic patients is highly desirable because it would be non-invasive and more closely mimic normal physiology, but this route of administration typically results in low bioavailability due to low pH and enzymatic degradation along the gastrointestinal tract. To explore an alternative approach that may mitigate these obstacles and also facilitate local synthesis of new therapeutic protein molecules in the small intestine, we engineered the food-grade bacterium Lactococcus lactis (NZ9000) for nisin-inducible expression and secretion of a bioactive single-chain insulin (SCI) analog, SCI-57. We show that the addition of nisin during early-log phase has a modest inhibitory effect on cell growth but induction during mid-log phase has a negligible impact on proliferation, suggesting a tradeoff between cell growth rate and duration of induction. We find that a signal peptide such as usp45 is necessary for secretion of SCI-57 into the medium; furthermore, we demonstrate that this secreted SCI-57 is biologically active, as assessed by the ability of conditioned L. lactis medium to stimulate Akt signaling in differentiated 3T3-L1 adipocytes. Finally, we show that the biological activity of SCI-57 was enhanced by near-neutral or slightly alkaline pH during induction, which is comparable to the pH in the small intestine, and by removal of a C-terminal purification tag. This study demonstrates that food-grade bacteria can be engineered to secrete bioactive insulin analogs and opens up the possibility of oral insulin delivery using live microorganisms.

摘要

口服胰岛素给糖尿病患者是非常理想的,因为它是非侵入性的,更能模拟正常的生理过程,但这种给药途径通常由于胃肠道内的低 pH 值和酶降解而导致生物利用度低。为了探索一种替代方法,可能减轻这些障碍,并促进在小肠中局部合成新的治疗性蛋白质分子,我们设计了食品级细菌乳球菌(NZ9000),用于诱导表达和分泌生物活性的单链胰岛素(SCI)类似物,SCI-57。我们表明,在对数早期添加乳链菌素对细胞生长有适度的抑制作用,但在对数中期诱导对增殖几乎没有影响,这表明细胞生长速率和诱导持续时间之间存在权衡。我们发现,诸如usp45 等信号肽对于 SCI-57 分泌到培养基中是必需的;此外,我们证明,这种分泌的 SCI-57 是具有生物活性的,因为条件培养基能够刺激分化的 3T3-L1 脂肪细胞中的 Akt 信号。最后,我们表明,在诱导过程中接近中性或略碱性 pH 值增强了 SCI-57 的生物活性,这与小肠内的 pH 值相当,并且通过去除 C 末端纯化标签也增强了生物活性。这项研究表明,食品级细菌可以被工程化以分泌生物活性的胰岛素类似物,并为使用活微生物进行口服胰岛素递送开辟了可能性。

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