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脂肪酰化增强了胱氨酸结肽的细胞内化和胞质分布。

Fatty acylation enhances the cellular internalization and cytosolic distribution of a cystine-knot peptide.

作者信息

Gao Xinxin, Mazière Ann De, Beard Rhiannon, Klumperman Judith, Hannoush Rami N

机构信息

Department of Early Discovery Biochemistry, Genentech, South San Francisco, CA, USA.

Department of Cell Biology, University Medical Center Utrecht, Utrecht, the Netherlands.

出版信息

iScience. 2021 Oct 5;24(11):103220. doi: 10.1016/j.isci.2021.103220. eCollection 2021 Nov 19.

Abstract

Delivering peptides into cells could open up possibilities for targeting intracellular proteins. Although fatty acylation of peptide therapeutics improves their systemic half-life, it remains unclear how it influences their cellular uptake. Here, we demonstrate that a fatty acylated peptide exhibits enhanced cellular internalization and cytosolic distribution compared to the un-acylated version. By using a cystine-knot peptide as a model system, we report an efficient strategy for site-specific conjugation of fatty acids. Peptides modified with fatty acids of different chain lengths entered cells through clathrin-mediated and macropinocytosis pathways. The cellular uptake was mediated by the length of the hydrocarbon chain, with myristic acid conjugates displaying the highest distribution across the cytoplasm including the cytosol, and endomembranes of the ER, Golgi and mitochondria. Our studies demonstrate how fatty acylation improves the cellular uptake of peptides, and lay the groundwork for future development of bioactive peptides with enhanced intracellular distribution.

摘要

将肽递送至细胞中可为靶向细胞内蛋白质开辟可能性。尽管肽疗法的脂肪酰化改善了它们的全身半衰期,但尚不清楚其如何影响细胞摄取。在此,我们证明与未酰化的肽相比,脂肪酰化肽表现出增强的细胞内化和胞质分布。通过使用胱氨酸结肽作为模型系统,我们报道了一种脂肪酸位点特异性偶联的有效策略。用不同链长脂肪酸修饰的肽通过网格蛋白介导的内吞作用和巨胞饮作用途径进入细胞。细胞摄取由烃链长度介导,肉豆蔻酸偶联物在包括胞质溶胶以及内质网、高尔基体和线粒体的内膜在内的整个细胞质中显示出最高的分布。我们的研究证明了脂肪酰化如何改善肽的细胞摄取,并为未来开发具有增强细胞内分布的生物活性肽奠定了基础。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/86d9/8529511/8bf027c4bc12/fx1.jpg

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