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含TAT的蛋白质和肽在活细胞中的货物依赖摄取模式及生物利用度

Cargo-dependent mode of uptake and bioavailability of TAT-containing proteins and peptides in living cells.

作者信息

Tünnemann Gisela, Martin Robert M, Haupt Simone, Patsch Christoph, Edenhofer Frank, Cardoso M Cristina

机构信息

Max Delbrück Center for Molecular Medicine, Robert-Rössle-Str. 10, Berlin 13125, Germany.

出版信息

FASEB J. 2006 Sep;20(11):1775-84. doi: 10.1096/fj.05-5523com.

Abstract

Cell-penetrating peptides (CPPs) are capable of introducing a wide range of cargoes into living cells. Descriptions of the internalization process vary from energy-independent cell penetration of membranes to endocytic uptake. To elucidate whether the mechanism of entry of CPP constructs might be influenced by the properties of the cargo, we used time lapse confocal microscopy analysis of living mammalian cells to directly compare the uptake of the well-studied CPP TAT fused to a protein (>50 amino acids) or peptide (<50 amino acids) cargo. We also analyzed various constructs for their subcellular distribution and mobility after the internalization event. TAT fusion proteins were taken up largely into cytoplasmic vesicles whereas peptides fused to TAT entered the cell in a rapid manner that was dependent on membrane potential. Despite their accumulation in the nucleolus, photobleaching of TAT fusion peptides revealed their mobility. The bioavailability of internalized TAT peptides was tested and confirmed by the strong inhibitory effect on cell cycle progression of two TAT fusion peptides derived from the tumor suppressor p21(WAF/Cip) and DNA Ligase I measured in living cells.

摘要

细胞穿透肽(CPPs)能够将多种物质导入活细胞。内化过程的描述各不相同,从与能量无关的细胞膜穿透到内吞摄取。为了阐明CPP构建体的进入机制是否可能受所载物质特性的影响,我们使用活的哺乳动物细胞的延时共聚焦显微镜分析,直接比较了与蛋白质(>50个氨基酸)或肽(<50个氨基酸)所载物质融合的、经过充分研究的CPP TAT的摄取情况。我们还分析了各种构建体在内化事件后的亚细胞分布和移动性。TAT融合蛋白主要被摄取到细胞质囊泡中,而与TAT融合的肽则以依赖于膜电位的快速方式进入细胞。尽管TAT融合肽在核仁中积累,但光漂白显示了它们的移动性。通过在活细胞中测量源自肿瘤抑制因子p21(WAF/Cip)和DNA连接酶I的两种TAT融合肽对细胞周期进程的强烈抑制作用,测试并证实了内化TAT肽的生物利用度。

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