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通过模拟合成细胞外基质中的隐匿信号来激活隐藏信号。

Activating hidden signals by mimicking cryptic sites in a synthetic extracellular matrix.

机构信息

Department of Chemistry and Macromolecules Innovation Institute, Virginia Tech, Blacksburg, VA, USA.

Department of Chemical Engineering, Ben-Gurion University of the Negev, Beer-Sheva, Israel.

出版信息

Nat Commun. 2023 Jun 19;14(1):3635. doi: 10.1038/s41467-023-39349-w.

Abstract

Cryptic sites are short signaling peptides buried within the native extracellular matrix (ECM). Enzymatic cleavage of an ECM protein reveals these hidden peptide sequences, which interact with surface receptors to control cell behavior. Materials that mimic this dynamic interplay between cells and their surroundings via cryptic sites could enable application of this endogenous signaling phenomenon in synthetic ECM hydrogels. We demonstrate that depsipeptides ("switch peptides") can undergo enzyme-triggered changes in their primary sequence, with proof-of-principle studies showing how trypsin-triggered primary sequence rearrangement forms the bioadhesive pentapeptide YIGSR. We then engineered cryptic site-mimetic synthetic ECM hydrogels that experienced a cell-initiated gain of bioactivity. Responding to the endothelial cell surface enzyme aminopeptidase N, the inert matrix transformed into an adhesive synthetic ECM capable of supporting endothelial cell growth. This modular system enables dynamic reciprocity in synthetic ECMs, reproducing the natural symbiosis between cells and their matrix through inclusion of tunable hidden signals.

摘要

隐匿位点是埋藏在天然细胞外基质 (ECM) 中的短信号肽。ECM 蛋白的酶切揭示了这些隐藏的肽序列,它们与表面受体相互作用,控制细胞行为。通过隐匿位点模拟细胞与其周围环境之间这种动态相互作用的材料,可以使内源性信号现象在合成 ECM 水凝胶中的应用成为可能。我们证明了 depsipeptides(“开关肽”)可以在其一级序列中发生酶触发的变化,初步研究表明胰蛋白酶触发的一级序列重排如何形成生物粘附五肽 YIGSR。然后,我们设计了模仿隐匿位点的合成 ECM 水凝胶,这些水凝胶经历了细胞起始的生物活性获得。响应内皮细胞表面酶氨基肽酶 N,惰性基质转化为具有粘附性的合成 ECM,能够支持内皮细胞生长。该模块化系统在合成 ECM 中实现了动态互反性,通过包含可调隐藏信号,再现了细胞与其基质之间的自然共生关系。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/d271/10279755/86ebb180aae2/41467_2023_39349_Fig1_HTML.jpg

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