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细胞内外极性的相互作用使通过分层基质进行深度机械感知成为可能。

Reciprocal intra- and extra-cellular polarity enables deep mechanosensing through layered matrices.

机构信息

Department of Mechanical Engineering & Materials Science, Washington University in St. Louis, St. Louis, MO, USA.

Department of Mechanical Engineering & Materials Science, Washington University in St. Louis, St. Louis, MO, USA.

出版信息

Cell Rep. 2023 Apr 25;42(4):112362. doi: 10.1016/j.celrep.2023.112362. Epub 2023 Apr 5.

Abstract

Adherent cells migrate on layered tissue interfaces to drive morphogenesis, wound healing, and tumor invasion. Although stiffer surfaces are known to enhance cell migration, it remains unclear whether cells sense basal stiff environments buried under softer, fibrous matrix. Using layered collagen-polyacrylamide gel systems, we unveil a migration phenotype driven by cell-matrix polarity. Here, cancer (but not normal) cells with stiff base matrix generate stable protrusions, faster migration, and greater collagen deformation because of "depth mechanosensing" through the top collagen layer. Cancer cell protrusions with front-rear polarity produce polarized collagen stiffening and deformations. Disruption of either extracellular or intracellular polarity via collagen crosslinking, laser ablation, or Arp2/3 inhibition independently abrogates depth-mechanosensitive migration of cancer cells. Our experimental findings, validated by lattice-based energy minimization modeling, present a cell migration mechanism whereby polarized cellular protrusions and contractility are reciprocated by mechanical extracellular polarity, culminating in a cell-type-dependent ability to mechanosense through matrix layers.

摘要

黏附细胞在分层组织界面上迁移,从而驱动形态发生、创伤愈合和肿瘤侵袭。尽管已知较硬的表面会增强细胞迁移,但仍不清楚细胞是否能感知埋藏在较软的纤维基质下的基底硬环境。通过使用分层胶原-聚丙烯酰胺凝胶系统,我们揭示了一种由细胞-基质极性驱动的迁移表型。在这里,具有硬基底基质的癌症(而非正常)细胞会产生稳定的突起,迁移速度更快,并且由于通过顶层胶原层进行“深度机械感知”,胶原变形更大。具有前后极性的癌细胞突起会产生极化的胶原变硬和变形。通过胶原交联、激光消融或 Arp2/3 抑制破坏细胞外或细胞内极性,都会独立地阻止癌症细胞的深度机械敏感迁移。我们的实验结果通过基于晶格的能量最小化建模得到了验证,提出了一种细胞迁移机制,其中极化的细胞突起和收缩性通过机械细胞外极性相互作用,最终导致细胞对基质层进行机械敏感的能力具有细胞类型依赖性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ec80/11246724/15f6fb12f055/nihms-2004351-f0002.jpg

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