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Merck
  • Distinct biological events generated by ECM proteolysis by two homologous collagenases.

Distinct biological events generated by ECM proteolysis by two homologous collagenases.

Proceedings of the National Academy of Sciences of the United States of America (2016-09-16)
Inna Solomonov, Eldar Zehorai, Dalit Talmi-Frank, Sharon G Wolf, Alla Shainskaya, Alina Zhuravlev, Elena Kartvelishvily, Robert Visse, Yishai Levin, Nir Kampf, Diego Adhemar Jaitin, Eyal David, Ido Amit, Hideaki Nagase, Irit Sagi
要旨

It is well established that the expression profiles of multiple and possibly redundant matrix-remodeling proteases (e.g., collagenases) differ strongly in health, disease, and development. Although enzymatic redundancy might be inferred from their close similarity in structure, their in vivo activity can lead to extremely diverse tissue-remodeling outcomes. We observed that proteolysis of collagen-rich natural extracellular matrix (ECM), performed uniquely by individual homologous proteases, leads to distinct events that eventually affect overall ECM morphology, viscoelastic properties, and molecular composition. We revealed striking differences in the motility and signaling patterns, morphology, and gene-expression profiles of cells interacting with natural collagen-rich ECM degraded by different collagenases. Thus, in contrast to previous notions, matrix-remodeling systems are not redundant and give rise to precise ECM-cell crosstalk. Because ECM proteolysis is an abundant biochemical process that is critical for tissue homoeostasis, these results improve our fundamental understanding its complexity and its impact on cell behavior.

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Sigma-Aldrich
モノクロナール抗MAPキナーゼ, 活性化 (二リン酸化型ERK-1&2) マウス宿主抗体, clone MAPK-YT, ascites fluid
Sigma-Aldrich
ラクトアルブミン酵素加水分解物, powder, BioReagent, suitable for cell culture
Sigma-Aldrich
抗MAPキナーゼ(ERK-1, ERK-2) ウサギ宿主抗体, whole antiserum