Cells respond to deletion of CAV1 by increasing synthesis of extracellular matrix

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Abstract

A range of cellular functions have been attributed to caveolae, flask-like invaginations of the plasma membrane. Here, we have used RNA-seq to achieve quantitative transcriptional profiling of primary embryonic fibroblasts from caveolin 1 knockout mice (CAV1-/- MEFs), and thereby to gain hypothesis-free insight into how these cells respond to the absence of caveolae. Components of the extracellular matrix were decisively over-represented within the set of genes displaying altered expression in CAV1-/- MEFs when compared to congenic wild-type controls. This was confirmed biochemically and by imaging for selected examples. Up-regulation of components of the extracellular matrix was also observed in a second cell line, NIH-3T3 cells genome edited to delete CAV1. Up-regulation of components of the extracellular matrix was detected in vivo by assessing collagen deposition and compliance of CAV1-/- lungs. We discuss the implications of these findings in terms of the cellular function of caveolae.

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Mendoza-Topaz, C., Nelson, G., Howard, G., Hafner, S., Rademacher, P., Frick, M., & Nichols, B. J. (2018). Cells respond to deletion of CAV1 by increasing synthesis of extracellular matrix. PLoS ONE, 13(10). https://doi.org/10.1371/journal.pone.0205306

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