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Development of immortalized mouse aortic endothelial cell lines. | LitMetric

AI Article Synopsis

  • The study focuses on overcoming the difficulties of isolating and maintaining primary mouse aortic endothelial cells (MAECs), which often lose their characteristics during culture.
  • A new method was developed to create immortalized MAEC (iMAEC) lines by using a retrovirus to maintain their properties and phenotypes effectively.
  • The results show that these iMAECs retain key endothelial cell markers and functional abilities, allowing researchers to advance studies in vascular biology and ailments related to the circulatory system.

Article Abstract

Background: The understanding of endothelial cell biology has been facilitated by the availability of primary endothelial cell cultures from a variety of sites and species; however, the isolation and maintenance of primary mouse aortic endothelial cells (MAECs) remain a formidable challenge. Culturing MAECs is difficult as they are prone to phenotypic drift during culture. Therefore, there is a need to have a dependable in vitro culture system, wherein the primary endothelial cells retain their properties and phenotypes.

Methods: Here, we developed an effective method to prepare immortalized MAEC (iMAEC) lines. Primary MAECs, initially isolated from aortic explants, were immortalized using a retrovirus expressing polyoma middle T-antigen. Immortalized cells were then incubated with DiI-acetylated-low density lipoprotein and sorted via flow cytometry to isolate iMAECs.

Results: iMAECs expressed common markers of endothelial cells, including PECAM1, eNOS, VE-cadherin, and von Willebrand Factor. iMAECs aligned in the direction of imposed laminar shear and retained the ability to form tubes. Using this method, we have generated iMAEC lines from wild-type and various genetically modified mice such as p47phox-/-, eNOS-/-, and caveolin-1-/-.

Conclusion: In summary, generation of iMAEC lines from various genetically modified mouse lines provides an invaluable tool to study vascular biology and pathophysiology.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC4230636PMC
http://dx.doi.org/10.1186/2045-824X-6-7DOI Listing

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