I just read this paper
Article Biomaterials for Integration with 3-D Bioprinting
mentioning that
"Migration of cells in 3-D can be
expedited or minimized depending on the ratios of
matrix components such as collagens and glycosami-
noglycans."
referring to
Article Bioprinting living structures
but in the referred paper I didn't find further explanation of how is the cell migration is influenced by ECM composition
Could somebody offer a more detailed explanation on relation between ECM composition and cell migration?
Thanks a lot! both papers are very helpful. But how exactly can I control cell migration with component of glycosaminoglycans? If I increase GAG component how will the cell migration be affected, up or down?
Thanks a lot! both papers are very helpful. But how exactly can I control cell migration with component of glycosaminoglycans? If I increase GAG component how will the cell migration be affected, more or less migration? Mohsen Ghorbian
Karen A. Darbinyan- Badges
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