BACKGROUND: Given the diversity of species from which adipose-derived stromal cells are derived and studied, the authors set out to delineate the differences in the basic cell biology that may exist across species. Briefly, the authors found that significant differences exist with regard to proliferation and osteogenic potentials of adipose-derived stromal cells across species. METHODS: Adipose-derived stromal cells were derived from human, mouse, and canine sources as previously described. Retinoic acid, insulin-like growth factor-1, and bone morphogenetic protein-2 were added to culture medium; proliferation and osteogenic differentiation were assessed by standardized assays. In vivo methods included seeding 150,000 adipose-derived stromal cells on a biomimetic scaffold and analyzing healing by micro-computed tomography and histology. RESULTS: Adipose-derived stromal cells from all species had the capability to undergo osteogenic differentiation. Canine adipose-derived stromal cells were the most proliferative, whereas human adipose-derived stromal cells were the most osteogenic (p < 0.05). Human cells, however, had the most significant osteogenic response to osteogenic media. Retinoic acid stimulated osteogenesis in mouse and canine cells but not in human adipose-derived stromal cells. Insulin-like growth factor-1 enhanced osteogenesis across all species, most notably in human- and canine-derived cells. CONCLUSIONS: Adipose-derived stromal cells derived from human, mouse, and canine all have the capacity to undergo osteogenic differentiation. Canine adipose-derived stromal cells appear to be the most proliferative, whereas human adipose-derived stromal cells appear to be the most osteogenic. Different cytokines and chemicals can be used to modulate this osteogenic response. These results are promising as attempts are made to optimize tissue-engineered bone using adipose-derived stromal cells.
BACKGROUND: Given the diversity of species from which adipose-derived stromal cells are derived and studied, the authors set out to delineate the differences in the basic cell biology that may exist across species. Briefly, the authors found that significant differences exist with regard to proliferation and osteogenic potentials of adipose-derived stromal cells across species. METHODS:Adipose-derived stromal cells were derived from human, mouse, and canine sources as previously described. Retinoic acid, insulin-like growth factor-1, and bone morphogenetic protein-2 were added to culture medium; proliferation and osteogenic differentiation were assessed by standardized assays. In vivo methods included seeding 150,000 adipose-derived stromal cells on a biomimetic scaffold and analyzing healing by micro-computed tomography and histology. RESULTS:Adipose-derived stromal cells from all species had the capability to undergo osteogenic differentiation. Canineadipose-derived stromal cells were the most proliferative, whereas humanadipose-derived stromal cells were the most osteogenic (p < 0.05). Human cells, however, had the most significant osteogenic response to osteogenic media. Retinoic acid stimulated osteogenesis in mouse and canine cells but not in humanadipose-derived stromal cells. Insulin-like growth factor-1 enhanced osteogenesis across all species, most notably in human- and canine-derived cells. CONCLUSIONS:Adipose-derived stromal cells derived from human, mouse, and canine all have the capacity to undergo osteogenic differentiation. Canineadipose-derived stromal cells appear to be the most proliferative, whereas humanadipose-derived stromal cells appear to be the most osteogenic. Different cytokines and chemicals can be used to modulate this osteogenic response. These results are promising as attempts are made to optimize tissue-engineered bone using adipose-derived stromal cells.
Authors: Shailesh Agarwal; Shawn J Loder; Christopher Breuler; John Li; David Cholok; Cameron Brownley; Jonathan Peterson; Hsiao H Hsieh; James Drake; Kavitha Ranganathan; Yashar S Niknafs; Wenzhong Xiao; Shuli Li; Ravindra Kumar; Ronald Tompkins; Michael T Longaker; Thomas A Davis; Paul B Yu; Yuji Mishina; Benjamin Levi Journal: Mol Ther Date: 2017-07-15 Impact factor: 11.454
Authors: Michael T Chung; Andrew S Zimmermann; Kevin J Paik; Shane D Morrison; Jeong S Hyun; David D Lo; Adrian McArdle; Daniel T Montoro; Graham G Walmsley; Kshemendra Senarath-Yapa; Michael Sorkin; Robert Rennert; Hsin-Han Chen; Andrew S Chung; Dean Vistnes; Geoffrey C Gurtner; Michael T Longaker; Derrick C Wan Journal: Stem Cells Transl Med Date: 2013-09-09 Impact factor: 6.940
Authors: Warren L Grayson; Bruce A Bunnell; Elizabeth Martin; Trivia Frazier; Ben P Hung; Jeffrey M Gimble Journal: Nat Rev Endocrinol Date: 2015-01-06 Impact factor: 43.330
Authors: Jonathan R Peterson; Oluwatobi N Eboda; R Cameron Brownley; Katherine E Cilwa; Lauren E Pratt; Sara De La Rosa; Shailesh Agarwal; Steven R Buchman; Paul S Cederna; Michael D Morris; Stewart C Wang; Benjamin Levi Journal: Stem Cells Dev Date: 2015-01-15 Impact factor: 3.272
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Authors: Jonathan R Peterson; Oluwatobi Eboda; Shailesh Agarwal; Kavitha Ranganathan; Steven R Buchman; Min Lee; Stewart C Wang; Yuji Mishina; Benjamin Levi Journal: Stem Cells Transl Med Date: 2014-09-17 Impact factor: 6.940
Authors: Alexis Donneys; Jordan T Blough; Noah S Nelson; Joseph E Perosky; Sagar S Deshpande; Stephen Y Kang; Peter A Felice; Christian Figueredo; Jonathan R Peterson; Kenneth M Kozloff; Benjamin Levi; Douglas B Chepeha; Steven R Buchman Journal: Head Neck Date: 2015-07-15 Impact factor: 3.147
Authors: Jonathan R Peterson; Sara De La Rosa; Hongli Sun; Oluwatobi Eboda; Katherine E Cilwa; Alexis Donneys; Michael Morris; Steven R Buchman; Paul S Cederna; Paul H Krebsbach; Stewart C Wang; Benjamin Levi Journal: Ann Surg Date: 2014-05 Impact factor: 12.969
Authors: Sagar S Deshpande; Alexis Donneys; Stephen Y Kang; Erin E Page; Peter A Felice; Lauren Kiryakoza; Noah S Nelson; Jose Rodriguez; Samir S Deshpande; Steven R Buchman Journal: Microvasc Res Date: 2014-08-27 Impact factor: 3.514