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2 research outputs found

Mesenchymal stem cells are short-lived and do not migrate beyond the lungs after intravenous infusion

Author: Baan C.C. (Carla)
Benseler V. (Volker)
Dahlke M.H. (Marc)
Eggenhofer E. (Elke)
Geissler E.K. (Edward)
Hoogduijn M.J. (Martin)
Kroemer H.K. (Heyo)
Popp F. (Felix)
Schlitt H.J. (Hans)
Publication venue: 'Frontiers Media SA'
Publication date: 01/12/2012
Field of study

Mesenchymal stem cells (MSC) are under investigation as a therapy for a variety of disorders. Although animal models show long term regenerative and immunomodulatory effects of MSC, the fate of MSC after infusion remains to be elucidated. In the present study the localization and viability of MSC was examined by isolation and re-culture of intravenously infused MSC. C57BL/6 MSC (500,000) constitutively expressing DsRed-fluorescent protein and radioactively labeled with Cr-51 were infused via the tail vein in wild-type C57BL/6 mice. After 5 min, 1, 24, or 72 h, mice were sacrificed and blood, lungs, liver, spleen, kidneys, and bone marrow removed. One hour after MSC infusion the majority of Cr-51 was found in the lungs, whereas after 24 h Cr-51 was mainly found in the liver. Tissue cultures demonstrated that viable donor MSC were present in the lungs up to 24 h after infusion, after which they disappeared. No viable MSC were found in the other organs examined at any time. The induction of ischemia-reperfusion injury in the liver did not trigger the migration of viable MSC to the liver. These results demonstrate that MSC are short-lived after i.v. infusion and that viable MSC do not pass the lungs. Cell debris may be transported to the liver. Long term immunomodulatory and regenerative effects of infused MSC must therefore be mediated via other cell types

Erasmus University Digital Repository

Mesenchymal stem cells in solid organ transplantation (MiSOT) fourth meeting: Lessons learned from first clinical trials

Author: Ancans J. (Janis)
Aran J.M. (Josep)
Baan C.C. (Carla)
Benseler V. (Volker)
Betjes M.G.H. (Michiel)
Casiraghi F. (Federica)
Christ B. (Bruno)
Dahlke M.H. (Marc)
Deans R. (Robert)
Delarosa O. (Olga)
Detry J-M.R. (Jean-Marie)
Dor F.J.M.F. (Frank)
Eggenhofer E. (Elke)
Engela A.U. (Anja)
Farré R. (Ramon)
Fillenberg B. (Barbara)
Franquesa M. (Marcella)
Gotti E. (Eliana)
Grinyo J. (Josep)
Hoogduijn M.J. (Martin)
Introna M. (Martino)
Johnson C. (Claire)
Kooten C. (Cees) van
Mahon B. (Bernard)
Mensah F.K.F. (Fane )
Obermajer N. (Natasha)
Perico N. (Norberto)
Pileggi A. (Antonello)
Pinxteren J. (Jef)
Popp F. (Felix)
Portero-Sanchez I. (Isabel)
Pulin A. (Andrey)
Rabelink T.J. (Ton)
Rambaldi A. (Alessandro)
Reading C.L. (Chris )
Reinders M.E. (Marlies)
Remuzzi G. (Giuseppe)
Roemeling-Vanrhijn M. (Marieke)
Sanchez-Fueyo A. (Albert)
Shagidulin M. (Murat)
Torras J.
Publication venue: 'Ovid Technologies (Wolters Kluwer Health)'
Publication date: 15/08/2013
Field of study

The Fourth Expert Meeting of the Mesenchymal Stem Cells in Solid Organ Transplantation (MiSOT) Consortium took place in Barcelona on October 19 and 20, 2012. This meeting focused on the translation of preclinical data into early clinical settings. This position paper highlights the main topics explored on the safety and efficacy of mesenchymal stem cells as a therapeutic agent in solid organ transplantation and emphasizes the issues (proper timing, concomitant immunossupression, source and immunogenicity of mesenchymal stem cells, and oncogenicity) that have been addressed and will be followed up by the MiSOT Consortium in future studies

Erasmus University Digital Repository