In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome

Oscar E. Simonson; Dimitrios Mougiakakos; Nina Heldring; Giulio Bassi; Henrik J. Johansson; Magnus Dalén; Regina Jitschin; Sergey Rodin; Matthias Corbascio; Samir El Andaloussi; Oscar P.B. Wiklander; Joel Z. Nordin; Johan Skog; Charlotte Romain; Tina Koestler; Laila Hellgren-Johansson; Petter Schiller; Per Olof Joachimsson; Hans Hägglund; Mattias Mattiasmattsson; Janne Lehtiö; Omid R. Faridani; Rickard Sandberg; Olle Korsgren; Mauro Krampera; Daniel J. Weiss; Karl Henrik Grinnemo; Katarina Le Blanc

doi:10.5966/sctm.2015-0021

In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome

Oscar E. Simonson, Dimitrios Mougiakakos, Nina Heldring, Giulio Bassi, Henrik J. Johansson, Magnus Dalén, Regina Jitschin, Sergey Rodin, Matthias Corbascio, Samir El Andaloussi, Oscar P.B. Wiklander, Joel Z. Nordin, Johan Skog, Charlotte Romain, Tina Koestler, Laila Hellgren-Johansson, Petter Schiller, Per Olof Joachimsson, Hans Hägglund, Mattias MattiasmattssonJanne Lehtiö, Omid R. Faridani, Rickard Sandberg, Olle Korsgren, Mauro Krampera, Daniel J. Weiss, Karl Henrik Grinnemo, Katarina Le Blanc

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120 Citas (Scopus)

Resumen

Mesenchymal stromal cells (MSCs) have been investigated as a treatment for various inflammatory diseases because of their immunomodulatory and reparative properties.However,manybasic questions concerning theirmechanisms of action after systemic infusion remain unanswered. We performed a detailed analysis of the immunomodulatory properties and proteomic profile of MSCs systemically administered to two patients with severe refractory acute respiratory distress syndrome (ARDS) on a compassionate use basis and attempted to correlate these with in vivo anti-inflammatory actions. Both patients received 2×10⁶ cells per kilogram, and each subsequently improved with resolution of respiratory, hemodynamic, and multiorgan failure. In parallel, a decrease was seen in multiple pulmonary and systemic markers of inflammation, including epithelial apoptosis, alveolar-capillary fluid leakage, and proinflammatory cytokines, microRNAs, and chemokines. In vitro studies of theMSCs demonstrated a broad antiinflammatory capacity, including suppression of T-cell responses and induction of regulatory phenotypes in T cells,monocytes, and neutrophils. Some of these in vitro potency assessments correlated with, and were relevant to, the observed in vivo actions. These experiences highlight both the mechanistic information that can be gained from clinical experience and the value of correlating in vitro potency assessments with clinical effects. The findings also suggest, but do not prove, a beneficial effect of lung protective strategies using adoptively transferred MSCs in ARDS. Appropriate randomized clinical trials are required to further assess any potential clinical efficacy and investigate the effects on in vivo inflammation.

Idioma original	Inglés
Páginas (desde-hasta)	1199-1213
Número de páginas	15
Publicación	Stem Cells Translational Medicine
Volumen	4
N.º	10
DOI	https://doi.org/10.5966/sctm.2015-0021
Estado	Publicada - 1 oct. 2015
Publicado de forma externa	Sí

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Simonson, O. E., Mougiakakos, D., Heldring, N., Bassi, G., Johansson, H. J., Dalén, M., Jitschin, R., Rodin, S., Corbascio, M., El Andaloussi, S., Wiklander, O. P. B., Nordin, J. Z., Skog, J., Romain, C., Koestler, T., Hellgren-Johansson, L., Schiller, P., Joachimsson, P. O., Hägglund, H., ... Le Blanc, K. (2015). In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome. Stem Cells Translational Medicine, 4(10), 1199-1213. https://doi.org/10.5966/sctm.2015-0021

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title = "In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome",

abstract = "Mesenchymal stromal cells (MSCs) have been investigated as a treatment for various inflammatory diseases because of their immunomodulatory and reparative properties.However,manybasic questions concerning theirmechanisms of action after systemic infusion remain unanswered. We performed a detailed analysis of the immunomodulatory properties and proteomic profile of MSCs systemically administered to two patients with severe refractory acute respiratory distress syndrome (ARDS) on a compassionate use basis and attempted to correlate these with in vivo anti-inflammatory actions. Both patients received 2×106 cells per kilogram, and each subsequently improved with resolution of respiratory, hemodynamic, and multiorgan failure. In parallel, a decrease was seen in multiple pulmonary and systemic markers of inflammation, including epithelial apoptosis, alveolar-capillary fluid leakage, and proinflammatory cytokines, microRNAs, and chemokines. In vitro studies of theMSCs demonstrated a broad antiinflammatory capacity, including suppression of T-cell responses and induction of regulatory phenotypes in T cells,monocytes, and neutrophils. Some of these in vitro potency assessments correlated with, and were relevant to, the observed in vivo actions. These experiences highlight both the mechanistic information that can be gained from clinical experience and the value of correlating in vitro potency assessments with clinical effects. The findings also suggest, but do not prove, a beneficial effect of lung protective strategies using adoptively transferred MSCs in ARDS. Appropriate randomized clinical trials are required to further assess any potential clinical efficacy and investigate the effects on in vivo inflammation.",

keywords = "Acute respiratory distress syndrome, Bone marrow stromal cells, Cell transplantation, Cellular therapy, Clinical translation, Pulmonary diseases, Respiratory tract, Stem cells",

author = "Simonson, {Oscar E.} and Dimitrios Mougiakakos and Nina Heldring and Giulio Bassi and Johansson, {Henrik J.} and Magnus Dal{\'e}n and Regina Jitschin and Sergey Rodin and Matthias Corbascio and {El Andaloussi}, Samir and Wiklander, {Oscar P.B.} and Nordin, {Joel Z.} and Johan Skog and Charlotte Romain and Tina Koestler and Laila Hellgren-Johansson and Petter Schiller and Joachimsson, {Per Olof} and Hans H{\"a}gglund and Mattias Mattiasmattsson and Janne Lehti{\"o} and Faridani, {Omid R.} and Rickard Sandberg and Olle Korsgren and Mauro Krampera and Weiss, {Daniel J.} and Grinnemo, {Karl Henrik} and {Le Blanc}, Katarina",

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doi = "10.5966/sctm.2015-0021",

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Simonson, OE, Mougiakakos, D, Heldring, N, Bassi, G, Johansson, HJ, Dalén, M, Jitschin, R, Rodin, S, Corbascio, M, El Andaloussi, S, Wiklander, OPB, Nordin, JZ, Skog, J, Romain, C, Koestler, T, Hellgren-Johansson, L, Schiller, P, Joachimsson, PO, Hägglund, H, Mattiasmattsson, M, Lehtiö, J, Faridani, OR, Sandberg, R, Korsgren, O, Krampera, M, Weiss, DJ, Grinnemo, KH & Le Blanc, K 2015, 'In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome', Stem Cells Translational Medicine, vol. 4, n.º 10, pp. 1199-1213. https://doi.org/10.5966/sctm.2015-0021

TY - JOUR

T1 - In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome

AU - Simonson, Oscar E.

AU - Mougiakakos, Dimitrios

AU - Heldring, Nina

AU - Bassi, Giulio

AU - Johansson, Henrik J.

AU - Dalén, Magnus

AU - Jitschin, Regina

AU - Rodin, Sergey

AU - Corbascio, Matthias

AU - El Andaloussi, Samir

AU - Wiklander, Oscar P.B.

AU - Nordin, Joel Z.

AU - Skog, Johan

AU - Romain, Charlotte

AU - Koestler, Tina

AU - Hellgren-Johansson, Laila

AU - Schiller, Petter

AU - Joachimsson, Per Olof

AU - Hägglund, Hans

AU - Mattiasmattsson, Mattias

AU - Lehtiö, Janne

AU - Faridani, Omid R.

AU - Sandberg, Rickard

AU - Korsgren, Olle

AU - Krampera, Mauro

AU - Weiss, Daniel J.

AU - Grinnemo, Karl Henrik

AU - Le Blanc, Katarina

PY - 2015/10/1

Y1 - 2015/10/1

N2 - Mesenchymal stromal cells (MSCs) have been investigated as a treatment for various inflammatory diseases because of their immunomodulatory and reparative properties.However,manybasic questions concerning theirmechanisms of action after systemic infusion remain unanswered. We performed a detailed analysis of the immunomodulatory properties and proteomic profile of MSCs systemically administered to two patients with severe refractory acute respiratory distress syndrome (ARDS) on a compassionate use basis and attempted to correlate these with in vivo anti-inflammatory actions. Both patients received 2×106 cells per kilogram, and each subsequently improved with resolution of respiratory, hemodynamic, and multiorgan failure. In parallel, a decrease was seen in multiple pulmonary and systemic markers of inflammation, including epithelial apoptosis, alveolar-capillary fluid leakage, and proinflammatory cytokines, microRNAs, and chemokines. In vitro studies of theMSCs demonstrated a broad antiinflammatory capacity, including suppression of T-cell responses and induction of regulatory phenotypes in T cells,monocytes, and neutrophils. Some of these in vitro potency assessments correlated with, and were relevant to, the observed in vivo actions. These experiences highlight both the mechanistic information that can be gained from clinical experience and the value of correlating in vitro potency assessments with clinical effects. The findings also suggest, but do not prove, a beneficial effect of lung protective strategies using adoptively transferred MSCs in ARDS. Appropriate randomized clinical trials are required to further assess any potential clinical efficacy and investigate the effects on in vivo inflammation.

AB - Mesenchymal stromal cells (MSCs) have been investigated as a treatment for various inflammatory diseases because of their immunomodulatory and reparative properties.However,manybasic questions concerning theirmechanisms of action after systemic infusion remain unanswered. We performed a detailed analysis of the immunomodulatory properties and proteomic profile of MSCs systemically administered to two patients with severe refractory acute respiratory distress syndrome (ARDS) on a compassionate use basis and attempted to correlate these with in vivo anti-inflammatory actions. Both patients received 2×106 cells per kilogram, and each subsequently improved with resolution of respiratory, hemodynamic, and multiorgan failure. In parallel, a decrease was seen in multiple pulmonary and systemic markers of inflammation, including epithelial apoptosis, alveolar-capillary fluid leakage, and proinflammatory cytokines, microRNAs, and chemokines. In vitro studies of theMSCs demonstrated a broad antiinflammatory capacity, including suppression of T-cell responses and induction of regulatory phenotypes in T cells,monocytes, and neutrophils. Some of these in vitro potency assessments correlated with, and were relevant to, the observed in vivo actions. These experiences highlight both the mechanistic information that can be gained from clinical experience and the value of correlating in vitro potency assessments with clinical effects. The findings also suggest, but do not prove, a beneficial effect of lung protective strategies using adoptively transferred MSCs in ARDS. Appropriate randomized clinical trials are required to further assess any potential clinical efficacy and investigate the effects on in vivo inflammation.

KW - Acute respiratory distress syndrome

KW - Bone marrow stromal cells

KW - Cell transplantation

KW - Cellular therapy

KW - Clinical translation

KW - Pulmonary diseases

KW - Respiratory tract

KW - Stem cells

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U2 - 10.5966/sctm.2015-0021

DO - 10.5966/sctm.2015-0021

M3 - Artículo

C2 - 26285659

AN - SCOPUS:84939823410

SN - 2157-6564

VL - 4

SP - 1199

EP - 1213

JO - Stem Cells Translational Medicine

JF - Stem Cells Translational Medicine

IS - 10

ER -

In vivo effects of mesenchymal stromal cells in two patients with severe acute respiratory distress syndrome

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