Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions

Ali Shokoohmand; Nikita M Patel; Lorena Braid; Massimo Dominici; Tracy S P Heng; James A Ankrum; Jayita Barua; Andrés Caicedo; Michael Creane; Lindsay Davies; Claudia C Dos Santos; Sara Rolandsson Enes; Karen English; Dominique Farge; María Fernández-García; Jacques Galipeau; Nadir Kadri; Maroun Khoury; Stephen Kilfeather; Mauro Krampera; Anna Krasnodembskaya; Manoj Lalu; Katarina Le Blanc; Guido Moll; Jan Nolta; Cecilia O'Kane; Patricia R M Rocco; Yufang Shi; Daniel J Weiss; Sowmya Viswanathan

doi:10.1016/j.jcyt.2025.102007

Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions

Ali Shokoohmand
, Nikita M Patel
, Lorena Braid
, Massimo Dominici
, Tracy S P Heng
, James A Ankrum
, Jayita Barua
, Andrés Caicedo
, Michael Creane
, Lindsay Davies
, Claudia C Dos Santos
, Sara Rolandsson Enes
, Karen English
, Dominique Farge
, María Fernández-García
, Jacques Galipeau
, Nadir Kadri
, Maroun Khoury
, Stephen Kilfeather
, Mauro Krampera

Anna Krasnodembskaya, Manoj Lalu, Katarina Le Blanc, Guido Moll, Jan Nolta, Cecilia O'Kane, Patricia R M Rocco, Yufang Shi, Daniel J Weiss, Sowmya Viswanathan

Research output: Contribution to journal › Article › peer-review

Abstract

The in vivo fate of mesenchymal stromal cells (MSCs), including their clearance, interaction with host tissues, and persistence, remains incompletely understood following systemic or local clinical administration to patients. Although immune-mediated clearance mechanisms, such as triggering of the instant blood-mediated inflammatory reaction, activation of coagulation and complement pathways, apoptosis and efferocytosis have been identified, their contributions to MSC function and efficacy are still under investigation. To address these knowledge gaps, an international panel of experts in MSC biology and clinical regenerative medicine convened to assess current evidence and define key unanswered questions. Discussions were structured around three thematic domains: (i) biodistribution and mechanisms of action following systemic delivery; (ii) biological implications of local or depot-based administration and (iii) the dynamics of MSC persistence and clearance in vivo. A major focus was on the role of MSC apoptosis and its immunological consequences, particularly interactions between apoptotic MSCs, phagocytes and endothelial barriers. This perspective highlights the most urgent research questions identified during the meeting and in follow-up discussions and proposes experimental strategies to move beyond traditional cell tracking toward interrogating functional persistence, immune modulation and delivery context. Addressing these gaps will deepen our understanding of MSC behavior in vivo and guide the development of safer, more predictable and more effective MSC-based interventions.

Original language	English
Article number	102007
Journal	Cytotherapy
Early online date	15 Nov 2025
DOIs	https://doi.org/10.1016/j.jcyt.2025.102007
Publication status	Early online date - 15 Nov 2025

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Shokoohmand, A., Patel, N. M., Braid, L., Dominici, M., Heng, T. S. P., Ankrum, J. A., Barua, J., Caicedo, A., Creane, M., Davies, L., Dos Santos, C. C., Enes, S. R., English, K., Farge, D., Fernández-García, M., Galipeau, J., Kadri, N., Khoury, M., Kilfeather, S., ... Viswanathan, S. (2025). Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions. Cytotherapy, Article 102007. Advance online publication. https://doi.org/10.1016/j.jcyt.2025.102007

@article{07bf67e83fa04431a7cec496592fc8c4,

title = "Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions",

abstract = "The in vivo fate of mesenchymal stromal cells (MSCs), including their clearance, interaction with host tissues, and persistence, remains incompletely understood following systemic or local clinical administration to patients. Although immune-mediated clearance mechanisms, such as triggering of the instant blood-mediated inflammatory reaction, activation of coagulation and complement pathways, apoptosis and efferocytosis have been identified, their contributions to MSC function and efficacy are still under investigation. To address these knowledge gaps, an international panel of experts in MSC biology and clinical regenerative medicine convened to assess current evidence and define key unanswered questions. Discussions were structured around three thematic domains: (i) biodistribution and mechanisms of action following systemic delivery; (ii) biological implications of local or depot-based administration and (iii) the dynamics of MSC persistence and clearance in vivo. A major focus was on the role of MSC apoptosis and its immunological consequences, particularly interactions between apoptotic MSCs, phagocytes and endothelial barriers. This perspective highlights the most urgent research questions identified during the meeting and in follow-up discussions and proposes experimental strategies to move beyond traditional cell tracking toward interrogating functional persistence, immune modulation and delivery context. Addressing these gaps will deepen our understanding of MSC behavior in vivo and guide the development of safer, more predictable and more effective MSC-based interventions.",

author = "Ali Shokoohmand and Patel, \{Nikita M\} and Lorena Braid and Massimo Dominici and Heng, \{Tracy S P\} and Ankrum, \{James A\} and Jayita Barua and Andr{\'e}s Caicedo and Michael Creane and Lindsay Davies and \{Dos Santos\}, \{Claudia C\} and Enes, \{Sara Rolandsson\} and Karen English and Dominique Farge and Mar{\'i}a Fern{\'a}ndez-Garc{\'i}a and Jacques Galipeau and Nadir Kadri and Maroun Khoury and Stephen Kilfeather and Mauro Krampera and Anna Krasnodembskaya and Manoj Lalu and Blanc, \{Katarina Le\} and Guido Moll and Jan Nolta and Cecilia O'Kane and Rocco, \{Patricia R M\} and Yufang Shi and Weiss, \{Daniel J\} and Sowmya Viswanathan",

year = "2025",

month = nov,

day = "15",

doi = "10.1016/j.jcyt.2025.102007",

language = "English",

journal = "Cytotherapy",

issn = "1465-3249",

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Shokoohmand, A, Patel, NM, Braid, L, Dominici, M, Heng, TSP, Ankrum, JA, Barua, J, Caicedo, A, Creane, M, Davies, L, Dos Santos, CC, Enes, SR, English, K, Farge, D, Fernández-García, M, Galipeau, J, Kadri, N, Khoury, M, Kilfeather, S, Krampera, M, Krasnodembskaya, A, Lalu, M, Blanc, KL, Moll, G, Nolta, J, O'Kane, C, Rocco, PRM, Shi, Y, Weiss, DJ & Viswanathan, S 2025, 'Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions', Cytotherapy. https://doi.org/10.1016/j.jcyt.2025.102007

TY - JOUR

T1 - Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions

AU - Shokoohmand, Ali

AU - Patel, Nikita M

AU - Braid, Lorena

AU - Dominici, Massimo

AU - Heng, Tracy S P

AU - Ankrum, James A

AU - Barua, Jayita

AU - Caicedo, Andrés

AU - Creane, Michael

AU - Davies, Lindsay

AU - Dos Santos, Claudia C

AU - Enes, Sara Rolandsson

AU - English, Karen

AU - Farge, Dominique

AU - Fernández-García, María

AU - Galipeau, Jacques

AU - Kadri, Nadir

AU - Khoury, Maroun

AU - Kilfeather, Stephen

AU - Krampera, Mauro

AU - Krasnodembskaya, Anna

AU - Lalu, Manoj

AU - Blanc, Katarina Le

AU - Moll, Guido

AU - Nolta, Jan

AU - O'Kane, Cecilia

AU - Rocco, Patricia R M

AU - Shi, Yufang

AU - Weiss, Daniel J

AU - Viswanathan, Sowmya

PY - 2025/11/15

Y1 - 2025/11/15

N2 - The in vivo fate of mesenchymal stromal cells (MSCs), including their clearance, interaction with host tissues, and persistence, remains incompletely understood following systemic or local clinical administration to patients. Although immune-mediated clearance mechanisms, such as triggering of the instant blood-mediated inflammatory reaction, activation of coagulation and complement pathways, apoptosis and efferocytosis have been identified, their contributions to MSC function and efficacy are still under investigation. To address these knowledge gaps, an international panel of experts in MSC biology and clinical regenerative medicine convened to assess current evidence and define key unanswered questions. Discussions were structured around three thematic domains: (i) biodistribution and mechanisms of action following systemic delivery; (ii) biological implications of local or depot-based administration and (iii) the dynamics of MSC persistence and clearance in vivo. A major focus was on the role of MSC apoptosis and its immunological consequences, particularly interactions between apoptotic MSCs, phagocytes and endothelial barriers. This perspective highlights the most urgent research questions identified during the meeting and in follow-up discussions and proposes experimental strategies to move beyond traditional cell tracking toward interrogating functional persistence, immune modulation and delivery context. Addressing these gaps will deepen our understanding of MSC behavior in vivo and guide the development of safer, more predictable and more effective MSC-based interventions.

AB - The in vivo fate of mesenchymal stromal cells (MSCs), including their clearance, interaction with host tissues, and persistence, remains incompletely understood following systemic or local clinical administration to patients. Although immune-mediated clearance mechanisms, such as triggering of the instant blood-mediated inflammatory reaction, activation of coagulation and complement pathways, apoptosis and efferocytosis have been identified, their contributions to MSC function and efficacy are still under investigation. To address these knowledge gaps, an international panel of experts in MSC biology and clinical regenerative medicine convened to assess current evidence and define key unanswered questions. Discussions were structured around three thematic domains: (i) biodistribution and mechanisms of action following systemic delivery; (ii) biological implications of local or depot-based administration and (iii) the dynamics of MSC persistence and clearance in vivo. A major focus was on the role of MSC apoptosis and its immunological consequences, particularly interactions between apoptotic MSCs, phagocytes and endothelial barriers. This perspective highlights the most urgent research questions identified during the meeting and in follow-up discussions and proposes experimental strategies to move beyond traditional cell tracking toward interrogating functional persistence, immune modulation and delivery context. Addressing these gaps will deepen our understanding of MSC behavior in vivo and guide the development of safer, more predictable and more effective MSC-based interventions.

U2 - 10.1016/j.jcyt.2025.102007

DO - 10.1016/j.jcyt.2025.102007

M3 - Article

C2 - 41420629

SN - 1465-3249

JO - Cytotherapy

JF - Cytotherapy

M1 - 102007

ER -

Fate and function of exogenously administered mesenchymal stromal cells: current insights and future directions

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