Infrapatellar fat pad-derived mesenchymal stem cell-based spheroids enhance their therapeutic efficacy to reverse synovitis and fat pad fibrosis

Dimitrios Kouroupis; Melissa A. Willman; Thomas M. Best; Lee D. Kaplan; Diego Correa

doi:10.1186/s13287-020-02107-6

Stem Cell Research & Therapy (Jan 2021)

Infrapatellar fat pad-derived mesenchymal stem cell-based spheroids enhance their therapeutic efficacy to reverse synovitis and fat pad fibrosis

Dimitrios Kouroupis,
Melissa A. Willman,
Thomas M. Best,
Lee D. Kaplan,
Diego Correa

Affiliations

Dimitrios Kouroupis: Department of Orthopedics, UHealth Sports Medicine Institute, University of Miami, Miller School of Medicine
Melissa A. Willman: Diabetes Research Institute & Cell Transplantation Center, University of Miami, Miller School of Medicine
Thomas M. Best: Department of Orthopedics, UHealth Sports Medicine Institute, University of Miami, Miller School of Medicine
Lee D. Kaplan: Department of Orthopedics, UHealth Sports Medicine Institute, University of Miami, Miller School of Medicine
Diego Correa: Department of Orthopedics, UHealth Sports Medicine Institute, University of Miami, Miller School of Medicine

DOI: https://doi.org/10.1186/s13287-020-02107-6
Journal volume & issue: Vol. 12, no. 1
pp. 1 – 19

Abstract

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Abstract Background To investigate the in vitro and in vivo anti-inflammatory/anti-fibrotic capacity of IFP-MSC manufactured as 3D spheroids. Our hypothesis is that IFP-MSC do not require prior cell priming to acquire a robust immunomodulatory phenotype in vitro in order to efficiently reverse synovitis and IFP fibrosis, and secondarily delay articular cartilage damage in vivo. Methods Human IFP-MSC immunophenotype, tripotentiality, and transcriptional profiles were assessed in 3D settings. Multiplex secretomes were assessed in IFP-MSC spheroids [Crude (non-immunoselected), CD146+ or CD146− immunoselected cells] and compared with 2D cultures with and without prior inflammatory/fibrotic cell priming. Functionally, IFP-MSC spheroids were assessed for their immunopotency on human PBMC proliferation and their effect on stimulated synoviocytes with inflammation and fibrotic cues. The anti-inflammatory and anti-fibrotic spheroid properties were further evaluated in vivo in a rat model of acute synovitis/fat pad fibrosis. Results Spheroids enhanced IFP-MSC phenotypic, transcriptional, and secretory immunomodulatory profiles compared to 2D cultures. Further, CD146+ IFP-MSC spheroids showed enhanced secretory and transcriptional profiles; however, these attributes were not reflected in a superior capacity to suppress activated PBMC. This suggests that 3D culturing settings are sufficient to induce an enhanced immunomodulatory phenotype in both Crude and CD146-immunoselected IFP-MSC. Crude IFP-MSC spheroids modulated the molecular response of synoviocytes previously exposed to inflammatory cues. Therapeutically, IFP-MSC spheroids retained substance P degradation potential in vivo, while effectively inducing resolution of inflammation/fibrosis of the synovium and fat pad. Furthermore, their presence resulted in arrest of articular cartilage degradation in a rat model of progressive synovitis and fat pad fibrosis. Conclusions 3D spheroids confer IFP-MSC a reproducible and enhanced immunomodulatory effect in vitro and in vivo, circumventing the requirement of non-compliant cell priming or selection before administration and thereby streamlining cell products manufacturing protocols.

Published in Stem Cell Research & Therapy

ISSN: 1757-6512 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Medicine: Medicine (General); Science: Chemistry: Organic chemistry: Biochemistry
Website: https://stemcellres.biomedcentral.com

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