Epigenetic and in vivo comparison of diverse MSC sources reveals an endochondral signature for human hematopoietic niche formation

Reinisch, Andreas; Etchart, Nathalie; Thomas, Daniel; Hofmann, Nicole A.; Fruehwirth, Margareta; Sinha, Subarna; Chan, Charles K.; Senarath-Yapa, Kshemendra; Seo, Eun Young; Wearda, Taylor; Hartwig, Udo F.; Beham‐Schmid, Christine; Trajanoski, Slave; Lin, Qiong; Wagner, Wolfgang; Dullin, Christian; Alves, Frauke; Andreeff, Michael; Weissman, Irving L.; Longaker, Michael T.; Schallmoser, Katharina; Majeti, Ravindra; Strunk, Dirk

doi:10.1182/blood-2014-04-572255

Cited by 207 publications

(250 citation statements)

References 49 publications

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“…Similarly, Noël et al [81] showed by microarray from Passage 1 (P1) BM-MSC and Ad-MSC that genes involved in chondro/osteogenesis, such as HES1, DLX5, TWIST1, BGLAP, OSX, SOX9, WNT5A, TGFΒ1 and VEGF were upregulated in BM-MSC. These results were confirmed recently in Reinisch et al [47] , which showed that genes related to chondro/osteogenesis such as RUNX2, RUNX3, BGLAP, MMP13, ITGA10, DLX5, DLX6, SPP1, BGLAP, ALPL, SPP1, COL2A, COL10A, and ACAN were upregulated in BM-MSC compared to Ad-MSC. The same researchers also confirmed that hemato/angiogenic genes such as INHBA, FZD1, TLR4, DGFC, ANGPT1, VEGFA, CTGF, and VEGFC were also upregulated in BM-MSC, confirming Brocher's results [42,47] .…”

Section: Bm-msc and Ad-msc Gene Signaturesupporting

confidence: 78%

“…The analysis of this literature underlines considerable variations between results obtained from different research teams that may be linked to the heterogeneity in (i) donors and donors' characteristics (e.g., health status, gender, age), (ii) in vitro/ex vivo protocols (e.g., sample isolation sites and methods, [33][34][35][36][37][38] , which represents the most robust comparison as they are not biased by inter-individual variabilities, in particular age, gender and health status. Nine studies comparing age-matched donors were also retained, which include 1 study on female donors only [39] , 1 study on 50% male and 50% female donors [40] , 2 studies on a close but not identical number of females and males [41,42] , and 5 studies on donors matched for age but without specifying the gender [43][44][45][46][47] . Finally, 4 studies compared the two types of MSC isolated from healthy donors, but with unknown age and gender [48][49][50][51] .…”

Section: Methodsmentioning

confidence: 99%

“…Therefore, only 4 papers were kept for this review. In these articles, BM-and Ad-MSC were expanded with a known and limited number of passages (P1 to P3), were grown in minimal conditions without induction towards lineage and were directly compared [39,42,47,81] .…”

Section: Bm-msc and Ad-msc Gene Signaturementioning

confidence: 99%

“…According to the selection criteria of this review (i.e., age and gender matching donors), 6 articles have been selected [39,[42][43][44]47,81] . From these 6 publications however, 2 were discarded because the number of cell passages was either too large or not clearly specified [43] (using P2 to P6 cells without additional clarification), which can cause artefactual background, or because the comparison was not performed with non-induced BM-MSC and Ad-MSC (comparing only differentiated cells) [44] .…”

Section: Bm-msc and Ad-msc Gene Signaturementioning

confidence: 99%

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Cell therapy for bone fracture repair: A comparative preclinical review of mesenchymal stromal cells from bone marrow and from adipose tissue

et al. 2015

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Abstract:Over the last decade, there has been an increasing interest among researchers for human mesenchymal stromal cells (MSC). Their regenerative properties, multilineage differentiation capacity and immunomodulatory properties make them promising candidates for treatment in various conditions. Emerging biotechnology companies specialized in cellular and regenerative therapies have been focusing their interest on MSC-based therapies, and their use in clinical trials has steadily increased. Notably, MSC are currently tested in clinical trials addressing unmet medical needs in the field of bone fracture repair and more specifically in non-union and delayed union fractures where the bone repair process is impaired. Although MSC can be isolated from various tissues, the most commonly studied sources are bone marrow (BM) and adipose tissue (Ad). In this article, we reviewed the literature directly comparing BM-and Ad-MSC for their in vitro characteristics and in vivo osteogenic potential to determine which source of MSC would be more appropriate for bone fracture repair. As considerable variations in experimental settings between studies were found, our review was based on studies meeting specific sets of criteria, notably regarding donors' age and gender. This review of side-by-side comparisons suggests that while BM-and Ad-MSC share common general characteristics, BM-MSC have a higher intrinsic osteogenic capacity in vitro and bone repair potential in vivo. Keywords: adipose tissue-derived mesenchymal stromal cells, bone marrow-derived mesenchymal stromal cells, MSC, proliferation, yield, immunophenotype, osteogenic differentiation, in vivo, preclinical, regenerative medicine, cell therapy, human, review *Correspondence to: Enrico Bastianelli, Bone Therapeutics S.A., PWTC, 37 rue Auguste Piccard, 6041 Gosselies, Belgium; Email: enrico.bastianelli@bonetherapeutics.com All authors contributed equally to this work.

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Section: Bm-msc and Ad-msc Gene Signaturesupporting

confidence: 78%

Section: Methodsmentioning

confidence: 99%

Section: Bm-msc and Ad-msc Gene Signaturementioning

confidence: 99%

Section: Bm-msc and Ad-msc Gene Signaturementioning

confidence: 99%

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Cell therapy for bone fracture repair: A comparative preclinical review of mesenchymal stromal cells from bone marrow and from adipose tissue

et al. 2015

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“…Charles Chan has led our group in finding the mouse skeletal stem cell (SSC) that not only selfrenews but also gives rise at the single-cell level to osteocytes, chondrocytes, and up to four distinct marrow stromal cells (124). Placed under the kidney capsule in large cell numbers, SSCs form bone and cartilage in a morphologically correct manner (124)(125)(126)(127), with a bone marrow cavity containing host-derived HSCs and blood vessels. Of the stromal cell subsets, at least one was in the Whitlock clones (121), and at least three of the stroma support HSCs and hematopoiesis (124-127).…”

Section: Wwwannualreviewsorg • How One Thing Led To Anothermentioning

confidence: 99%

How One Thing Led to Another

Weissman

2016

Annu. Rev. Immunol.

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I started research in high school, experimenting on immunological tolerance to transplantation antigens. This led to studies of the thymus as the site of maturation of T cells, which led to the discovery, isolation, and clinical transplantation of purified hematopoietic stem cells (HSCs). The induction of immune tolerance with HSCs has led to isolation of other tissue-specific stem cells for regenerative medicine. Our studies of circulating competing germline stem cells in colonial protochordates led us to document competing HSCs. In human acute myelogenous leukemia we showed that all preleukemic mutations occur in HSCs, and determined their order; the final mutations occur in a multipotent progenitor derived from the preleukemic HSC clone. With these, we discovered that CD47 is an upregulated gene in all human cancers and is a “don't eat me” signal; blocking it with antibodies leads to cancer cell phagocytosis. CD47 is the first known gene common to all cancers and is a target for cancer immunotherapy.

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Early molecular events duringin vitrochondrogenesis

Karlsen

Jakobsen

Brinchmann

2016

The Biology and Therapeutic Application of Mesenchymal Cells

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Epigenetic and in vivo comparison of diverse MSC sources reveals an endochondral signature for human hematopoietic niche formation

Abstract: Key Points Epigenetics and in vivo behavior can distinguish MSCs from different sources. BM-derived MSCs form a hematopoietic niche via a vascularized cartilage intermediate.

Cited by 207 publications

References 49 publications

Cell therapy for bone fracture repair: A comparative preclinical review of mesenchymal stromal cells from bone marrow and from adipose tissue

Cell therapy for bone fracture repair: A comparative preclinical review of mesenchymal stromal cells from bone marrow and from adipose tissue

How One Thing Led to Another

Early molecular events duringin vitrochondrogenesis

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