Targeting of chondrocyte plasticity via connexin43 modulation attenuates cellular senescence and fosters a pro-regenerative environment in osteoarthritis

Varela‐Eirin, Marta; Varela-Vázquez, Adrián; Guitián-Caamaño, Amanda; Paı́no, Carlos Luis; Mato, Virginia; Largo, Raquel; Aasen, Trond; Tabernero, Arantxa; Fonseca, Eduardo; Kandouz, Mustapha; Caeiro, José Ramón; Blanco, Alfonso; Mayán, M.D.

doi:10.1038/s41419-018-1225-2

Cited by 71 publications

(66 citation statements)

References 114 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Reduced Cx43 is considered a marker for senescence in fibroblasts [285], glomerular mesangial cells [286], and hematopoietic stem cells (HSCs) [287], although upregulation of Cx43 increases senescence of chondrocytes [288]. Cx43 prevents senescence in HSCs by forming Fig.…”

Section: Connexin 43mentioning

confidence: 99%

Mitochondria and metabolic transitions in cardiomyocytes: lessons from development for stem cell-derived cardiomyocytes

Garbern

Lee

2021

Stem Cell Res Ther

View full text Add to dashboard Cite

Current methods to differentiate cardiomyocytes from human pluripotent stem cells (PSCs) inadequately recapitulate complete development and result in PSC-derived cardiomyocytes (PSC-CMs) with an immature or fetal-like phenotype. Embryonic and fetal development are highly dynamic periods during which the developing embryo or fetus is exposed to changing nutrient, oxygen, and hormone levels until birth. It is becoming increasingly apparent that these metabolic changes initiate developmental processes to mature cardiomyocytes. Mitochondria are central to these changes, responding to these metabolic changes and transitioning from small, fragmented mitochondria to large organelles capable of producing enough ATP to support the contractile function of the heart. These changes in mitochondria may not simply be a response to cardiomyocyte maturation; the metabolic signals that occur throughout development may actually be central to the maturation process in cardiomyocytes. Here, we review methods to enhance maturation of PSC-CMs and highlight evidence from development indicating the key roles that mitochondria play during cardiomyocyte maturation. We evaluate metabolic transitions that occur during development and how these affect molecular nutrient sensors, discuss how regulation of nutrient sensing pathways affect mitochondrial dynamics and function, and explore how changes in mitochondrial function can affect metabolite production, the cell cycle, and epigenetics to influence maturation of cardiomyocytes.

show abstract

Section: Connexin 43mentioning

confidence: 99%

Mitochondria and metabolic transitions in cardiomyocytes: lessons from development for stem cell-derived cardiomyocytes

Garbern

Lee

2021

Stem Cell Res Ther

View full text Add to dashboard Cite

show abstract

“…Cellular senescence is regarded as detrimental for tissue repair and regeneration since it induces replicative aging in cells, which directly contributes to their loss of regenerative capacity in tissue repair . Additionally, SASP proteins released by senescent cells can disrupt tissue homeostasis and potentially act on neighboring cells in a paracrine signaling manner . Thus, induction of cell senescence in the reprograming of fibroblast into OB appears contradictory.…”

Section: Discussionmentioning

confidence: 99%

“…[43][44][45][46] Additionally, SASP proteins released by senescent cells can disrupt tissue homeostasis and potentially act on neighboring cells in a paracrine signaling manner. 45,[47][48][49] Thus, induction of cell senescence in the reprograming of fibroblast into OB appears contradictory. Nevertheless, emerging evidence in embryonic and adult tissues indicates that cell senescence is beneficial in tissue homeostasis.…”

Section: Discussionmentioning

confidence: 99%

Reprogramming of human fibroblasts into osteoblasts by insulin-like growth factor-binding protein 7

Chiu

Lee

et al. 2020

Stem Cells Translational Medicine

View full text Add to dashboard Cite

The induced pluripotent stem cell (iPSC) is a promising cell source for tissue regeneration. However, the therapeutic value of iPSC technology is limited due to the complexity of induction protocols and potential risks of teratoma formation. A trans‐differentiation approach employing natural factors may allow better control over reprogramming and improved safety. We report here a novel approach to drive trans‐differentiation of human fibroblasts into functional osteoblasts using insulin‐like growth factor binding protein 7 (IGFBP7). We initially determined that media conditioned by human osteoblasts can induce reprogramming of human fibroblasts to functional osteoblasts. Proteomic analysis identified IGFBP7 as being significantly elevated in media conditioned with osteoblasts compared with those with fibroblasts. Recombinant IGFBP7 induced a phenotypic switch from fibroblasts to osteoblasts. The switch was associated with senescence and dependent on autocrine IL‐6 signaling. Our study supports a novel strategy for regenerating bone by using IGFBP7 to trans‐differentiate fibroblasts to osteoblasts.

show abstract

“…For example, deletion of the gap junction channel protein connexin43 attenuates cellular senescence and promotes chondrocyte regeneration in osteoarthritis. 46 The power of CRISPR-mediated gene deletion to ‘cleanly’ dissect the contribution of closely related family members to cartilage biology was nicely demonstrated in a study of the WNT signalling pathway members. 47 Here, CRISPR was used to delete three WNT family members independently, thereby allowing the investigators to separately determine the contribution of each WNT factor to chondrocyte differentiation.…”

Section: Crispr Applications In Basic Orthopaedic Researchmentioning

confidence: 99%

Applications of CRISPR for musculoskeletal research

Fitzgerald

2020

Bone & Joint Research

View full text Add to dashboard Cite

The ability to edit DNA at the nucleotide level using clustered regularly interspaced short palindromic repeats (CRISPR) systems is a relatively new investigative tool that is revolutionizing the analysis of many aspects of human health and disease, including orthopaedic disease. CRISPR, adapted for mammalian cell genome editing from a bacterial defence system, has been shown to be a flexible, programmable, scalable, and easy-to-use gene editing tool. Recent improvements increase the functionality of CRISPR through the engineering of specific elements of CRISPR systems, the discovery of new, naturally occurring CRISPR molecules, and modifications that take CRISPR beyond gene editing to the regulation of gene transcription and the manipulation of RNA. Here, the basics of CRISPR genome editing will be reviewed, including a description of how it has transformed some aspects of molecular musculoskeletal research, and will conclude by speculating what the future holds for the use of CRISPR-related treatments and therapies in clinical orthopaedic practice. Cite this article: Bone Joint Res 2020;9(7):351–359.

show abstract

Targeting of chondrocyte plasticity via connexin43 modulation attenuates cellular senescence and fosters a pro-regenerative environment in osteoarthritis

Cited by 71 publications

References 114 publications

Mitochondria and metabolic transitions in cardiomyocytes: lessons from development for stem cell-derived cardiomyocytes

Mitochondria and metabolic transitions in cardiomyocytes: lessons from development for stem cell-derived cardiomyocytes

Reprogramming of human fibroblasts into osteoblasts by insulin-like growth factor-binding protein 7

Applications of CRISPR for musculoskeletal research

Contact Info

Product

Resources

About