NF-κB activation impairs somatic cell reprogramming in ageing

Abstract: Ageing constitutes a critical impediment to somatic cell reprogramming. We have explored the regulatory mechanisms that constitute age-associated barriers, through derivation of induced pluripotent stem cells (iPSCs) from individuals with premature or physiological ageing. We demonstrate that NF-κB activation blocks the generation of iPSCs in ageing. We also show that NF-κB repression occurs during cell reprogramming towards a pluripotent state. Conversely, ageing-associated NF-κB hyperactivation impairs the g… Show more

“…4 Accordingly, we have provided evidence for a direct regulation of DOT1L and YY1 genes by NF-kB, and a striking over-expression of DOT1L in NGPS fibroblasts, suggesting that these proteins might be relevant effectors of NF-kB role in cellular reprogramming as well as in NF-kB-driven alterations. 2 Additionally, the administration of a specific DOT1L chemical inhibitor remarkably increased the reprogramming efficiency of NGPS fibroblasts. 2 Furthermore, the parallelism observed between rejuvenation and reprogramming enhancement through NF-kB inhibition suggested that DOT1L could be a novel target for rejuvenation-based approaches (Fig.…”

“…2 Additionally, the administration of a specific DOT1L chemical inhibitor remarkably increased the reprogramming efficiency of NGPS fibroblasts. 2 Furthermore, the parallelism observed between rejuvenation and reprogramming enhancement through NF-kB inhibition suggested that DOT1L could be a novel target for rejuvenation-based approaches (Fig. 1).…”

“…We also extended these results to cells from patients with other progeroid syndromes and from physiologically aged donors, thereby supporting the key relevance of NF-kB signaling in the maintenance of cellular identity. 2 Nevertheless, the putative NF-kB targets controlling this newly identified ageassociated reprogramming barrier were completely unknown. In this regard, previous studies have uncovered new chromatin-modifying proteins such as DOT1L and YY1 that function as reprogramming repressors.…”

“…2 The methylation of H3K79 by DOT1L which is a conserved epigenetic mark in many eukaryotic epigenomes, increases progressively along the aging process, suggesting that DOT1L might function as a vital clock, ticking the hours impassively. 6 The results discussed herein demonstrate the critical involvement of DOT1L in aging pathogenesis and provide the first in vivo evidence about the efficacy of DOT1L-inhibitory strategies to treat ageassociated alterations, demonstrating the utility of studying age-associated reprogramming barriers for the development of anti-aging therapies.…”

“…2 Our studies in this regard were first focused on the generation of iPSCs from fibroblasts of patients with NestorGuillermo progeria syndrome (NGPS), a severe disease caused by a homozygous mutation in the BANF1 gene (c.34G>C; p.A12T). 3 We found that NGPS fibroblasts showed an increased NF-kB signaling in comparison with control cells, which could contribute to their premature senescence phenotype.…”

Reprogramming aging through DOT1L inhibition

“…4 Accordingly, we have provided evidence for a direct regulation of DOT1L and YY1 genes by NF-kB, and a striking over-expression of DOT1L in NGPS fibroblasts, suggesting that these proteins might be relevant effectors of NF-kB role in cellular reprogramming as well as in NF-kB-driven alterations. 2 Additionally, the administration of a specific DOT1L chemical inhibitor remarkably increased the reprogramming efficiency of NGPS fibroblasts. 2 Furthermore, the parallelism observed between rejuvenation and reprogramming enhancement through NF-kB inhibition suggested that DOT1L could be a novel target for rejuvenation-based approaches (Fig.…”

“…2 Additionally, the administration of a specific DOT1L chemical inhibitor remarkably increased the reprogramming efficiency of NGPS fibroblasts. 2 Furthermore, the parallelism observed between rejuvenation and reprogramming enhancement through NF-kB inhibition suggested that DOT1L could be a novel target for rejuvenation-based approaches (Fig. 1).…”

“…We also extended these results to cells from patients with other progeroid syndromes and from physiologically aged donors, thereby supporting the key relevance of NF-kB signaling in the maintenance of cellular identity. 2 Nevertheless, the putative NF-kB targets controlling this newly identified ageassociated reprogramming barrier were completely unknown. In this regard, previous studies have uncovered new chromatin-modifying proteins such as DOT1L and YY1 that function as reprogramming repressors.…”

“…2 The methylation of H3K79 by DOT1L which is a conserved epigenetic mark in many eukaryotic epigenomes, increases progressively along the aging process, suggesting that DOT1L might function as a vital clock, ticking the hours impassively. 6 The results discussed herein demonstrate the critical involvement of DOT1L in aging pathogenesis and provide the first in vivo evidence about the efficacy of DOT1L-inhibitory strategies to treat ageassociated alterations, demonstrating the utility of studying age-associated reprogramming barriers for the development of anti-aging therapies.…”

“…2 Our studies in this regard were first focused on the generation of iPSCs from fibroblasts of patients with NestorGuillermo progeria syndrome (NGPS), a severe disease caused by a homozygous mutation in the BANF1 gene (c.34G>C; p.A12T). 3 We found that NGPS fibroblasts showed an increased NF-kB signaling in comparison with control cells, which could contribute to their premature senescence phenotype.…”

Reprogramming aging through DOT1L inhibition

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