DNMT1 maintains progenitor function in self-renewing somatic tissue

Sen, George L.; Reuter, Jason; Webster, Daniel E.; Zhu, Lilly; Khavari, Paul A.

doi:10.1038/nature08683

Cited by 401 publications

(450 citation statements)

References 37 publications

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“…This review will focus primarily on changes in histone modifications. However, we also note that regulators of DNA methylation are required for the function of a variety of adult stem cells (Zhao et al, 2003;Ma et al, 2009;Trowbridge et al, 2009;Sen et al, 2010;Trowbridge and Orkin, 2010;Wu et al, 2010), and that they complex with chromatin modifiers to elicit changes in chromatin state (Jones et al, 1998;Nan et al, 1998;Fuks et al, 2003). In addition, chromatin remodeling factors are also important for stem and progenitor cell function (Lessard et al, 2007;Ho et al, 2009;Ho and Crabtree, 2010), suggesting that several epigenetic mechanisms could coordinately control adult stem cell gene expression programs during organismal aging.…”

Section: Epigenetic Regulation Of Aging Stem Cellsmentioning

confidence: 73%

Epigenetic regulation of aging stem cells

2011

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Section: Epigenetic Regulation Of Aging Stem Cellsmentioning

confidence: 73%

Epigenetic regulation of aging stem cells

2011

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“…We now clearly demonstrate a crucial role for CD98hc in maintaining basal keratinocyte functions throughout the epidermis, including IFE and HF, via its ability to mediate integrin signaling. Because most of the human malignancies arise in actively self-renovating sites of epithelial tissues (Sen et al, 2010), integrin signaling is thought to play an important role in formation and maintenance of epithelial cancers (White et al, 2004;Kass et al, 2007). Considering the physiological role of CD98hc in mammalian epithelial tissue formation and homeostasis, and the fact that enhanced expression of CD98hc epithelial neoplasias is indicative of malignant evolution (Cantor and Ginsberg, 2012), it could be hypothesized that novel studies on such a multifunctional protein would pave the way to new discoveries.…”

Section: Discussionmentioning

confidence: 99%

CD98hc (SLC3A2) regulation of skin homeostasis wanes with age

Boulter¹,

Estrach²,

Errante³

et al. 2013

J Cell Biol

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Skin aging is linked to reduced epidermal proliferation and general extracellular matrix atrophy. This involves factors such as the cell adhesion receptors integrins and amino acid transporters. CD98hc (SLC3A2), a heterodimeric amino acid transporter, modulates integrin signaling in vitro. We unravel CD98hc functions in vivo in skin. We report that CD98hc invalidation has no appreciable effect on cell adhesion, clearly showing that CD98hc disruption phenocopies neither CD98hc knockdown in cultured keratinocytes nor epidermal 1 integrin loss in vivo. Instead, we show that CD98hc deletion in murine epidermis results in improper skin homeostasis and epidermal wound healing. These defects resemble aged skin alterations and correlate with reduction of CD98hc expression observed in elderly mice. We also demonstrate that CD98hc absence in vivo induces defects as early as integrin-dependent Src activation. We decipher the molecular mechanisms involved in vivo by revealing a crucial role of the CD98hc/integrins/Rho guanine nucleotide exchange factor (GEF) leukemia-associated RhoGEF (LARG)/RhoA pathway in skin homeostasis. Finally, we demonstrate that the deregulation of RhoA activation in the absence of CD98hc is also a result of impaired CD98hc-dependent amino acid transports.

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“…To test whether the downregulation of miR-200 family members in SNU484-LPCX cells resulted from miR-200 promoter hypermethylation, we treated SNU484-LPCX cells with 5-aza-2 0 -deoxycytidine. 5-aza-2 0 -deoxycytidine is an irreversible inhibitor of maintenance DNA methyltransferase, which is an enzyme that transfers methyl groups to newly synthesized DNA strands (Sen et al, 2010). Treatment with 5-aza-2 0 -deoxycytidine for 4 days did not increase the expression of miR-200 family members in SNU484-LPCX cells, indicating that promoter hypermethylation is not involved in the downregulation of miR-200 family member expression in SNU484-LPCX cells (Supplementary Figure 7).…”

Section: Regulation Of the Mir-200 Promoter By Smad3mentioning

confidence: 99%

Smad3 regulates E-cadherin via miRNA-200 pathway

Ahn

Young

et al. 2011

Oncogene

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To identify potential microRNA (miRNA) links between Smad3, a mediator of TGF-b (transforming growth factor-b) signaling, and E-cadherin, we characterized the miRNA profiles of two gastric cancer cell lines: SNU484-LPCX, which does not express Smad3, and SNU484-Smad3, in which Smad3 is overexpressed. We found that among differentially expressed miRNAs, miR-200 family members are overexpressed in SNU484-Smad3 cells. Subsequent studies, including analysis of the effects of silencing Smad3 in SNU484-Smad3 cells and a luciferase reporter assay, revealed that Smad3 directly binds to a Smad-binding element located in the promoter region of miR-200b/a, where it functions as a transcriptional activator. TGF-b did not affect the regulatory role of Smad3 in transcription of miR-200 and expression of epithelial-mesenchymal transition markers. We conclude that Smad3 regulates, at the transcriptional level, miR-200 family members, which themselves regulate ZEB1 and ZEB2, known transcriptional repressors of E-cadherin, at the posttranscriptional level in a TGF-b-independent manner. This represents a novel link between Smad3 and posttranscriptional regulation by miRNAs in epithelial-mesenchymal transition in gastric cancer cells.

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DNMT1 maintains progenitor function in self-renewing somatic tissue

Cited by 401 publications

References 37 publications

Epigenetic regulation of aging stem cells

Epigenetic regulation of aging stem cells

CD98hc (SLC3A2) regulation of skin homeostasis wanes with age

Smad3 regulates E-cadherin via miRNA-200 pathway

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