Transcriptional Regulation of the <i>SCL</i> Locus: Identification of an Enhancer That Targets the Primitive Erythroid Lineage In Vivo

Delabesse, Éric; Ogilvy, Sarah; Chapman, Michael A.; Piltz, Sandie; Göttgens, Berthold; Green, Anthony

doi:10.1128/mcb.25.12.5215-5225.2005

Cited by 57 publications

(93 citation statements)

References 73 publications

(65 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Previous systematic analysis of the 50 kb of the mouse Tal1/ Pdzk1ip1 coregulatory domain ‫01מ(‬ kb to +40 kb relative to promoter 1a) has identified multiple Tal1 regulatory elements Sinclair et al 1999;Göttgens et al 2000Göttgens et al , 2002aDelabesse et al 2005). Within this well-characterized region, two novel DNaseI hypersensitive sites were identified as significantly enriched (+29 and +32) and investigated in functional assays.…”

Section: Resultsmentioning

confidence: 99%

“…Elements at +1 and +3, relative to the mouse exon 1a, have been shown to target the expression of Tal1 to the developing spinal cord in transgenic mice , while the +23 directs expression to specific regions within the brain (Göttgens et al 2000). The region at ‫9מ‬ functions as an enhancer in hematopoietic cell lines , and the +40 region is active in the primitive erythroid lineage (Delabesse et al 2005). The mouse +12 region is homologous to the human +14 region, which has been identified as an TAL1 transcriptional repressor (Courtes et al 2000).…”

Section: Resultsmentioning

confidence: 99%

“…The Tal1 (formerly known as Scl) locus was used to establish the protocol, which was then further validated by successfully mapping known DNaseI hypersensitive sites across 240 kb of the human ␣-globin locus. Previous studies have systematically dissected the transcriptional regulation of the mouse Tal1 locus and have identified multiple conserved regulatory elements that direct expression in transgenic mice to subdomains of the Tal1 expression pattern (Göttgens et al , 2000(Göttgens et al , 2002bSanchez et al 1999Sanchez et al , 2001Sinclair et al 1999;Delabesse et al 2005). Similarly, the regulatory elements within the ␣-globin locus have been extensively characterized using both biological and bioinformatics approaches (Yagi et al 1986;Higgs et al 1990;Vyas et al 1992;Hughes et al 2005).…”

mentioning

confidence: 99%

See 2 more Smart Citations

Identifying gene regulatory elements by genomic microarray mapping of DNaseI hypersensitive sites

Follows

Dhami²,

Göttgens³

et al. 2006

Genome Res.

View full text Add to dashboard Cite

The identification of cis-regulatory elements is central to understanding gene transcription. Hypersensitivity of cis-regulatory elements to digestion with DNaseI remains the gold-standard approach to locating such elements. Traditional methods used to identify DNaseI hypersensitive sites are cumbersome and can only be applied to short stretches of DNA at defined locations. Here we report the development of a novel genomic array-based approach to DNaseI hypersensitive site mapping (ADHM) that permits precise, large-scale identification of such sites from as few as 5 million cells. Using ADHM we identified all previously recognized hematopoietic regulatory elements across 200 kb of the mouse T-cell acute lymphocytic leukemia-1 (Tal1) locus, and, in addition, identified two novel elements within the locus, which show transcriptional regulatory activity. We further validated the ADHM protocol by mapping the DNaseI hypersensitive sites across 250 kb of the human TAL1 locus in CD34 + primary stem/progenitor cells and K562 cells and by mapping the previously known DNaseI hypersensitive sites across 240 kb of the human ␣-globin locus in K562 cells. ADHM provides a powerful approach to identifying DNaseI hypersensitive sites across large genomic regions.

show abstract

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

mentioning

confidence: 99%

See 1 more Smart Citation

Identifying gene regulatory elements by genomic microarray mapping of DNaseI hypersensitive sites

Follows

Dhami²,

Göttgens³

et al. 2006

Genome Res.

View full text Add to dashboard Cite

show abstract

“…Previous studies, such as those of the globin gene loci (77)(78)(79)(80)(81), the GATA1 and SCL/Tal1 gene loci (82)(83)(84)(85)(86)(87)(88)(89)(90)(91)(92)(93), and the erythropoietin gene locus (83), characterized enhancers as distantly located, positively acting cis-regulatory elements (77,80). Recent studies have shown that enhancers have additional, complex roles in cellular gene regulation.…”

Section: Discussionmentioning

confidence: 99%

Identification of Biologically Relevant Enhancers in Human Erythroid Cells

Steiner

Bogardus

et al. 2013

Journal of Biological Chemistry

View full text Add to dashboard Cite

Background: Programs of cellular development and differentiation are controlled by enhancers. Results: Human erythroid cell type-specific enhancers are marked by p300 and groups of transcription factors. Conclusion: Enhancers are important regulators of species-specific erythroid cell structure and function. Significance: Deciphering how nonpromoter regulatory elements control gene expression in erythroid cells is important for understanding inherited and acquired hematologic disease.

show abstract

“…If the regulatory proteins of a cell as a whole are considered an input, the output is determined by the DNA sequences of the CRMs and their accessibility to transcription factor complex binding. Therefore in terms of a pression that mirrors the developmental and spatial expression patterns of the endogenous genes they regulate (Delabesse et al, 2005;Gottgens et al, 2000;Gottgens et al, 2004;Sanchez et al, 1999;Silberstein et al, 2005). Genes are equipped with multiple, disparate CRMs, each several hundred base pairs long.…”

Section: Overviewmentioning

confidence: 99%

Gene regulatory networks governing haematopoietic stem cell development and identity

Pimanda¹,

Göttgens²

2010

Int. J. Dev. Biol.

View full text Add to dashboard Cite

Development can be viewed as a dynamic progression through regulatory states which characterise the various cell types within a given differentiation cascade. To understand the progression of regulatory states that define the origin and subsequent development of haematopoietic stem cells, the first imperative is to understand the ontogeny of haematopoiesis. We are fortunate that the ontogeny of blood development is one of the best characterized mammalian developmental systems. However, the field is still in its infancy with regard to the reconstruction of gene regulatory networks and their interactions with cell signalling cascades that drive a mesodermal progenitor to adopt the identity of a haematopoietic stem cell and beyond. Nevertheless, a framework to dissect these networks and comprehend the logic of its circuitry does exist and although they may not as yet be available, a sense for the tools that will be required to achieve this aim is also emerging. In this review we cover the fundamentals of network architecture, methods used to reconstruct networks, current knowledge of haematopoietic and related transcriptional networks, current challenges and future outlook.

show abstract

Transcriptional Regulation of the SCL Locus: Identification of an Enhancer That Targets the Primitive Erythroid Lineage In Vivo

Cited by 57 publications

References 73 publications

Identifying gene regulatory elements by genomic microarray mapping of DNaseI hypersensitive sites

Identifying gene regulatory elements by genomic microarray mapping of DNaseI hypersensitive sites

Identification of Biologically Relevant Enhancers in Human Erythroid Cells

Gene regulatory networks governing haematopoietic stem cell development and identity

Contact Info

Product

Resources

About