Defining the mammalian CArGome

Sun, Qiang; Chen, Guang; Streb, Jeffrey W.; Long, Xiaochun; Yang, Yumei; Stoeckert, Christian J.; Miano, Joseph M.

doi:10.1101/gr.4108706

Cited by 267 publications

(290 citation statements)

References 68 publications

(97 reference statements)

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“…93 Interestingly, a CArG box in the human T-cell leukemia virus-1 that deviates from the conventional sequences, shown in Figure 1, was shown to bind to and be activated by SRF. 94 This would suggest that the full complement of SRF-binding sites in the genome (ie, CArGome 22 ) may be more diverse than previously thought. Indeed, several putative SRF-binding 'CArG boxes' derived from genome-wide binding studies show sequences that diverge substantially from conventional CArG boxes.…”

Section: Srf and Hematopoietic System Diseasementioning

confidence: 92%

“…Cells of the dentate gyrus showed a reduction in F-actin, and biochemical data indicated decreases in gelsolin and altered phosphorylation of cofilin, two regulators of cytoskeletal dynamics. While both cofilin genes are direct targets of SRF, 22 the nature of SRF-dependent gelsolin expression is incompletely understood. SRF deletion in the perinatal hippocampus resulted in poor organization and aberrant synapses of the so-called mossy fibers, apparently because of their inability to respond appropriately to guidance cues that drive proper neuronal cell migration and organization.…”

Section: Srf and Nervous System Disease Central Nervous Systemmentioning

confidence: 99%

“…[19][20][21][22][23][24][25][26] Bioinformatic and wet-lab assays have disclosed a disproportionate number of SRFtarget genes encoding for elements of the actin cytoskeleton. 20,22,23,26 Evidence for the role of SRF in cytoskeletal processes stems from genetic ablation studies using slug, fly, and worm where loss of SRF function leads to defective animal/cellular locomotion (reviewed by Miano et al 27 ). In fact, SRF is essential for life processes in every species where it has been inactivated, including mice where global loss of SRF leads to incomplete gastrulation and embryonic arrest before organogenesis commences.…”

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confidence: 99%

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Role of serum response factor in the pathogenesis of disease

Miano

2010

Laboratory Investigation

118

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Serum response factor (SRF) is a ubiquitously expressed transcription factor that binds to a DNA cis element known as the CArG box, which is found in the proximal regulatory regions of over 200 experimentally validated target genes. Genetic deletion of SRF is incompatible with life in a variety of animals from different phyla. In mice, loss of SRF throughout the early embryo results in gastrulation defects precluding analyses in individual organ systems. Genetic inactivation studies using conditional or inducible promoters directing the expression of the bacteriophage Cre recombinase have shown a vital role for SRF in such cellular processes as contractility, cell migration, synaptic activity, inflammation, and cell survival. A growing number of experimental and human diseases are associated with changes in SRF expression, suggesting that SRF has a role in the pathogenesis of disease. This review summarizes data from experimental model systems and human pathology where SRF expression is either deliberately or naturally altered. Genomic DNA is a quaternary code comprising proteincoding and non-protein-coding sequences. While the protein-coding sequences are well-defined and increasingly understood, we are only beginning to elucidate the hidden information within the vast landscape of the non-proteincoding sequences. The field of comparative genomics has facilitated the identification of transcription factor-binding sites (TFBS) and microRNAs (miRs), which, aside from repetitive DNA sequences, are among the more easily decipherable non-protein-coding sequences in the human genome. Together, TFBS and miRs have essential roles in cell fate determination and cellular homeostasis of most life forms. Sequence variations (eg, single-nucleotide polymorphisms, SNPs) in the TFBS, miRs, and miR target sequences alter gene/protein expression and thus disturb homeostasis leading to disease. 1-4 A major imperative, therefore, is decoding the non-protein-coding genome relating to gene regulation to gain a full understanding of how DNA-binding transcription factors and the estimated one million or more TFBS direct normal biological processes.Serum response factor (SRF) is the founding member of the MADS-box family of transcription factors 5 and is one of the best understood DNA-binding proteins in the human proteome. The DNA-binding properties of SRF and its molecular cloning were first defined in the laboratory of Richard Treisman. 6,7 SRF has relatively low intrinsic transcriptional activity, but its interaction with over 60 cofactors confers strong transactivation potential in a cell-and context-specific manner. At least two major signaling pathways converge upon SRF to direct the programs of gene expression. 8,9 The classic pathway involves growth factor stimulation and mitogen-activated protein kinase signaling leading to the phosphorylation of the SRF cofactor, ELK1, and the activation of growth-related genes. 10,11 The second regulatory pathway occurs through Rho-dependent changes in actin dynamics. 12 In this pathway, si...

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Section: Srf and Hematopoietic System Diseasementioning

confidence: 92%

Section: Srf and Nervous System Disease Central Nervous Systemmentioning

confidence: 99%

mentioning

confidence: 99%

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Role of serum response factor in the pathogenesis of disease

Miano

2010

Laboratory Investigation

118

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“…This may rule out a predominant role of Srf or Mal in their transcriptional regulation in Mks, in contrast to other cell types. 7,20 Expression level of Kindlin-3, which is abundantly expressed in Mks and platelets, was also unaffected. Expression levels were normalized to Gapdh and results were expressed relative to the level of each gene in wild-type Mks (set to 1) (n ¼ 3 per genotype).…”

Section: Po005 By Mann-whitney Test)mentioning

confidence: 93%

The serum response factor (SRF)/megakaryocytic acute leukemia (MAL) network participates in megakaryocyte development

et al. 2010

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“…Levels of cofilin phosphorylation following organ culture were similar in stretched WT and KO portal veins and were reduced to Ͻ50% in the absence of stretch in both genotypes. Expression of the cofilin gene is, like SM22 and desmin, regulated by myocardin and serum response factor (25), and the protein level of cofilin is therefore sensitive to mechanical stretch (3). Furthermore, the Rho kinase inhibitor Y-27632 had similar effects on contractile responses in depolarized WT and KO portal veins.…”

Section: Discussionmentioning

confidence: 99%

Differential dependence of stretch and shear stress signaling on caveolin-1 in the vascular wall

Albinsson¹,

Nordström²,

Swärd³

et al. 2008

American Journal of Physiology-Cell Physiology

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The role of caveolae in stretch- versus flow-induced vascular responses was investigated using caveolin 1-deficient [knockout (KO)] mice. Portal veins were stretched longitudinally for 5 min (acute) or 72 h (organ culture). Basal ERK1/2 and Akt phosphorylation were increased in organ-cultured KO veins, as were protein synthesis and vessel wall cross sections. Stretch stimulated acute phosphorylation of ERK1/2 and long-term phosphorylation of focal adhesion kinase (FAK) and cofilin but did not affect Akt phosphorylation. Protein synthesis, and particularly synthesis of smooth muscle differentiation markers, was increased by stretch. These effects did not differ in portal veins from KO and control mice, which also showed the same contractile response to membrane depolarization and inhibition by the Rho kinase inhibitor Y-27632. KO carotid arteries had increased wall cross sections and responded to pressurization (120 mmHg) for 1 h with increased ERK1/2 but not Akt phosphorylation, similar to control arteries. Shear stress by flow for 15 min, on the other hand, increased phosphorylation of Akt in carotids from control but not KO mice. In conclusion, caveolin 1 contributes to low basal ERK1/2 and Akt activity and is required for Akt-dependent signals in response to shear stress (flow) but is not essential for trophic effects of stretch (pressure) in the vascular wall.

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Defining the mammalian CArGome

Cited by 267 publications

References 68 publications

Role of serum response factor in the pathogenesis of disease

Role of serum response factor in the pathogenesis of disease

The serum response factor (SRF)/megakaryocytic acute leukemia (MAL) network participates in megakaryocyte development

Differential dependence of stretch and shear stress signaling on caveolin-1 in the vascular wall

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