Mapping and Functional Analysis of Cis-regulatory Elements in Mouse Photoreceptors PDF Download
Are you looking for read ebook online? Search for your book and save it on your Kindle device, PC, phones or tablets. Download Mapping and Functional Analysis of Cis-regulatory Elements in Mouse Photoreceptors PDF full book. Access full book title Mapping and Functional Analysis of Cis-regulatory Elements in Mouse Photoreceptors by Andrew Everett Oliver Hughes. Download full books in PDF and EPUB format.
Author: Andrew Everett Oliver Hughes
Publisher:
ISBN:
Category : Electronic dissertations
Languages : en
Pages : 152
Get Book Here
Book Description
Photoreceptors are light-sensitive neurons that mediate vision, and they are the most commonly affected cell type in genetic forms of blindness. In mice, there are two basic types of photoreceptors, rods and cones, which mediate vision in dim and bright environments, respectively. The transcription factors (TFs) that control rod and cone development have been studied in detail, but the cis-regulatory elements (CREs) through which these TFs act are less well understood. To comprehensively identify photoreceptor CREs in mice and to understand their relationship with gene expression, we performed open chromatin (ATAC-seq) and transcriptome (RNA-seq) profiling of FACS-purified rods and cones. We find that rods have significantly fewer regions of open chromatin than cones (as well as >60 additional cell types and tissues), and we demonstrate that this uniquely closed chromatin architecture depends on the rod master regulator Nrl. Finally, we find that regions of rod- and cone-specific open chromatin are enriched for distinct sets of TF binding sites, providing insight into the cis-regulatory grammar of these cell types.We also sought to understand how the regulatory activity of rod and cone open chromatin regions is encoded in DNA sequence. Cone-rod homeobox (CRX) is a paired-like homeodomain TF and master regulator of both rod and cone development, and CRX binding sites are by far the most enriched TF binding sites in photoreceptor CREs. The in vitro DNA binding preferences of CRX have been extensively characterized, but how well in vitro models of TF binding site affinity predict in vivo regulatory activity is not known. In addition, paired-class homeodomain TFs bind DNA as both monomers and dimers, but whether monomeric and dimeric CRX binding sites have distinct regulatory activities is not known. To address these questions, we used a massively parallel reporter assay to quantify the activity of thousands native and mutant CRX binding sites in explanted mouse retinas. These data reveal that dimeric CRX binding sites encode stronger enhancers than monomeric CRX binding sites. Moreover, the activity of half-sites within dimeric CRX binding sites is cooperative and spacing-dependent. In addition, saturating mutagenesis of 195 CRX binding sites reveals that, while TF binding site affinity and activity are moderately correlated across mutations within individual CREs, they are poorly correlated across mutations from distinct CREs. Accordingly, we show that accounting for baseline CRE activity improves the prediction of the effects of mutations in regulatory DNA from sequence-based models. Taken together, these data demonstrate that the activity of CRX binding sites depends on multiple layers of sequence context, providing insight into photoreceptor gene regulation and illustrating functional principles of homeodomain TF binding sites.
Author: Andrew Everett Oliver Hughes
Publisher:
ISBN:
Category : Electronic dissertations
Languages : en
Pages : 152
Get Book Here
Book Description
Photoreceptors are light-sensitive neurons that mediate vision, and they are the most commonly affected cell type in genetic forms of blindness. In mice, there are two basic types of photoreceptors, rods and cones, which mediate vision in dim and bright environments, respectively. The transcription factors (TFs) that control rod and cone development have been studied in detail, but the cis-regulatory elements (CREs) through which these TFs act are less well understood. To comprehensively identify photoreceptor CREs in mice and to understand their relationship with gene expression, we performed open chromatin (ATAC-seq) and transcriptome (RNA-seq) profiling of FACS-purified rods and cones. We find that rods have significantly fewer regions of open chromatin than cones (as well as >60 additional cell types and tissues), and we demonstrate that this uniquely closed chromatin architecture depends on the rod master regulator Nrl. Finally, we find that regions of rod- and cone-specific open chromatin are enriched for distinct sets of TF binding sites, providing insight into the cis-regulatory grammar of these cell types.We also sought to understand how the regulatory activity of rod and cone open chromatin regions is encoded in DNA sequence. Cone-rod homeobox (CRX) is a paired-like homeodomain TF and master regulator of both rod and cone development, and CRX binding sites are by far the most enriched TF binding sites in photoreceptor CREs. The in vitro DNA binding preferences of CRX have been extensively characterized, but how well in vitro models of TF binding site affinity predict in vivo regulatory activity is not known. In addition, paired-class homeodomain TFs bind DNA as both monomers and dimers, but whether monomeric and dimeric CRX binding sites have distinct regulatory activities is not known. To address these questions, we used a massively parallel reporter assay to quantify the activity of thousands native and mutant CRX binding sites in explanted mouse retinas. These data reveal that dimeric CRX binding sites encode stronger enhancers than monomeric CRX binding sites. Moreover, the activity of half-sites within dimeric CRX binding sites is cooperative and spacing-dependent. In addition, saturating mutagenesis of 195 CRX binding sites reveals that, while TF binding site affinity and activity are moderately correlated across mutations within individual CREs, they are poorly correlated across mutations from distinct CREs. Accordingly, we show that accounting for baseline CRE activity improves the prediction of the effects of mutations in regulatory DNA from sequence-based models. Taken together, these data demonstrate that the activity of CRX binding sites depends on multiple layers of sequence context, providing insight into photoreceptor gene regulation and illustrating functional principles of homeodomain TF binding sites.
Author: Karen Ann Lawrence
Publisher:
ISBN:
Category : Electronic dissertations
Languages : en
Pages : 132
Get Book Here
Book Description
Crx is the principal transcription factor of the photoreceptor transcriptional network and is a key regulator of photoreceptor differentiation and survival. Mice mutant for Crx lack functional photoreceptors and are blind at birth. Mutations in human CRX are associated with several retinal diseases including autosomal dominant cone-rod dystrophy 2 and Leber's congenital amaurosis, a severe form of blindness in newborns. Given the importance of Crx in photoreceptor development and maintenance, genome-wide mapping of Crx binding sites was used to facilitate identification of photoreceptor cis-regulatory elements. ChIP-seq against Crx identified thousands of cis-regulatory regions around photoreceptor genes in adult mouse retina. Crx directly regulates downstream photoreceptor transcription factors and their target genes via a network of spatially distributed regulatory elements around each locus. Crx-bound regions act in a synergistic fashion to activate transcription and contain multiple Crx binding sites which interact in a spacing- and orientation-dependent manner to fine-tune transcript levels. Crx ChIP-seq was also performed on Nrl-/- retinas which represent an enriched source of cone photoreceptors. Comparison with the wild-type ChIP-seq dataset identified numerous rod- and cone-specific Crx-bound regions as well as many shared elements. Thus, Crx combinatorially orchestrates the transcriptional networks of both rods and cones by coordinating the expression of photoreceptor genes including most retinal disease genes. This study pinpoints thousands of non-coding regions of relevance to both Mendelian and complex retinal disease and allows prioritization of human retinal disease genes which has already resulted in identification of FAM161A and MAK, novel disease genes implicated in retinitis pigmentosa.
Author: Tapas Kumar Kundu
Publisher: Springer Science & Business Media
ISBN: 9400745257
Category : Medical
Languages : en
Pages : 698
Get Book Here
Book Description
Epigenetics fine-tunes the life processes dictated by DNA sequences, but also kick-starts pathophysiological processes including diabetes, AIDS and cancer. This volume tracks the latest research on epigenetics, including work on new-generation therapeutics.
Author: G. Berlucchi
Publisher: Springer Science & Business Media
ISBN: 3642654959
Category : Medical
Languages : en
Pages : 758
Get Book Here
Book Description
Author: Evelyne Sernagor
Publisher: Cambridge University Press
ISBN: 1139459732
Category : Medical
Languages : en
Pages : 369
Get Book Here
Book Description
This advanced text, first published in 2006, takes a developmental approach to the presentation of our understanding of how vertebrates construct a retina. Written by experts in the field, each of the seventeen chapters covers a specific step in the process, focusing on the underlying molecular, cellular, and physiological mechanisms. There is also a special section on emerging technologies, including genomics, zebrafish genetics, and stem cell biology that are starting to yield important insights into retinal development. Primarily aimed at professionals, both biologists and clinicians working with the retina, this book provides a concise view of vertebrate retinal development. Since the retina is 'an approachable part of the brain', this book will also be attractive to all neuroscientists interested in development, as processes required to build this exquisitely organized system are ultimately relevant to all other parts of the central nervous system.
Author: Kim-Anh Do
Publisher: Cambridge University Press
ISBN: 1107027527
Category : Mathematics
Languages : en
Pages : 499
Get Book Here
Book Description
This book describes the integration of high-throughput bioinformatics data from multiple platforms to inform our understanding of the functional consequences of genomic alterations.
Author: Helga Kolb
Publisher:
ISBN:
Category :
Languages : en
Pages :
Get Book Here
Book Description
Author: Nadav Ahituv
Publisher: Springer Science & Business Media
ISBN: 1461416833
Category : Medical
Languages : en
Pages : 289
Get Book Here
Book Description
In Gene Regulatory Sequences and Human Disease, the Editor will introduce the different technological advances that led to this breakthrough. In addition, several examples will be provided of nucleotide variants in noncoding sequences that have been shown to be associated with various human diseases.
Author: B. Wissinger
Publisher: Karger Medical and Scientific Publishers
ISBN: 3805575785
Category : Medical
Languages : en
Pages : 230
Get Book Here
Book Description
The objective of this publication is to enhance mutual understanding and communication between ophthalmologists, molecular geneticists, genetic counselors and biomedical researchers. In the introductory chapter, current genetic paradigms and experimental genetic approaches relevant to the nature of hereditary disorders are discussed. The following contribution on the epidemiology of hereditary ocular disorders provides an excellent reference to geneticists as well as clinicians. Myopia is presented as an example of a complex clinical phenotype where genes and environment interact. Further molecular ophthalmogenetic topics, such as corneal dystrophies, cataract, glaucoma, opticus neuropathy, non-syndromic and syndromic pigmentary retinopathies, defects of vitamin A metabolism and macular dystrophies including age-related macular degeneration, are investigated in depth. The volume concludes with a survey of color vision deficiencies, a discussion of animal models and gene therapy, and a useful description of technical devices supporting patients who are losing sight.
Author: Roland W. Herzog
Publisher: World Scientific
ISBN: 9814280917
Category : Medical
Languages : en
Pages : 415
Get Book Here
Book Description
1. Non-viral gene therapy / Sean M. Sullivan -- 2. Adenoviral vectors / Stuart A. Nicklin and Andrew H. Baker -- 3. Retroviral vectors and integration analysis / Cynthia C. Bartholomae [und weitere] -- 4. Lentiviral vectors / Janka Matrai, Marinee K.L. Chuah and Thierry VandenDriessche -- 5. Herpes simplex virus vectors / William F. Goins [und weitere] -- 6. Adeno-Associated Viral (AAV) vectors / Nicholas Muzyczka -- 7. Regulatory RNA in gene therapy / Alfred. S. Lewin -- 8. DNA integrating vectors (Transposon, Integrase) / Lauren E. Woodard and Michele P. Calos -- 9. Homologous recombination and targeted gene modification for gene therapy / Matthew Porteus -- 10. Gene switches for pre-clinical studies in gene therapy / Caroline Le Guiner [und weitere] -- 11. Gene therapy for central nervous system disorders / Deborah Young and Patricia A. Lawlor -- 12. Gene therapy of hemoglobinopathies / Angela E. Rivers and Arun Srivastava -- 13. Gene therapy for primary immunodeficiencies / Aisha Sauer, Barbara Cassani and Alessandro Aiuti -- 14. Gene therapy for hemophilia / David Markusic, Babak Moghimi and Roland Herzog -- 15. Gene therapy for obesity and diabetes / Sergei Zolotukhin and Clive H. Wasserfall -- 16. Gene therapy for Duchenne muscular dystrophy / Takashi Okada and Shin'ichi Takeda -- 17. Cancer gene therapy / Kirsten A.K. Weigel-Van Aken -- 18. Gene therapy for autoimmune disorders / Daniel F. Gaddy, Melanie A. Ruffner and Paul D. Robbins -- 19. Gene therapy for inherited metabolic storage diseases / Cathryn Mah -- 20. Retinal diseases / Shannon E. Boye, Sanford L. Boye and William W. Hauswirth -- 21. A brief guide to gene therapy treatments for pulmonary diseases / Ashley T. Martino, Christian Mueller and Terence R. Flotte -- 22. Cardiovascular disease / Darin J. Falk, Cathryn S. Mah and Barry J. Byrne
