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Fibrosis

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Cover of 'Fibrosis'

Table of Contents

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    Book Overview
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    Chapter 1 Human Fibrotic Diseases: Current Challenges in Fibrosis Research
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    Chapter 2 The Bleomycin Model of Pulmonary Fibrosis
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    Chapter 3 Intradermal Injections of Bleomycin to Model Skin Fibrosis
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    Chapter 4 Assessing the Effects of Fibrosis on Lung Function by Light Microscopy-Coupled Stereology
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    Chapter 5 Transplanting Human Skin Grafts onto Nude Mice to Model Skin Scars
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    Chapter 6 Hypertrophic Scarring in the Rabbit Ear: A Practical Model for Studying Dermal Fibrosis
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    Chapter 7 Mouse and Rat Models of Induction of Hepatic Fibrosis and Assessment of Portal Hypertension
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    Chapter 8 Mouse Models of Corneal Scarring
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    Chapter 9 Modeling Cardiac Fibrosis in Mice: (Myo)Fibroblast Phenotype After Ischemia
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    Chapter 10 Characterization of Mesenchymal-Fibroblast Cells Using the Col1a2 Promoter/Enhancer
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    Chapter 11 Isolation and Culture of Primary Murine Hepatic Stellate Cells
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    Chapter 12 Isolation and Culture of Adipose-Derived Stromal Cells from Subcutaneous Fat
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    Chapter 13 Isolation of Live Fibroblasts by Fluorescence-Activated Cell Sorting
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    Chapter 14 Detection of Infiltrating Mast Cells Using a Modified Toluidine Blue Staining
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    Chapter 15 Cell-Populated Collagen Lattice Models
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    Chapter 16 Traction Force Measurement Using Deformable Microposts
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    Chapter 17 Mechanical Deformation of Cultured Cells with Hydrogels
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    Chapter 18 Preparation of Decellularized Lung Matrices for Cell Culture and Protein Analysis
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    Chapter 19 Type I Collagen Purification from Rat Tail Tendons
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    Chapter 20 Purification of Human Plasma/Cellular Fibronectin and Fibronectin Fragments
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    Chapter 21 Laser Capture Microdissection of Tissue Sections for High-Throughput RNA Analysis
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    Chapter 22 Collagen Quantification in Tissue Specimens
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    Chapter 23 Methods for the Assessment of Active Transforming Growth Factor-β in Cells and Tissues
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    Chapter 24 Visualizing In Vitro Type I Collagen Fibrillogenesis by Transmission Electron Microscopy
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    Chapter 25 Histological and Electron Microscope Staining for the Identification of Elastic Fiber Networks
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    Chapter 26 Method for Picrosirius Red-Polarization Detection of Collagen Fibers in Tissue Sections
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    Chapter 27 Probing Collagen Organization: Practical Guide for Second-Harmonic Generation (SHG) Imaging
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    Chapter 28 Methods for Quantifying Fibrillar Collagen Alignment
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    Chapter 29 Exploring the Nano-Surface of Collagenous and Other Fibrotic Tissues with AFM
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    Chapter 30 Spectral Unmixing Methods and Tools for the Detection and Quantitation of Collagen and Other Macromolecules in Tissue Specimens
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    Chapter 31 Simple Analysis of Deposited Gene Expression Datasets for the Non-Bioinformatician: How to Use GEO for Fibrosis Research
Attention for Chapter 10: Characterization of Mesenchymal-Fibroblast Cells Using the Col1a2 Promoter/Enhancer
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Chapter title
Characterization of Mesenchymal-Fibroblast Cells Using the Col1a2 Promoter/Enhancer
Chapter number 10
Book title
Fibrosis
Published in
Methods in molecular biology, January 2017
DOI 10.1007/978-1-4939-7113-8_10
Pubmed ID
Book ISBNs
978-1-4939-7112-1, 978-1-4939-7113-8
Authors

Ian M. H. Li, Amy L. Horwell, Grace Chu, Benoit de Crombrugghe, George Bou-Gharios

Abstract

Excessive deposition of extracellular matrix (ECM) is a common hallmark of fibrotic diseases in various organs. Chiefly among this ECM are collagen types I and III, secreted by local fibroblasts, and other mesenchymal cells recruited for repair purposes. In the last two decades, the search for a fibroblast-specific promoter/enhancer has intensified in order to control the regulation of ECM in these cells and limit the scarring of the fibrotic process. In our previous work, we characterized an enhancer region 17 kb upstream of the Col1a2 gene transcription start site. This enhancer in transgenic mice is expressed mainly in mesenchymal cells during development and in adults upon injury. When driving transgenes such as beta-galactosidase or luciferase, this construct acts as an informative reporter of collagen transcription and is predictive of collagen type I deposition. In this chapter, we provide detailed protocols for identifying similar enhancers and using the sequence to generate a construct for transfection and producing transgenic animals. We also provided information on the use of luminescence in transgenic mice, tissue processing, as well as using cre/lox system to obtain conditional gain and loss of function in mice.

Mendeley readers

Mendeley readers

The data shown below were compiled from readership statistics for 14 Mendeley readers of this research output. Click here to see the associated Mendeley record.

Geographical breakdown

Country Count As %
Unknown 14 100%

Demographic breakdown

Readers by professional status Count As %
Student > Ph. D. Student 6 43%
Student > Master 4 29%
Professor > Associate Professor 1 7%
Unknown 3 21%
Readers by discipline Count As %
Biochemistry, Genetics and Molecular Biology 6 43%
Pharmacology, Toxicology and Pharmaceutical Science 2 14%
Agricultural and Biological Sciences 1 7%
Social Sciences 1 7%
Medicine and Dentistry 1 7%
Other 0 0%
Unknown 3 21%