Nonsense mutation correction in human diseases : an approach for targeted medicine /

Nonsense Mutation Correction in Human Diseases: An Approach for Targeted Medicine provides an introduction on genetic diseases, discusses the prevalence of nonsense mutations, the consequences of a nonsense mutation for the expression of the mutant gene, and the presentation of the nonsense-mediated...

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Detalles Bibliográficos
Clasificación:Libro Electrónico
Autores principales: Benhabiles, Hana (Autor), Jia, Jieshuang (Autor), Lejeune, Fabrice (Autor)
Formato: Electrónico eBook
Idioma:Inglés
Publicado: London : Acedemic Press is an imprint of Elsevier, [2016]
Temas:
Genetic disorders.
Mutation (Biology)
Targeted Gene Repair
Genetic Diseases, Inborn
Mutation
Codon, Nonsense
Nonsense Mediated mRNA Decay
Maladies g�en�etiques.
Mutation (Biologie)
HEALTH & FITNESS > Diseases > General.
MEDICAL > Clinical Medicine.
MEDICAL > Diseases.
MEDICAL > Evidence-Based Medicine.
MEDICAL > Internal Medicine.
Genetic disorders
Acceso en línea:Texto completo

MARC

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100 1 |a Benhabiles, Hana,  |e author. 
245 1 0 |a Nonsense mutation correction in human diseases :  |b an approach for targeted medicine /  |c Hana Benhabiles, Jieshuang Jia, Fabrice Jejeune. 
264 1 |a London :  |b Acedemic Press is an imprint of Elsevier,  |c [2016] 
300 |a 1 online resource (ix, 180 pages) 
336 |a text  |b txt  |2 rdacontent 
337 |a computer  |b c  |2 rdamedia 
338 |a online resource  |b cr  |2 rdacarrier 
588 0 |a Online resource; title from PDF title page (EBSCO, viewed March 16, 2016). 
504 |a Includes bibliographical references and index. 
520 |a Nonsense Mutation Correction in Human Diseases: An Approach for Targeted Medicine provides an introduction on genetic diseases, discusses the prevalence of nonsense mutations, the consequences of a nonsense mutation for the expression of the mutant gene, and the presentation of the nonsense-mediated mRNA decay (NMD). It presents the mechanism of action and rationale associated with each strategy to correct nonsense mutations with the results of clinical trials to further support this basis. In addition, the book shows how it may be possible to combine several of these strategies to ultimately improve the efficiency of correction, also suggesting the future goals and objectives to improve treatment modalities in this evolving sphere of personalized medicine. 
505 0 |a Cover; Title Page; Copyright Page; Contents; About the Authors; Acknowledgments; Chapter 1 -- General Aspects Related to Nonsense Mutations; 1 -- Premature termination codon, nonsense mutation, and consequences on gene expression; 2 -- Pre-mRNA splicing mechanism; 2.1 -- Generalities; 2.2 -- Categories of Alternative Splicing; 2.3 -- Regulation of Splicing; 2.4 -- Pathologies Associated with Splicing Defaults; 3 -- Nonsense-mediated mRNA decay (NMD) mechanism; 3.1 -- Generalities; 3.2 -- Main proteins involved in NMD; 3.2.1 -- UPF1/RENT1/SMG2; 3.2.2 -- UPF2/RENT2/SMG3; 3.2.3 -- UPF3/UPF3a/Rent3A. 
505 8 |a 3.2.4 -- UPF3X/UPF3b/Rent3B3.2.5 -- Suppressor of Morphogenesis in Genitalia 1 (SMG1)/ATX/Lambda-Iota Protein Kinase C-Interacting Protein (LIP); 3.2.6 -- SMG5/EST1B; 3.2.7 -- SMG6/EST1A/hSmg5/7a; 3.2.8 -- SMG7/EST1C; 3.2.9 -- SMG8/Amplified in Breast Cancer Gene 2 and SMG9; 3.3 -- EJC-Dependent Model; 3.4 -- Model Involving the Distance Between the Stop Codon and the Position of the poly(A) Binding Protein C1; 3.5 -- Natural Substrates of NMD; 3.6 -- Regulation; 3.6.1 -- Autoregulation; 3.6.2 -- Tissue Specificity; 3.6.3 -- Inhibition During Apoptosis; 3.6.4 -- miRNA; 3.6.5 -- Phosphorylation. 
505 8 |a 3.6.6 -- Regulation by Availability of NMD Factors3.7 -- UPF2, UPF3X/UPF3b Independent Pathway; 3.8 -- Pathologies Associated with NMD Defaults; 4 -- Correction of nonsense mutations, a case of targeted therapy; References; Chapter 2 -- Pathologies Susceptible to be Targeted for Nonsense Mutation Therapies; 1 -- Rare diseases; 1.1 -- Duchenne Muscular Dystrophy (DMD); 1.2 -- Cystic Fibrosis (CF); 1.3 -- Spinal Muscular Atrophy; 2 -- Frequent diseases; 2.1 -- Cancers; 2.2 -- Metabolic Diseases; 2.3 -- Neurologic Disorders; References; Chapter 3 -- Strategies to Correct Nonsense Mutations. 
505 8 |a 1 -- The exon skipping1.1 -- Principle; 1.2 -- Examples; 1.3 -- Weaknesses; 2 -- Trans-splicing; 2.1 -- Principle; 2.2 -- An Example of Trans-Splicing Used as Therapeutic Approach for Duchenne Muscular Dystrophy; 2.3 -- Weaknesses; 3 -- PTC-readthrough; 3.1 -- Principle; 3.1.1 -- Aminoglycoside Molecules; 3.1.2 -- Nonaminoglycoside Molecules; 3.2 -- Weaknesses; 4 -- NMD inhibition; 4.1 -- Principle; 4.2 -- Examples; 4.3 -- Weaknesses; 5 -- Pseudouridylation at the PTC; 5.1 -- Principle; 5.2 -- Weaknesses; 6 -- Gene therapy; 6.1 -- Principle; 6.2 -- Weaknesses; 7 -- Cell therapy; 7.1 -- Principle; 7.2 -- Weaknesses. 
505 8 |a 8 -- Genome editing8.1 -- Zinc Finger Nucleases; 8.1.1 -- Weaknesses; 8.2 -- Transcription Activator-Like Effector Nucleases; 8.2.1 -- Weaknesses; 8.3 -- CRISPR/Cas9; 8.3.1 -- Illustration; 8.3.2 -- Weaknesses; 9 -- Combinatory approaches to improve nonsense mutation therapies; 9.1 -- Activation of Both Transcription and Readthrough; 9.2 -- Inhibition of NMD and Activation of Readthrough; 9.3 -- Gene Therapy/Genome Editing/Pseudouridylation at the PTC and Cell Therapy; References; Chapter 4 -- Conclusions; 1 -- Summary on the different strategies and their results. 
505 8 |a 2 -- Personalized/targeted medicine versus traditional medicine. 
650 0 |a Genetic disorders. 
650 0 |a Mutation (Biology) 
650 1 2 |a Targeted Gene Repair  |0 (DNLM)D052416 
650 2 |a Genetic Diseases, Inborn  |0 (DNLM)D030342 
650 2 |a Mutation  |0 (DNLM)D009154 
650 2 2 |a Codon, Nonsense  |0 (DNLM)D018389 
650 2 2 |a Nonsense Mediated mRNA Decay  |0 (DNLM)D059365 
650 6 |a Maladies g�en�etiques.  |0 (CaQQLa)201-0024547 
650 6 |a Mutation (Biologie)  |0 (CaQQLa)201-0017096 
650 7 |a HEALTH & FITNESS  |x Diseases  |x General.  |2 bisacsh 
650 7 |a MEDICAL  |x Clinical Medicine.  |2 bisacsh 
650 7 |a MEDICAL  |x Diseases.  |2 bisacsh 
650 7 |a MEDICAL  |x Evidence-Based Medicine.  |2 bisacsh 
650 7 |a MEDICAL  |x Internal Medicine.  |2 bisacsh 
650 7 |a Genetic disorders  |2 fast  |0 (OCoLC)fst00940009 
650 7 |a Mutation (Biology)  |2 fast  |0 (OCoLC)fst01031152 
700 1 |a Jia, Jieshuang,  |e author. 
700 1 |a Lejeune, Fabrice,  |e author. 
776 0 8 |i Print version:  |a Benhabiles, Hana.  |t Nonsense mutation correction in human diseases.  |d London : Acedemic Press is an imprint of Elsevier, [2016]  |z 9780128044681  |z 0128044683  |w (OCoLC)946815702 
856 4 0 |u https://sciencedirect.uam.elogim.com/science/book/9780128044681  |z Texto completo 

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