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دانلود کتاب Carbohydrates in Drug Discovery and Development: Synthesis and Application

دانلود کتاب کربوهیدرات ها در کشف و توسعه دارو: سنتز و کاربرد

Carbohydrates in Drug Discovery and Development: Synthesis and Application

مشخصات کتاب

Carbohydrates in Drug Discovery and Development: Synthesis and Application

ویرایش: 1 
نویسندگان:   
سری:  
ISBN (شابک) : 0128166754, 9780128166758 
ناشر: Elsevier 
سال نشر: 2020 
تعداد صفحات: 695 
زبان: English 
فرمت فایل : PDF (درصورت درخواست کاربر به PDF، EPUB یا AZW3 تبدیل می شود) 
حجم فایل: 22 مگابایت 

قیمت کتاب (تومان) : 56,000



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توجه داشته باشید کتاب کربوهیدرات ها در کشف و توسعه دارو: سنتز و کاربرد نسخه زبان اصلی می باشد و کتاب ترجمه شده به فارسی نمی باشد. وبسایت اینترنشنال لایبرری ارائه دهنده کتاب های زبان اصلی می باشد و هیچ گونه کتاب ترجمه شده یا نوشته شده به فارسی را ارائه نمی دهد.


توضیحاتی در مورد کتاب کربوهیدرات ها در کشف و توسعه دارو: سنتز و کاربرد



کربوهیدرات ها در کشف و توسعه دارو: سنتز و کاربرد پیشرفت های مهم در سنتز، زیست شناسی و کاربردهای زیست پزشکی کربوهیدرات ها، همراه با جنبه های درمانی و دارویی شیمی کربوهیدرات ها را بررسی می کند. علاوه بر پیشرفت در ساخت الیگوساکاریدها، شیمیدانان همچنین در توانایی جمع آوری گلیکوپپتیدها و گلیکوپروتئین ها پیشرفت کرده اند. این کتاب جنبه‌های پیشرفته کربوهیدرات‌ها را پوشش می‌دهد، که با یک مقدمه کوتاه، نام‌گذاری و طبقه‌بندی شروع می‌شود که با بحث در مورد روش‌شناسی تشکیل پیوند گلیوزیدی، پروتکل‌های اخیر برای سنتز O-گلیکوزیدها، N-گلیکوزیدها، تیوگلیکوزیدها و C-گلیکوزیدها، درون مولکولی دنبال می‌شود. تحویل آگلیکون (IAD)، اصلاح کربوهیدرات، و موارد دیگر.

نوشته شده توسط تیمی از کارشناسان بین المللی که فعالانه بر روی جنبه های مختلف شیمی کربوهیدرات مصنوعی کار می کنند، این کتاب منبع ارزشمندی برای شیمیدانان کربوهیدرات، شیمیدانان محصولات طبیعی است. شیمیدان‌های دارویی، شیمی‌دانان آلی مصنوعی و بیوشیمی‌دانانی که در صنعت و دانشگاه کار می‌کنند.


توضیحاتی درمورد کتاب به خارجی

Carbohydrates in Drug Discovery and Development: Synthesis and Application examines important developments in the synthesis, biology and biomedical applications of carbohydrates, along with the therapeutic and pharmacological aspects of carbohydrate chemistry. In addition to the advancement in construction of oligosaccharides, chemists are also making strides in the ability to assemble glycopeptides and glycoproteins. This book covers advanced aspects of carbohydrates, starting with a brief introduction, nomenclature and classification that is followed by a discussion of glyosidic bond formation methodology, recent protocols for the synthesis of O-glycosides, N-glycosides, thioglycosides and C-glycosides, Intramolecular Aglycon Delivery (IAD), carbohydrate modification, and more.

Written by a team of international experts actively working on different aspect of synthetic carbohydrate chemistry, this book is an invaluable resource for carbohydrate chemists, natural products chemists, medicinal chemists, synthetic organic chemists and biochemists working in industry and academia.



فهرست مطالب

Cover
CARBOHYDRATES IN
DRUG DISCOVERY AND
DEVELOPMENT:
SYNTHESIS AND APPLICATION
Copyright
Contributors
Foreword
Preface
Abbreviations
Chapter One - Recent trends and challenges on carbohydrate-based molecular scaffolding: general consideration toward impact of ca...
	1 - Introduction
	2 - Biological significance of carbohydrates and their impact in drug discovery
		2.1 - Carbohydrates on cell surface
		2.2 - Carbohydrate for genetic information
		2.3 - Importance of furanose structure
		2.4 - Heparin: a natural anticoagulant
	3 - Carbohydrate-based drugs
		3.1 - Naturally occurring carbohydrates and their derivatives as drug candidates
		3.2 - Carbohydrate scaffolds in nature and their impact in drug development
		3.3 - Carbohydrate-based antibiotics
		3.4 - Carbohydrate-based anti-cancer agents
		3.5 - Carbohydrate-based anti-diabetic agents
			3.5.1 - Glycosidase inhibitors with anti-diabetic effects
			3.5.2 - Sodium dependent glucose co-transporter inhibitors
		3.6 - Carbohydrate-based anti-tubercular agents
		3.7 - Carbohydrate-based anti-parasitic agents
		3.8 - Carbohydrate-containing molecules as anti-HIV agents
		3.9 - Carbohydrate-based anti-coagulants
		3.10 - Carbohydrate-mimetics as potential sialyltransferase inhibitors
		3.11 - Carbohydrate-based potential glycosidase inhibitors
		3.12 - Cardiac glycosides as therapeutics
		3.13 - Carbohydrate-based molecules with miscellaneous activities
	4 - Carbohydrate-based metallo drugs
	5 - Carbohydrate-based vaccines
	6 - Conclusions and future perspective
	Acknowledgments
	References
Chapter Two - Heparin mimetics as tools for modulation of biology and therapy
	1 - Introduction
	2 - Heparin mimetics as anti-coagulants
	3 - Heparin mimetics as growth factor binders
	4 - Heparin mimetics as heparanase inhibitors
	5 - Conclusion and future perspectives
	Acknowledgments
	References
Chapter Three - Bioactive C-glycosides inspired from natural products towards therapeutics
	1 -
Introduction
	2 - Glycosides in nature
	3 -
C-Glycosides: an introduction
	4 -
Synthesis of bioactive C-glycosides
	5 -
C-Glycoside: Dapagliflozin, a novel drug in the market for diabetes
		5.1 - Proximal ring modifications in Dapagliflozin
		5.2 - Modification in the glycone part of Dapagliflozin
	6 -
C-Glycosides of flavones
	7 -
C-Glycosides of chalcones
	8 -
C-glycosides of xanthones
	9 -
C-Glycosides inspired from Adenophostin A
	10 -
C-Glycosides of KRN 7000
		10.1 - Sugar ring annulation for the access to C-glycosides
	11 -
C-Glycosides: annulating glycone and aglycone part, an illustration
	12 -
C-1 functionalized building blocks for synthesis of C-Glycosides
		12.1 - Applications of C-1 functionalized building blocks
	13 -
Conclusions and future perspectives
	References
Chapter Four - 3-Deoxy-d-manno-oct-2-ulosonic acid (Kdo) derivatives in antibacterial drug discovery
	1 -
Introduction
	2 -
Total syntheses of Kdo
		2.1 - Total synthesis of Kdo from D-arabinose
		2.2 - Total synthesis of Kdo from d-mannose
		2.3 - Total synthesis of Kdo from d-mannitol
		2.4 - Total synthesis of Kdo from other precursors
	3 -
Synthesis of Kdo derivatives as potential inhibitors of Kdo-processing enzymes
		3.1 - Total synthesis of 2-deoxy-β-Kdo
		3.2 - Synthesis of 2-deoxy-β-Kdo derivatives
		3.3 - Synthesis of Kdo C-glycosides
		3.4 - Synthesis of Kdo O-glycosides
		3.5 - Synthesis of miscellaneous Kdo derivatives
	4 -
Kdo derivatives for LPS labeling of living organisms
	5 -
Conclusions and future perspectives
	References
Chapter Five - Sialic acid-containing molecules in drug discovery and development
	1 - Introduction
	2 - Some representative characteristics of sialic acids
		2.1 - Sialic acid as terminal sugars
		2.2 - Sialic acid has great structural complexity
		2.3 - Occurrence of sialic acids
		2.4 - Sialic acids have a great biological significance
		2.5 - Biosynthesis of diverse sialosides in eukarotic and prokaryotic system
		2.6 - Enzymatic synthesis of sialylated glycans
	3 - Common synthetic routes for sialic acid containing molecules
		3.1 - Chemical glycosylation
			3.1.1 - Modifications at C-1
			3.1.2 - Modifications at C-2: leaving groups
		3.2 - Chemo-enzymatic synthesis for the designing sialoside libraries
	4 - Sialic acid-containing molecules in drug development
	5 - Synthesis of some commercially available drugs
		5.1 - Zanamivir and oseltamivir as neuraminidase inhibitors
		5.2 - Synthesis of zanamivir from N-acetylneuraminic acid (NANA) by the Merck Frosst Centre, Canada
		5.3 - Scalable route to zanamivir by Glaxo
		5.4 - First scalable synthesis of oseltamivir phosphate from (-)-quinic acid by Gilead Sciences Inc
	6 - Sialic acid in neurobiology: opportunity and challenges
		6.1 - Disorders associated with sia
			6.1.1 - Sialic acid storage disorder
			6.1.2 - Sialuria and salla disease
			6.1.3 - Guillain–barré syndrome
			6.1.4 - Miller fisher syndrome
			6.1.5 - Schrizophenia
			6.1.6 - Autism spectrum disorder (ASD)
			6.1.7 - Alzheimer’s disease (AD)
		6.2 - Uses in neurobiology
			6.2.1 - As biomarker
			6.2.2 - ‘Sia’ as drug for disorders
	7 - Conclusions and future perspective
	Acknowledgments
	References
Chapter Six - Glycan microarray: Toward drug discovery and development
	1 - Introduction
	2 - Fabrication of glycan microarrays
	3 - Detection of glycan microarrays
	4 - Biomedical applications of glycan microarrays
		4.1 - Cancer
		4.2 - Infectious diseases
		4.3 - Autoimmune diseases
		4.4 - Vaccine development
		4.5 - Enzyme inhibitors
	5 - Conclusions
	References
Chapter Seven - Recent developments in the synthesis of biologically relevant inositol derivatives
	1 -
Introduction
	2 -
Structure, nomenclature of myo-inositol and associated implications for synthesis
	3 -
Inositols and their derivatives: the biological and medicinal context
	4 -
Strategies for the synthesis of inositol derivatives
		4.1 - Necessity versus current state of art
		4.2 - Synthesis of inositol derivatives from myo-inositol– relative reactivity of the hydroxyl groups
		4.3 - Synthesis of enantiomeric myo-inositol derivatives from chiral precursors
		4.4 - Enantiomeric inositol derivatives from myo-inositol
		4.5 - Resolution of racemic myo-inositol derivatives by conversion to separable diastereomers
		4.6 - Enzyme mediated resolution of racemic myo-inositol derivatives
		4.7 - Desymmetrization of symmetric myo-inositol derivatives
		4.8 - Phosphorylation of inositol derivatives
	5 -
Conclusions and future outlook
	References
Chapter Eight - Iminosugars
	1 -
General introduction
		1.1 - Glycoconjugate processing enzymes
		1.2 - Inhibitors of glycosidases
		1.3 - Classifications of carbohydrate-derived inhibitors
		1.4 - Iminosugars
	2 -
Iminosugars as inhibitors glycosidases
		2.1 - Mode of action
		2.2 - Structural basis for glycosidase inhibition by iminosugars
	3 -
Classification of naturally occuring iminosugars
		3.1 - Natural polyhydroxypiperidines and their source of isolation
		3.2 - Natural polyhydroxypyrrolidines and their source of isolation
		3.3 - Naturally occurring polyhydroxyindolizidines and their source of isolation
		3.4 - Naturally occurring polyhydroxypyrrolizidines and their source of isolation
		3.5 - Naturally occurring nortropanes and their source of isolation
	4 -
Iminosugars as inhibitors of glycosidases
		4.1 - Iminosugars as inhibitors of α-glucosidases
		4.2 - Iminosugars as inhibitors of β-glucosidases
		4.3 - Iminosugars as inhibitors of α-galactosidases
		4.4 - Iminosugars as inhibitors of β-galactosidases
		4.5 - Iminosugars as inhibitors of mannosidases
		4.6 - Iminosugars as inhibitors of α-L-fucosidases
		4.7 - Iminosugars as inhibitors of α-l-rhamnosidoses
		4.8 - Iminosugars as inhibitors of β-N-acetylhexosaminidases
		4.9 - Iminosugars as inhibitors of glycogen phosphorylase
	5 -
Iminosugars as antivirals
	6 -
Iminosugars as pharmacological chaperones for lysosomal storage diseases
	7 -
Conclusions and future scope
	References
Chapter Nine - Carbohydrate-protein interactions: Enhancing multivalency effects through statistical rebinding
	1 -
Introduction
		1.1 - ConA
		1.2 - DC-SIGN
		1.3 - PNA
		1.4 - Jack bean α-mannosidase
	2 -
Conclusion and future perspectives
	References
Chapter Ten - Carbo-click in drug discovery and development: Opportunities and challenges
	1 -
Introduction
	2 -
Carbo-click in drug discovery and development
		2.1 - Traizolyl glycoconjugates as enzyme inhibitors
			2.1.1 - Carbonic anhydrase inhibitor
			2.1.2 - Glycosyl transferase inhibitors
			2.1.3 - Trypanosoma cruzi trans-sialidase (TcTS) inhibitor
			2.1.4 - Glycosidase inhibition activity
			2.1.5 - Neuraminidase inhibitors
				2.1.5.1 - Zanamivir based neuraminidase inhibitors
				2.1.5.2 - DANA based neuraminidase inhibitors
				2.1.5.3 - Sialic Acid based Neuraminidase inhibitors
			2.1.6 - Glycogen phosphorylase inhibitor
			2.1.7 - Protein tyrosine phosphatases (PTPs) inhibitors
		2.2 - Pharmacological applications of click chemistry
			2.2.1 - Anti-cancer activities
			2.2.2 - Anti-leishmanial activity
			2.2.3 - Anti-fungal and anti-bacterial activities
	3 -
Conclusion and future perspectives
	Acknowledgments
	References
Chapter Eleven - Glycohybrid molecules in medicinal chemistry: Present status and future prospective
	1 -
Introduction
	2 -
Bioactive carbohybrid molecules
		2.1 - Anticancer activity
			2.1.1 - Antiviral activity
		2.2 - Immunomodulatory activity
		2.3 - PTP1B inhibitors
		2.4 - Carbonic anhydrase inhibitor
		2.5 - Antimalarial activity
		2.6 - Antifungal activity
		2.7 - Antibacterial activity
		2.8 - Glycosidase inhibitor activity
		2.9 - Galectin-3 inhibitors
		2.10 - Anti-inflammatory
	3 -
Conclusion and future prospective
	References
Chapter Twelve - Biologically active carbohydrate-containing macrocycles
	1 -
Introduction
		1.1 - Macrocyclic carbohydrates isolated from plants
		1.2 - Macrocyclic carbohydrates isolated from microorganisms
		1.3 - Natural carbohydrate-based macrocycles as drug candidate
		1.4 - Macrocyclic carbohydrates used for the drug delivery
		1.5 - Macrocyclic carbohydrates as marketed drugs
		1.6 - Macrocyclic carbohydrates as antibiotics
		1.7 - Macrocyclic carbohydrates as anti-fungal drugs
		1.8 - Macrocyclic carbohydrates as immune suppressants or immunomodulators
	2 -
Synthesis of some macrocyclic carbohydrates
		2.1 - Synthesis of carbohydrate macrocycles possesing sugar part as core molecule
	3 -
Conclusions and future perspectives
	Acknowledgment
	References
Chapter Thirteen - Carbohydrate-based antibiotics: Opportunities and challenges
	1 -
Introduction
		1.1 - Carbohydrates-containing antibiotics
	2 -
Aminoglycoside antibiotics
		2.1 - Recent progress in design of novel aminoglycosides
	3 -
Nucleoside antibiotics
		3.1 - Pyrimidine analogues
		3.2 - Fluorinated pyrimidines
		3.3 - Thiopurines
	4 -
Macrolide antibiotics
	5 - Glycopeptide antibiotics
	6 - Conclusions and future perspectives
	References
Chapter Fourteen - Carbohydrate-based anti-bacterial and anti-cancer vaccines
	1 -
Introduction
	2 -
Carbohydrates as biologically relevant molecules and their impact on carbohydrate as antigens
	3 -
Glycoconjugate vaccines
		3.1 - Challenges associated with carbohydrate-based vaccines
		3.2 - Design of glycoconjugate vaccines
			3.2.1 - Synthesis of glycoconjugates as vaccine candidates
		3.3 - Anti bacterial glycoconjugate vaccine
		3.4 - Anti-tumour and anti-cancer carbohydrate vaccines
	4 -
Conclusions and future perspectives
	References
Chapter Fifteen - Opportunity of plant oligosaccharides and polysaccharides in drug development
	1 -
Introduction
	2 -
Biological and pharmacological significance
		2.1 - Starch and its products
		2.2 - Monosaccharide based natural polyols
		2.3 - Cellulose and its derivatives
		2.4 - Exudate gums
		2.5 - Glycoconjugates
	3 -
Plant oligosaccharide based molecules
	4 -
Plant polysaccharide based drugs
		4.1 - Antidiabetic activity
		4.2 - Immunomodulatory activity
	5 -
Structure-activity relationship
	6 -
Polysaccharides in drug delivery
	7 -
Bioactive polysaccharides: Structural aspects
	8 -
Conclusions
	9 -
Future perspectives
	References
Chapter N-acetylgalactosamine (GalNAc)-conjugates: Delivering oligonucleotide drugs to the liver
	1 - Introduction
		1.1 - Oligonucleotide therapeutics
		1.2 - Oligonucleotide therapeutics: Mode of action
		1.3 - Oligonucleotide therapeutics: Challenges
		1.4 - Medicinal chemistry of therapeutic oligonucleotides
		1.5 - Phosphate-backbone modifications
		1.6 - Sugar modifications
		1.7 - Combining the sugar and phosphate-backbone modifications
		1.8 - Complete replacement of the sugar-phosphate backbone
		1.9 - Nucleobase modifications
		1.10 - Covalent-conjugate approach: GalNAc-conjugates
		1.11 - GalNAc-conjugates: mechanism of liver-specific delivery
		1.12 - GalNAc-conjugates: design
			1.12.1 - Triantennary GalNAc
			1.12.2 - Monomeric linear GalNAc
		1.13 - Further improvements in GalNAc-oligonucleotide conjugates
	2 - Clinical status of GalNAc-conjugated oligonucleotide drugs
	3 - Conclusions and future perspectives
	References
Index
Back Cover




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