Nanomaterials for drug delivery and therapy /

Detalles Bibliográficos
Clasificación:Libro Electrónico
Otros Autores: Grumezescu, Alexandru Mihai (Editor )
Formato: Electrónico eBook
Idioma:Inglés
Publicado: Amsterdam, Netherlands : Elsevier, 2019.
Temas:
Nanostructured materials > Therapeutic use.
Drug delivery systems.
Nanomedicine.
Nanotechnology.
Nanomedicine
Drug Delivery Systems
Nanotechnology
Nanomat�eriaux > Emploi en th�erapeutique.
Syst�emes d'administration de m�edicaments.
Nanom�edecine.
Nanotechnologie.
MEDICAL > Pharmacology.
Drug delivery systems
Acceso en línea:Texto completo

MARC

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020 |a 9780128166291  |q (electronic bk.) 
020 |a 0128166290  |q (electronic bk.) 
020 |z 9780128165058  |q (print) 
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035 |a (OCoLC)1090139178  |z (OCoLC)1090441504  |z (OCoLC)1090545837  |z (OCoLC)1090758989  |z (OCoLC)1090853090 
050 4 |a R857.N34 
072 7 |a MED  |x 071000  |2 bisacsh 
082 0 4 |a 615.6  |2 23 
245 0 0 |a Nanomaterials for drug delivery and therapy /  |c edited by Alexandru Mihai Grumezescu. 
264 1 |a Amsterdam, Netherlands :  |b Elsevier,  |c 2019. 
300 |a 1 online resource 
336 |a text  |b txt  |2 rdacontent 
337 |a computer  |b c  |2 rdamedia 
338 |a online resource  |b cr  |2 rdacarrier 
500 |a Includes index. 
588 0 |a Print version record. 
505 0 |a Front Cover; Nanomaterials for Drug Delivery and Therapy; Copyright Page; Contents; List of Contributors; Foreword; Preface; 1 Cell and organ drug targeting; 1.1 Introduction; 1.2 Why Targeting Cell and Organ Is Required?; 1.3 Strategies for Drug Targeting; 1.3.1 Passive Targeting; 1.3.2 Inverse Targeting; 1.3.3 Active Targeting; 1.3.3.1 First order targeting; 1.3.3.2 Second order targeting; 1.3.3.3 Third order targeting; 1.3.3.4 Ligand mediated targeting; 1.3.4 Physical Targeting; 1.3.5 Dual Targeting; 1.3.6 Double Targeting; 1.4 Carriers for Drug Targeting 
505 8 |a 1.4.1 The Microparticles: Microspheres and Microcapsules1.4.1.1 Application of microparticles as a carrier for targeted drug delivery; 1.4.1.1.1 Ophthalmic drug delivery; 1.4.1.1.2 Gene delivery; 1.4.1.1.3 Drug delivery for anticancer therapy; 1.4.1.1.4 Vaginal drug delivery; 1.4.1.2 Pros and cons of microparticulate delivery system; 1.4.2 Nanocarriers; 1.4.2.1 Vital nanocarriers; 1.4.2.2 Application of nanoparticles as a carrier for targeted drug delivery; 1.4.2.2.1 Intratumoral drug delivery; 1.4.2.2.2 Intrahepatic drug delivery; 1.4.2.2.3 Intracellular drug delivery 
505 8 |a 1.4.2.2.4 Targeted drug delivery to the brain1.4.2.3 Pros and cons of nanocarriers; 1.4.3 Vesicular Carriers; 1.4.3.1 Liposomes; 1.4.3.1.1 Application of liposomes; 1.4.3.2 Niosomes; 1.4.3.2.1 Application of niosomes as a carrier for targeted drug delivery; 1.4.3.3 Ufasomes; 1.4.3.3.1 Application of ufasomes as a carrier for targeted drug delivery; 1.4.3.4 Pharmacosomes; 1.4.3.4.1 Application of pharmacosome in targeted delivery; 1.4.3.5 Virosomes; 1.4.3.5.1 Application of virosomes in targeted drug delivery; 1.4.3.6 Cubosomes; 1.4.3.6.1 Application of cubosomes in targeted drug delivery 
505 8 |a 1.4.3.7 Pros and cons of vesicular carriers1.4.4 Cells as the Carriers for Targeted Drug Delivery; 1.4.4.1 Neutrophils; 1.4.4.2 Lymphocytes; 1.4.4.3 Fibroblasts; 1.4.4.4 Artificial cells; 1.4.4.5 Resealed erythrocytes; 1.4.4.6 Nanoerythrosomes; 1.4.4.7 Pros and cons of cell-based carriers; 1.4.5 Miscellaneous Carrier Systems; 1.4.5.1 Quantum dot; 1.4.5.2 Prodrug(s); 1.4.5.3 Monoclonal antibodies; 1.5 Future Perspectives; References; 2 Characterization of pharmaceutical nanocarriers: in vitro and in vivo studies; 2.1 Introduction; 2.2 Characterization; 2.2.1 In Vitro Parameters 
505 8 |a 2.2.1.1 Presence of nanocarriers2.2.1.2 Size; 2.2.1.2.1 Photon correlation spectroscopy; 2.2.1.2.2 Transmission electron microscopy; 2.2.1.2.3 Laser diffraction study; 2.2.1.2.4 Turbidity method; 2.2.1.2.5 Nuclear magnetic resonance; 2.2.1.2.6 Filtration; 2.2.1.2.7 Optical microscopy; 2.2.1.3 Morphology; 2.2.1.3.1 Electron microscopy; 2.2.1.3.2 Atomic force microscopy; 2.2.1.4 Zeta potential; 2.2.1.5 Surface hydrophobicity; 2.2.1.5.1 Hydrophobic interaction chromatography; 2.2.1.6 Entrapment/incorporation efficiency; 2.2.1.7 Drug content; 2.2.1.8 Solubility study 
650 0 |a Nanostructured materials  |x Therapeutic use. 
650 0 |a Drug delivery systems. 
650 0 |a Nanomedicine. 
650 0 |a Nanotechnology. 
650 1 2 |a Nanomedicine  |0 (DNLM)D050997 
650 2 2 |a Drug Delivery Systems  |0 (DNLM)D016503 
650 2 |a Nanotechnology  |0 (DNLM)D036103 
650 6 |a Nanomat�eriaux  |0 (CaQQLa)201-0258061  |x Emploi en th�erapeutique.  |0 (CaQQLa)201-0373975 
650 6 |a Syst�emes d'administration de m�edicaments.  |0 (CaQQLa)000260397 
650 6 |a Nanom�edecine.  |0 (CaQQLa)201-0448752 
650 6 |a Nanotechnologie.  |0 (CaQQLa)201-0225435 
650 7 |a MEDICAL  |x Pharmacology.  |2 bisacsh 
650 7 |a Nanotechnology  |2 fast  |0 (OCoLC)fst01032639 
650 7 |a Drug delivery systems  |2 fast  |0 (OCoLC)fst00898667 
650 7 |a Nanomedicine  |2 fast  |0 (OCoLC)fst01744350 
700 1 |a Grumezescu, Alexandru Mihai,  |e editor. 
776 0 8 |i Print version:  |a Grumezescu, Alexandru Mihai.  |t Nanomaterials for drug delivery and therapy  |z 9780128165058  |w (OCoLC)1085965515 
856 4 0 |u https://sciencedirect.uam.elogim.com/science/book/9780128165058  |z Texto completo 

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