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Cytochrome P450 2D6: Structure, Function, Regulation and Polymorphism [Kõva köide]

  • Formaat: Hardback, 508 pages, kõrgus x laius: 280x210 mm, kaal: 1474 g, 16 Tables, black and white; 30 Illustrations, color; 182 Illustrations, black and white
  • Ilmumisaeg: 09-Mar-2016
  • Kirjastus: CRC Press Inc
  • ISBN-10: 1466597879
  • ISBN-13: 9781466597877
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Cytochrome P450 2D6: Structure, Function, Regulation and PolymorphismSuurem pilt
  • Formaat: Hardback, 508 pages, kõrgus x laius: 280x210 mm, kaal: 1474 g, 16 Tables, black and white; 30 Illustrations, color; 182 Illustrations, black and white
  • Ilmumisaeg: 09-Mar-2016
  • Kirjastus: CRC Press Inc
  • ISBN-10: 1466597879
  • ISBN-13: 9781466597877
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Teised raamatud sellest sooduspakkumisest: Kevadine sooduspakkumine - kuni 31. maini üle miljoni raamatu kuni 25% soodsamalt
Püsilink: https://www.kriso.ee/db/9781466597877.html
Märksõnad:
Cytochromes are proteins that catalyze electron transfer reactions of well-known metabolic pathways and are classified in various superfamilies. The CYP, or P450, superfamily accounts for 90% of the oxidative metabolism of clinical drugs. One member of this superfamily, P450 2D6 (or CYP2D6), singlehandedly metabolizes about 25% of all medications in the human liver. Cytochrome P450 2D6: Structure, Function, Regulation, and Polymorphism reviews the current knowledge of CYP2D6 as well as the maturing body of evidence indicating its significance to clinical and pharmacological researchers and practitioners.

This book focuses on the critical role CYP2D6 plays in the human liver. It examines the genetic, epigenetic, physiological, pathological, and structural factors of the gene that govern the highly variable metabolism of a number of drugs in clinical use. It highlights the impact of the functional roles of CYP2D6 on clinical practice and drug development and also discusses implications for precise medicine, strategies to avoid adverse drug reactions, and paths for future research.

Cytochrome P450 2D6 is a unique, valuable book focusing on a single but immensely powerful human gene. It provides the first single source of comprehensive information on CYP2D6 that serves as an important reference for medical, biomedical, pharmaceutical, and nursing researchers, practitioners, and students.
Preface xiii
Author xv
Chapter 1 Introduction to Human Cytochrome P450 Superfamily 1(100)
1.1 The Cytochrome P450s in Nature
1(2)
1.2 Human CYP Superfamily
3(19)
1.2.1 Members of the CYP Superfamily: Family, Subfamily, Clan, and Motif
3(12)
1.2.2 Subcellular Location of CYPs
15(1)
1.2.3 CYP-Mediated Metabolism of Xenobiotics and Endogenous Compounds
16(1)
1.2.4 Structural Features of CYPs
17(2)
1.2.5 Inhibition of CYPs
19(1)
1.2.6 Regulation of CYPs via Nuclear Receptors, miRNAs, Inflammation, and Cytokines
19(2)
1.2.7 Phenotypes and Polymorphisms of CYPs
21(1)
1.2.8 CYP-Related Diseases
22(1)
1.3 Human CYP1 Family
22(4)
1.3.1 CYP1A1 (Aryl Hydrocarbon Hydroxylase)
23(1)
1.3.2 CYP1A2 (Aryl Hydrocarbon Hydroxylase)
24(1)
1.3.3 CYP1B1 (Aryl Hydrocarbon Hydroxylase)
25(1)
1.4 Human CYP2ABFGST Cluster: CYP2A6, 2A7, 2A13, 2B6, 2F1, and 2S1
26(6)
1.4.1 CYP2A6 (Coumarin 7-Hydroxylase)
26(2)
1.4.2 CYP2A7
28(1)
1.4.3 CYP2A13
28(1)
1.4.4 CYP2B6
29(2)
1.4.5 CYP2F1
31(1)
1.4.6 CYP2S1
31(1)
1.5 Human CYP2C Cluster: CYP2C8, 2C9, 2C18, and 2C19
32(4)
1.5.1 CYP2C8
32(1)
1.5.2 CYP2C9
33(2)
1.5.3 CYP2C18 (S-Mephenytoin Hydroxylase)
35(1)
1.5.4 CYP2C19
35(1)
1.6 Other Human CYP2 Family Members
36(4)
1.6.1 CYP2D6
36(1)
1.6.2 CYP2E1
37(1)
1.6.3 CYP2J2
37(1)
1.6.4 CYP2R1
38(1)
1.6.5 CYP2U1
39(1)
1.6.6 CYP2W1
39(1)
1.7 Human CYP3A Cluster: CYP3A4, 3A5, 3A7, and 3A43
40(4)
1.7.1 CYP3A4
40(3)
1.7.2 CYP3A5
43(1)
1.7.3 CYP3A7
43(1)
1.7.4 CYP3A43
44(1)
1.8 Human CYP4ABXZ Cluster: CYP4A11, 4A22, 4B1, 4X1, and 4Z1
44(1)
1.8.1 CYP4A11 (20-Hydroxyeicosatetraenoic Acid Synthase, Fatty Acid ω-Hydroxylase, and Lauric Acid ω-Hydroxylase)
44(1)
1.8.2 CYP4A22 (Fatty Acid ω-Hydroxylase and Lauric Acid ω-Hydroxylase)
45(1)
1.8.3 CYP4B1
45(1)
1.9 Human CYP4F Cluster: CYP4F2, 4F3, 4F8, 4F11, 4F12, and 4F22
45(2)
1.9.1 CYP4F2 (20-Hydroxyeicosatetraenoic Acid Synthase, Arachidonic Acid ω-Hydroxylase, and Leukotriene-B4 ω-Hydroxylase 1)
45(1)
1.9.2 CYP4F3
46(1)
1.9.3 CYP4F8
46(1)
1.9.4 CYP4F11 (Phylloquinone ω-Hydroxylase and 3-Hydroxy Fatty Acid ω-Hydroxylase)
46(1)
1.9.5 CYP4F12
46(1)
1.9.6 CYP4F22
47(1)
1.10 Other Human CYP4 Family Members
47(1)
1.10.1 CYP4V2 (Docosahexaenoic Acid ω-Hydroxylase)
47(1)
1.10.2 CYP4X1
47(1)
1.10.3 CYP4Z1
47(1)
1.11 Human CYP5 Family
48(1)
1.11.1 CYP5A1 (Thromboxane A Synthase 1, TBXAS1)
48(1)
1.12 Human CYP7 Family
48(1)
1.12.1 CYP7A1 (Cholesterol 7α-Hydroxylase)
48(1)
1.12.2 CYP7B1 (Oxysterol 7α-Hydroxylase 1)
49(1)
1.13 Human CYP8 Family
49(1)
1.13.1 CYP8A1 (Prostaglandin I2 Synthase, PGIS/PTGIS)
49(1)
1.13.2 CYP8B1 (Sterol 12α-Hydroxylase)
50(1)
1.14 Human CYP11 Family
50(2)
1.14.1 CYP11A1 (Cholesterol Side-Chain Cleavage Enzyme)
50(1)
1.14.2 CYP11B1 (Steroid 11β-Hydroxylase)
51(1)
1.14.3 CYPI1B2 (Aldosterone Synthase/Steroid 11β/18-Hydroxylase)
51(1)
1.15 Human CYP17 Family
52(1)
1.15.1 CYP17A1 (Steroid 17α-Monooxygenase, 17α-Hydroxylase, 17,20 Lyase, and 17,20 Desmolase)
52(1)
1.16 Human CYP19 Family
53(1)
1.16.1 CYP19A1 (Aromatase)
53(1)
1.17 Human CYP20 Family
54(1)
1.17.1 CYP20A1
54(1)
1.18 Human CYP21 Family
54(1)
1.18.1 CYP21A2 (Steroid 21-Hydroxylase)
54(1)
1.19 Human CYP24 Family
54(1)
1.19.1 CYP24A1 (1,25-Dihydroxyvitamin D3 24-Hydroxylase, Vitamin D 24-Hydroxylase/ Vitamin D3 24-Hydroxylase)
54(1)
1.20 Human CYP26 Family
55(2)
1.20.1 CYP26A1 (Retinoic Acid 4-Hydroxylase)
56(1)
1.20.2 CYP26B1
56(1)
1.20.3 CYP26C1
57(1)
1.21 Human CYP27 Family
57(2)
1.21.1 CYP27A1 (Sterol 27-Hydroxylase)
57(1)
1.21.2 CYP27B1 (Mitochondria) 25-Hydroxyvitamin D 1α-Hydroxylase)
58(1)
1.21.3 CYP27C1
58(1)
1.22 Human CYP39A1, 46A1, and 51A1
59(1)
1.22.1 CYP39A1 (Oxysterol 7α-Hydroxylase 2)
59(1)
1.23 Human CYP46 Family
59(1)
1.23.1 CYP46A1 (Cholesterol 24-Hydroxylase)
59(1)
1.24 Human CYP51 Family
59(1)
1.24.1 CYP51A1 (Lanosterol 14α-Demethylase/Sterol 14α-Demethylase)
59(1)
1.25 Highlights of This Book
60(1)
References
60(41)
Chapter 2 Mammalian CYP2D Members: A Comparison of Structure, Function, and Regulation 101(38)
2.1 Introduction
101(1)
2.2 Rat Cyp2d Subfamily: Cyp2d1, 2d2, 2d3, 2d4, and 2d5
102(17)
2.2.1 Tissue Distribution of Rat Cyp2ds
102(10)
2.2.2 Substrates of Rat Cyp2ds
112(1)
2.2.3 Differences in Rat Cyp2d-Dependent Metabolism
113(1)
2.2.4 Dark Agouti Rats as a Cyp2d2-Deficient Model
114(3)
2.2.5 Regulation of Rat Cyp2ds
117(1)
2.2.6 Inhibitors of Rat CYP2ds and Cyp2d-Mediated Drug-Drug Interactions
118(1)
2.3 Mouse Cyp2d Subfamily: Cyp2d9-2d13, 2d22, 2d26, 2d34, and 2d40
119(2)
2.3.1 Tissue Distribution of Mouse Cyp2ds
119(1)
2.3.2 Substrate Specificity of Mouse Cyp2ds
120(1)
2.3.3 Cyp2d Knockout and CYP2D6 Transgenic Mouse Model
120(1)
2.4 Bovine CYP2D14
121(1)
2.5 Dog CYP2D15
121(4)
2.5.1 Cloning and Purification of Dog CYP2D15
122(1)
2.5.2 Tissue Distribution of Dog CYP2D15
122(1)
2.5.3 Substrate Specificity of Dog CYP2D15
122(2)
2.5.4 Induction of Dog CYP2D15
124(1)
2.5.5 Inhibitors of Dog CYP2D15
125(1)
2.6 Guinea Pig Cyp2d16
125(1)
2.6.1 Tissue Distribution of Guinea Pig Cyp2d16
125(1)
2.6.2 Substrate Specificity of Guinea Pig Cyp2d16
125(1)
2.6.3 Regulation of Guinea Pig Cyp2d16
125(1)
2.7 Macaque CYP2D17, 2D29, 2D42, and 2D44
126(1)
2.7.1 Cynomolgus Monkey CYP2D17 and 2D44
126(1)
2.7.2 Japanese Monkey CYP2D29
127(1)
2.8 Marmoset CYP2D8, 2DI9, and 2D30
127(1)
2.9 Rabbit CYP2D23 and CYP2D24
128(1)
2.10 Pig CYP2D25
128(1)
2.10.1 Cloning and Purification of Pig CYP2D25
128(1)
2.10.2 Catalytic Activity of Pig CYP2D25
128(1)
2.11 Syrian Hamster Cyp2d27
129(1)
2.12 Chicken CYP2D49
129(1)
2.13 Horse CYP2D50
129(1)
2.14 Conclusions and Future Perspectives
130(1)
References
130(9)
Chapter 3 Substrates of Human CYP2D6 139(150)
3.1 Introduction
139(1)
3.2 Probes of CYP2D6
139(2)
3.2.1 Sparteine and Debrisoquine
139(1)
3.2.2 Dextromethorphan
140(1)
3.2.3 Bufuralol and Tramadol
140(1)
3.3 Therapeutic Drugs as Substrates of CYP2D6
141(91)
3.3.1 Drugs Acting on the Central Nervous System
141(36)
3.3.1.1 Tricyclic Antidepressants
141(5)
3.3.1.2 Selective Serotonin Reuptake Inhibitors
146(5)
3.3.1.3 Other Antidepressants
151(2)
3.3.1.4 Antipsychotics
153(9)
3.3.1.5 Hypnotics
162(1)
3.3.1.6 Opioids and Opioid Receptor Antagonists
162(3)
3.3.1.7 Antiemetics
165(4)
3.3.1.8 Antimigraine Drugs
169(1)
3.3.1.9 Antiparkinsonism Agents
170(1)
3.3.1.10 Centrally Acting Cholinesterase Inhibitors
171(4)
3.3.1.11 Drugs for Senile Dementia
175(1)
3.3.1.12 Drugs for the Treatment of Attention-Deficit/Hyperactivity Disorder
175(1)
3.3.1.13 Nonnarcotic Analgesics
175(1)
3.3.1.14 Drugs for Huntington's Disease Chorea
176(1)
3.3.2 Cardiovascular Drugs
177(25)
3.3.2.1 Antianginal Drugs
177(3)
3.3.2.2 Antiarrhythmics
180(10)
3.3.2.3 Antiplatelet Agents
190(3)
3.3.2.4 β-Blockers
193(5)
3.3.2.5 Calcium Channel Blockers
198(4)
3.3.3 Antihistamines
202(6)
3.3.3.1 Azelastine
203(1)
3.3.3.2 Chlorpheniramine
203(1)
3.3.3.3 Cinnarizine and Flunarizine
203(1)
3.3.3.4 Diphenhydramine
204(1)
3.3.3.5 Loratadine
204(1)
3.3.3.6 Mequitazine
205(1)
3.3.3.7 Oxatomide
205(2)
3.3.3.8 Terfenadine
207(1)
3.3.4 Anti-HIV Agents
208(7)
3.3.4.1 HIV Protease Inhibitors
208(2)
3.3.4.2 Nonnucleoside Reverse Transcriptase Inhibitors
210(5)
3.3.5 Antimalarial Drugs
215(2)
3.3.5.1 Amodiaquine
215(1)
3.3.5.2 Chloroquine
215(1)
3.3.5.3 Halofantrine
215(2)
3.3.5.4 Phenoxypropoxybiguanides
217(1)
3.3.6 Hypolipidemic Agents
217(1)
3.3.6.1 Fluvastatin
217(1)
3.3.6.2 Pactimibe
218(1)
3.3.7 Muscarinic Receptor Antagonists
218(1)
3.3.7.1 Tolterodine
218(1)
3.3.8 Nonsteroidal Anti-Inflammatory Drugs
218(2)
3.3.8.1 Acetaminophen
218(2)
3.3.8.2 Indomethacin
220(1)
3.3.9 Oral Hypoglycemic Drugs
220(1)
3.3.9.1 Phenformin
220(1)
3.3.10 Selective Estrogen Receptor Modulators
221(6)
3.3.10.1 Tamoxifen
222(4)
3.3.10.2 Droloxifene
226(1)
3.3.10.3 Enclomifene
226(1)
3.3.10.4 Lasofoxifene
226(1)
3.3.11 Selective Phosphodiesterase Type 5 Inhibitors
227(1)
3.3.12 Other Drugs and Compounds
227(5)
3.4 Drugs of Abuse as Substrates of CYP2D6
232(4)
3.4.1 Amphetamine Derivatives
232(1)
3.4.2 β-Carbolines
232(1)
3.4.3 Designer Drugs
233(1)
3.4.4 Indolealkylamines
234(2)
3.5 Fluorescent Probes as Substrates of CYP2D6
236(1)
3.6 Plant Alkaloids, Toxicants, and Environmental Compounds as Substrates of CYP2D6
237(3)
3.6.1 Plant Alkaloids
237(1)
3.6.2 Neurotoxin
237(1)
3.6.3 Herbicides and Pesticides
238(2)
3.7 Endogenous Compounds as Substrates of CYP2D6
240(5)
3.7.1 5-Methoxyindolethylamine
240(1)
3.7.2 Tyramines
240(1)
3.7.3 Steroids and Neurosteroids
241(3)
3.7.4 Endogenous Morphine
244(1)
3.7.5 Endocannabinoid Arachidonoylethanolamide (Anandamide)
244(1)
3.8 Structure-Activity Relationships of CYP2D6 Substrates
245(1)
3.9 Conclusions and Future Directions
246(10)
References
256(33)
Chapter 4 Inhibitors of Human CYP2D6 289(26)
4.1 Introduction
289(1)
4.2 Selective Inhibitors of CYP2D6
289(10)
4.3 Mechanism-Based Inhibitors of CYP2D6
299(1)
4.3.1 Paroxetine
299(1)
4.3.2 Cimetidine
299(1)
4.3.3 Metoclopramide
299(1)
4.3.4 Pimozide
300(1)
4.3.5 Other Compounds
300(1)
4.4 Reversible and Mixed-Type Inhibitors of CYP2D6
300(7)
4.4.1 Central Nervous System Drugs
300(3)
4.4.1.1 Antipsychotics
300(1)
4.4.1.2 SSRIs
301(1)
4.4.1.3 Tricyclic Antidepressants
302(1)
4.4.1.4 Other Antidepressants
302(1)
4.4.1.5 Narcotics
302(1)
4.4.1.6 Other Central Nervous System Drugs
302(1)
4.4.2 H1 Receptor Antagonists
303(1)
4.4.3 Antifungal Agents
304(1)
4.4.4 Anti-HIV Agents
304(1)
4.4.5 Steroids
304(1)
4.4.6 Other Drugs
304(2)
4.4.7 Amphetamine Analogs
306(1)
4.4.8 Natural and Herbal Compounds
307(1)
4.5 Structure-Activity Relationships of CYP2D6 Inhibitors
307(1)
4.6 Conclusions and Future Directions
308(1)
References
308(7)
Chapter 5 Regulation of Human CYP2D6 315(26)
5.1 Introduction
315(1)
5.2 Effects of Physiological Factors on CYP2D6 Activity
316(2)
5.2.1 Gender
316(1)
5.2.2 Developmental Changes (Ontogeny) of CYP2D6 Expression and Activity
316(1)
5.2.3 Pregnancy Induces CYP2D6
317(1)
5.2.4 Fasting
318(1)
5.3 Effects of Environmental Factors on CYP2D6 Activity
318(2)
5.3.1 Smoking
318(1)
5.3.2 Alcoholic Cirrhosis
319(1)
5.3.3 Herbal Medicines
319(1)
5.4 Human CYP2D6 Is Largely Uninducible by Prototypical Inducers of CYPs
320(1)
5.4.1 In Vitro Studies
320(1)
5.4.2 In Vivo Studies
320(1)
5.5 Transcriptional and Posttranscriptional Regulation of CYP2D6 by HNF-4α and FXR
321(2)
5.5.1 Transcriptional Regulation of CYP2D6 by HNF-4α
321(1)
5.5.2 Transcriptional Regulation of CYP2D6 by FXR
322(1)
5.6 Posttranslational Regulation of CYP2D6
323(1)
5.7 Genome-Wide Association Studies on the Regulation of CYP2D6
323(1)
5.8 Effects of Diseases on CYP2D6 Expression and Activity
324(3)
5.8.1 Liver Diseases
324(2)
5.8.2 Chronic Renal Failure
326(1)
5.8.3 Diabetes
326(1)
5.8.4 Rheumatoid Arthritis
327(1)
5.8.5 Cytokines and Inflammation
327(1)
5.9 Conclusions and Future Directions
327(1)
References
327(14)
Chapter 6 Structure and Function of Human CYP2D6 341(74)
6.1 Introduction
341(1)
6.2 Pharmacophore Models and Structural Requirements of CYP2D6 Ligands
341(2)
6.3 Homology Modeling Studies of Human CYP2D6
343(3)
6.3.1 Homology Models Derived from Bacterial CYPs
343(1)
6.3.2 Homology Models Derived from Rabbit CYP2C5 Structures
344(2)
6.4 Site-Directed Mutagenesis Studies of CYP2D6
346(12)
6.4.1 Pro34
346(1)
6.4.2 Gly42
346(1)
6.4.3 Ala90
347(1)
6.4.4 Asp100
347(1)
6.4.5 Thr107
347(1)
6.4.6 Phe120, Phe481, and Phe483
348(1)
6.4.7 Trp128
349(1)
6.4.8 Val136
350(1)
6.4.9 Glu156
350(1)
6.4.10 Gly169
350(1)
6.4.11 Glu216 and Asp301
350(3)
6.4.12 Lys281
353(1)
6.4.13 Glu222
353(1)
6.4.14 Arg296
353(1)
6.4.15 Ser304
353(1)
6.4.16 Thr309 and Thr312
354(1)
6.4.17 His324
355(1)
6.4.18 Val338
356(1)
6.4.19 Met374
356(1)
6.4.20 Glu410
356(1)
6.4.21 Arg440
356(1)
6.4.22 Ser486
356(2)
6.5 Studies Using Aryldiazene Probes
358(1)
6.6 Antibody Studies of Human CYP2D6
359(1)
6.7 Other Molecular Modeling Studies
360(1)
6.8 X-Ray Crystallographic Study of Human CYP2D6 and Functional Implications
360(7)
6.8.1 Secondary Structure of CYP2D6 in Comparison with CYP2C9
360(1)
6.8.2 Active-Site Cavity of CYP2D6
361(1)
6.8.3 Key Active-Site Amino Acids of CYP2D6
362(2)
6.8.3.1 Ile106
362(1)
6.8.3.2 Leu213 and Val308
362(1)
6.8.3.3 Glu216
362(1)
6.8.3.4 Asp301
362(1)
6.8.3.5 Thr309
363(1)
6.8.3.6 Met374
363(1)
6.8.3.7 Phe120, Phe481, and Phe483
364(1)
6.8.3.8 Arg441
364(1)
6.8.4 Heme-Binding Site
364(1)
6.8.5 Access and Egress Channels
364(1)
6.8.6 Binding Region for Cytochrome P450 Reductase
365(1)
6.8.7 Plasticity of CYP2D6
365(1)
6.8.8 A Comparison of the Homology Model and Crystal Structure of CYP2D6
366(1)
6.8.9 Binding of Atypical Substrates to Human CYP2D6
366(1)
6.9 Bindings Modes of the Substrates and Inhibitors with CYP2D6
367(40)
6.9.1 Binding Modes of the Substrates with CYP2D6 Active Site
368(7)
6.9.2 Binding Modes of the Inhibitor with the CYP2D6 Active Site
375(32)
6.10 Conclusions and Future Directions
407(1)
References
407(8)
Chapter 7 Clinical Pharamcogenomics of Human CYP2D6 415(68)
7.1 Introduction
415(1)
7.2 Interindividual Variability in CYP2D6 Expression and Activity
416(1)
7.3 Alleles of the CYP2D6 Gene
416(14)
7.3.1 Null Alleles of CYP2D6
416(11)
7.3.1.1 Null Alleles Attributed to Single Base Mutation or Small Insertions/Deletions
425(1)
7.3.1.2 Nonfunctional Full-Length Coded Alleles
426(1)
7.3.1.3 Deletion of the Entire Gene
426(1)
7.3.1.4 Formation of Hybrid Genes
426(1)
7.3.2 Alleles with Partial or Residual Function
427(2)
7.3.3 Alleles with Largely Normal or Increased Activity
429(1)
7.3.4 Duplication and Multiduplication of CYP2D6
429(1)
7.4 Ethnic Variation in the Distribution of CYP2D6 Polymorphisms
430(1)
7.5 Antianginal Drugs
431(1)
7.5.1 Perhexiline
431(1)
7.6 Antiarrhythmic Drugs
431(5)
7.6.1 Flecainide
432(1)
7.6.2 Mexiletine
433(1)
7.6.3 Propafenone
434(1)
7.6.4 Vernakalant
435(1)
7.7 Antidepressants
436(7)
7.7.1 Tricyclic Antidepressants
436(3)
7.7.1.1 Amitriptyline and Nortriptyline
436(1)
7.7.1.2 Clomipramine
436(1)
7.7.1.3 Doxepin
437(1)
7.7.1.4 Imipramine and Desipramine
437(1)
7.7.1.5 Maprotiline
438(1)
7.7.1.6 Trimipramine
438(1)
7.7.2 Selective Serotonin Reuptake Inhibitors
439(3)
7.7.2.1 Citalopram
439(1)
7.7.2.2 Fluvoxamine
439(1)
7.7.2.3 Fluoxetine
440(1)
7.7.2.4 Paroxetine
441(1)
7.7.2.5 Sertraline
441(1)
7.7.3 Other Antidepressants
442(1)
7.7.3.1 Mianserin
442(1)
7.7.3.2 Mirtazapine
442(1)
7.7.3.3 Venlafaxine
442(1)
7.7.3.4 Miscellaneous Antidepressants
443(1)
7.8 Antipsychotics
443(6)
7.8.1 Aripiprazole
443(1)
7.8.2 Chlorpromazine
444(1)
7.8.3 Haloperidol
444(2)
7.8.4 Perphenazine
446(1)
7.8.5 Risperidone
446(1)
7.8.6 Thioridazine
447(1)
7.8.7 Zuclopenthixol
447(1)
7.8.8 Miscellaneous and Atypical Antipsychotics
448(1)
7.8.8.1 Clozapine
448(1)
7.8.8.2 Olanzapine
448(1)
7.8.8.3 Miscellaneous Antipsychotics
448(1)
7.9 Centrally Acting Cholinesterase Inhibitors
449(1)
7.9.1 Donepezil
449(1)
7.9.2 Galantamine
449(1)
7.10 Drugs for the Treatment of Attention-Deficit/Hyperactivity Disorder
449(2)
7.10.1 Atomoxetine
449(2)
7.11 Drugs for the Treatment of Senile Dementia
451(1)
7.11.1 Nicergoline
451(1)
7.12 Antimuscarinic Drugs
451(1)
7.12.1 Tolterodine
451(1)
7.13 Antiemetics
451(1)
7.13.1 Dolasetron
451(1)
7.13.2 Ondansetron
451(1)
7.13.3 Tropisetron
451(1)
7.14 Antihistamine
452(1)
7.14.1 Chlorpheniramine
452(1)
7.14.2 Diphenhydramine
452(1)
7.14.3 Loratadine
452(1)
7.15 β-Blockers
452(2)
7.15.1 Carvedilol
452(1)
7.15.2 Metoprolol
453(1)
7.15.3 Propranolol
454(1)
7.15.4 Timolol
454(1)
7.16 Opioids
454(4)
7.16.1 Codeine
455(1)
7.16.2 Dihydrocodeine
455(1)
7.16.3 Hydrocodone
455(1)
7.16.4 Oxycodone
456(1)
7.16.5 Methadone
456(1)
7.16.6 Tramadol
457(1)
7.17 Oral Hypoglycemic Drugs
458(1)
7.17.1 Phenformin
458(1)
7.18 Selective Estrogen Receptor Modulators
459(1)
7.18.1 Tamoxifen
459(1)
7.19 Other Drugs
460(1)
7.19.1 Cevimeline
460(1)
7.19.2 Darifenacin
460(1)
7.19.3 Tetrabenazine
460(1)
7.19.4 Vortioxetine
460(1)
7.20 Conclusions and Future Perspectives
460(3)
References
463(20)
Chapter 8 General Discussion about Human CYP2D6 483(12)
References
489(6)
Index 495
Shufeng Zhou is the associate vice president of Global Medical Development and associate dean of international research in the College of Pharmacy of the University of South Florida in Tampa. He earned his PhD in pharmacology from the University of Auckland in New Zealand. His major research interests are systems pharmacology, drug metabolism and drug transport, pharmacokinetics/pharmacometrics, pharmacogenomics, nanomedicine, and Chinese medicine. He has published more than 450 peer-reviewed papers, 20 books and book chapters, and more than 440 conference abstracts. He was one of the Highly Cited Researchers of 2014 according to Thomson Reuter and has given more than 150 invited seminars and keynote presentations to academic institutions, government agencies, and high-profile international conferences. He serves as an editor or the editor in chief of at least 21 biomedical journals and is an editorial board member of more than 75 medical and pharmacological journals. He has received several national and international awards, is a voting member of US Pharmacopeia, a consultant for the World Health Organization and the Food and Drug Administration, and a council member or chair of several national and international professional societies.