Signposts to Chiral Drugs: Organic Synthesis in Action - Rilegato

Recensione

From the reviews:

“In this timely book, Šunjić and Parnham provide an exciting selection of major achievements in drug development and unfold 15 intriguing success stories of aliskiren, vancomycin, paclitaxel, menthol, efavirenz, and others from the perspective of a medicinal chemist. ... This book will be most appealing to undergraduate and graduate students with an interest in synthesis and stereochemistry ... . it should be considered an instructive teaching supplement that underscores the general significance and impact of creative synthetic chemistry and stimulates further discussion in the classroom.” (Christian Wolf, Journal of the American Chemical Society, September, 2011)

“The subject of the book are chiral drugs. ... Each chapter can be read separately and consists of an abstract, introduction, the main part with the synthetic approach to a certain drug, conclusion and references. ... References are relevant and up-to date. A long list of abbreviations and acronyms is provided at the beginning ... . The book will be very useful to synthetic organic and medicinal chemists in innovative pharmaceutical companies and to scientists and ambitious students of chemistry and pharmacy.” (Branka Zorc, Acta Pharmaceutica, Vol. 61, 2011)

“This ... volume will be of interest to those working in synthetic organic chemistry, particularly in the medicinal chemistry area, and having as their aim the discovery of new drug entities for the pharmaceutical industries. ... there is also a useful summary of synthetic methods and concepts that are developed in the individual chapters, together with a useful index. The standard of presentation is very high, with many clearly presented reaction schemes, and each chapter has a comprehensive list of references to the specific area.” (D. W. Allen, Inflammopharmacology, Vol. 19, 2011)

Contenuti

1. Organic synthesis in drug discovery and development

1.      Introduction

2.      Synthetic organic chemistry in drug R&D process

3.      New concepts in drug discovery process

         3.1.   The impact of natural products upon modern drug discovery

3.2.    Biology oriented and DNA-templated synthesis in drug discovery

         3.3.   Incorporation of genomics in drug discovery

4.      Conclusion

References

2. Aliskiren fumarate

1.                 Introduction

2.            Renin and the mechanism of action of aliskiren

3.            Structural characteristics and synthetic approaches to aliskiren

3.1       Strategy based on visual imagery, starting from Nature’s chiral pool; a Dali-like presentation of objects

3.2 Fine-tuning of the chiral ligand for the Rh complex; hydrogenation of the selected substrate with extreme enantioselectivities

4.            Conclusion

References

3. (R)-K-13675

3.1   Introduction

3.2   Peroxisome proliferator-activated receptor a (PPARa) agonists.

3.2.1 b-Phenylpropionic acids

3.2.2 a-Alkoxy-b-arylpropionic acids

3.2.3 a-Aryloxy-b-phenyl propionic acids.

3.2.4 Oxybenzoylglycine derivatives.

3.3 Non-hydrolytic anomalous lactone ring-opening

3.4 Mitsunobu reaction in the ether bond formation

3.5 Conclusion

References

4. Sitagliptin phosphate monohydrate

4.1 Introduction

4.2 Endogenous glucoregulatory peptide hormones and dipeptidyl peptidase IV (DPP4) inhibitors

4.3 Synthesis with C-acyl mevalonate as the N-acylating agent

4.4   Highly enantioselective hydrogenation of unprotected b-enamino amides and the use of Josiphos-ligands

4.5 Ammonium chloride, an effective promoter of catalytic enantioselective hydrogenation

4.6 Conclusion

References

5. Biaryl unit in valsartan and vancomycin 

5.1 Introduction

5.2   Angiotensin AT1 receptor, G-protein coupled receptors (GPCRs).

5.3 Cu-promoted catalytic decarboxylative biaryl synthesis, biomimetic type aerobic decarboxylation

5.4 Stereoselective approach to axially chiral biaryl system; the case of vancomycin

5.5 Conclusion

References

6. 3-Amino-1,4-benzodiazepines

6.1 Introduction

6.2 3-Amino-1,4-benzodiazepine derivatives, g-secretase inhibitors

6.3 Configurational stability; racemization and enantiomerization

6.4 Crystallization induced asymmetric transformation

6.5 Asymmetric Ireland-Cleisen rearrangement

6.6 Hydroboration of the terminal C=C bond; anti-Markovnikov hydratation

6.7 Crystallization-induced asymmetric transformation in the synthesis of L-768,673

6.8 Conclusion

References

7. Sertraline

7.1 Introduction

7.2 Synaptosomal serotonin uptake and its selective inhibitors (SSRI)

7.3 Action of sertraline and its protein target

7.4 General synthetic route

7.5 Stereoselective reduction of ketones and imines under kinetic and thermodynamic control

7.5.1 Diastereoselectivity of hydrogenation of rac-tetralone-methylimine; the old (MeNH2/TiCl4/toluene) method is improved by using MeNH2/EtOH-Pd/CaCO3, 60-65 oC in a telescoped process

7.5.2 Kinetic resolution of racemic methylamine; hydrosylilation by (R,R)-(EBTHI)TiF2 /PhSiH3 catalytic system

7.5.3 Catalytic epimerization of the trans- to the cis-isomer of sertraline

7.5.4 Stereoselective reduction of tetralone by chiral diphenyloxazaborolidine

7.6. Desymmetrization of oxabenzonorbornadiene, Suzuki coupling of arylboronic acids and vinyl halides

7.7 Pd-Catalyzed (Tsuji-Trost) coupling of arylboronic acids and allylic esters

7.8 Simulated moving bed (SMB) in the commercial production of sertraline

7.9 Conclusion

References

8. 1,2-Dihydroquinolines