東華大學圖書館 |

Drug design = from structure and mode-of-action to rational design concepts /

紀錄類型:	書目-電子資源 : Monograph/item
正題名/作者:	Drug design/ by Gerhard Klebe.
其他題名:	from structure and mode-of-action to rational design concepts /
作者:	Klebe, Gerhard.
出版者:	Berlin, Heidelberg :Springer Berlin Heidelberg : : 2024.,
面頁冊數:	xxviii, 686 p. :ill. (chiefly color), digital ;24 cm.
內容註:	Preface -- Introduction -- Part I Fundamentals of drug research -- 1 Drug research yesterday, today, tomorrow -- 2 In the beginning there was serendipity -- 3 Examples of classical drug research -- 4 Protein-ligand interactions as the basis of drug action -- 5 Optical activity and biological action -- Part II The search for lead structure -- 6 The classical search for lead structure -- 7 Screening technologies for lead structure search -- 8 The optimisation of lead structure -- 9 The design of prodrugs -- 10 Peptidomimetics. 6 The classical search for lead structure -- 7 Screening technologies for lead structure search -- 8 Lead structure optimisation -- 9 Design of prodrugs -- 10 Peptidomimetics.Part III Experimental and theoretical methods -- 11 Combinatorics: chemistry with large numbers -- 12 Genetic engineering in drug discovery -- 13 Experimental methods for structure elucidation -- 14 Description of the structure of biomolecules -- 15 Molecular modelling -- 16 Conformational analysis -- Part IV Quantitative structure-activity relationships and design methods -- 17 Pharmacophore hypotheses, molecular comparisons and database searches -- 18 Quantitative structure-activity relationships -- 19 From in vitro to in vivo: optimising ADME tox properties -- 20 Protein modelling and structure-based drug design -- 21 An example: structure-based design of inhibitors of tRNA-guanine transglycosylase -- Part V Successes in rational drug design -- 22 How drugs work: targets for therapy -- 23 Inhibitors for hydrolases with acyl enzyme intermediates -- 24 Inhibitors of aspartyl proteases -- 25 Inhibitors of hydrolytically cleaving metalloenzymes -- 26 Inhibitors for transferases -- 27 Inhibitors for oxidoreductases -- 28 Agonists and antagonists for nuclear receptors -- 29 Agonists and antagonists of membrane receptors -- 30 Ligands for channels, pores and transporters -- 31 Ligands for surface receptors -- 32 Biopharmaceuticals: peptides, proteins, nucleotides and macrolides as active substances.
Contained By:	Springer Nature eBook
標題:	Drugs - Design. -
電子資源:	https://doi.org/10.1007/978-3-662-68998-1
ISBN:	9783662689981

Drug design = from structure and mode-of-action to rational design concepts /
Klebe, Gerhard.

Drug designfrom structure and mode-of-action to rational design concepts /[electronic resource] :by Gerhard Klebe. - Berlin, Heidelberg :Springer Berlin Heidelberg :2024. - xxviii, 686 p. :ill. (chiefly color), digital ;24 cm.

Preface -- Introduction -- Part I Fundamentals of drug research -- 1 Drug research yesterday, today, tomorrow -- 2 In the beginning there was serendipity -- 3 Examples of classical drug research -- 4 Protein-ligand interactions as the basis of drug action -- 5 Optical activity and biological action -- Part II The search for lead structure -- 6 The classical search for lead structure -- 7 Screening technologies for lead structure search -- 8 The optimisation of lead structure -- 9 The design of prodrugs -- 10 Peptidomimetics. 6 The classical search for lead structure -- 7 Screening technologies for lead structure search -- 8 Lead structure optimisation -- 9 Design of prodrugs -- 10 Peptidomimetics.Part III Experimental and theoretical methods -- 11 Combinatorics: chemistry with large numbers -- 12 Genetic engineering in drug discovery -- 13 Experimental methods for structure elucidation -- 14 Description of the structure of biomolecules -- 15 Molecular modelling -- 16 Conformational analysis -- Part IV Quantitative structure-activity relationships and design methods -- 17 Pharmacophore hypotheses, molecular comparisons and database searches -- 18 Quantitative structure-activity relationships -- 19 From in vitro to in vivo: optimising ADME tox properties -- 20 Protein modelling and structure-based drug design -- 21 An example: structure-based design of inhibitors of tRNA-guanine transglycosylase -- Part V Successes in rational drug design -- 22 How drugs work: targets for therapy -- 23 Inhibitors for hydrolases with acyl enzyme intermediates -- 24 Inhibitors of aspartyl proteases -- 25 Inhibitors of hydrolytically cleaving metalloenzymes -- 26 Inhibitors for transferases -- 27 Inhibitors for oxidoreductases -- 28 Agonists and antagonists for nuclear receptors -- 29 Agonists and antagonists of membrane receptors -- 30 Ligands for channels, pores and transporters -- 31 Ligands for surface receptors -- 32 Biopharmaceuticals: peptides, proteins, nucleotides and macrolides as active substances.

This English-language textbook, based on the successful German edition 'Wirkstoffdesign', brings the subject of drug design back to the cutting edge of research. The reader learns about new methods in genetic engineering and the expanded range of structural biological methods. Especially in the last 10 years, many complex target structures such as G-protein coupled receptors or ion channels have been elucidated by using these methods. The reader learns how these long-sought complex structures with classical drugs look like and how the therapeutic effect is achieved. This textbook is aimed at students of pharmacy, chemistry and the life sciences, but also at career changers and medicinal chemists in research and development departments of the pharmaceutical industry. Conceptually, it is very different from classical textbooks on pharmaceutical chemistry. It focuses on the path to a new drug substance. The selection of case studies is based on didactic aspects and attempts to give a broad overview of methods and strategies without forgetting to look back at the beginnings of this field of work. Thus, the arc spans from the history of drug research, the mechanisms of action of drugs and the methods for lead structure search and optimisation to structure determination methods, modelling, molecular dynamics and QSAR methods to structure- and computer-aided design. Videos via app: simply download the SN More Media app free of charge, scan a link with the play button or use the printed QR code and immediately play the video on your smartphone or tablet.

ISBN: 9783662689981

Standard No.: 10.1007/978-3-662-68998-1doiSubjects--Topical Terms:

664528
Drugs
--Design.

LC Class. No.: RS420

Dewey Class. No.: 615.19

Drug design = from structure and mode-of-action to rational design concepts /
LDR:04644nmm a2200337 a 4500 001 2389552
003 DE-He213
005 20250205115222.0
006 m d
007 cr nn 008maaau
008 250916s2024 gw s 0 eng d
020 $a 9783662689981 $q (electronic bk.)
020 $a 9783662689974 $q (paper)
024 7 $a 10.1007/978-3-662-68998-1 $2 doi
035 $a 978-3-662-68998-1
040 $a GP $c GP
041 1 $a eng $h ger
050 4 $a RS420
072 7 $a MMG $2 bicssc
072 7 $a MED071000 $2 bisacsh
072 7 $a MKG $2 thema
082 0 4 $a 615.19 $2 23
090 $a RS420 $b .K63 2024
100 1 $a Klebe, Gerhard. $3 767670
240 1 0 $a Wirkstoffdesign. $l English
245 1 0 $a Drug design $h [electronic resource] : $b from structure and mode-of-action to rational design concepts / $c by Gerhard Klebe.
260 $a Berlin, Heidelberg : $b Springer Berlin Heidelberg : $b Imprint: Springer, $c 2024.
300 $a xxviii, 686 p. : $b ill. (chiefly color), digital ; $c 24 cm.
505 0 $a Preface -- Introduction -- Part I Fundamentals of drug research -- 1 Drug research yesterday, today, tomorrow -- 2 In the beginning there was serendipity -- 3 Examples of classical drug research -- 4 Protein-ligand interactions as the basis of drug action -- 5 Optical activity and biological action -- Part II The search for lead structure -- 6 The classical search for lead structure -- 7 Screening technologies for lead structure search -- 8 The optimisation of lead structure -- 9 The design of prodrugs -- 10 Peptidomimetics. 6 The classical search for lead structure -- 7 Screening technologies for lead structure search -- 8 Lead structure optimisation -- 9 Design of prodrugs -- 10 Peptidomimetics.Part III Experimental and theoretical methods -- 11 Combinatorics: chemistry with large numbers -- 12 Genetic engineering in drug discovery -- 13 Experimental methods for structure elucidation -- 14 Description of the structure of biomolecules -- 15 Molecular modelling -- 16 Conformational analysis -- Part IV Quantitative structure-activity relationships and design methods -- 17 Pharmacophore hypotheses, molecular comparisons and database searches -- 18 Quantitative structure-activity relationships -- 19 From in vitro to in vivo: optimising ADME tox properties -- 20 Protein modelling and structure-based drug design -- 21 An example: structure-based design of inhibitors of tRNA-guanine transglycosylase -- Part V Successes in rational drug design -- 22 How drugs work: targets for therapy -- 23 Inhibitors for hydrolases with acyl enzyme intermediates -- 24 Inhibitors of aspartyl proteases -- 25 Inhibitors of hydrolytically cleaving metalloenzymes -- 26 Inhibitors for transferases -- 27 Inhibitors for oxidoreductases -- 28 Agonists and antagonists for nuclear receptors -- 29 Agonists and antagonists of membrane receptors -- 30 Ligands for channels, pores and transporters -- 31 Ligands for surface receptors -- 32 Biopharmaceuticals: peptides, proteins, nucleotides and macrolides as active substances.
520 $a This English-language textbook, based on the successful German edition 'Wirkstoffdesign', brings the subject of drug design back to the cutting edge of research. The reader learns about new methods in genetic engineering and the expanded range of structural biological methods. Especially in the last 10 years, many complex target structures such as G-protein coupled receptors or ion channels have been elucidated by using these methods. The reader learns how these long-sought complex structures with classical drugs look like and how the therapeutic effect is achieved. This textbook is aimed at students of pharmacy, chemistry and the life sciences, but also at career changers and medicinal chemists in research and development departments of the pharmaceutical industry. Conceptually, it is very different from classical textbooks on pharmaceutical chemistry. It focuses on the path to a new drug substance. The selection of case studies is based on didactic aspects and attempts to give a broad overview of methods and strategies without forgetting to look back at the beginnings of this field of work. Thus, the arc spans from the history of drug research, the mechanisms of action of drugs and the methods for lead structure search and optimisation to structure determination methods, modelling, molecular dynamics and QSAR methods to structure- and computer-aided design. Videos via app: simply download the SN More Media app free of charge, scan a link with the play button or use the printed QR code and immediately play the video on your smartphone or tablet.
650 0 $a Drugs $x Design. $3 664528
650 1 4 $a Pharmacology. $3 634543
650 2 4 $a Pharmaceutics. $3 3538434
650 2 4 $a Pharmacy. $3 636101
650 2 4 $a Medicinal Chemistry. $3 892420
650 2 4 $a Chemistry. $3 516420
650 2 4 $a Life Sciences. $3 890838
710 2 $a SpringerLink (Online service) $3 836513
773 0 $t Springer Nature eBook
856 4 0 $u https://doi.org/10.1007/978-3-662-68998-1
950 $a Medicine (SpringerNature-11650)