| Current
Organic Chemistry
ISSN: 1385-2728
Current Organic
Chemistry
Volume 12, Number 5, March 2008
Contents
Bioorganic Chemistry
Guest Editor: Harri Lönnberg
Editorial Pp. 342
Synthesis of 4'-C-modified 2'-Deoxyribonucleoside
Analogues and Oligonucleotides Pp. 343-354
Karl-Heinz Jung and Andreas Marx
[Abstract]
Peptide Backbone Modifications Pp. 355-385
Jan Deska and Uli Kazmaier
[Abstract]
General Articles
Transition Metal Catalyzed Asymmetric Oxidation of
Sulfides Pp. 386-404
Konstantin P. Bryliakov and Evgenii P. Talsi
[Abstract]
Catalytic Tandem Organic Sequences through Selective
Boron Addition Chemistry Pp. 405-423
Jesus Ramírez, Vanesa Lillo, Anna M. Segarra and
Elena Fernández
[Abstract]
Stable Isotope Coded Labeling Reagents for Quantitative
Proteomics Pp. 424-440
Zuly Rivera-Monroy, Guenther K. Bonn and András
Guttman
[Abstract]
Abstracts
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Editorial
This issue constitutes Part II of the thematic issue of Bioorganic
Chemistry. It contains two timely reviews that highlight backbone
modifications in oligonucleotides and peptides. The first
of them, contributed by Jung and Marx, compiles the synthetic
studies of 4´-substituted nucleosides and their incorporation
into oligonucleotides. These structural modifications have
gained interest for the reason that they may protect the oligonucleotide
backbone toward enzymatic degradation and simultaneously allow
introduction of conjugate groups in a manner that does not
hamper hybridization. Accordingly, the physico-chemical properties
of the oligonucleotide may conveniently be tuned by 4´-substitution.
The review by Deska and Kazmaier, in turn, concerns backbone
modifications of peptides. While human proteins and peptides
are composed almost exclusively of 20 common L-amino acids,
the amino acid content of peptide-based secondary metabolites
of lower organisms is much more versatile, and many of such
abnormal peptide structures exhibit pharmacological properties.
For this reason, and to obtain appropriate chemical models
for structural motives of proteins, synthesis of backbone
modified peptide has received wide interest. The results of
these synthetic efforts are compiled. I thank the contributors
for their thorough work. Hopefully many of the readers of
Current Organic Chemistry will find these reviews interesting.
Harri Lönnberg
Department of Chemistry
University of Turku
FIN-20014 Turku
Finland
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Synthesis of 4'-C-modified 2'-Deoxyribonucleoside
Analogues and Oligonucleotides
Karl-Heinz Jung and Andreas Marx
4'-C-Modified nucleotides and oligonucleotides have been
explored extensively recently. The motivations for these investigations
drive from the development of new drugs to investigations
of complex biological processes. This review covers the common
strategies for the synthesis of 4'-C-modified nucleosides
that have been subsequently incorporated into oligonucleotides.
After a brief depiction of two mainly followed routes for
the generation of 4'-C-modified nucleosides, the synthetic
efforts of the modified nucleotides are grouped into those
bearing hydrophobic or polar modifications. Subsequently strategies
for the incorporation of the respective nucleotides into oligonucleotides
by automated DNA synthesis are discussed.
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Peptide Backbone Modifications
Jan Deska and Uli Kazmaier
The selective introduction or manipulation of side chains
in a peptide represents a severe synthetic challenge. During
the last years numerous different approaches towards the targeted
modification of small to medium-sized peptides have been developed
which should be presented in this review. Focusing on the
manipulation of the peptide backbone, procedures concerning
selective N-alkylation, C-alkylation and
C=O-thionation are described.
[Back to top]
Transition Metal Catalyzed Asymmetric Oxidation of
Sulfides
Konstantin P. Bryliakov and Evgenii P. Talsi
In the past two decades, chiral sulfoxides have been finding
increasing use, reflecting growing interest both in convenient
auxiliaries in asymmetric synthesis and products with biological
properties containing a chiral sulfinyl group. In 1984, groups
of Kagan and Modena discovered that titanium(IV) isopropoxide
- diethyltartrate based systems (also known as “modified
Katsuki-Sharpless reagents”) are capable of asymmetric
oxidizing of prochiral sulfides by alkylhydroperoxides. Later,
catalytic versions of the titanium tartrate systems were developed
(with up to 90 % yield and 90 % ee for certain sulfides)
that remain the most applied systems for asymmetric sulfoxidations.
However, the low turnover numbers (5-20), complexity and expensiveness
of such systems stimulated the search for other transition
metal based catalytic systems. This review will cover the
progress in transition metal catalyzed asymmetric sulfides
oxidations achieved since the discoveries of early 1980s to
the present days.
[Back to top]
Catalytic Tandem Organic Sequences through Selective
Boron Addition Chemistry
Jesus Ramírez, Vanesa Lillo, Anna M. Segarra and
Elena Fernández
Transition metal-catalyzed addition of a mono- and a diboron
reagent to unsaturated carbon-carbon bonds provides an efficient
and convenient route for the preparation of mono- and diboronic
compounds. These compounds are versatile intermediates for
the purposes of organic synthesis. Catalytic control of the
chemo-, regio- and diastereoselective C-B formation enables
access to highly selective functionalized molecules by consecutive
tandem sequences. Mechanistic insights involving concatenated
reactions through boron chemistry are reviewed and discussed
with particular emphasis on the role of the catalytic systems,
the scope of the substrates and reagents, and the origin of
the asymmetric induction. Recent developments in the cascade
reaction from borylation or the formation of carbocycles via
multiple carborhodation steps triggered by the rhodium-catalyzed
intermolecular addition of organoboron are not covered, however,
since they have been the object of other reviews [1].
[Back to top]
Stable Isotope Coded Labeling Reagents for Quantitative
Proteomics
Zuly Rivera-Monroy, Guenther K. Bonn and András
Guttman
One of the most important subjects in contemporary
proteomics is the relative and absolute quantification of
gene expression at the protein level. The application of stable-isotope
coded tagging in conjunction with high performance bioanalytical
methods such as liquid chromatography and mass spectrometry
for the separation and identification of proteins and peptides
has proven successful to reveal global changes in protein
expression in both comparative and absolute manners. The rapid
progress in the field is evidenced by the introduction of
quite a few stable isotope labeled novel reagents for protein
and peptide tagging with particular structural characteristics.
In this review we focus on the chemical design, structure
and synthesis of the most important of such tagging reagents,
also addressing their advantages and limitations in quantitative
proteomics.
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