Thiophene 1
Thiophene 1
Thiophene 1
ChemInform Abst ract : Synt hesis of Novel 2-Aminot hiophene-3-carboxylat es by Variat ions of t he Gew…
Ralf Lyssy
Available online at www.derpharmachemica.com
ISSN 0975-413X
CODEN (USA): PCHHAX
ABSTRACT
Thiophene nucleus has been established as the potential entity in the largely growing chemical
world of heterocyclic compounds possessing promising pharmacological characteristics. The
similar compounds synthesized through different routes bear variable magnitudes of biological
activities. The knowledge of various synthetic pathways and the diverse physicochemical
parameters of such compounds draw the especial attention of medicinal chemists to produce
combinatorial library and carry out exhaustive efforts in the search of lead molecules. The
present review provides a broad view of the synthesis and properties of compounds having
thiophene nucleus.
INTRODUCTION
As the world’s population increases and health problems expand accordingly, need to discover
new therapeutics will become even more diring. The design of drug molecules arguably offers
some of the greatest hopes for success in present and future era. Heterocyclic compounds are
widely distributed in nature and are essential for life. There are vast numbers of
pharmacologically active heterocyclic compounds many of which are in regular clinical use[1].
The investigational approaches towards Structure- Activity Relationship focusing the search of
optimized candidates have become immensely important.
Thiophene belongs to a class of heterocyclic compounds containing a five membered ring made
up of one sulphur as heteroatom with the formula C4H4S. Thiophene and its derivatives exist in
petroleum or coal. Thiophene is taken from the word theion, the Greek word for sulfur, and
another Greek word phaino which means shinning. Thiophene structure can be found in certain
natural products and is also incorporated in several pharmacologically active compounds.
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4 3
5 2
S
1
Thiophene
In medicinal chemistry, thiophene derivatives have been very well known for their therapeutic
applications. The simple thiophenes are stable liquids which closely resemble the corresponding
benzene compounds in boiling point and even in smell[2]. They occur in coal tar distillates. The
discovery of thiophene in coal tar benzene provides one of the classic anecdotes of organic
chemistry.
Thiophene was discovered as a contaminant in benzene[3]. It was observed that isatin (1H-
indole-2, 3- Dione) forms a blue dye if it is mixed with sulfuric acid and crude benzene. Victor
Meyer was able to isolate the substance responsible for this reaction. The compound was found
to be a heterocyclic compound- Thiophene.
Thiophene has a structure that is analogous to structure of pyrrole, and due to pie electron cloud,
it behave like extremely reactive benzene derivative.
An alternative route that has been used is the Friedel- Crafts acylation followed by Wolff-
Kishner reduction. Thiophene acylate preferentially in the α-position and thus 2-acyl-5-
alkylthiophenes can also be accessed by this route from 2-alkyl thiophenes. When both α-
positions are alkyl substituted, acylation occurs in the β-position to produce 3-acyl-2, 5-
dialkylthiophenes such as 2, 5-dimethyl- 3-acetylthiophene (1).
COCH 3
H3C CH3
S
1
Synthetic approaches to the construction of thiophene and substituted thiophene have been
efficiently developed. Thiophene ring can be constructed from non-heterocyclic precursors by
two reaction pathways[5]:
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Depending upon the following reaction pathways, various synthetic procedures have been
developed, leading to different substituted thiophene.
OH CH3
O P4 S10
0
250 S
O
HO
Paal Thiophene Synthesis
Source of sulfur used are traditionally phosphorus sulfides, latterly Lawesson’s reagent(LR)[6],
or bis(trimethylsilyl) sulfide[7].
S
S
P O
P CH3
S
S
H3C
O
Lawesson’s Reagent
Paal and Knorr individually described the initial examples of condensation reactions between 1,
4- diketones and primary amines, which became to known as the Paal- Knorr pyrrole
synthesis[8]. The basic mechanism of this synthetic procedure involves cyclization of 1,4-
diketones, either in the presence of a primary amine (Paal- Knorr pyrrole synthesis), in the
presence of a sulphur source (Paal Thiophene synthesis), or by dehydration of the diketone itself
(Paal Furan synthesis)[9].
Reagents such as phosphorus pentasulfide or Lawesson's reagent act as sulfurizing agents as well
as dehydrating agents, allowing a reaction pathway that could lead first to the formation of
furans. This hypothesis was tested by Campaigne and coworkers in 1952. They were able to
prove that Paal Thiophene Synthesis could not proceed via furan as intermediate. Instead it went
through the formation of a thione. To prove this they conducted parallel experiments. Direct
comparisons were made between the reactions of 2,5-hexanedione and 1,2- dibenzoylethane with
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P2S5 and the reactions of 2,5-dimethylfuran and 2,5-diphenylfuran under the Paal Thiophene
Synthesis conditions. Reactions utilizing the diketones provided a greater yield of the thiophene
suggesting that the furan is not an essential intermediate in the reaction pathway, but rather a by-
product[10].
R R O
R R
O
O P2S5
P2S5
R S
R S
R
R
Based on the above observations, it was proposed that the mechanism involves initial formation
of thione (X = O or S), which is followed by tautomerization and cyclization. Aromaticity drives
the facile elimination of either H2O or H2S resulting in the thiophene product.
.
H3C H3C :SH H3C S
CH3 CH3 CH3
CH3
O P2S5 S XH
H3C
X X H
X
H3C S
CH3
This synthetic method for thiophene had been subjected to considerable variations and
improvements over time. The standard procedure for the Paal Thiophene Synthesis is to use
phosphorus pentasulphide as the sulphur atom source. The product is always a mixture
containing furan due to the dehydrating effect of P2S5 as an additional property.
A number of other reagents had been developed to take care of the sulphur source and
dehydration. Hydrogen sulphide, in the presence of an acid catalyst, was found to be more
efficient than phosphorus pentasulphide at converting ketones to thione.
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R2 COOMe O
HS S
R2
O R3 R1
O
R1 R3 OH
Fiesselmann Thiophene Synthesis proceeds through consecutive base-catalyzed 1, 4- conjugate
addition reactions to form thioacetal. Treatment with stronger base results in the formation of an
enolate while intramolecular reaction through Dieckmann condensation leads to the formation of
a ketone. Eliminating methylthioglycolate and tautomerization propelled by aromaticity provides
the 3-hydroxyl thiophene dicarboxylate.
OCH3 OCH3
- O OCH 3 O
S
CH3 S S -
- H3CO O
H3CO O
H 3COOC S
H3COOC
O CH3
COOCH3
+
COOCH3 H
COOCH3
O OCH3
OH -HSCH2COOCH3
S O NaOMe
S S
Tautomerism Rearrangement H CO
3 OH
S
COOCH3 S H3COOC
COOCH3
COOCH3 COOCH3
Therefore, thiophene can be synthesized from reactions of thioglycolic acid derivatives and β -
keto esters, α, β -dihalo esters and α - and β -halovinyl esters, along with the corresponding
nitriles, ketones and aldehydes. Furthermore, a variety of α-mercaptocarbonyl systems can be
used in place of the thioglycolic acid derivatives and this extends the applicability of this
reaction[9].
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R1
R1 O S8
NC
R2 X
+ X Amine
R2 S
NH2
The first step in the mechanism of the Gewald reaction is the Knoevenagel condensation of an
activated nitrile with a ketone or aldehyde to produce an acrylonitrile. The product of this
condensation is then thiolated at the methylene position. The sulfurated compound initially
decays to the mercaptide compound which then undergoes a cyclization reaction via mercaptide
attack at the cyano group. Base-catalyzed tautomerization affords the 2-aminothiophene[14].
+
R' S
O N O -
R N
R + OR" -H2O S H
R"O N R"O
R' O
O R R'
S
H2N R'
O R
OR"
Reaction mechanism involved in Gewald Aminothiophene Synthesis
OEt
O EtO S HO O
O
O S
O
O OH
NaOEt, EtOH
Ph Ph
Et CH3
S
ii) Using carbon disulfide
2-alkylthiophenes[21] can be synthesized by the addition of a carbanion to carbon disulfide with
a subsequent S-alkylation.
CH 3CO
O
S
CS 2 , K 2 CO 3
S
DMF
O H 3C
O
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R2 Br
NO 2
Ph
O R1
N
DBU, PhH N
O 2N S S
DBU
S S
ii) Thiophene can be synthesized by passing a mixture of acetylene and hydrogen sulfide through
a tube containing alumina at 400°C. This method is commercially used.
S
HC CH +
H 2S H2 +
iii) Thiophene may also be prepared by heating sodium succinate with phosphorous trisulphide.
+ P2S 3
Na OOC
S
+
COONa
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R R
R1
I R1
CuI S
R2
I + K2S
MeCN
o
R3 140 C(sealed), 24hr R R3
2
ii) An efficient one-step method for the synthesis of highly substituted thiophenes from
thiomorpholides and α-haloketones has been developed[24].
Ar O Ar
Br
S K 2 CO 3
R N
N
+ O Toluene
6-8hrs S
R'
R'
O
R
iii) Conditions for the palladium-catalyzed direct arylation of a wide range of heterocycles with
aryl bromides employ a stoichiometric ratio of both coupling partners, as well as a
substoichiometric quantity of pivalic acid, which results in significantly faster reactions.
An evaluation of the influence of the nature of the aryl halide has also been carried out[25].
S S
R Pd(OAc) R Ar
Ar Br 2
+ K 2 CO 3 Y
Y
Y= CH(R= alkyl, CHO, COOEt, OMe); N (R= H, Alkyl)
R R'O
R"
AuCl
0
S Toluene, 25 C, 2hr R
S
OR' R"
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desulfuration[29] have been carried out. Coordination chemistry of such compounds has
received recent attention because of its relevance to metal-catalysed hydro desulfuration of fossil
fuels[30].
Coordination can occur through sulfur atom, through the 2- and 5- carbon or both(η1) or through
π- clouds of C(2)= C(3) or C(4)= C(5) bonds (η2) or both(η4).
Thiophene-based compounds have also found widespread use in modern drug design[32],
biodiagnostics[33], electronic and optoelectronic devices[34] and conductive and
electroluminescent polymers[35]. Also several reviews of various aspects of thiophene
coordination and reactivity in transition metal complexes have been reported[36].
Thiophene is considered aromatic, although theoretical calculations suggest that the degree of
aromaticity is less than that of benzene. This could be demonstrated by its ability to undergo
substitution reaction.
Thiophene is a toxic and flammable aromatic compound. It is insoluble in water but soluble in
most organic solvents including alcohol and ether. Melting Point of thiophene is -38°C while
boiling point is 84°C.
Critical temperature of Thiophene has been determined by sealed- tube method and is found to
be 579.4K. From the heat of combustion and from the values of thermochemical bond energies, a
resonance energy of 20 Kcal./mol was calculated for thiophene. Dipole moments were used in
connection with estimation of electron distribution and substituent effect in thiophene and for
conformation of molecular orbital calculations(MO)[37].
Table1: Dipole moment of thiophene(in debyes)
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The "electron pairs" on sulfur are significantly delocalized in the pi electron system[38].
Thiophene has a higher degree of stabilization than the analogous furan. This is due to the fact
that sulphur has a lager bonding radius (length) and therefore sulphur could tolerate a positive
charge better as a result of inductive pull towards sulphur[39]. These contributions to its stability
can be envisaged from the canonical form of thiophene.
+
- -
S
.. S
.. +
A B
Thiophenes do not undergo the oxidation typical of a sulfides. Thiophene undergoes electrophilic
substitution: nitration, sulfonation, halogenation, Friedel-Crafts acylation etc. Even the thiophene
can undergo Reimer-Tiemann reaction and coupling diazonium salts formation.
Considerable recent attention has been given to investigations into modifications of substituents
in the presynthesized thiophene structure. In addition many studies were devoted to the use of
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various thiophene derivatives in the synthesis of linearly and angularly polyannelated, including
previously unknown heterocyclic systems.
O2N
S
Piperidine
Br N NO2
S
CH3OH
80% S
S
COCH3
ii) Sulfonation
Sulfonation of thiophene by sulphuric acid gives thiophene-2-sulfonic acid. and 2-
chlorosulfonation[45] is efficient.
PCl5 , ClSO 3 H
70% S
S
SO2Cl
iii) Nitration
Nitration of thiophene should be carried out in the absence of nitrous acid as it can lead to an
explosive reaction[46]. To prevent this, acety1 nitrate or nitronium tetraflouroborate[47] are
satisfactory. The major 2-nitro-product is accompanied by approximately 10% of the 3- nitro
isomer[48].
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NO2
Conc.HNO 3 , (CH 3 CO) 2O
70% S
+ S
S
NO2
iv) Halogenation
At room temperature halogenation of thiophene occurs readily and is rapid even at –300 C in the
dark. The rate of halogenation of thiophene, at 250 C, is about 108times that of benzene[49].
I2 , HNO 3 (aq.)
90% S
S
I
Br
2XBr
48% S
S
Br
Cl
SnCl 2 , CH 2 Cl 2
(CH3 COO) 4 Pb S
S
Cl
d. Addition at sulfur
Thiophene sulfur can add electrophilic species. Thiophenium salts[53] though not formed
efficiently from thiophene itself, are produced in high yields with polyalky1-substituted
thiophenes[54]. The sulfur in such salts is probably tetrahedral i.e. the sulfur is sp3 hybridised.
H3C H3C
CH3 CH3
MeoSO2F
H3C H3C
NaPF6 +
S S
CH3 - CH3
MePF6
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are widely used. Thiophene nucleus is one of the most important heterocycles exhibiting
remarkable pharmacological activities. Thiophene moiety carrying compounds exhibit various
activities like for example 1-[1- (2, 5- dimethylthiophen- 3- yl) ethyl]- 1-hydroxyurea (2) shows
antiinflammatory activity; the maleate salt of 1-(2,5-dimethylthiophen- 3- yl)- 3-(5- methyl- 1 H-
imidazol- 4- yl) propan-1-one (3) act as serotonin antagonists and is used in the treatment of
Alzheimer’s disease. The latter has also been employed in the formulation of inks for computer
printers by the Xerox Group[55] and as a raw material for herbicides/ pesticides[56].
H2NOC S
N OH
N
S O
NH
(2) (3)
2-butylthiophene (4) has been employed as a raw material in the synthesis of anticancer agents
and 2-octylthiophene (5) has been employed in the synthesis of anti-atherosclerotic agents such
as (6).
S S
(4) (5)
H 11 C 8 S
NH
H 5 C 2 OOC
(6)
It also has applications in metal complexing agents and in the development of insecticides. The
higher alkylated thiophenes (7) also have other uses like 2-hexylthiophene has been used
extensively as a raw material in patents relating to liquid crystals.
S
NH
R
OH
OH R= C2H5-C6H13
(7)
As far as biological activity is concerned, fused hetero-aromatic systems are often of greater
interest than monocyclic compounds.
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Thiophene can be fused with various heterocyclic systems giving rise to various new
heterocyclic system with enhanced biological activity. Thienopyrimidines occupy a special
position among these compounds.
Along with some other pyrimidine systems containing an annelated five-membered hetero-
aromatic ring, thienopyrimidine are structural analogs of biogenic purines and can be considered
as potential nucleic acid antimetabolites.
CONCLUSION
The analytical and other informational data, available in literature so far, have rendered
thiophenes significantly important class of heterocyclic compounds and their applications in ever
challenging chemotherapy of various ailments/ infections etc. since last two decades immensely
hiked interests of medicinal chemist and biochemist.
This particular review article, in reference, would extend great deal of help to researchers in
reckoning and determining the best and most productive, economical, suggestive and conclusive
access to various thiophenes of clinical importance superseding other compounds of their class.
Acknowledgement
The authors are thankful to librarians of various Institutions & libraries like Jamia Hamdard New
Delhi, National Medical Library New Delhi, NISCAIR New Delhi, CDRI Lucknow, IVRI
Bareilly and to the Teerthanker Mahaveer College of Pharmacy, Teerthanker Mahaveer
University, Moradabad for providing literature survey facility to carry out the work.
REFERENCE
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