unsaturated ketone, alkene, 5-membered ringc286/retro.pdf · · 2000-11-151 Organic Synthesis and...
Transcript of unsaturated ketone, alkene, 5-membered ringc286/retro.pdf · · 2000-11-151 Organic Synthesis and...
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Organic Synthesis and Carbon-Carbon Bond Forming Reactions 1. To introduce basic concepts of organic synthesis: Retrosynthesis – thinking backwards from relatively complex molecules to simpler ones – the disconnection approach.
Target Molecule Precursors Solomons p169 - 172
n.b.
2. To classify and extend the main carbon-carbon bond forming reactions (CCBFR) introduced in CHE1C1Y.
3. To illustrate the importance of organic synthesis with real examples. Organic Synthesis Introduction Why bother?! Ca. 7 million organic compounds known – most have been made by synthesis rather than isolated from nature. Reasons for Synthesising Organic Compounds:
a) Proof of structure of a natural compound by ‘putting it together’ from simpler molecules.
b) To prepare compounds that are useful to mankind e.g. pharmaceuticals, polymers, dyes etc.
c) To prepare specific compounds to study reaction mechanisms or biological metabolism (e.g. labelled compounds).
d) For the intellectual challenge – new problems demand new solutions and can lead to the development of NEW CHEMISTRY, reagents etc.
When faced with the challenge of preparing a specific organic compound ho do we go about it? This is the art of synthesis! e.g. How might we attempt to make Z jasmone – an important constituent of many perfumes?
O
?α,β unsaturated ketone, alkene, 5-membered ring
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In fact one synthesis uses the following as carbon sources
O
O
H
H
H H
Br
CH2O
CH2O
It is not clear from this however, how the chemistry might be done! Therefore just being given the starting materials is not sufficient to help plan a synthesis. Note the importance of CCBFR. We need a logical planning method. Retrosynthetic Analysis (The Disconnection Approach) Originated by E.J. Corey (Nobel Prize 1990) p169 – 172 p259 – 260 p354 – 359 Definition of Terms Target Molecule (TM) – the compound we wish to prepare e.g.
O
methylphenyl ketone(acetophenone)
Retrosynthetic Analysis – the process of WORKING BACKWARDS from the TM in order to devise a suitable synthetic route (or routes) on paper. Note:
denotes disconnection of TM to its most immediate precursor.
Multiple steps are required so this needs to be repeated.
TM 1st Precursor 2nd Precursor Starting compounds- readily available
After writing possible routes we would need to evaluate each one before deciding which to follow.
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Readily Available Starting Materials (RASM) – cheap, commercially available compounds. Disconnection – a paper operation involving an imagined cleavage of a bond (yielding ‘synthons’) to suggest a method and possible SM’s for making the bond, ultimately leading to possible SM’s for the overall synthesis.
X Y X+ + Y-
X- + Y+
X + Y
OR
OR
Note: There must be a good chemical reaction corresponding to the reverse of the disconnections. Synthon – an idealised fragment, usually a cation or anion, resulting from a disconnection.
X+ Y-
X- Y+
X Y Usually synthons don’t exist as such, but help in the correct choice of reagent. In our example:
O
OLooks possible because it implieselectrophilic attack on benzene ring
O Does not look so good (nucleophilicattack less usual)
Synthetic Equivalent – the actual compounds used to function as synthons.
OO
Cl AlCl3 Friedel Crafts reagent
Functional Group Interconversion (FGI) – the process of writing one functional group for another to help synthetic planning and to help disconnection. Note, there must be a good reaction in the reverse (forward!) direction.
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e.g. NH2
NO2
O N O
Easy! Nitration of benzene (HNO3/H2SO4)
easy
reduction(Sn/HCl)
?
FGI
Alternative synthesis of
O
FGI
HO H HO H
CH3
CH3MgBrH
O
Many ways to make alcohols (e.g. via Grignard reagents) - suggests alternative synthesis to Friedel Crafts. In planning a synthetic strategy, apart from devising a means of constructing the carbon skeleton with the required functionality as above, there are other subtle factors, which we must address.
O HO H HO H
X X X
Y
YAND NOT
AND NOT
enantiomers
Control of Regiochemistry
Control of Stereochemistry
(Good summary p169 – 172, 259 – 260, 354 – 359)
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We will illustrate this approach with examples, starting with synthesis of benzene derivatives. Starting point is usually fairly obvious – simple benzene derivatives or perhaps benzene itself. The Synthesis of Substituted Benzene Derivatives (Solomons p655 – 695) Reactions are usually straightforward (SEAr) and you will have met most of them before. Synthesis is simplified because the nature of the starting materials is usually clear. Thus, most reactions correspond to the following disconnection:
X
X SEAr
Example 1 1st decision – which bond to disconnect first!
NH2SEAr 1
Br
Br
NH2
Problem! No good synthetic equivalentfor NH2
+
(but o/p directing effect of Br sub is OK)
NH2
Br
Br+ - can use Br2/FeBr3o/p directing effect of NH2 is OKBUT, problem is overbromination
NH2
Br
BrBr
However, we can carry out monobromination on the N-acyl derivative of the amine:
NH2
Br
NHCOCH 3 NHCOCH 3
Br
OHBr2
(some o-isomer - separate)
then we can remove the protecting group (HO-/H2O) to give the required product.
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So formally:
NH2
Br
NHCOCH 3NHCOCH 3
Br
FGINH2 NO2
FGI FGI
HNO3/H2SO4Sn/HClCH3COClBr2OH
Is there an alternative route? Try a different FGI!
NH2
Br
FGI
NO2
NO2
Br Br
NO2
Br
YES
NO
o/p directing effect of Br is OK
NO2 group is m-directingtherefore not a good disconnection
Example 2 OHO
Br
FGI
Br
O
Br
NOsynthons are OK butdirecting effect of acylis meta, therefore no good
Br
Ogood synthonsdirecting effect of Br OK
Synthesis
Br
O
Br
HO
Br
Br2/FeBr3 CH3COCl
AlCl3
NaBH4
racemate!(some o-isomer,separate)
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Example 3
CH3CONH OH
FGI
NH2 OH
FGI
NO2 OH
OHSO3H N2 NH2NO2
HONOH2O, boilKOH, heatH2SO4, SO3
NO2+
Sn/HCl
(CH3CO)2O
Guidelines for designing a synthesis
1 Use retrosynthetic analysis to work backwards from TM to the precursors and eventually to RASM.
2 Locate the functional groups in the TM – for most functional groups
there are good DISCONNECTIONS (the reverse of real chemical reactions).
3 Examine all possible disconnections – check which are chemically sound
(correspond to known reactions, reagents, directing effects etc.)
4 If you can make no progress try FGI: (NO2/NH2; CH3/COOH; C-Br/C-OH; CHO/CH2OH etc.)
5 Having obtained precursors to TM, repeat the process on these
intermediates. Clearly you will need a good knowledge of your basic chemistry and an appreciation of reaction mechanisms, directing effects etc. With Aromatic systems the SM’s are usually fairly obvious. Usually benzene or a benzene derivative such as toluene, phenol etc. bond to be disconnected is almost always the bond joining the aromatic ring to the rest of the molecule. Also FGI’s often correspond to some simple types of reaction e.g. reduction (NO2 to NH2), oxidation (CH3 to COOH), diazonium chemistry (NH2 → N2
+ → Ar-X).
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In aromatic chemistry CCBFR revolve around: 1) Friedel Crafts type reactions
Ar HROCl
Ar COR
2) Displacements on aromatic diazonium salts
Ar N2
CN
CuCNAr C N
(3) Not forgetting Grignard reagents + carbonyls) With aliphatic acyclic and cyclic systems – the process is not always as straightforward – need to consider a greater array of CCBFR’s and FGI’s. Retrosynthesis In An Aliphatic Molecule – A Guide To Alternative Disconnections. Retrosynthetic analysis 1
Ph
OH
Ph
Ph
OHPh
PhBr
PhPh
OH
Ph
OPhBrMg
PhBrMgPh
O
Ph
Path A
O
Ph
synthetic equiv.?(can't think of one) OK
B
(+H+)
Ph
Synthesis
OH
MgBr
Ph
H2O
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Retrosynthetic analysis 2
Ph
OH
Ph
Ph Ph
Ph
O
Ph
Path A
synthetic equiv.?(can't think of one)
B
Ph
Synthesis
OH
MgBr
Ph
H2O
OH
Ph Ph
OH
Ph
OMgBr
Ph
OMgBr
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Retrosynthetic analysis 3
Ph
OH
Ph
Ph
O
Ph
synthetic equiv.?(can't think of one)
Path AB
Synthesis
Ph
(+H+)
OH
MgBr
Ph
H2O
Ph
OH
Ph
PhBr
Ph
OH
Ph
Ph
OPhBrMg
Ph
OPhBrMg
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Retrosynthetic analysis 4
Ph
OH
Ph
Ph
O
Ph
Ph
OH
Ph
Ph
O
Ph
PhBr
Ph
O
Ph
Ph
Ph
O
Ph
Path AB
Ph CH3
O
Synthesis
NaBH4
CO2Et
Ph
OBr
FGI
PhBrPh CH3
O
not great, but see later
base
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Retrosynthetic analysis 5
Ph
OH
Ph
Ph
O
Ph
LiCu(CH2CH2Ph)2
H
Ph
Li + BrCH2CH2PhOH
LiCH2CH2Ph
Ph
Synthesis
Ph
O
Ph
Ph
O
CuI
Ph
NaBH4
FGI
Ph
O
Ph
OLiCu
CH2CH2Ph
CH2CH2Ph
Ph
O
Ph
We shall discuss possible synthesis later, but we will concentrate on CCBFR in aliphatic systems. Review and extend CCBFR from 1C1Y, in particular: Aldol and Claisen condensations Alkylation of β-keto esters (RCHOCH2CO2R’) Grignard reactions And illustrate their use in synthesis.
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Classification of CCBFR in aliphatic chemistry
There are several ways of doing this. We shall consider the following: a) Carbanion Alkylation
C R X C R
i) Alkylation of enolate ions
O
+ R X RO
p 867 - 879
ii) Alkylation of acetylide or cyanide
R C C + R' X R R'
N C R' X+ R CN
p 321 - 322
p 804
iii) Organometallic alkylation
R Mg X +O R
OH p 483
Note iv) Direct alkylation of carbanions is possible in some cases
R2CuLi + R' X R R'
Where R' = methyl or 1o alkyl halide
p 167 - 169
(Not a typical substitution mechanism!) b) Carbonyl Addition And Carbonyl Substitution Reactions
i) Aldol and related reactions (Addn)
O2
OOHp 762 - 774
ii) Claisen condensation and related reactions (Subn)
O
O2 O
O Op 860 - 867
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iii) Organometallic reactions (Addn)
O+ RMgBr
OH
Rp 483 - 492
iv) Acetylide/cyanide addition
O
O
R
N
OH
OH CN
R
+
+
p 492
p 732 - 734
v) Wittig reaction (Addn)
O+ R CHPPh3
O
R
PPh3
R
+ POPh3
p 734 - 737
c) Conjugate Addition Reactions - ‘Michael’ (1,4 Addition)
O
O
+ CH(CO2Et)2
RMgBrR2CuLi better
O
CO2Et
CO2Et
O
R
p 774 - 778 882 - 884
p 777
d) Reaction Of Alkenes, Alkynes And Aromatics
i) Pericyclic reactions:
Cycloadditions
Diels Alder
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Electrocyclic reactions
(MJC)
Sigmatropic reactions
Cope Rearrangement
ii) Friedel Crafts and related reactions
RCOR
O
iii) Addition of carbenes to alkenes
R2C:R R
Simmons Smith (carbenoid)
In the main we will be looking at ionic reactions.
C C C C
In CCBFR the carbonyl group is very important
O Oδ+
O
δ-
as an electrophile as a nucleophile
Also in CCBFR, organometallic compounds are important. e.g.
δ- δ+
RMgBr - Grignard Reagents, Lithium alkyls LiR etc
R2CuLi - Organocuprates
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Carbonyl Chemistry for Forming C-C Bonds Carbonyl compounds having an α-hydrogen act as weak (protic) acids and react with a base to yield enolate anions.
OO
H
HH
O
H
H
H
H
base + base-H
enolate anion
OH
OH H H
Ka = [H+][CH3COCH2-]
Compare pKa acetone = 19.3 ethane = 60 (approx)
[CH3COCH3]pKa = logKa
Presence of neighbouring carbonyl group increases the acidity of a ketone over an alkane by a factor of 1040! The use of such enolate anions from carbonyl compounds is fundamental to organic synthesis and you will already have met them as intermediates in the aldol reaction and claisen condensation. When we have two carbonyl groups adjacent to a methylene group, the acidity of the α-H is greatly increased. Because of the acidity of their methylene (CH2) hydrogens, malonic esters, ethylacetoacetate and β-dicarbonyl compounds etc are often called active hydrogen compounds .
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Active Methylene Compounds
H3C C CH2
OC OEt
O
EtO C CH2
OC OEt
O
H3C C CH2
OC CH 3
O
OCO2Me
O
O
ethylacetoacetate (ethyl 3-oxobutanoate)
diethyl malonate (diethyl propandioate)
acetyl acetone (2,4-pentandione)
2-methoxycarbonylcyclohexanone
1,3-cyclohexanedione
H3C C CH 2
OC OEt
O
EtO C CH2
OC OEt
O
H3C C CH2
OC CH 3
O
H3C CCH3
O
CH 3 C OEt
O
RCOOH
C C HH
CH3CH2OH
HOH
CH3CH3
pKa
9 (2 x ketones)
11 (1 x ketone, 1 x ester)
13 (2 x ester)
19
25
Compare:
5
16
16
25
60
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Such compounds are often used in synthesis because:
1) They are readily made and cheap 2) The anion can be generated quantitatively 3) Self condensation does not occur with 1 mole of base – OH is
deprotonated 4) The site of deprotonation is unambiguous 5) The enolate ions formed on deprotonation can be alkylated and acylated
offering useful products. Example:
OEt
O O
OEt
O O
OEt
O O
OEt
O O
pKa 20
OEt
O O
NaOEt
(pKa EtOH = 16)
pKa 11
Reactions of Active Methylene Compounds
1) Carbanion Alkylation Most important use is for preparation of ketones (from β-keto esters RCOCH2CO2Et) and of acids from malonic esters (CH2(CO2R)2).
OEt
O O
OEt
O O
ROEt
O O
R OH
O
O O
RHO
O O
R
O
O O
R
H
OH1) NaOEt
2) RBr
O
EtO
R
H
H
OH
O
heat
R
decarboxylation
H
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Note:
OEt
O O O
O
R
O
is the synthetic equivalent to
CO2Et group is used to activate α-carbon atom
OEt
O O
R RBr
So Retrosynthesis
synthetic equivs
OR2R1
O
Why not just use ?
Seems OK but problems
O
1) In unsymmetrical case, which α-position reacts?
2) Product may alkylate
OEt
O O
may prefer to react with starting ketone or product
The use of activating group stabilises the required enolate
so that conversion is complete with EtO
reaction with SM cannot therefore occur
The alkyl halide is added in a separate step-no base remains to form anionof product
Note. The activating group is easily removed
3)
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Acids
CO2Et
CO2Et
1) NaOEt
2) RBr
CO2Et
CO2EtR
1) KOH
2) H+/∆ R COOH +CO2
1) NaOEt2) R'Br
CO2Et
CO2Et
R
R'
1) KOH
2) H+/∆R'R
COOH +CO2
Note: with 2 equivalents of NaOEt and a dihalide (e.g. Br(CH2)4Br) - can get cycloalkanecarboxylic acids.e.g.
COOH
So Retrosynthesis:
R CH2CO2HCO2Et
CO2Et
O
R
C18H37
C2H5
CO2H
R-Br
+ CH2CO2H
Practice with
Note: FGI’s can be carried out on intermediates/products. Note especially:
CO2Et
CO2Et
R2
R1
CH2OH
CH2OH
R2
R1FGI
(LiAlH4)
1,3 diol
Helps in the synthesis of 1,3 diols.
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Enolate Anions as Ambident Nucleophiles e.g.
H3C CO
CH 2
H3CO
CH 2
H3C
O
CH 2
reacts as alkoxide
reacts as carbanion
Site of alkylation depends, in part, on substrate
Alkyl halides C-alkylation
H3C CO
CH2
O-alkylation
RBr CH3COCH2R
(CH3)3SiCl
Si(CH3)3SiCl
silyl enol ether
(strong Si-O bond formed
2. Reaction of Active Methylene Compounds with Carbonyl Compounds (Knoevenagel Condensation)
CO2Et
CO2EtH
R H
O
CO2Et
CO2EtR
O H
H
CO2Et
CO2EtR
HO HRCH C(CO2Et)2
H
RCH CHCO 2H
-H2O
(i) OH(ii) H(iii) heat
Usually uses weak base/weak acid as catalyst, (R2NH/HOAc). Any combination of stabilising groups can be used (CN, CO2Et etc).
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3. Michael Reaction with Active Methylene Compounds (Conjugate Addition Reaction)
Carbanions derived from active methylene compounds react with α,β-unsaturated compounds by 1,4-(conjugate) addition known as Michael addition.
CO2Et
CO2EtH
O
H3C
CO2Et
CO2EtH
O
H3C
CO2Et
CO2EtH
O
H3CCO2H
O
H3C
CO2H
O
H3C
O
H3C
O
H3COH
O
CO2Et
CO2Et
In retrosynthesis terms
(i) OH(ii) H(iii) heat
H
H
O
CO2H
O
CO2H
O
CO2Et
Question
How would you prepare
CO2Et
?
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4. Dianions in Synthesis
We have discussed the regioselective reactions of this active methylene carbon (C-2) in ethylacetoacetate. Can regiospecifically trap C-4 via the dianion.
OEt
O O
OEt
O O
or 2 x LiNiPr2 (LDA)lithium diisoprpylamide
1)NaH, 2) BuLi
OMe
O O
1) RX (1 equiv)2) H
pKa 20 pKa 11
least acidic forms most reactive anion
Need two equivalents of base and second one needs to be strong (pKa>20)
pKa 30
OMe
O O
OMe
O OR
LiN
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Carbonyl Addition and Carbonyl Substitution – Aldol and Claisen Reactions. Usually self-condensations, these reactions combine nucleophilic attack and α-substitution as the first step. The Aldol Condensation of Aldehydes and Ketones
H3C CO
HH2C C
O
H
H2C CO
H
H3C CO
HCH2 C
O
HCH3CO
H
CH2 CO
HCH3COH
H
CH3CH CHCHO
CH CO
H
OH
H2O
CH3COH
H
-H2Omore vigorousconditions (heat)
General for aldehydes and ketones withα-H
NB ReversibleProduct favoured with RCH2CHOSM favoured with R2CHCHO
2-butenal
3-hydroxybutanalaldol
H
Reason for dehydration1) Acidity of α-H2) Stability of conjugated product
OH
Note the Aldol condensation can also be performed with acid catalysis in which dehydration usually follows (enol form is involved – mechanism p 773). NB dehydration drives the reaction when the equilibrium is unfavourable.
CH2 CO
HCH3COH
CH 3
H3C CO
CH 3
H3C
H3C
CH 3
O
OH O
OH
O
2%98%
OH O
-H2O
good yield
O
In retrosynthesis terms
O
FGIRecognise aldol oraldol product
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kinetic enolate
RO
proton removed from least hindered site
H
RO
Hence different products from acid and basic conditions
thermodynamically preferred enol
O OH
Unsymmetrical ketone? Regioselectivity is a problem!
-H2O
O
ROH
OH
O O
strong base
Claisen Condensation of Esters
H3C OEt
O
H2C OEt
O
H2C OEt
O
H2C OEt
O
H3C OEt
OH3C CH2
O
OEtCO 2Et
H2C CH 2
OCO2Et
H3C CHO
CO2Et
not complete deprotonationEtOH pKa = 16CH3CO2Et pKa = 25
EtO
pKa 11, drives reaction
H
Note: the only difference between the Aldol and Claisen reaction is the fate of the tetrahedral intermediate – Claisen expels alkoxide, Aldol alkoxide is protonated.
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Mixed Aldol and Mixed Claisen Condensations These are not very useful generally as there are four potential products. However, they can be useful if one component has no α-H. Mixed Aldol
O O
PhCHO
PhEtO
ClaisenSchmidtcondensation
Mixed Claisen Condensations Only successful when one of the ester components has no α-H e.g. PhCO2Et OR HCOOEt.
Ph OEt
O
H OEt
O
OEt
O O
O
H OEt
OO O
OO
CO2EtCO 2Et
1) EtO
2) H
Can also carry out mixed Claisen between ester and ketone
O
CO 2Et
CO2Et
1) EtO
2) H favoured because removalof proton from here drives equilibrium
O O
CO 2Et
Synthesis of dimedone
2 x H
aldol Michael
O O
(i) OH(ii) H
(iii) heat
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C-C Bond Formation to Make Rings Intramolecular Aldol Reactions and Claisen Condensations When certain dicarbonyl compounds are treated with base intramolecular Aldol reactions can occur. Similarly diesters can undergo intramolecular Claisen Condensations (this reactions is known as the Dieckmann cyclisation). Aldol
O
O O
OH
O
O
O
O
OH
O
OO
NaOH
EtOH
HO O
-H2O
5 and 6 membered rings preferred
The intramolecular Aldol condensation forms the basis of a very useful method for making rings – The Robinson Annulation Reaction:
O O
O
OEt
O O
OEt
O
Michael
O
CO2Etintramolecular
aldol
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Intramolecular Claisen Condensations – The Dieckmann Cyclisation Reaction works best with 1,6 or 1,7 diesters to give 5 or 6 membered rings.
OMe
O
OMe
O
OMe
O
OMe
O
O
OMe
O
OMe
O
O
NaOMe1
MeOH
6
OCO2Me1
7
cyclic β-ketoesters
can be functionalisedand decarboxylated
Regioselective Formation of Enolate Ions (p786)
OWeak base
Protic solvent
OLiNiPr2
DME(MeOCH2CH2OMEaprotic)
OLi
Thermodynamically favoured
(More stable due to more substituted double bond)
Kinetically FavouredSterically hindered base rapidly removes proton fromless substituted α position (where there are more of themalso)
Alkylation is regiospecific:
OLiCH3I
O
ClSiMe3but
OSiMe3 This kinetic enolate, trappedas the TMS ether can beregenerated with F
(Si-F very strong)
OSiMe3 O O
Ph
OH
F
PhCHO
Other Useful CCBFR’s
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The Wittig Reaction (p 734)
R R'
O+
R'' R'''
X PPh3
BaseR'
R
R'''
R''+ OPPh3
Very useful method for alkene synthesis as the position of the double bond is known. The first step is formation of a Phosphorus Ylide (a neutral compound with C- and P+).
Ph3P: BrCH2CO2Et CHCO2Et.Br
H
Ph3P
Base
Ph3P CHCO2EtPh3P CHCO2Et
Does not contribute much
OH
O PPh3
CO2Et
CH3CH CHCO2Et
RCOR' + H R R'
H
OH
R R'
OH
O
HgSO4
H20
Acetylene anion as a synthon for CH3C=O H
Dithiane Anions Acyl anion equivalents which exhibit Umpolung (reversed polarity p 907). Two S atoms attached to the same carbon atom of a 1,3-dithiane cause the H atoms to be more acidic (pKa ≅ 32) than normal alkyl C-H.
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1,3-dithianes are easily prepared from aldehydes, they are thioacetals.
RCHO +SH SH
H+BuLi S S
RS SR H
R'X
S SR R'
1) R'CHO
2) Hg2+/H20R
O
R'
OH
Hg2+/H20
R R'
O
1,2 -di O
Radical Dimerisation Reactions Leading To 1,2-diO Pattern 1. Pinacol Formation
Retrosynthesis
OHC
OHC
OHC
OHC
Synthesis
OMg/ether
electron transfer
OC
OC
MgOC
OC
Mg
HH2O
OHC
OHC
O e-O
31
2. Acyloin Condensation Similar to ester dimerisation, used traditionally to make large rings.
(CH 2)n
CO2Et
CO2Et
2 x Na(CH 2)n
OOEt
OEtO
(CH2)n
OOEt
OEtO
(CH 2)n
O
O
2 x Na
(CH2)n
O
O
(CH 2)n
O
O
HH2O
(CH 2)n
OH
O
2-hydroxy ketone (acyloin)
Now improved by addition of Me3SiCl which traps the intermediate dianion.
RCO2Et
Na
Me3SiCl
R
R
OSiMe3
OSiMe3
H2O R
R
O
OH