353 Winter 2010 FINAL
Here is an post-mortem analysis / "how to" for this exam. The questions are split by the sections. At the start of each section are a few suggestions of what to look for or how to tackle the question type.
RELATIVE
PROPERTIES:
Identify the controlling feature, which is not always as obvious as it may
appear. Look for two pairs of similar systems to compare that have minimal
differences in structure. If a compound is named, draw it out. If a reaction
is involved, identify the type of reaction and then what the controlling factors
are.
Qu1: B
Acidity...
if you know your pKa's then this is easy : aldehyde = 17, terminal alkyne = 25 and ketone =20. Remember the lower the pKa the stronger
the acid, so iii > i >ii.
What if you don't remember your pKas ? (why not ?) Then you'll
need to deduce it. Think
of the simple acid equation HA <=> H+ A-
then look for factors that stabilise A-.....Note that two of the systems have
the acidic H that are alpha to a carbonyl group. In the aldehyde i and the ketone iii, the conjugate bases (they are enolates) can be resonance stablised by the C=O group. The difference between the aldehyde and ketone is the difference between the effect that the -H and the -R group has. Since an alkyl group (-R) is slightly electron donating, it will destabilise the conjugate base making the parent ketone iii less acidic than the aldehyde i. Now for the terminal alkyne.... loss of the proton also gives a carbanion (sp hybridised) but there is no resonance stabilisation of the -ve charge, hence it's the least acidic. Overall then in terms of acidity, i > iii > ii.
Qu2: E
The reaction is electrophilic aromatic substitution, a nitration and we need to look at the substituent
effects on the aromatic ring. The halide group in i is a slightly electron withdrawing group via inductive effects - it's a deactivating
group. The nitro group in ii is a strongly deactivating group due to resonance
and inductive effects. The hydroxy group in iii is strongly activating due to resonance. So the reactivity is iii > i > ii.
Qu3: E
The reactivity of carbonyl groups towards an organometallic reagent, a Grignard reagent, looking at the relative reactivity of i ester, ii amide,
and iii acyl halide.
Electronic factors need to be considered. First compare i and ii, esters tend to be more reactive than amides because the N is a better electron donor than an O (think about the electronegativity) and the N group is a poorer leaving group than the similar O group. Both factors make the amide less reactive than the ester. Now compare iii and i. Acyl halides are typically more reactive than esters due to the properties of the bromine atom (size, electronegativity). Hence
in terms of reactivity iii > i > ii.
Qu4: E
The reactivity of carbonyl groups towards an organometallic reagent, a metal hydride, looking at the relative reactivity of substituted aromatic systems i an aldehyde, ii a methyl substituted ketone
and iii a chloro substituted aldehyde.
Electronic and steric factors need to be considered. First compare the two aldehydes i and iii. The ortho-Cl in iii is an electron withdrawing substituent and so it will make the aldehyde C=O more +ve and hence more electrophilic and more reactive. Now compare i and ii, an aldehyde and a ketone. Simple aldehydes are usually more reactive than simple ketones because the extra alkyl group of a ketone electronically and sterically makes the carbonyl less reactive. In ii we also have an ortho-methyl group which due to it's weakly electron donating characteristics will make the carbonyl even less reactive. So overall, iii > i > ii.
Qu5: A
We are looking at the basicity of a series of substituted aromatic N systems. First let's compare i and ii. Both are substituted anilines, hence it's the aromatic substituent effects we need to focus on and how that affects the N lone pair availability. Electron donors will add electron density to the system making the electrons more available and therefore more basic. In the two structures : i has a para-methoxy group (strong electron donating), and ii has a bromine (weakly electron withdrawing). Now for iii an amide where the N lone pair is involved in resonance with the carbonyl group making the electrons less available. Therefore the basicity is i > ii > iii.
Qu6: D
The systems are substituted alkenes and alkynes... electrophilic
addition of HBr to an alkene or alkyne. A closer look at the structures shows that the three systems have similar base structures except that
i is an alkyne rather than an alkene and that there is a methoxy substitutent in ii otherwise the chains are the same. So iii will give a simple secondary carbocation upon reaction with HBr. In ii the methoxy substituent will impact the stability of the cation. An alkoxy group,
RO- is able to stabilise the +ve charge by resonance so ii will be
more reactive than iii (think of the electron donating alkoxy group making
the C=C more electron rich). For alkynes the low stability of the vinyl carbocation makes alkynes less reactive than alkenes... so ii > iii >i.
Qu7: E
Acidity...
if you know your pKa's then this is easy : diketone =9, beta-ketoester =11 and carboxylic acid = 5. Remember the lower the pKa the stronger
the acid, so iii > i >ii.
What if you don't remember your pKas ? (why not ?) Then you'll
need to deduce it. Think
of the simple acid equation HA <=> H+ A-
then look for factors that stabilise A-.....So the carboxylic acid iii is the most acidic (-ve charge on electronegative oxygen atom plus resonance to another oxygen atom. For the other two systems, the acidic H is alpha to at least one carbonyl group, i.e. they are enolate systems. In these active methylenes, remember that ketones stabilise the enolate better than esters because the alkoxy group (RO-) in an ester is also in competing resonance with the carbonyl. So overall, iii > i >ii.
Qu8: E
Resonance energy indicates the stability of the conjugated system. Aromatic systems have high stablisation and therefore high resonance energies. Since naphthalene iii is a polycyclic aromatic with the larger conjugated system, it will have the highest resonance energy than benzene itself, i. If we now compare benzene i and pyridine ii, then we need to recall that benzene is more aromatic than pyridine and therefore benzene has the higher resonance energy, hence iii > i > ii.
Qu9: A
First identify the alpha
positions. i is a ketone, with adjacent CH2 and CH3groups meaning a total of
5 enolisable H. ii is an aromatic ketone so the C=O group is attached to a phenyl ring and a CH3group meaning a total of
3 enolisable H. iii is diaromatic ketone with two adjacent phenyl groups and
hence no enolisable H,
so i > ii > iii.
Qu10: C
These are Diels-Alder reactions. In terms of stereoisomers we need to think about (i) regioselectivity and (ii) endo/exo selectivity. Reaction of i can give a single regio isomer but as either endo or exo. The reaction of ii can give two regio isomers depending on the relative positions of the methyl group from the diene and the dienophile and each of these has both an endo and exo isomer. iii is not a conjugated diene, so it does not react with the dienophile. Hence ii > i > iii.
STRUCTURES and PROPERTIES:
You need to know about functional groups and reactions, and how to apply concepts
related to structure such as stereochemistry, acidity/basicity and reactivity etc.
Qu11: AD
Achiral molecules don't rotate plane polarised light.... but all the examples have chirality centers, so we need to identify the meso compounds. Assign the configurations as R or S at the chirality centers....The group priority order is Ph > CPh(H)CH3 > CH3 > H. Note that A can be identified as meso by virtue of the fact that each of the substituents are opposite in 3D space across the center C-C to the like group.
Qu12: BC or BE
Enantiomers are non-superimposable mirror images and therefore have opposite configurations are all chirality centers.
Qu13: BCE
The required trans-alkene (Ph(CH3)C=C(CH3)Ph) reacts with H2 / metal catalyst via a syn addition to give two enantiomers.
Qu14:CE
In order for two of these structures to rotate light in the same direction, they will need to have the same configurations.
Qu15: B
All the structures contain N atoms, but only 3 are amines... the lone pairs on N in amines makes them basic. The primary amine in B is the most basic because there is no resonance of the N sp3 lone pair with the pi system (as there is in A). In D the lone pair is in an sp2 hybrid and is therefore closer to the N nucleus and less available.
Qu16: CE
The formal charge on the N in the neutral amines in A, B and D is zero. In a nitro group, C, and an ammonium group, E the N has a +1 formal charge.
Qu17: ABE
Primary and secondary amines react with nitrous acid (formed from NaNO2 and H+) to give diazonium salts.
Qu18: B
Acidity...
of carbonyl (enolate) systems. In general terms, aldehydes > ketones > esters in terms of their ability to stabilise enolates so the beta-ketoaldehyde B is the most acidic of these systems.
Qu19: E
Across the set of 5 compounds most of the H are alpha-hydrogens next two carbonyl groups except E where they are only next to one carbonyl (hence less resonance stabilisation of the conjugate base).
Qu20: D
Sodium borohydride is a milder hydride reagent that reduces aldehydes and ketones or more reactive carbonyls but not ester or less reactive carbonyls. Hence the diester, D, is the only system that would not be reduced.
Qu21: CD
Systems where a carboxylic acid group is beta to another carbonyl group can be decarboxylated. Carboxylic acid derivatives (e.g. esters) are readily hydrolysed to carboxylic acids under these conditions.
AROMATICITY and RESONANCE:
Best method is to work through the molecules and decide on the aromaticity based on the four criteria (cyclic, planar, conjugated pi system with 4n+2 pi electrons).
Qu23: ACD
B and E do not have cyclic pi systems (note the sp3 C in the ring) and are therefore nonaromatic. D is aromatic because the boron atom has an empty p orbital available to contribute to the pi system and the carbanion adds 2 e to the 4 from the 2 C=C to make a 6 pi system.
Qu24: AD
Antiaromatic systems satisfy the first three aromaticity criteria but are 4n systems and therefore do not meet the Huckel rule. B is aromatic (one S lone pair is in the 6e pi system), C is aromatic because the boron atom has an empty p orbital contributed to the conjugation of to the 2e pi system) and E is aromatic because the carbocation center has an empty p orbital contributed to the conjugation of to the 2e pi system).
Qu25: A
B is a cyclic, conjugated pi system with 4 pi electrons and is therefore antiaromatic. C is a cyclic, conjugated pi system with 6 pi electrons and is therefore aromatic. D and E are not conjugated systems.
Qu26: C
In order to be aromatic hydrocarbons, they can only contain C and H atoms, no heteroatoms such as N. If n=2 in the Huckel rule it means we need 10 pi electrons. A is 10 pi electrons, but non planar and therefore is non-aromatic. B is not a conjugated system, D is not a hydrocarbon and E has 14 pi electrons (i.e. an n=3 aromatic system).
Qu27: ACD
B has an aromatic tautomer but not an aromatic resonance structure. Remember that atoms can not move in resonance contributors. The sp3 carbon in E prevents the aromatic character. In A, C and D the charge separation in the resonance contributor can create an aromatic system. In A and D these are 5 membered anionic rings and in C its a 7 membered cationic ring.
Qu28: AD
B and E are all non-aromatic as drawn due to the sp3 C centers in the cyclic systems. The lone pair on the N in C is part of the aromatic system and therefore has a non-aromatic conjugate acid.
Qu29: AC
B, D and E are aromatic as drawn. Removal of H+ from the structure A and C gives a anionic and neutral aromatic system respectively.
STARTING MATERIALS AND PRODUCTS:
If you are trying to find the product, then you should probably just work forwards through the sequence of reactions.
If you are looking for the starting material, then working backwards is probably the best way to go....
Basically depends on the need to know and identify the reactions, this is often triggered by looking at the functional groups in the molecules.
Qu30: C
Working forwards, the peracid reacts with the alkene to give an epoxide. The Grignard reagent will then react with the epoxide at the least hindered end to form a tertiary alcohol (B or C). B has the -OH on the wrong carbon atom, and D has the wrong regiochemistry in the epoxide opening step.
Qu31: B
Working forwards, hydroboration and oxidation of the alkene gives the anti-Markovnikov primary alcohol. PDC is an oxidising agent giving the aldehyde which is then treated with an ylid in a Wittig reaction to give the alkene. A has too many carbon atoms and C comes from the wrong regiochemistry in the first step.
Qu32: A
Working forwards, thionyl chloride reacts with the carboxylic acid to make the acid chloride. This then reacts with the secondary amine to give the N,N-dimethyl amide.
Qu33:B
Working forwards, the aromatic ester undergoes an electrophilic
aromatic substitution, specifically Friedel-Crafts
alkylation on the more reactive ring (left RO- substituted aromatic) giving a para methyl group. This is followed by another electrophilic
aromatic substitution, specifically nitration again on the more activated ring. A and D have the wrong regiochemistry for both the electrophilic aromatic substitutions since the carbonyl group deactivates that ring. C has the wrong regiochemistry for nitration since both the methyl and the alkoxy group activates the other ring. E has the wrong regiochemistry since the first reaction is directed para by the alkoxy group.
Qu34: D
Working backwards, the last step is hot acidic permanganate that has caused the oxidation of a benzylic substituent to give the benzoic acid. Step 1 is an electrophilic
aromatic substitution, specifically Friedel-Crafts
alkylation giving the t-butyl group. Remember that these alkylations only work on activated aromatics and that t-butyl groups can't be oxidised by permanganate.
Qu35: C
Working backwards, the product is a 1,2-diol. Looking at the reagents, this has come from the ring opening of an epoxide via what amounts to an anti-addition. Analysis of the diol product indicate the regio and stereochemistry on the required alkene.
Qu36: A
Working backwards, LDA is lithium isopropyl amide, a strong base, so it looks like we are making an anion, probably an enolate and then methylating it via an SN2 reaction. This methyl group is attached to the carbon alpha to the ketone. The 2nd step, acidic hydrolysis is not easy to make sense of on its own, but if we look at the first step, we should be able to make some sense of it. The dicarbonyl is being treated with base, so again it's enolate chemistry and it is being used to make the 5 membered ring via a double alkylation. This means the 1,4-dibromide A is what we are looking for.
Qu37: D
Working backwards, looking at the product and the 3rd set of reagents, it looks like we made the two ethyl esters probably from the carboxylic acids (it looks like a Fischer esterification). Based on the 2nd step, this was the ozonolysis of an with an oxidative work-up to give the dicarboxylic acid, so we can reveal the starting alkene by reconnecting the carbonyl groups. Looking at step 1, the cyclopentadiene and heat suggests we did a Diels-Alder reaction, so reverse the arrows in the product to reveal the starting material, D.
Qu38: A
Working forwards, the aldehyde ester will be reduced by the excess hydride to the 1,3-diol. Reaction of the 1,3-diol with the ketone will form a cyclic ketal. The key here is getting the right number of atoms in each ring. B would be formed by reaction with cyclohexanone with 1,2-ethanediol. D has too many carbon atoms (it would be formed by reaction with cyclohexanone), and E has too few carbon atoms (it would be formed by reaction with cyclopentanone with 1,2-ethanediol).
REAGENTS FOR SYNTHESIS:
Need to be able to look at reactions, looking at the functional groups in the starting materials and products to think about
how you have got there.
How well do you know your reagents
? Look at what has actually happened in terms of the reaction functional
group transformation and then first look for any regiochemical issues
then finally the stereochemistry last (it's the hardest to sort out).
Qu39: B
In order to convert benzene into the m-nitrobenzoic acid we need to introduce a carbon substituent and a nitro group. The key issues are the Friedel-Crafts don't work on deactivated aromatics and nitro groups and carboxylic acid groups interfere with Grignard reactions. These factors rule out A, C and D. E does not work because aryl bromides don't react with carbon dioxide. The route that works is a Friedel-Crafts acylation to methyl ketone (m-director) then permanganate oxidation, under these conditions (acidic
and heated) will oxidise the substituent to a carboxylic acid group. Then an electrophilic
aromatic substitution, specifically nitration using nitric and sulfuric acids.
Qu40: A
In order to convert 2-pentyne into the appropriate pentan-2,3-diol, we first need to interpret the Fischer projection. The implication is that we either make the cis-alkene (catalytic hydrogenation using Lindlar's catalyst) and then do a anti addition to give the diol or make the trans-alkene (Na
/ NH3 is a dissolving metal reduction) and do an syn-addition to get the diol. Cold alkali permanganate or osmium tetroxide / aq NaOH gives a diol via syn-addition. B gives an alcohol not a diol, C and D give the wrong stereochemistry, and E has the wrong nucleophile in the last step (it needs water not methanol).
Qu41: D
We need to convert the carboxylic acid group into a primary alcohol via a reduction, but in order to do this, we will need to protect the aldehyde first and then deprotect it after the reduction since the aldehyde is more reactive than the acid. A and B have the steps in the wrong order. C is a reduction followed by oxidation so it would give the dialdehyde. E does not give the desired product because NaBH4 is not a strong enough reducing agent to reduce the acid.
Qu42: B
In order to convert methylbenzene into (2-methyl-1-propenyl)benzene a quick analysis shows that we need to make a new CC bond and add a total of 3 new C atoms. Two possible routes spring to mind, via a Grignard reagent / elimination route or via a Wittig reaction : B radically brominates the benzylic position then prepares the ylid ready for the Wittig reaction. A fails because the first reaction would not give the required benzyl halide (HCl does not undergo radical reactions so this is not a good route to the required halide). C does not work because Grignards don't react well with halides and it certainly would not give an alkene. Similarly for D.... for the last step to cause an elimination to give an alkene, we would need an alcohol from step 3. Again for E oxidation to the acid then reduction to the primary alcohol followed by conversion to the bromide is fine, but again Grignards don't react well with halides and it certainly would not give an alkene at the end.
Qu43: A
Qu44:C
In order to convert methylbenzene into triphenylmethanol, a quick analysis shows that we need to add two more phenyl groups, probably via Grignard chemistry with a carbonyl group (since it's common). This is achieved in C where the starting material is oxidised to benzoic acid, converted to the methyl ester and then reacted with excess phenyl magnesium bromide to give the required tertiary alcohol.
EXPLANATION OF PHENOMENA
Qu45: D
When temperature affects product distribution is this way, we typically have a case of kinetic and thermodynamic control. At the lower temperature, the reaction is under kinetic control where it is the rate of formation of the carbocation intermediate that is important and this is affected by the stability of the carbocation.
Qu46: D
There are four structural criteria for aromaticity. [14]-annulene implies that is has 14 pi electrons which means that it satisfies the Huckel rule (where n=3). An inspection of the structure, shows that is does contain a cycle of conjugated pi systems. So it appears that the planarity is the issue. In [14]-annulene, it is the H atoms in the interior of the ring that are too close to each other (i.e. steric strain) that destabilises the planar conformation.
Qu47: B
When ranking basicity, looking at the availability of the lone pair electrons is the best approach. For N1, the pyridine N, the lone pair is in an sp2 hybrid orbital that is perpendicular to the aromatic pi system. For N2, the amino group N, the lone pair is in a p orbital that is involved in a resonance interaction with the aromatic pi system. Therefore, N1 lone pair electrons are more available than those on N2 and so N1 is more basic than N2. This means that on protonation of N1 to give it's conjugate acid, the amine group can stabilise the positive charge due to its electron donating character.
Qu48: C
The reaction shown is a hydride reduction of the ketone to a secondary alcohol via a nucleophilic addition. The key thing is to remember that the attacking species is an H- (not the HO- group), this H is the one attached to the same carbon atom as the -OH group. In the major product, this H has added to the bottom face due to the steric hindrance caused by the methyl substituent on the bridging carbon that partially blocks the top face.
Qu49: C
The key difference between X and Y is the alkene C=C, a question all about substituent effects. This means that the substituent in X is really just an alkyl group while that it Y is a conjugated nitrile. Alkyl groups are weak electron donors and direct ortho / para while nitriles are strong electron withdrawers and direct meta.
Qu50: E
LiAlH4 reduces amides to amines. Since this is a cyclic amide, the product will be the cyclic amine.
![[Chem 353 Home]](../mol.gif)
Return to Homepage