Section F: organic functional groups

Question 1

why do we study functional groups?

Answer 1

• functional groups have a characteristic chemical behaviour
• the same functional group in different molecules behaves in the same way
• several functional groups in one molecules usually behave independently of one another
• knowledge of functional groups helps understand the metabolism of molecules and simplifies our understanding of how biomolecules react

Question 2

which molecules does electrophilic addition involve?

Answer 2

alkenes

Question 3

which molecules are formed by the electrophilic addition of alkenes?

Answer 3

alcohols and alkyl halides

Question 4

what is Markovnikov’s rule?

Answer 4

for the addition of hydrogen halides to alkenes, the H adds to the C with the most H atoms attached ie. the reaction proceeds in such a way as to involve the most stable carbocation

Question 5

define ‘regioselectivity’

Answer 5

the preference of one direction of chemical bond making or breaking over all others, resulting in the formation of a single regioisomer

Question 6

describe the biosynthesis of cholesterol

Answer 6

• squalene —> cholesterol
• cascade reaction
• multiple electrophilic additions occur
• reactions are linked so that the product of one is the starting material for the next ie. each electrophilic reaction generates a carbocation that acts as an electrophile in the subsequent reaction
• the active site of the enzyme bends squalene into a particular conformation
• this brings together parts of the molecule that will react with each other

Question 7

which molecules are formed by an elimination reaction?`

Answer 7

alkenes

Question 8

which reaction does the extension of glycogen involve?

Answer 8

nucleophilic substitution

Question 9

what is the reaction for the extension of glycogen?

Answer 9

UDP-glucose + glycogen (n residues) —> UDP + glycogen (n+1 residues)

Question 10

what is the function of UDP in the extension of glycogen?

Answer 10

• it tags glucose to signal to the enzyme
• it activates glucose to take part in the reaction
• it is a very good leaving group

Question 11

why does the SN2 reaction favour primary over tertiary molecules?

Answer 11

there is no steric hindrance of the molecule with a primary molecule, which there would be with the bulky alkyl groups of a tertiary molecule

Question 12

why does the SN1 reaction favour tertiary over primary molecules?

Answer 12

the alkyl groups of the tertiary molecule stabilise the carbocation intermediate by the inductive effect

Question 13

describe the SN2 reaction

Answer 13

• bimolecular nucleophilic substitution
• one step
• both species involved in the rate-determining step ie. rate of reaction depends on both [Nu] and [L]
• attack from the back side
• in transition state, both Nu and L are partially bonded to the central carbon
• fastest when the substrate is primary and slowest when it is tertiary
• needs reasonably strong nucleophile
• sterospecific
• results in an inversion of configuration
• one pure enantiomer as a substrate gives one pure enantiomer as the product

Question 14

describe the SN1 reaction

Answer 14

• unimolecular nucleophilic substitution
• two steps
• the rate of reaction depends only on [substrate] and not on [Nu]
• the bond between carbon and the leaving group is broken before the entry of the nucleophile
• fastest when the substrate is tertiary and slowest when it is primary
• nucleophile can be weaker
• results in racemisation in which a pure enantiomer gives a mix of both enantiomers

Question 15

what is the effect of using a protic solvent on the rate of SN2 and SN1` reactions?

Answer 15

SN2 - the rate of reaction is decreased since the solvent would form a solvent cage around the nucleophile, reducing its nucleophilicity and preventing any reaction; alternatively, the protons could combine directly with the nucleophile

SN1 - the solvent helps to stabilise the leaving group and carbocation, increasing the rate of reaction

Question 16

what is the effect of the solvent cage on both SN2 and SN1 reactions?

Answer 16

SN2 - solvent cage around the nucleophile reduces its nucleophilicity and, since nucleophile must be relatively strong, will decrease the rate of reaction

SN1 - the solvent cage would also decrease the nucleophilicity of the nucleophile, but the reaction would still be favourable overall:

• the intermediate carbocation is stabilised, lowering its energy on an energy diagram
• the nucleophile is also stabilised, increasing the height of the peak slightly
• but, since the intermediate carbocation energy level has been decreased, the absolute peak height is still lower
• therefore no effect on the kinetics of the reaction

Question 17

give an example of an SN2 reaction

Answer 17

norepinephrine —> epinephrine (adrenaline)

in which SAM is activated by methylation

Question 18

give an example of an SN1 reaction

Answer 18

geranyl diphosphate —> geraniol

in which OPP is an excellent leaving group

Question 19

give an example of a polar protic and aprotic solvent

Answer 19

polar - H2O

aprotic - diethyl ether CH3CH2OCH2CH3

Question 20

which two reactions are competing mechanisms?

Answer 20

elimination and substitution

Question 21

which two reactions are ‘opposites’?

Answer 21

electrophilic addition and elimination

Question 22

what is the difference between E2 and E1?

Answer 22

E2 - one step

E1 - two steps; removal of leaving group is the rate-determining step

Question 23

what is Zaitser’s rule?

Answer 23

the carbon most likely to lose a hydrogen is the one with fewer hydrogens (due to hyperconjugation)

Question 24

how is a primary alcohol oxidised?

Answer 24

primary alcohol —> aldehyde —> carboxylic acid

Question 25

how is a secondary alcohol oxidised?

Answer 25

secondary alcohol —> ketone

Question 26

which oxidising agent is used to convert an alcohol into a carboxylic acid?

Answer 26

(Cr2O7)2-/H+ (dilute H2SO4) = breathaliser

Question 27

which oxidising agent is used to convert an alcohol into a ketone?

Answer 27

AgNO3/NH3 or H2O = Tollen’s reagent

Question 28

how can weak nucleophiles undergo carbonyl addition?

Answer 28

they require activation of the carbonyl group by acid catalysis, protonating oxygen

Question 29

name two reducing agents

Answer 29

LiAl4 and NaBH4

Question 30

what conditions are required for the conversion of Ar=O into Ar-OOH?

Answer 30

1. LiAlH4/THF

2. H+/H2O

Question 31

what conditions are required for the conversion of CH3CH=CHCH=O?

Answer 31

1. NaBH4/EtOH

2. H+/H2O

Question 32

which reducing agent is found in nature?

Answer 32

NADH

Question 33

how are hemiacetals formed?

Answer 33

by the nucleophilic attack of an alcohol

Question 34

what is formed by the polymerisation of α-D-glucose?

Answer 34

helical structure of amylose or glycogen

Question 35

what is α-D-glucose?

Answer 35

-OH group is axially positioned

Question 36

what is formed by the polymerisation of β-D-glucose?

Answer 36

the straight polymer of cellulose

Question 37

what is β-D-glucose?

Answer 37

-OH group is equatorially positioned

Question 38

define ‘pyranose’

Answer 38

a collective term for carbohydrates that have a chemical structure that includes a six-membered ring consisting of five carbon atoms and one oxygen atom

Question 39

define ‘tautomers’

Answer 39

isomers of a compound that differ only in the position of the protons and electrons