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Organic

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1 , 2 , or , 3 amines: amines in which 1, 2, or 3 hydrogens of NH3 are replaced ... 3 different groups bonded to N is chiral and exists as a pair of enantiomers and, ... – PowerPoint PPT presentation

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Title: Organic


1
  • Organic
  • Chemistry

William H. Brown Christopher S. Foote
2
  • Amines

Chapter 22
3
Structure Classification
  • Amines are classified as
  • 1, 2, or , 3 amines amines in which 1, 2, or
    3 hydrogens of NH3 are replaced by alkyl or aryl
    groups

4
Structure Classification
  • Amines are further divided into aliphatic,
    aromatic, and heterocyclic amines
  • aliphatic amine an amine in which nitrogen is
    bonded only to alkyl groups
  • aromatic amine an amine in which nitrogen is
    bonded to one or more aryl groups

5
Structure Classification
  • heterocyclic amine an amine in which nitrogen is
    one of the atoms of a ring

6
Structure Classification
  • Example classify each amino group by type

7
Structure Classification
  • Aliphatic amines replace the suffix -e of the
    parent alkane by -amine

8
Nomenclature
  • The IUPAC system retains the name aniline

9
Nomenclature
  • Among the various functional groups discussed in
    the text, -NH2 is one of the lowest in order of
    precedence

10
Nomenclature
  • Common names for most aliphatic amines are
    derived by listing the alkyl groups bonded to
    nitrogen in one word ending with the suffix -amine

11
Nomenclature
  • When four groups are bonded to nitrogen, the
    compound is named as a salt of the corresponding
    amine

12
Chirality of Amines
  • if we consider the unshared pair of electrons on
    nitrogen as a fourth group, then the arrangement
    of groups around N is approximately tetrahedral
  • an amine with 3 different groups bonded to N is
    chiral and exists as a pair of enantiomers and,
    in principle, can be resolved

13
Chirality of Amines
  • in practice, however, they cannot be resolved
    because they undergo pyramidal inversion, which
    converts one enantiomer to the other

14
Chirality of Amines
  • pyramidal inversion is not possible with
    quaternary ammonium ions, and their salts can be
    resolved

15
Physical Properties
  • Amines are polar compounds, and both 1 and 2
    amines form intermolecular hydrogen bonds
  • N-H----N hydrogen bonds are weaker than O-H----O
    hydrogen bonds because the difference in
    electronegativity between N and H (3.0 - 2.1
    0.9) is less than that between O and H (3.5 -
    2.1 1.4)

16
NMR Spectroscopy
  • 1H-NMR
  • the chemical shift of amine hydrogens is
    variable, and may be found in the region ? 0.5 to
    5.0 depending on the solvent, concentration, and
    temperature
  • they generally appear as singlets
  • 13C-NMR
  • carbons bonded to nitrogen are generally shifted
    approximately 20 ppm downfield relative to their
    signal in an alkane of comparable structure

17
IR Spectroscopy
  • 1 and 2 amines show N-H stretching absorption
    in the region 3300 - 3500 cm-1
  • 1 amines show two bands in this region
  • 2 amines show only one band in this region

18
Basicity
  • All amines are weak bases, and aqueous solutions
    of amines are basic

19
Basicity
  • it is more common to discuss the basicity of
    amines by reference to the acid ionization
    constant of the corresponding conjugate acid
  • for any acid-conjugate base pair

20
Basicity
  • using values of pKa, we can compare the acidities
    of amine conjugate acids with other acids

21
Basicity-Aliphatic Amines
  • Aliphatic Amines

22
Basicity-Aromatic Amines
  • Aromatic amines

23
Basicity-Aromatic Amines
  • aromatic amines are considerably weaker bases
    than aliphatic amines

24
Basicity-Aromatic Amines
  • Aromatic amines are weaker bases than aliphatic
    amines because of two factors
  • resonance stabilization of the free base, which
    is lost on protonation

25
Basicity-Aromatic Amines
  • resonance delocalization of the electron pair on
    nitrogen by interaction with the pi system of the
    aromatic ring decreases basicity

26
Basicity-Aromatic Amines
  • the greater electron-withdrawing inductive effect
    of the sp2 carbon of an aromatic amine compared
    with the sp3 carbon of an aliphatic amine also
    decreases basicity
  • Electron-releasing, such as alkyl groups,
    increase the basicity of aromatic amines
  • Electron-withdrawing groups, such as halogens,
    the nitro group, and a carbonyl group decrease
    the basicity of aromatic amines by a combination
    of resonance and inductive effects

27
Basicity-Aromatic Amines
  • 4-nitroaniline is a weaker base than
    3-nitroaniline

28
Basicity-Aromatic Amines
  • Heterocyclic aromatic amines are weaker bases
    than heterocyclic aliphatic amines

29
Basicity-Aromatic Amines
  • in pyridine, the unshared pair of electrons on N
    is not part of the aromatic sextet
  • pyridine is a weaker base than heterocyclic
    aliphatic amines because the free electron pair
    on N lies in an sp2 hybrid orbital (33 s
    character) and is held more tightly to the
    nucleus than the free electron pair on N in an
    sp3 hybrid orbital (25 s character)

30
Basicity-Aromatic Amines
  • Imidazole

31
Basicity-Guanidine
  • Guanidine is the strongest base among neutral
    organic compounds
  • its basicity is due to the delocalization of the
    positive charge over the three nitrogen atoms

32
Reaction with Acids
  • All amines, whether soluble or insoluble in
    water, react quantitatively with strong acids to
    form water-soluble salts

33
Preparation
  • We have already covered these methods
  • nucleophilic ring opening of an epoxide by
    ammonia and amines (11.9B)
  • addition of ammonia and 1 and 2 amines to
    aldehydes and ketones to give an imine followed
    by reduction of the imine to an amine (16.10)
  • reduction of an amide by LiAlH4 (18.11B)
  • reduction of a nitrile to a 1 amine (18.11C)
  • Hofmann rearrangement of a 1 amide (18.12)
  • nitration of an arene followed by reduction of
    the NO2 group to a 1 amine (21.1B)

34
Preparation
  • Alkylation of ammonia and amines by SN2
  • unfortunately, such alkylations give mixtures of
    products through a series of proton transfer and
    nucleophilic substitution reactions

35
Preparation via Azides
  • Alkylation of azide ion

36
Preparation via Azides
  • alkylation of azide ion

37
Reaction with HNO2
  • Nitrous acid is a weak acid, most commonly
    prepared by treating aqueous NaNO2 aqueous H2SO4
    or HCl
  • In its reactions with amines, it
  • participates in proton-transfer reactions
  • is a source of the nitrosyl cation, NO, a weak
    electrophile

38
Reaction with HNO2
  • NO is formed in the following way
  • we study the reactions of HNO2 with 1, 2, and
    3 aliphatic and aromatic amines

39
Amines with HNO2
  • 3 aliphatic amines, whether water-soluble or
    water-insoluble, are protonated to form
    water-soluble salts
  • 3 aromatic amines NO is a weak electrophile
    and, as such, participates in EAS
  • 2 aliphatic and aromatic amines react with NO
    to give N-nitrosoamines

40
RNH2 with HNO2
  • 1 aliphatic amines give a mixture of
    unrearranged and rearranged substitution and
    elimination products, all of which are produced
    by way of a diazonium ion and its loss of N2 to
    give a carbocation
  • Diazonium ion an RN2 or ArN2 ion

41
1 RNH2 with HNO2
  • Formation of a diazonium ion
  • Step 1 reaction of a 1 amine with the nitrosyl
    cation
  • Step 2 protonation followed by loss of water

42
1 RNH2 with HNO2
  • Aliphatic diazonium ions are unstable and lose N2
    to give a carbocation which may
  • 1. lose a proton to give an alkene
  • 2. react with a nucleophile to give a
    substitution product
  • 3. rearrange and then react by 1 and/or 2

43
1 RNH2 with HNO2
  • Tiffeneau-Demjanov reaction treatment of a
    ?-aminoalcohol with HNO2 gives a ketone and N2

44
1 RNH2 with HNO2
  • reaction with NO gives a diazonium ion
  • concerted loss of N2 and rearrangement followed
    by proton transfer gives the ketone

45
1 ArNH2 with HNO2
  • The -N2 group of an arenediazonium salt can be
    replaced in a regioselective manner by these
    groups

46
1 ArNH2 with HNO2
  • A 1 aromatic amine can be converted to a phenol

47
1 ArNH2 with HNO2
  • Problem what reagents and experimental
    conditions will bring about this conversion?

48
1 ArNH2 with HNO2
  • Problem Show how to bring about each conversion

49
Hofmann Elimination
  • Hofmann elimination thermal decomposition of a
    quaternary ammonium hydroxide to give an alkene
  • Step 1 formation of a 4 ammonium hydroxide

50
Hofmann Elimination
  • Step 2 thermal decomposition of the 4 ammonium
    hydroxide

51
Hofmann Elimination
  • Hofmann elimination is regioselective - the major
    product is the least substituted alkene
  • Hofmanns rule any ?-elimination that occurs
    preferentially to give the least substituted
    alkene as the major product is said to follow
    Hofmanns rule

52
Hofmann Elimination
  • the regioselectivity of Hofmann elimination is
    determined largely by steric factors, namely the
    bulk of the -NR3 group
  • hydroxide ion preferentially approaches and
    removes the least hindered hydrogen and, thus,
    gives the least substituted alkene
  • bulky bases such as (CH3) 3CO-K give largely
    Hofmann elimination with alkyl halides

53
Cope Elimination
  • Cope elimination thermal decomposition of an
    amine oxide
  • Step 1 oxidation of a 3 amine gives an amine
    oxide
  • Step 2 if the amine oxide has at least one
    ?-hydrogen, it undergoes thermal decomposition to
    give an alkene

54
Cope Elimination
  • Cope elimination shows syn stereoselectivity but
    little or no regioselectivity
  • mechanism a cyclic flow of electrons in a
    six-membered transition state

55
Prob 22.24
  • From each pair, select the stronger base.

56
Prob 22.25
  • Calculate the ratio of morpholine to its
    conjugate acid at pH 7.0. At what pH are the
    concentrations of morpholine and its conjugate
    acid equal?

57
Prob 22.26
  • Which of the nitrogens of pyridoxamine is the
    stronger base? Explain.

58
Prob 22.27
  • Which of the nitrogens in epibatidine is the
    stronger base? How many stereocenters are present
    in epibatidine?

59
Prob 22.29
  • Complete each acid-base reaction and predict
    whether equilibrium lies to the left or right.

60
Prob 22.29 (contd)
  • Complete each acid-base reaction and predict
    whether equilibrium lies to the left or right.

61
Prob 22.29 (contd)
  • Complete each acid-base reaction and predict
    whether equilibrium lies to the left or right.

62
Prob 22.30
  • Provide an explanation for fact that
    quinuclidine is a considerably stronger base than
    triethylamine.

63
Prob 22.31
  • Devise a chemical procedure to separate a
    mixture of these three compounds and recover each
    in pure form.

64
Prob 22.33
  • Show how to convert each compound to benzylamine.

65
Prob 22.34
  • Propose a structural formula for acetylcholine
    chloride.

66
Prob 22.35
  • Show how the hydroxylated compound can be
    transformed into an alkyldiazonium ion, an active
    carcinogen, in the presence of an acid catalyst.

67
Prob 22.36
  • Analyze the mechanism of each rearrangement, and
    list their similarities and differences.

68
Prob 22.37
  • Propose a mechanism for this conversion. Account
    for the stereospecificity of the reaction.

69
Prob 22.38
  • Propose structural formulas for compound A and B.

70
Prob 22.39
  • Propose a structural formula for C10H16.

71
Prob 22.41
  • Propose a mechanism for pyrolysis of this ester.

72
Prob 22.43
  • Show how propranil can be synthesized from
    benzene and propanoic acid.

73
Prob 22.44
  • Show to bring about each step in this synthesis.

74
Prob 22.45
  • Show how to bring about this synthesis.

75
Prob 22.46
  • Show how to bring about the conversion of phenol
    to 4-methoxybenzylamine.

76
Prob 22.47
  • Show how to prepare methylparaben from toluene.

77
Prob 22.48
  • Show how to synthesize this 3 amine from benzene.

78
Prob 22.49
  • Show how to prepare N-methylmorpholine from the
    named starting materials.

79
Prob 22.50
  • Given this retrosynthetic analysis, propose a
    synthesis for tridemorph, a systemic agricultural
    fungicide.

80
Prob 22.51
  • Propose a mechanism for this example of a Ritter
    reaction. What would be the product of a Ritter
    reaction using acetonitrile?

81
Prob 22.52
  • Show how each of these diamines can be prepared
    from acetonitrile.

82
Prob 22.53
  • Given this retrosynthetic analysis, propose a
    synthesis for the intravenous anesthetic propofol.

83
Prob 22.54
  • Given this retrosynthetic analysis, propose a
    synthesis for propoxyphene.

84
Amines
End Chapter 22
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