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A new role for l-ascorbic acid: michael donor to α,β-unsaturated carbonyl compounds
7rhakhm Vd. 39, No. 13. pp. 2137 to 2145. 1983 Pnatcd In GreoI Britain.
-/83
A NEW ROLE FOR L-ASCORBIC ACID:
$3.00 + .a3 F’qamon Prm Ltd.
MICHAEL DONOR TO o,B-UNSATURATED
CARBONYL COMPOUNDS1
GABOR FODOR", REGINA ARNOLD AND TIVADAR MOHACSI National Foundation for Cancer Research Laboratory at the Department of Chemistry, West Virginia University, Morgantown, WV
26506
ISABELLA KARLE AND JUDITH FLIPPEN-ANDERSON Laboratory for the Structure of Matter, Naval Research Laboratory, Washington, DC 20375
(Receivedin USA
14 January 1983)
Abstract - In a novel Michael-type reaction L-ascorbic acid (1) undergoes addition to acrolein to give the tricyclic hemiacetal lactone 3. The constitution and relative configuration of 3 was studied by a combination of NMR and IR spectroscopy. Ultimately, the structure of 3 was determined by X-ray crystallography. The absolute stereochemistry follows from the known chirality of C-4 and C-5 of L-ascorbic acid. A mechanism for the reaction, including its steric course, is proposed. Methyl vinyl ketone reacts with 1 in a similar fashion to give diketo lactone derivative 4. Upon the action of methanolic hydrogen chloride on 5 one anomer, the tricyclic methyl ketal lactone 5, forms. Structure 5 is closely related to 3. Synthetic and possible biological applications of the new reaction are-discussed. Recently one of us and his associates found
saturated lactone.
that L-ascorbic acid (1) undergoes enediol
the primary product (m.p. 114-116")
The elemental analysis of
acetal formation with 1,2-dicarbonyl
corresponds to the monohydrate of a 1:l adduct
compounds like methylglyoxal and their 2-4 vinylogues e.g., 4-keto'2-pentenal.
between acrolein and -1. However, the adduct can be dehydrated to product 2 (m.p. 150-152') via
In contrast, we now observed that acrolein
the ternary azeotrope with ethanol and
reacts with ascorbic acid in water to give a
benzene.
crystalline product that shows no olefinic
is the 1:l adduct.
protons and carbons, respectively, lnthe and "C
NMR spectrum.
'H
Both 2 and its monohydrate show identical
A single carbonyl
13C NMR spectra in DMSO-d. (Fig. 3).
band appears at 1780 cm-' in the IR and a signal at 175
Elemental analysis confirms that 2
A
noticeable feature is that most of the major
ppm in the r'C NMR spectrum.
signals appear as narrowly spaced "doublets"
These values suggest the presence of a
in the proton decoupled spectrum.
2137
This
2138
G. FODORet al.
points
to
isomers of
2 can
is
presence
are
of
in
with
that
MS0
solution.
(Fig.
from
4)
which
findings
hemiacetal
the
aldehyde
crystals
of
recrystallization
2 were
from
a structure
study
are
obtained
thus
crystallizes
feasible.
described
in
in
Details
the
of
c = 10.318(4)
the
monoclinic
A,
independent
A,
B -
using
structure
was
were
for
each
from
observed to
in
hydroxyl the
of
and
also
resultant
refinement
by
for
did
not
data
atoms
were after
the
C
well
coordinates
hydrogen
give
z1 IFoI-IFcl Z/F 1
on in
the
that
1,
I
using final
good
and O-9 on O-12. these
R factors,
Table and
1 lists
the
Beq values
for final for
our
analysis.
of
in FIp,.
1,
experimentally The molecule
b-membered
the
is
has
ring
and
consistent
cyclic
hemiacetal
the
configurations were
The absolute
C-4
the
rational
by
configu-
the
and C-5
to
at
established
by using
atoms
2’6.02’9]
know” of
ascorbic
new ehiral
name of
dodecane.
throughout
request
centers.
1.3,7-trioxa-
the
Chemical name:
This
numbering
text.
However,
upon
Abstracts
suggcstcd
the
(3S,3aR,SaS,6R)-hexahydro-
R and 3.94% refined “on-
which
Fig.
2 fiall
within
The angles
around
C-2,
indicate
that
form
in
and angles
values.
the
without ring
(the
has
C-2,
C-9,
34.1(5)O).
Both
conformation
the
C-2,
C-6
the
“flaps”;
by C-2,
O-3,
and C-2
is
C-2,
bond
C-4
and C-5
of
and C-9 The ring
O-1
packing
rings torsion is
intermolecular
the
the
in
also angle
influenced hydrogen
are
of
is
in a”
(the
the
bonds.
rings
by C-6,
the H-6,
two
Crystal
presence O-5
5-
C-6,
-31.2(5)‘). the
from
formed
five-membered
between
by
&r
about
atoms
formed
other
cc.*
is is
plane
one
plane
In the
5-
twisted
these
of
junction is
rings
that
out
the
angle
and are
such
chair
junction
5-membered
is
out
at
able
The h-
flattened
torsion
C-6
and C-9 was
strain.
ring
O-9
expected C-6
fusion
h-membered
are
system
a somewhat
envelope
C-8
ring
The ring
and
O-3,
fused
significant
conformation. membered
ring.
the
a
centers
was deduced
membered 3.24%
the
This
of
as a reference
C-7, and Rw -
so
WFO =
R+.
on O-5
to
stereodiagram
The relative
chiral
membered
parameters
map showed
calculated
of
[
X-ray
to
and COH angles
a disordered
Zw(jFo\-iFc/)’
the
the product
2-(3-oxopropyl)-3-oxo-I.-gulono-
illustrated
were
on just
refine
hydrogens
parameters
R =
five
elucidated addition
one
Bond distances
The hydrogens
difference the
factors
hydrogen
the
[3,4-blpyran-S-one.
deviations
positional
O-H distances
and indicated
where
from
3,5a,8-trihydroxy-211,5H-furo-[3’,2’:2,3]furo-
map calculated
refined.
A subsequent
for
using
unreasonable.
Structure
and a
and calculated
the
rings.
of
14.3.2.0
w
Hydrogen
their
oxygens
positions
thermal
has
from
structure
following
802
the
rings,
(2).
the
were calculated All
the
was used
minimized
standard
refinement.
cycles
then
were
estimated
a difference
and 0 atoms were
the
&oxo-(55,9S,12R)-trihydroxy-(2R,6E)-tricyclo-
refined
weights,
in
5-membered
We choose
thermal were
of
coordinates.
fused
acid
was
the
Gilardi7.
the
several
and
atoms
available
analysis
shown
chirality
The
methods
procedure
intensity)
according
located
are
by computer
ration
a graphite
The function
where
collected
symbolic
and
least-squares
least-squares
in
that
draw”
lac tone
non-centrosymmetric
C and 0 atom
0RFXLS3.
(derived
for
observed
for
atoms,
“on-hydrogen
formula
3,6-ketal
A,
beam. the
The coordinates
full-matrix
used
using for
group
diffracto-
with
incident
solved
Cw(IF,I-IF&)‘,
of
the
procedure5
crystals.
program6
coordinates
carbon
Anisotropic
the
factors
structural
with
and 2 = 2.
X-ray
CuKa radiation on
space
101.8(l)’
reflections
monochromator
the
between
two
-3
b = 7.526(S)
on a NICOLET P3F automatic
by
comparison
determined
following
The compound
a = 6.293(3)
addition
to
map coordinates
for
three
P21 with
refined
hydrogens.
parameters
be
by X-ray
became
Crystalloarauhv.
factors
difference
the bonded
The X-ray
paragraph.
meter
the
by
methanol-ether,
determination
crystallography
802
hydrogens
authors.
Single
X-Ray
atoms,
the
structure
group
acrolein.
this
hydrogen
hydroxyl
between
These
a cyclic
arises
related
mutarotatio”
an equilibrium
3 in
consistent
two closely
Indeed,
be observed
of
moiety
of
solutio”.
indicative
isomers
of
the
in
of is
3
a donor
A new role for L-ascorbic acid
2139
Table 1.
Fractional Coordinates and Equivalent Isotropic Thermal Parameters with e.s.d.'s in Parentheses. --.\*om x 2 v 8eq ~_____-0.3529(4) 0.2379(j) 0.1204(4) 0.2057(6) 0.4037(7) 0.6029(4) 0.3816(6) 0.24?6(4) 0.0714(7) -0.0665(5) 0.0834(5) -0.1240(4) 0.1752(7) O.U73(7) 0.4X5(6) 0.6042(4)
O(1) C(2) O(3) C(4) C(5) O(5) C(6) O(7) C(8) O(8) C(9) O(9) C(10) C(11) C(12) O(12)
0.5957(7) 0.759L 0.7605(7) 0.8843(9) 0.9697(8) O-8954(7) 0.9252(7) 1.0638(6) 0.990?(9) 1.0844(7) 0.7917(a) 0.7134(7) 0.7223(9) 0.5295(8) 0.5204(8) 0.6156(8)
2.5(l) 2.3(l) 2.9(l) 3.5(2) 2.9(l) 3.1(l) 2.8(l) 3.3(2) 3.0(l) 3.9(2) 2.6(l) 2.9(l) 3.1(l) 3.3(2) 3.2(l) 3.9(2)
----
--____
=
B eq
Fig.
0.1958(Z) 0.1806(3) 0.0505(2) -0.0302(4) 0.0552(4) 0.0337(3) 0.1955(4) 0.2375(3) 0.2762(4) 0.3054(3) 0.2762(4) 0.2319(3) 0.4137(4) 0.4059(4) 0.3256(4) 0.3970(3)
1.
; z r oii ai*.l. J 1.i
Stereodiar:ram of the structural formula and stercocnnfiguracion of 3 as rlr,~~r,:i:~i~d h':k-rav ~if~Fr;~ctior,.
d
10 1OQ.Z
Fig. C.
119.7 b01
aund lenp,ths (e.s.d. 0.003
X)
01-2-6 j-2-9
101.7 t12.e
and bond angles (e.s.d. 0.5*) in 3.
2140
G. FODORer al. Table 2.
Fractional Coordinates for H Atoms with e.s.d.'s in Parentheses.
Atom
x
Y
H(4) H(4) H(5) H(6) H(l0) H(lO) H(U) H(ll) H(l2) H(O5) H(O9) H(012)
0.248(9) 0.082(8) 0.410(8) 0.531(8) 0.302(9) 0.065(7) 0.120(8) 0.286(8) 0.479(8) .635 -.174 .682 .664
0.811(8) 0.979(8) 1.103(9) 0.907(9) 0.801(9) 0.736(9) 0.450(9) 0.478(8) 0.377(9) .945 .754 .616 .591
to the ring oxygen O-l with the He**0
-0.113(6) -0.063(6) 0.053(S) 0.261(S) 0.452(S) 0.471(S) 0.373(S) 0.506(6) 0.306(S) -.023 .159 .325 .478
DISCUSSION
distance at 2.10 A, the O***O distance at 2.84 A an
2
the O-H***0 angle at 166.7".
After the structure of the tricyclic O-9
lactone 2 was unequivocally determined tie
is a donor to O-5 with an H***O distance of
were able to confirm and complete the
1.99 A, and O***O distance of 2.72 A and an
interpretation of its spectra.
O-H.**0 angle of 151.4".
The hydrogen on
All major signals in the "C
NMR spectrum
O-12 appears to be disordered between two
have been assigned to the two anomers of 2.
positions.
The minor peaks can be attributed to a small
In one of its disordered
positions it does not form any hydrogen
amount of bicyclic lactone free aldehyde
bonds.
which is also formed in solution (Fig. 3).
In the other position it is a donor
to a hydrogen bond to O-9 with an He**0
The fact that 2 and its monohydrate have
distance of 1.84 A. an O***O distance of
identical NMR spectra in DMSO-d. indicates
2.74 A and an O-H***0 angle of 153.0".
The
only other intermolecular approach less than
that the water molecule is loosely bound to 2, since the DMSO-water interactions are
a van der Waals' separation is between C-2
stronger than the intermolecular association
and O-5 at 3.14 A.
of water and compound 2.
a. b. C.
d. e. f. g. h. i.
Fig. 3.
Proton decoupled "C
NMR spectrum of 3 in DMSO-de.
29.3, 29.9 32.0, 32.3 73.6 74.8 85.2, 85.3 87.2, 87.5 99.6, 100.0 106.0, 106.8 174.9. 175.1
A new role for L-ascorbic acid NXR spectrum
The “C
of
the monohydrate
Da0 shows the same pattern There are only
signals.
(2 2 ppm) downfield lactone
carbonyl
the conclusion Involved
as
the hydrate
in hydrogen
geometry
membered rings appears
the two fused
as a broadened
to
proton
reached
rapidly
Michael
and thereby
can be followed
escapes 4).
of
were taken at 365 nm, because
opposite
is larger
is
solvent
Time zero
refers
is added to -3.
is possible dissolved,
before
Since rotation
be determined
acid
completely of pure 1 at
experimentally.
The initial
reading
(t = 4.5)
but changes
rapidly
towards
positive
of
lead
Concerning
to the
ascorbic
that acid
1
acrolein
Hence the addition
The ultimate
involving
from the
from the side ring
C-3 and O-6 of ascorbic
to the thermod~namfcally of
Furthermore,
in the crystal
the two five-membered
hydroxyl
prefers
lattice,
is noteworthy
that
favored rings. the
an equatorial
away from the ketofuranose the Michael
-2b
Scheme
acts
the steric
one can infer
&s-junction
It
acid
a
nucleophilic
the product
C-2 of
leads
position
values.
ascorbic
to C-5 and C-6.
hemiacetal
is negative
J_.
stereoselective.
closure
no measurement
the sample is
the optical
t = 0 cannot
to the time the
to the keto
is essentially
of -_ 2b should
the reaction
configuration
the rotation lengths.
This
wherein
carbon
approaches
wave-
the conjugated
leading
A concerted
product
measurements
at shorter
to make C-2 the
of O-6 upon C-3 and O-3 upon the
course
The
,221.
reaction
tricyclic
the change of
(Fig.
(vie
In our case
around C-Z is
increased
aldehyde
the equilibrium
Las an
two potentially
whjch can attack
s
reaction
of _3.
O-3 and C-2. density
as the donor.
be observed
with
bond of acrolein
attack
In DMSO, however,
rotation
sites:
aldehyde
with a hydroxyl
We assume that
detection.
reactive
nucleophile
resonance.
in methanol.
nucleophile
double
a possible
can be regarded
ambident
sufficiently
five-
at 6 5.6.
of 2 cannot
in the
the anomerfc
the formation
the X-electron
the C-S proton
singlet
overlaps
The mutarotation is
of
for Due to
at 6 4.5,
- maybe
- which forms
of establishing
mechanism for
mono-
except
The C-l.? hemiacetal
This peak partly proton
singlet
be due to a
species
Scheme 1 outlines to
The C-6 proton
peak.
coupling
is negligible.
aldehydc
ascorbate-3-anion
the water
as a sharp
the rigid
is
bonding
of 2 and its
could
equilibrium.
molecule.
of
appears
process
rotation
levorotatory
the free
This allows
in DMSO-d6 are identical
the size
transient
C-5 and the
the C-5 hydroxyl
The ‘H NMRspectra hydrate
for
resonance. that
The negative
“doublet”
t.wo significant
shifts:
donor
a
with
in
2141
ring. addition
G. FODOR et al.
2142 step
takes
place
at
No basic
catalyst
was used
as
provides
sufficient
act
as
shifted
of
somewhat
in aqueous 10
with
solution
at
subsequent to
form
lactone
in a recent ascorbic line
acid
dimer
pcntacyclic
the
tendency
M_etil
with
;lroceeded
with
ascorbic
Clycosidation
a
affords
ketounderscore
there
Once
the
scope
of
this
compound
corresponds and
to the
the
have
carbonyl cm-‘).
(Fig.
5)
been
shows at
lactone
214.7
is In
sharp
singlet
the
177.9
6 2.1 to
singlet
at
can
d 4.4
are
ketone
Two hydroxyl
1.
carbons
singlet
to
a methoxyl
peak
appears
correct
the
at
in
the
tricyclic
perfect
the
lactone
‘H YX??
6 3.7
group; at
6) but
ppm and
The
another
6 1.4.
elemental
are
(Fig.
(112.8
a sharp
the TR
The analysts
agreement methyl
with
ketal
two (1700 in
to Tbl.s
signal
CH,OH 2aHCI
’ the is
at
s
108.3
(DMSO-d.)
belongs
to
the
function;
be ascribed proton
cm-‘,
D20
A hemiketal
-4.
a keto
_4
carbonyl
ppm.
by the
adjacent
proton.
There
structure
protons
CllHlsOI
the
carbonyl
instead.
the
lacks
in
ppm indicates
4
lactone.
In
hemiketal
IR spectrum
‘H NMR spectrum at
for
structure
ascorbic
ppm in addition
indicated
ppm.
cyclic
one
at
with
of
which
ketone.
NMR spectrum
only
carbonyl
consistent
the “C
isolated
and
a keto
present
shows
spectra
which cm-’
NMR spectrum
for
Two ketal
methyl
1700
of
2-(3-oxobutylj-3-oxo-
its
formed. in
The
resonance
carbon
or
bands
1760
adduct
the
L-gulonolactone, could
1:l
be
CloHI,O,
a,@-unsaturated
either
principle,
could for
“C
173.8
corresponding sharp
analyzed
at
ppm) are
spectrum
as Michael
at
no signal
resonance
114.8
Yethyl
serve
In the
is
methanol)
product
absorption
carbonyl.
we
(2% HCl in
a crystalline
carbonyl spectrum.
on C-3.
acid. to
4
acceptor.
acid
CH,=CH-C-CH,
L-
formation
the
was chosen
perfectly
fl
+
1
and C-3
was clarified,
new reaction
A crystalline
or
a
contains
as acceptor.
vinyl
that
pH _ 4,
pii 7.4.
The crystal-
group
investigate
ketone
at
in
Jackson
of
examples
hemiketal
acrolein
to
solution at
of
place
role two
acid,
also These
ketone
acid
takes
was described
synthesis 11
and a carbonyl
vinyl
reaction
the
towards
O-6
formation
The reaction
buffer
_1 is
A similar
dehydro-L-ascorbic
rings.
between
O-6
intermediate
structure, 12
furanose
exclusive
of
benzylation
examples
between
2-O-phosphate.
of
ascorbic
for
and C-3
3.
the
Earlier
was observed.
on
aqueous
O-6
was
C-2
In both
paper
by the 5.
upon
The formation
pH 4.
cyclization
bicyclic
between
product
completely
The preference
the
however,
acid
on the
a hemiketal
D1O.
3-(hydroxymethyl)indol
had reported acid.
disappear
with
in a phosphate
plays
are,
reactions.
C-2
in
and 6.8
confirmed
product
acid
L-ascorbic
L-ascorbic
cyclization
_1
and
example
There
analogous
6’ :
of
are
tricyclic
any
ascorbic
ascot-b&en: at
exchange
to
equilibria
stable
donor.
alkylated’
6 5.6
reaction
dissociation
find
where
a Michael
of
more
not
literature
of
various
the
We could
acid. water
dissociation
As the
towards
formation
the
Since
ascorbate-3-anions
“starters”. the
ascorbic
necessary.
a solirent,
progresses,
of
pH -. 4 of
is
to
the methyl the
the
resonances
Structure We are
2 is basing
C-4
on analogies
at
the
methyl
closely our
with ketal
related
to
configurational -3. carbon
compound assignments
The configuration was deduced
at from
2.
2143
A new role for L-ascorbic acid
180150. 120SO-
min
Fig. 4.
Mutarotation
of _? in DMSO (c,
1.5).
3.
b. C.
d.
I
e. f. 8. h.
5.
Proton
decoupled
“C
NMR spectrum
of
5 in
0
50
100
150
200 Fig.
I
I
I
wm
17.8 30.2 37.1 74.1 76.4 78.1 87.5 108.3
D.0
(D:p-dioxane
reference).
a.
a
b. c. d. e. f. 8. h. 1’:
23.3 31.2 35.1 53.9 73.2 75.5 77.6 86.6 114.8 112.8
k.
173.8
r* i 200 ppm
I
Fig.
6.
Proton
decoupled
100 ‘*C
NHR spectrum
I
I
I
150
50 of
2 In D,O
fD:p-dioxane
0 reference).
2144
G. FODORet
al.
Dteiding models and especially space filling
might be possible by co-administration of
Catali" models of the two possible anomets
cyclophosphamide and L-ascorbic acid.
of -5.
The methoxyl group in g-position is
much preferred stetically.
In the tetta-
hydropyran ring assuming a twist-boat
The
spectrum
of
the
shows
that
nated
by some
Similar methyl mixture
-5 is
the
material major
unteacted
attempts
glycoside of
crude
“C
to
resulted
NMR
potential structure could be transformed into
contami-
other functionalities.
-4. convert in
-3 into
a
intermediate for syntheses.
a syrupy
products which shows three
3.6) of the 'H NMR spectrum.
EXPERIMENTAL
After partial
chromatographic separation spectral data of the individuai fractions suggest that two anomeric C-12 methyl glycosides were formed together with a dimethyl acetal-methyl ketal derived from the aldehyde form of 2.
The
separation and purification of these products is in progress. Conclusions.
This is the first report on L-
ascorbic acid as a novel powerful Michael catbanion donor towards two reactive a.@ unsaturated carbonyl compounds.
Further
studies are already under way to evaluate the scope of
this reaction.
We are
interested in using biologically significant a,B-unsaturated aldehydes like 4-hydroxypentenal as acceptors.
Assuming
that
the
addition is reversible in UiUO a"
adduct with 4-hydtoxypentenal could have 13 cancetostatic activity. Unsaturated nittiles and esters. and also q&nones,
shall
be investigated as potential Michael acceptors. The fact that the reaction with actolein takes place under almost physiological conditions suggests that ascorbic acid might be useful as a detoxifying agent in vivo.
Acrolein is a metabolite of the
widely used anticancer agent cyclophosphamide.
Melting points were determined on an Electrothermal melting point apparatus and ate uncorrected. IR spectra were recorded on a Beckman IR 10 spectrophotometet. A PetkinElmer Model 141 M Polarimetet was used for the optical rotation measurements. 13c NMR spectra were taken on a Varian CFT-20 specttometer at 20 MHz. The ‘H NMR spectra were recorded on a Vatian EM-360 (60 MHz) spectto-
meter and on a Vatian Cm-20 spectrometer at go MHZ. Elemental analysis were performed by Galbtaith Laboratories, Inc., Knoxville, Tennessee. L-(+)-ascorbic acid, actolein (97%) and methyl vinyl ketone (technical grade) were purchased from Aldrich and used without further purification. A standard solution of Tillmans’ reagent (TR) i.e., 2,6dichlotoindophenol sodium salt,17 was used for the titration of _1.
Monohydrate
of 3. To a stirred solution of 20 g (0.11 mol) ascorbic acid (1) in 100 ml H1O under a Nz atmosphere 5.8 g (0.10 mol) actolein was added dropwise. Throughout and after the addition the temperature was not allowed to rise above 25”. A white ptecipitate usually formed within two hours. If not, crystallization was induced by seeding. The suspension was stirred at room temperature until titration (with TR solution) of alfquots taken from the supetnatant liquid indicated a quantitative consumption of 1. After being kept in the refrigerator overnight the solid was filtered, washed and dried. 13 g monohydrate of 3, m.p. 111-113’ was obtained. Recrystallization from 95% ethanol gave transparent prisms, m.p. 114-116”. The supetnatant liquid was freeze-dried and the residual solid recrystallized from 95% ethanol to afford a” additional crop (5.1 g) of the monohydrate. Total yield: 18.1 g, 72%. Anal. Calcd. for C.H,.zO,*HzO: Found : C. 43.24; H. 5.60; 0, 51.16. c, 43.37; H, 5.71; 0, 51.03.
Protection against some toxic side-effects
1,3,7-Trioxa-&oxo-
which have been linked to acrolein was
G+tricyclo-
achieved by co-administration of sodium 214 or N-acetylmetcaptoethane sulfonate 15 cysteine. In both cases a free sulfhydtyl group is believed to react with the double bond of actolein to form a non-toxic addition compound. non-toxic substance
We shall try to
explore the use of 3 as a new chital
distinct peaks in the methoxy region (6 3.4-
Michael
derivative with a chital tertiary hydtoxyl. The side chain or the lactone ring of such a
clearly
product
a Robinson
annellation leading to a cyclohexenone
conformation the B-methoxy group is placed in equatorial position.
In addition, compound 3 in the diketo form appears to be set up for
Since 2 proved to be a 16 , a similar protection
(5% 9% lZE)-trikydroxy-
[4.3.2.0
2J 6. 02, ‘I-dodecane
(25 (2).
10 g (0.04 mol) monohydrate of 2 was dissolved in 140 ml hot absolute ethanol, 50 ml dry benzene was added and the mixture was After removal of the ternary and distilled. binary azeottope the residual dry ethanol solution was concentrated to about 60 ml. Compound 2 crystallized as white needles, IR (~gt!, 7g, 75%. m.p. 150-152’. Yield: 3580-3100 (broad, vOH). 2960 and 1780 cm-‘.
'H NMR (DMSO-d., 80 MHz) 6 1.7-2.4 !m, 4H),
2145
A new role for L-ascorbic acid 3.8-4.3 (m, 3H), 4.45 (s, lH), 5.58 (br s, 2H, partially disappears upon addition of D*O), 6.4-6.8 (-2H. DnO exchangeable peaks). I'C NMR (DMSO-d.): see Fig. 3. [al;' = +34.4" + 0.3" (c, l-in methanol). Mutarotation (c, 1.5 in DMSO): [a]::. = -36 o + + 184' (4.5 min -+ 3 hrs); see Fig. 4. Anal. Calcd. for C. 46.55 H, 5.17 0, 48.28. CeH1207: Found: C, 46.34 H, 5.26 0, 48.05. 1.6 g (7 mmol) of 2 in Acetalization of 3. 25 ml 2% methanol?k hydrogen chloride was stirred at room temperature for 8 hours. The solution was neutralized with powdered silver carbonate, filtered and dried (NalSO,). The methanol was rerrPved in vacua. The residue, a colorless syrup, was subjected to column chromatography on neutral alumina with benzene-ethanol (3:l) as eluent. TLC on alumina sheets (using the same eluent) indicated that two materials with Rf 0.25 and Rf 0.13 had been separated. 'H NMR spectra of the two isolated syrupy products showed three methoxy methyls (6 3.4, 3.5, 3.6) for one material (Rf 0.25), while the other product (Rf 0.13) had one methoxy peak at 6 3.5. So far the purification and characterization has not been completed. 3,6-Hemiketal of 2-(3-oxobutyZl-3-0x0-G gulonolactone 12). It was found advantageous to introduce methyl vinyl ketone in he vapor phase following a method by DeBoer. 15 20 g (0.11 mol) ascorbic acid (1) was dissolved in 100 ml H=O. Dry nitrogen gas (flow rate ‘-40 ml/min) was bubbled through 8.8 g (0.12 mol) methyl vinyl ketone and then introduced into the ascorbic acid solution through a fritted disc. The temperature was kept below 25'. After about 10 hours all the ketone - except for a small residue of non-volatile materialhad been transferred. Stirring of the homogeneous reaction mixture at 0" was continued until titration of aliquots indicated a constant amount (26%) of unreacted 1. Hence the conversion of 1 was 74%. Some inreacted methyl vinyl ketone had to be removed in UQCUO before the reaction mixture was freeze-dried. The crude product was extracted with hot ethyl acetate (ratio: 10 ml per 1 g). A white crystalline solid separated from the extract. After cooling and filtration 13.7 g of product 3 were obtained. The yield was 66% based on 1 consumed. Recrystallization from ethyi acetate yielded transparent crystals, m.p. 134-136". Direct recrystallization of the crude product from ethyl acetate gave pure 4 in a somewhat lower yield. IR (KBr) 7380, 3260, 3010, 2950, 2900, 1760 and 1700 cm-'. 'H NMR (DMSO-d., 80 MHz) 6 1.87 (m, 2H), 2.07 (s, 3H), 2.5 (m. 2H), 3.8-4.2 (m. 3H), 4.43 (s. 1H). 5.62 (br s, 2H), 6.79 (s, 1H). The signals at 5.62 and 6.79 disappear completely upon addition of D?O. "C NMR (D,O): See Fig. 5. [ali = +41" + 0.3" (c, 1 in methanol). Anal. Calcd. forC1aH1z.0,: C, 48.78; H. 5.69; 0, 45.53. Found: C. 48.91; H. 5.77; 0. 45.32. 1,3, ?-Trioza-&oxo- (5% SSI-dihydroxy-lZR(?)metbxy-12E(?I-methyZ(24 6l+tricycZo[4.3.2.0 2a6.02Jg]-dodecane 15). 1.5 g (6.1 mmol) of 4 was dissolved in ?5 ml anhydrous methanol containing 2% hydrogen chloride and stirred for 7 hours at room temperature. The yellow solution was neutralized with
powdered silver carbonate, cooled, filtered and dried (NazSOb). Removal of the solvent in vacua gave a syrup which partly crystallized. The crude product was recrystallized twice from ethyl acetate to'afford 0.5 g (31%) of pure 5, colorless crystals, m.p. 154-156'. IR (KBr): 3440. 3330, 2950 and 1730 cm-'. 'H NMR (DMSO-da, 60 MHz) 6 1.40 (s. 3H), 1.6-2.3 (m, 4H), 3.68 (s. 3H), 3.84.3 (m, 3H), 4.43 (s. lH), 5.3 and 5.82 (DIO see "C NMR (D,O) exchangeable protons). Fig. 6. [old = +53.7' + 0.3" (c, 1 in methanol). Anal. Calcd. for C1,H160,: C, 50.77; H. 6.15; 0, 43.08. Found: C, 50.69; H, 6.24; 0, 43.17. The work done at West Acknowledgements. Virginia University was supported entirely by a grant from the National Foundation for Cancer Research (NFCR). Thanks are due to Professor Albert Szent-Gysrgyi for calling our attention to the reaction of ascorbic acid with acrolein. REFERENCES 1.
Part of this work will be included in the Ph.D. dissertation of R.A.
2.
G. Fodor, R. Mujumdar and J. R. Butterick in "Submolecular Biology and Cancer", Ciba Foundation Series 67, Excerpta Medica, Amsterdam (1979). PP. 165-174.
3.
G. Fodor, J. R. Butterick, A. Springsteen and H. Mathelier, ORGN 286 in "Book of Abstracts" , Joint Congress of the American Chemical Society and the Chemical Society of Japan, Honolulu, Hawaii (1979).
4.
A. Szent-Gy&gyi and G. Fodor, US Patents 4.238.500 and 4,287.205.
5.
J. Karle and I. L. Karle, Acti Cryst. 2, 849 (1966).
6.
W. R. Busing, K. 0. Martin, H. A. Levy, R. D. Ellison, W. C. Hamilton, J. A. Ibers, C. K. Johnson and W. E. Thiessen, ORXFLS3, Oak Ridge National Laboratory, TN (1975).
7.
R. D. Cilardi. ncta mst. (1973).
8.
C. K. Johnson, ORTEP. Report ORNL-3794 Oak Ridge National Laboratory, TN (1965).
9.
G. Kiss and ti. Neukom, Helv. 2, 989 (1966).
m,
2089
Chim. Acta
10.
K. C. A. Jackson and J. K. N. Jones, Canad. J. &em. 42, 560 (1965).
11.
Y. Sekine. T. Futatsugi, T. Hata and F. Cramer, J. tig. Chem. 9, 3453 (1982).
12.
J. Hvoslef, Acta Cryst.
13.
P. J. Conroy, J. T. Nodes, T. F. Slater and G. W. White, Eur. J. Can. 12, 55(1977).
14.
N. Brock. J. Stekar, J. Pohl, U. Niemeyer and G. Scheffler, Arzneim.-Forsch. 2, 659 (1979).
15.
M.
m,
916 (1972).
J. Berrigan, H. L. Gurtoo. S. D.Sharma. R. F. Struck and A. J. Marinello, Biochem. and Biophys. Res. Conrun. 93. 797 (1980).
16.
R. Veltri. private communication.
17.
K. Schank. Synthesis.
18.
C. D. DeBoer. J. Org. Chem. 2. (1974).
181 (1972). 2426
-/83
A NEW ROLE FOR L-ASCORBIC ACID:
$3.00 + .a3 F’qamon Prm Ltd.
MICHAEL DONOR TO o,B-UNSATURATED
CARBONYL COMPOUNDS1
GABOR FODOR", REGINA ARNOLD AND TIVADAR MOHACSI National Foundation for Cancer Research Laboratory at the Department of Chemistry, West Virginia University, Morgantown, WV
26506
ISABELLA KARLE AND JUDITH FLIPPEN-ANDERSON Laboratory for the Structure of Matter, Naval Research Laboratory, Washington, DC 20375
(Receivedin USA
14 January 1983)
Abstract - In a novel Michael-type reaction L-ascorbic acid (1) undergoes addition to acrolein to give the tricyclic hemiacetal lactone 3. The constitution and relative configuration of 3 was studied by a combination of NMR and IR spectroscopy. Ultimately, the structure of 3 was determined by X-ray crystallography. The absolute stereochemistry follows from the known chirality of C-4 and C-5 of L-ascorbic acid. A mechanism for the reaction, including its steric course, is proposed. Methyl vinyl ketone reacts with 1 in a similar fashion to give diketo lactone derivative 4. Upon the action of methanolic hydrogen chloride on 5 one anomer, the tricyclic methyl ketal lactone 5, forms. Structure 5 is closely related to 3. Synthetic and possible biological applications of the new reaction are-discussed. Recently one of us and his associates found
saturated lactone.
that L-ascorbic acid (1) undergoes enediol
the primary product (m.p. 114-116")
The elemental analysis of
acetal formation with 1,2-dicarbonyl
corresponds to the monohydrate of a 1:l adduct
compounds like methylglyoxal and their 2-4 vinylogues e.g., 4-keto'2-pentenal.
between acrolein and -1. However, the adduct can be dehydrated to product 2 (m.p. 150-152') via
In contrast, we now observed that acrolein
the ternary azeotrope with ethanol and
reacts with ascorbic acid in water to give a
benzene.
crystalline product that shows no olefinic
is the 1:l adduct.
protons and carbons, respectively, lnthe and "C
NMR spectrum.
'H
Both 2 and its monohydrate show identical
A single carbonyl
13C NMR spectra in DMSO-d. (Fig. 3).
band appears at 1780 cm-' in the IR and a signal at 175
Elemental analysis confirms that 2
A
noticeable feature is that most of the major
ppm in the r'C NMR spectrum.
signals appear as narrowly spaced "doublets"
These values suggest the presence of a
in the proton decoupled spectrum.
2137
This
2138
G. FODORet al.
points
to
isomers of
2 can
is
presence
are
of
in
with
that
MS0
solution.
(Fig.
from
4)
which
findings
hemiacetal
the
aldehyde
crystals
of
recrystallization
2 were
from
a structure
study
are
obtained
thus
crystallizes
feasible.
described
in
in
Details
the
of
c = 10.318(4)
the
monoclinic
A,
independent
A,
B -
using
structure
was
were
for
each
from
observed to
in
hydroxyl the
of
and
also
resultant
refinement
by
for
did
not
data
atoms
were after
the
C
well
coordinates
hydrogen
give
z1 IFoI-IFcl Z/F 1
on in
the
that
1,
I
using final
good
and O-9 on O-12. these
R factors,
Table and
1 lists
the
Beq values
for final for
our
analysis.
of
in FIp,.
1,
experimentally The molecule
b-membered
the
is
has
ring
and
consistent
cyclic
hemiacetal
the
configurations were
The absolute
C-4
the
rational
by
configu-
the
and C-5
to
at
established
by using
atoms
2’6.02’9]
know” of
ascorbic
new ehiral
name of
dodecane.
throughout
request
centers.
1.3,7-trioxa-
the
Chemical name:
This
numbering
text.
However,
upon
Abstracts
suggcstcd
the
(3S,3aR,SaS,6R)-hexahydro-
R and 3.94% refined “on-
which
Fig.
2 fiall
within
The angles
around
C-2,
indicate
that
form
in
and angles
values.
the
without ring
(the
has
C-2,
C-9,
34.1(5)O).
Both
conformation
the
C-2,
C-6
the
“flaps”;
by C-2,
O-3,
and C-2
is
C-2,
bond
C-4
and C-5
of
and C-9 The ring
O-1
packing
rings torsion is
intermolecular
the
the
in
also angle
influenced hydrogen
are
of
is
in a”
(the
the
bonds.
rings
by C-6,
the H-6,
two
Crystal
presence O-5
5-
C-6,
-31.2(5)‘). the
from
formed
five-membered
between
by
&r
about
atoms
formed
other
cc.*
is is
plane
one
plane
In the
5-
twisted
these
of
junction is
rings
that
out
the
angle
and are
such
chair
junction
5-membered
is
out
at
able
The h-
flattened
torsion
C-6
and C-9 was
strain.
ring
O-9
expected C-6
fusion
h-membered
are
system
a somewhat
envelope
C-8
ring
The ring
and
O-3,
fused
significant
conformation. membered
ring.
the
a
centers
was deduced
membered 3.24%
the
This
of
as a reference
C-7, and Rw -
so
WFO =
R+.
on O-5
to
stereodiagram
The relative
chiral
membered
parameters
map showed
calculated
of
[
X-ray
to
and COH angles
a disordered
Zw(jFo\-iFc/)’
the
the product
2-(3-oxopropyl)-3-oxo-I.-gulono-
illustrated
were
on just
refine
hydrogens
parameters
R =
five
elucidated addition
one
Bond distances
The hydrogens
difference the
factors
hydrogen
the
[3,4-blpyran-S-one.
deviations
positional
O-H distances
and indicated
where
from
3,5a,8-trihydroxy-211,5H-furo-[3’,2’:2,3]furo-
map calculated
refined.
A subsequent
for
using
unreasonable.
Structure
and a
and calculated
the
rings.
of
14.3.2.0
w
Hydrogen
their
oxygens
positions
thermal
has
from
structure
following
802
the
rings,
(2).
the
were calculated All
the
was used
minimized
standard
refinement.
cycles
then
were
estimated
a difference
and 0 atoms were
the
&oxo-(55,9S,12R)-trihydroxy-(2R,6E)-tricyclo-
refined
weights,
in
5-membered
We choose
thermal were
of
coordinates.
fused
acid
was
the
Gilardi7.
the
several
and
atoms
available
analysis
shown
chirality
The
methods
procedure
intensity)
according
located
are
by computer
ration
a graphite
The function
where
collected
symbolic
and
least-squares
least-squares
in
that
draw”
lac tone
non-centrosymmetric
C and 0 atom
0RFXLS3.
(derived
for
observed
for
atoms,
“on-hydrogen
formula
3,6-ketal
A,
beam. the
The coordinates
full-matrix
used
using for
group
diffracto-
with
incident
solved
Cw(IF,I-IF&)‘,
of
the
procedure5
crystals.
program6
coordinates
carbon
Anisotropic
the
factors
structural
with
and 2 = 2.
X-ray
CuKa radiation on
space
101.8(l)’
reflections
monochromator
the
between
two
-3
b = 7.526(S)
on a NICOLET P3F automatic
by
comparison
determined
following
The compound
a = 6.293(3)
addition
to
map coordinates
for
three
P21 with
refined
hydrogens.
parameters
be
by X-ray
became
Crystalloarauhv.
factors
difference
the bonded
The X-ray
paragraph.
meter
the
by
methanol-ether,
determination
crystallography
802
hydrogens
authors.
Single
X-Ray
atoms,
the
structure
group
acrolein.
this
hydrogen
hydroxyl
between
These
a cyclic
arises
related
mutarotatio”
an equilibrium
3 in
consistent
two closely
Indeed,
be observed
of
moiety
of
solutio”.
indicative
isomers
of
the
in
of is
3
a donor
A new role for L-ascorbic acid
2139
Table 1.
Fractional Coordinates and Equivalent Isotropic Thermal Parameters with e.s.d.'s in Parentheses. --.\*om x 2 v 8eq ~_____-0.3529(4) 0.2379(j) 0.1204(4) 0.2057(6) 0.4037(7) 0.6029(4) 0.3816(6) 0.24?6(4) 0.0714(7) -0.0665(5) 0.0834(5) -0.1240(4) 0.1752(7) O.U73(7) 0.4X5(6) 0.6042(4)
O(1) C(2) O(3) C(4) C(5) O(5) C(6) O(7) C(8) O(8) C(9) O(9) C(10) C(11) C(12) O(12)
0.5957(7) 0.759L 0.7605(7) 0.8843(9) 0.9697(8) O-8954(7) 0.9252(7) 1.0638(6) 0.990?(9) 1.0844(7) 0.7917(a) 0.7134(7) 0.7223(9) 0.5295(8) 0.5204(8) 0.6156(8)
2.5(l) 2.3(l) 2.9(l) 3.5(2) 2.9(l) 3.1(l) 2.8(l) 3.3(2) 3.0(l) 3.9(2) 2.6(l) 2.9(l) 3.1(l) 3.3(2) 3.2(l) 3.9(2)
----
--____
=
B eq
Fig.
0.1958(Z) 0.1806(3) 0.0505(2) -0.0302(4) 0.0552(4) 0.0337(3) 0.1955(4) 0.2375(3) 0.2762(4) 0.3054(3) 0.2762(4) 0.2319(3) 0.4137(4) 0.4059(4) 0.3256(4) 0.3970(3)
1.
; z r oii ai*.l. J 1.i
Stereodiar:ram of the structural formula and stercocnnfiguracion of 3 as rlr,~~r,:i:~i~d h':k-rav ~if~Fr;~ctior,.
d
10 1OQ.Z
Fig. C.
119.7 b01
aund lenp,ths (e.s.d. 0.003
X)
01-2-6 j-2-9
101.7 t12.e
and bond angles (e.s.d. 0.5*) in 3.
2140
G. FODORer al. Table 2.
Fractional Coordinates for H Atoms with e.s.d.'s in Parentheses.
Atom
x
Y
H(4) H(4) H(5) H(6) H(l0) H(lO) H(U) H(ll) H(l2) H(O5) H(O9) H(012)
0.248(9) 0.082(8) 0.410(8) 0.531(8) 0.302(9) 0.065(7) 0.120(8) 0.286(8) 0.479(8) .635 -.174 .682 .664
0.811(8) 0.979(8) 1.103(9) 0.907(9) 0.801(9) 0.736(9) 0.450(9) 0.478(8) 0.377(9) .945 .754 .616 .591
to the ring oxygen O-l with the He**0
-0.113(6) -0.063(6) 0.053(S) 0.261(S) 0.452(S) 0.471(S) 0.373(S) 0.506(6) 0.306(S) -.023 .159 .325 .478
DISCUSSION
distance at 2.10 A, the O***O distance at 2.84 A an
2
the O-H***0 angle at 166.7".
After the structure of the tricyclic O-9
lactone 2 was unequivocally determined tie
is a donor to O-5 with an H***O distance of
were able to confirm and complete the
1.99 A, and O***O distance of 2.72 A and an
interpretation of its spectra.
O-H.**0 angle of 151.4".
The hydrogen on
All major signals in the "C
NMR spectrum
O-12 appears to be disordered between two
have been assigned to the two anomers of 2.
positions.
The minor peaks can be attributed to a small
In one of its disordered
positions it does not form any hydrogen
amount of bicyclic lactone free aldehyde
bonds.
which is also formed in solution (Fig. 3).
In the other position it is a donor
to a hydrogen bond to O-9 with an He**0
The fact that 2 and its monohydrate have
distance of 1.84 A. an O***O distance of
identical NMR spectra in DMSO-d. indicates
2.74 A and an O-H***0 angle of 153.0".
The
only other intermolecular approach less than
that the water molecule is loosely bound to 2, since the DMSO-water interactions are
a van der Waals' separation is between C-2
stronger than the intermolecular association
and O-5 at 3.14 A.
of water and compound 2.
a. b. C.
d. e. f. g. h. i.
Fig. 3.
Proton decoupled "C
NMR spectrum of 3 in DMSO-de.
29.3, 29.9 32.0, 32.3 73.6 74.8 85.2, 85.3 87.2, 87.5 99.6, 100.0 106.0, 106.8 174.9. 175.1
A new role for L-ascorbic acid NXR spectrum
The “C
of
the monohydrate
Da0 shows the same pattern There are only
signals.
(2 2 ppm) downfield lactone
carbonyl
the conclusion Involved
as
the hydrate
in hydrogen
geometry
membered rings appears
the two fused
as a broadened
to
proton
reached
rapidly
Michael
and thereby
can be followed
escapes 4).
of
were taken at 365 nm, because
opposite
is larger
is
solvent
Time zero
refers
is added to -3.
is possible dissolved,
before
Since rotation
be determined
acid
completely of pure 1 at
experimentally.
The initial
reading
(t = 4.5)
but changes
rapidly
towards
positive
of
lead
Concerning
to the
ascorbic
that acid
1
acrolein
Hence the addition
The ultimate
involving
from the
from the side ring
C-3 and O-6 of ascorbic
to the thermod~namfcally of
Furthermore,
in the crystal
the two five-membered
hydroxyl
prefers
lattice,
is noteworthy
that
favored rings. the
an equatorial
away from the ketofuranose the Michael
-2b
Scheme
acts
the steric
one can infer
&s-junction
It
acid
a
nucleophilic
the product
C-2 of
leads
position
values.
ascorbic
to C-5 and C-6.
hemiacetal
is negative
J_.
stereoselective.
closure
no measurement
the sample is
the optical
t = 0 cannot
to the time the
to the keto
is essentially
of -_ 2b should
the reaction
configuration
the rotation lengths.
This
wherein
carbon
approaches
wave-
the conjugated
leading
A concerted
product
measurements
at shorter
to make C-2 the
of O-6 upon C-3 and O-3 upon the
course
The
,221.
reaction
tricyclic
the change of
(Fig.
(vie
In our case
around C-Z is
increased
aldehyde
the equilibrium
Las an
two potentially
whjch can attack
s
reaction
of _3.
O-3 and C-2. density
as the donor.
be observed
with
bond of acrolein
attack
In DMSO, however,
rotation
sites:
aldehyde
with a hydroxyl
We assume that
detection.
reactive
nucleophile
resonance.
in methanol.
nucleophile
double
a possible
can be regarded
ambident
sufficiently
five-
at 6 5.6.
of 2 cannot
in the
the anomerfc
the formation
the X-electron
the C-S proton
singlet
overlaps
The mutarotation is
of
for Due to
at 6 4.5,
- maybe
- which forms
of establishing
mechanism for
mono-
except
The C-l.? hemiacetal
This peak partly proton
singlet
be due to a
species
Scheme 1 outlines to
The C-6 proton
peak.
coupling
is negligible.
aldehydc
ascorbate-3-anion
the water
as a sharp
the rigid
is
bonding
of 2 and its
could
equilibrium.
molecule.
of
appears
process
rotation
levorotatory
the free
This allows
in DMSO-d6 are identical
the size
transient
C-5 and the
the C-5 hydroxyl
The ‘H NMRspectra hydrate
for
resonance. that
The negative
“doublet”
t.wo significant
shifts:
donor
a
with
in
2141
ring. addition
G. FODOR et al.
2142 step
takes
place
at
No basic
catalyst
was used
as
provides
sufficient
act
as
shifted
of
somewhat
in aqueous 10
with
solution
at
subsequent to
form
lactone
in a recent ascorbic line
acid
dimer
pcntacyclic
the
tendency
M_etil
with
;lroceeded
with
ascorbic
Clycosidation
a
affords
ketounderscore
there
Once
the
scope
of
this
compound
corresponds and
to the
the
have
carbonyl cm-‘).
(Fig.
5)
been
shows at
lactone
214.7
is In
sharp
singlet
the
177.9
6 2.1 to
singlet
at
can
d 4.4
are
ketone
Two hydroxyl
1.
carbons
singlet
to
a methoxyl
peak
appears
correct
the
at
in
the
tricyclic
perfect
the
lactone
‘H YX??
6 3.7
group; at
6) but
ppm and
The
another
6 1.4.
elemental
are
(Fig.
(112.8
a sharp
the TR
The analysts
agreement methyl
with
ketal
two (1700 in
to Tbl.s
signal
CH,OH 2aHCI
’ the is
at
s
108.3
(DMSO-d.)
belongs
to
the
function;
be ascribed proton
cm-‘,
D20
A hemiketal
-4.
a keto
_4
carbonyl
ppm.
by the
adjacent
proton.
There
structure
protons
CllHlsOI
the
carbonyl
instead.
the
lacks
in
ppm indicates
4
lactone.
In
hemiketal
IR spectrum
‘H NMR spectrum at
for
structure
ascorbic
ppm in addition
indicated
ppm.
cyclic
one
at
with
of
which
ketone.
NMR spectrum
only
carbonyl
consistent
the “C
isolated
and
a keto
present
shows
spectra
which cm-’
NMR spectrum
for
Two ketal
methyl
1700
of
2-(3-oxobutylj-3-oxo-
its
formed. in
The
resonance
carbon
or
bands
1760
adduct
the
L-gulonolactone, could
1:l
be
CloHI,O,
a,@-unsaturated
either
principle,
could for
“C
173.8
corresponding sharp
analyzed
at
ppm) are
spectrum
as Michael
at
no signal
resonance
114.8
Yethyl
serve
In the
is
methanol)
product
absorption
carbonyl.
we
(2% HCl in
a crystalline
carbonyl spectrum.
on C-3.
acid. to
4
acceptor.
acid
CH,=CH-C-CH,
L-
formation
the
was chosen
perfectly
fl
+
1
and C-3
was clarified,
new reaction
A crystalline
or
a
contains
as acceptor.
vinyl
that
pH _ 4,
pii 7.4.
The crystal-
group
investigate
ketone
at
in
Jackson
of
examples
hemiketal
acrolein
to
solution at
of
place
role two
acid,
also These
ketone
acid
takes
was described
synthesis 11
and a carbonyl
vinyl
reaction
the
towards
O-6
formation
The reaction
buffer
_1 is
A similar
dehydro-L-ascorbic
rings.
between
O-6
intermediate
structure, 12
furanose
exclusive
of
benzylation
examples
between
2-O-phosphate.
of
ascorbic
for
and C-3
3.
the
Earlier
was observed.
on
aqueous
O-6
was
C-2
In both
paper
by the 5.
upon
The formation
pH 4.
cyclization
bicyclic
between
product
completely
The preference
the
however,
acid
on the
a hemiketal
D1O.
3-(hydroxymethyl)indol
had reported acid.
disappear
with
in a phosphate
plays
are,
reactions.
C-2
in
and 6.8
confirmed
product
acid
L-ascorbic
L-ascorbic
cyclization
_1
and
example
There
analogous
6’ :
of
are
tricyclic
any
ascorbic
ascot-b&en: at
exchange
to
equilibria
stable
donor.
alkylated’
6 5.6
reaction
dissociation
find
where
a Michael
of
more
not
literature
of
various
the
We could
acid. water
dissociation
As the
towards
formation
the
Since
ascorbate-3-anions
“starters”. the
ascorbic
necessary.
a solirent,
progresses,
of
pH -. 4 of
is
to
the methyl the
the
resonances
Structure We are
2 is basing
C-4
on analogies
at
the
methyl
closely our
with ketal
related
to
configurational -3. carbon
compound assignments
The configuration was deduced
at from
2.
2143
A new role for L-ascorbic acid
180150. 120SO-
min
Fig. 4.
Mutarotation
of _? in DMSO (c,
1.5).
3.
b. C.
d.
I
e. f. 8. h.
5.
Proton
decoupled
“C
NMR spectrum
of
5 in
0
50
100
150
200 Fig.
I
I
I
wm
17.8 30.2 37.1 74.1 76.4 78.1 87.5 108.3
D.0
(D:p-dioxane
reference).
a.
a
b. c. d. e. f. 8. h. 1’:
23.3 31.2 35.1 53.9 73.2 75.5 77.6 86.6 114.8 112.8
k.
173.8
r* i 200 ppm
I
Fig.
6.
Proton
decoupled
100 ‘*C
NHR spectrum
I
I
I
150
50 of
2 In D,O
fD:p-dioxane
0 reference).
2144
G. FODORet
al.
Dteiding models and especially space filling
might be possible by co-administration of
Catali" models of the two possible anomets
cyclophosphamide and L-ascorbic acid.
of -5.
The methoxyl group in g-position is
much preferred stetically.
In the tetta-
hydropyran ring assuming a twist-boat
The
spectrum
of
the
shows
that
nated
by some
Similar methyl mixture
-5 is
the
material major
unteacted
attempts
glycoside of
crude
“C
to
resulted
NMR
potential structure could be transformed into
contami-
other functionalities.
-4. convert in
-3 into
a
intermediate for syntheses.
a syrupy
products which shows three
3.6) of the 'H NMR spectrum.
EXPERIMENTAL
After partial
chromatographic separation spectral data of the individuai fractions suggest that two anomeric C-12 methyl glycosides were formed together with a dimethyl acetal-methyl ketal derived from the aldehyde form of 2.
The
separation and purification of these products is in progress. Conclusions.
This is the first report on L-
ascorbic acid as a novel powerful Michael catbanion donor towards two reactive a.@ unsaturated carbonyl compounds.
Further
studies are already under way to evaluate the scope of
this reaction.
We are
interested in using biologically significant a,B-unsaturated aldehydes like 4-hydroxypentenal as acceptors.
Assuming
that
the
addition is reversible in UiUO a"
adduct with 4-hydtoxypentenal could have 13 cancetostatic activity. Unsaturated nittiles and esters. and also q&nones,
shall
be investigated as potential Michael acceptors. The fact that the reaction with actolein takes place under almost physiological conditions suggests that ascorbic acid might be useful as a detoxifying agent in vivo.
Acrolein is a metabolite of the
widely used anticancer agent cyclophosphamide.
Melting points were determined on an Electrothermal melting point apparatus and ate uncorrected. IR spectra were recorded on a Beckman IR 10 spectrophotometet. A PetkinElmer Model 141 M Polarimetet was used for the optical rotation measurements. 13c NMR spectra were taken on a Varian CFT-20 specttometer at 20 MHz. The ‘H NMR spectra were recorded on a Vatian EM-360 (60 MHz) spectto-
meter and on a Vatian Cm-20 spectrometer at go MHZ. Elemental analysis were performed by Galbtaith Laboratories, Inc., Knoxville, Tennessee. L-(+)-ascorbic acid, actolein (97%) and methyl vinyl ketone (technical grade) were purchased from Aldrich and used without further purification. A standard solution of Tillmans’ reagent (TR) i.e., 2,6dichlotoindophenol sodium salt,17 was used for the titration of _1.
Monohydrate
of 3. To a stirred solution of 20 g (0.11 mol) ascorbic acid (1) in 100 ml H1O under a Nz atmosphere 5.8 g (0.10 mol) actolein was added dropwise. Throughout and after the addition the temperature was not allowed to rise above 25”. A white ptecipitate usually formed within two hours. If not, crystallization was induced by seeding. The suspension was stirred at room temperature until titration (with TR solution) of alfquots taken from the supetnatant liquid indicated a quantitative consumption of 1. After being kept in the refrigerator overnight the solid was filtered, washed and dried. 13 g monohydrate of 3, m.p. 111-113’ was obtained. Recrystallization from 95% ethanol gave transparent prisms, m.p. 114-116”. The supetnatant liquid was freeze-dried and the residual solid recrystallized from 95% ethanol to afford a” additional crop (5.1 g) of the monohydrate. Total yield: 18.1 g, 72%. Anal. Calcd. for C.H,.zO,*HzO: Found : C. 43.24; H. 5.60; 0, 51.16. c, 43.37; H, 5.71; 0, 51.03.
Protection against some toxic side-effects
1,3,7-Trioxa-&oxo-
which have been linked to acrolein was
G+tricyclo-
achieved by co-administration of sodium 214 or N-acetylmetcaptoethane sulfonate 15 cysteine. In both cases a free sulfhydtyl group is believed to react with the double bond of actolein to form a non-toxic addition compound. non-toxic substance
We shall try to
explore the use of 3 as a new chital
distinct peaks in the methoxy region (6 3.4-
Michael
derivative with a chital tertiary hydtoxyl. The side chain or the lactone ring of such a
clearly
product
a Robinson
annellation leading to a cyclohexenone
conformation the B-methoxy group is placed in equatorial position.
In addition, compound 3 in the diketo form appears to be set up for
Since 2 proved to be a 16 , a similar protection
(5% 9% lZE)-trikydroxy-
[4.3.2.0
2J 6. 02, ‘I-dodecane
(25 (2).
10 g (0.04 mol) monohydrate of 2 was dissolved in 140 ml hot absolute ethanol, 50 ml dry benzene was added and the mixture was After removal of the ternary and distilled. binary azeottope the residual dry ethanol solution was concentrated to about 60 ml. Compound 2 crystallized as white needles, IR (~gt!, 7g, 75%. m.p. 150-152’. Yield: 3580-3100 (broad, vOH). 2960 and 1780 cm-‘.
'H NMR (DMSO-d., 80 MHz) 6 1.7-2.4 !m, 4H),
2145
A new role for L-ascorbic acid 3.8-4.3 (m, 3H), 4.45 (s, lH), 5.58 (br s, 2H, partially disappears upon addition of D*O), 6.4-6.8 (-2H. DnO exchangeable peaks). I'C NMR (DMSO-d.): see Fig. 3. [al;' = +34.4" + 0.3" (c, l-in methanol). Mutarotation (c, 1.5 in DMSO): [a]::. = -36 o + + 184' (4.5 min -+ 3 hrs); see Fig. 4. Anal. Calcd. for C. 46.55 H, 5.17 0, 48.28. CeH1207: Found: C, 46.34 H, 5.26 0, 48.05. 1.6 g (7 mmol) of 2 in Acetalization of 3. 25 ml 2% methanol?k hydrogen chloride was stirred at room temperature for 8 hours. The solution was neutralized with powdered silver carbonate, filtered and dried (NalSO,). The methanol was rerrPved in vacua. The residue, a colorless syrup, was subjected to column chromatography on neutral alumina with benzene-ethanol (3:l) as eluent. TLC on alumina sheets (using the same eluent) indicated that two materials with Rf 0.25 and Rf 0.13 had been separated. 'H NMR spectra of the two isolated syrupy products showed three methoxy methyls (6 3.4, 3.5, 3.6) for one material (Rf 0.25), while the other product (Rf 0.13) had one methoxy peak at 6 3.5. So far the purification and characterization has not been completed. 3,6-Hemiketal of 2-(3-oxobutyZl-3-0x0-G gulonolactone 12). It was found advantageous to introduce methyl vinyl ketone in he vapor phase following a method by DeBoer. 15 20 g (0.11 mol) ascorbic acid (1) was dissolved in 100 ml H=O. Dry nitrogen gas (flow rate ‘-40 ml/min) was bubbled through 8.8 g (0.12 mol) methyl vinyl ketone and then introduced into the ascorbic acid solution through a fritted disc. The temperature was kept below 25'. After about 10 hours all the ketone - except for a small residue of non-volatile materialhad been transferred. Stirring of the homogeneous reaction mixture at 0" was continued until titration of aliquots indicated a constant amount (26%) of unreacted 1. Hence the conversion of 1 was 74%. Some inreacted methyl vinyl ketone had to be removed in UQCUO before the reaction mixture was freeze-dried. The crude product was extracted with hot ethyl acetate (ratio: 10 ml per 1 g). A white crystalline solid separated from the extract. After cooling and filtration 13.7 g of product 3 were obtained. The yield was 66% based on 1 consumed. Recrystallization from ethyi acetate yielded transparent crystals, m.p. 134-136". Direct recrystallization of the crude product from ethyl acetate gave pure 4 in a somewhat lower yield. IR (KBr) 7380, 3260, 3010, 2950, 2900, 1760 and 1700 cm-'. 'H NMR (DMSO-d., 80 MHz) 6 1.87 (m, 2H), 2.07 (s, 3H), 2.5 (m. 2H), 3.8-4.2 (m. 3H), 4.43 (s. 1H). 5.62 (br s, 2H), 6.79 (s, 1H). The signals at 5.62 and 6.79 disappear completely upon addition of D?O. "C NMR (D,O): See Fig. 5. [ali = +41" + 0.3" (c, 1 in methanol). Anal. Calcd. forC1aH1z.0,: C, 48.78; H. 5.69; 0, 45.53. Found: C. 48.91; H. 5.77; 0. 45.32. 1,3, ?-Trioza-&oxo- (5% SSI-dihydroxy-lZR(?)metbxy-12E(?I-methyZ(24 6l+tricycZo[4.3.2.0 2a6.02Jg]-dodecane 15). 1.5 g (6.1 mmol) of 4 was dissolved in ?5 ml anhydrous methanol containing 2% hydrogen chloride and stirred for 7 hours at room temperature. The yellow solution was neutralized with
powdered silver carbonate, cooled, filtered and dried (NazSOb). Removal of the solvent in vacua gave a syrup which partly crystallized. The crude product was recrystallized twice from ethyl acetate to'afford 0.5 g (31%) of pure 5, colorless crystals, m.p. 154-156'. IR (KBr): 3440. 3330, 2950 and 1730 cm-'. 'H NMR (DMSO-da, 60 MHz) 6 1.40 (s. 3H), 1.6-2.3 (m, 4H), 3.68 (s. 3H), 3.84.3 (m, 3H), 4.43 (s. lH), 5.3 and 5.82 (DIO see "C NMR (D,O) exchangeable protons). Fig. 6. [old = +53.7' + 0.3" (c, 1 in methanol). Anal. Calcd. for C1,H160,: C, 50.77; H. 6.15; 0, 43.08. Found: C, 50.69; H, 6.24; 0, 43.17. The work done at West Acknowledgements. Virginia University was supported entirely by a grant from the National Foundation for Cancer Research (NFCR). Thanks are due to Professor Albert Szent-Gysrgyi for calling our attention to the reaction of ascorbic acid with acrolein. REFERENCES 1.
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