Abstract
This invention relates to a method for preparing azithromycin dihydrate
from crude azithromycin by the gradual crystallization of azithromycin
from acetone by the addition of a minimal amount of water to effect
crystal formation is disclosed. This invention also relates to a method
of making azithromycin from desmethyl-azithromycin by dissolving desmethyl-azithromycin
in acetone, adding activated carbon, adding formaldehyde, adding formic
acid; refluxing the desmethyl-azithromycin acetone solution, adding
sodium hydroxide to induce precipitation of azithromycin, and isolating
azithromycin.
Claims
We claim:
1. A process for making azithromycin dihydrate, comprising the
steps of: (a) dissolving azithromycin in acetone; (b) maintaining
the solution of azithromycin and acetone temperature of about 20.degree.
C. to about 25.degree. C.; (c) adding water in two separate sequential
additions, a first addition of water and a second addition of water;
(d) adding water of the second addition at a rate of up to 0.2 volumes
of water per volume of acetone per hour; and (e) isolating the crystals
of azithromycin dihydrate.
2. The process of claim 1 wherein the first addition of water facilitates
the formation of a suspension.
3. The process of claim 2 wherein between about 0.4 to about 0.5
volumes of water per volume of water are added in the first addition
of water.
4. The process of claim 1 wherein the temperature is maintained
at about 20.degree. C.
5. The process of claim 1 wherein the first addition of the water
occurs over about 2 to about 3 hours.
6. The process of claim 1 wherein the solution formed after the
first addition of water is stirred for about 4 hours prior to the
second addition of water.
7. The process of claim 1 wherein the isolated azithromycin dihydrate
contains less than about 0.1% of isomers of azithromycin.
8. A method of making azithromycin from desmethyl-azithromycin
comprising the steps of: (a) dissolving desmethyl-azithromycin in
acetone; (b) refluxing the desmethyl-azithromycin acetone solution;
(c) adding formaldehyde; (d) adding formic acid; (e) adding activated
carbon; (f) adding sodium hydroxide to induce precipitation of azithromycin;
and isolating azithromycin.
9. The method of claim 8 wherein the isolated azithromycin is substantially
free of derivatives of azithromycin.
10. The method of claim 8 further comprising the step of heating
the desmethyl-azithromycin acetone solution.
11. The method of claim 8, wherein the desmethyl-azithromycin acetone
solution is heated to reflux.
13. The method of claim 8 further comprising the step of drying
azithromycin at about 40.degree. C.
Description
CROSS-REFERENCE TO RELATED APPLICATIONS
[0001] This application claims the benefit of provisional applications
serial Nos. 60/174,330, filed Jan. 4, 2000; and 60/220,681, filed
Jul. 25, 2000.
FIELD OF THE INVENTION
[0002] This invention relates to methods of preparing antibiotics,
and more particularly to a new method for the crystallization of
azithromycin dihydrate.
BACKGROUND OF THE INVENTION
[0003] Azithromycin, 9-deoxo-9a-aza-9a-methyl-9a-homoerythromycin
A, has the structural formula 1
[0004] and is a semi-synthetic macrolide antibiotic related to
erythromycin A. Azithromycin possesses broad-antibacterial activity,
and is useful for treating infections caused by susceptible microorganisms.
[0005] U.S. Pat. Nos. 4,517,359 and 4,474,768 describe methods
for the preparation of azithromycin. According to European Patent
Application EP 298 650 ("the EP '650 application"), the
azithromycin obtained by the methods of U.S. Pat. Nos. 4,517,359
and 4,474,768 is a hygroscopic monohydrate. Because of its hygroscopic
nature, the azithromyycin monohydrate is difficult to prepare and
maintain in a form having a constant, reproducible water-content,
and is particularly difficult to handle during formulation. The
EP '650 application describes a dihydrate form of azithromycin that
is less hygroscopic than the previously known azithromycin monohydrate.
The method described in the EP '650 application for making the dihydrate
form from the monohydrate is by crystallization from tetrahydrofuran,
hexane and water. It would be advantageous to be able to manyfacture
azithromycin dihydrate by a process which uses less potentially
toxic solvents.
[0006] Chinese Patent Application CN 1,093,370 ("the Chinese
'370 application") describes an azithromycin crystal having
water content of 4-6% and is characterized therein as being less
hygroscopic than the dihydrate described in the EP '650 application.
The method disclosed in the Chinese '370 application for making
the described form of azithromycin is by crystallization from acetone
and water.
[0007] A solvent system of acetone and water is also described
in the European Patent application 941,999 wherein azithromycin
dihydrate is precipitated from the acid salt by the addition of
base. It is known from the relevant literature that azithromycin
is not stable under acidic conditions and therefore potential undesirable
impurities may be obtained by the precipitation method described
by the EP '999 application.
[0008] Thus, there remains a need for a method of making azithromycin
dihydrate in high yields directly from crude azithromycin (without
the need to first isolate the monohydrate), under non-acidic conditions
which does not necessitate the use of solvent which have potential
toxicity problems in the production of pharmaceutical products.
[0009] By conventional methods of manufacture, azithromycin may
contain isomers of azithromycin in about 0.5% to about 1%. It would
be advantageous to have a method of removing possible isomers from
azithromycin such that the purity of azithromycin dihydrate may
be enhanced.
[0010] By conventional methods of manufacture, azithromycin may
contain an impurity which is a derivative of azithromycin. It would
be advantageous to have a method of making azithromycin which is
substantially free of impurities that are derivatives of azithromycin.
SUMMARY OF THE INVENTION
[0011] The present invention relates to a process for making azithromycin
dihydrate, comprising the steps of: (a) dissolving azithromycin
in acetone; (b) maintaining the solution of azithromycin and acetone
temperature of about 20.degree. C. to about 25.degree. C.; (c) adding
water in two separate sequential additions, a first addition of
water and a second addition of water; (d) adding water in the second
addition step at a rate of up to 0.2 volumes of water per volume
of acetone per hour; and (e) isolating the crystals of azithromycin
dihydrate. Preferably, between about 0.4 to about 0.5 volumes of
water per volume of water are added in the first addition of water.
Preferably, the first addition of the water occurs over about 2
to about 3 hours. Preferably, the solution formed after the first
addition of water is stirred for about 4 hours prior to the second
addition of water. Preferably, the isolated azithromycin dihydrate
contains less than 0.1% of isomers of azithromycin. More preferably,
the isolated azithromycin dihydrate contains less than about 0.05
to about 0.02% of isomers of azithromycin. Most preferably, the
isolated azithromycin dihydrate is substantially free of isomers
of azithromycin.
[0012] The present invention relates to a method of making azithromycin
from desmethyl-azithromycin comprising the steps of: (a) dissolving
desmethyl-azithromycin in acetone; (b) refluxing the desmethyl-azithromycin
acetone solution; (c) adding formaldehyde; (d) adding formic acid;
(e) adding activated carbon; (f) adding sodium hydroxide to induce
precipitation of azithromycin; and isolating azithromycin. Preferably,
the isolated azithromycin is substantially free of derivatives of
azithromycin.
[0013] The methods of the present invention are thus useful for
the manufacture of azithromycin dihydrate in high yield and purity.
DETAILED DESCRIPTION OF THE INVENTION
[0014] The present invention provides new processes for the manufacture
of azithromycin dihydrate wherein azithromycin dihydrate is made
directly from crude azithromycin, under non-acidic conditions in
unexpectedly high yields. Azithromycin for use as a starting material
in the presently claimed method may be prepared according to the
methods set forth in U.S. Pat. Nos. 4,517,359 and 4,474,768, the
contents of which are incorporated herein by reference.
[0015] It has been discovered that in making azithromycin dihydrate
by crystallization from acetone and water, that both (i) the temperature
for the addition of water to a solution of acetone and azithromycin,
and (ii) the addition profile for water during the precipitation
process are essential. Further, it has been discovered that the
present process for making azithromycin dihydrate, the purity of
azithromycin is enhanced by the removal of isomers of azithromycin
that may be present in the starting material.
[0016] Specifically, it has been discovered that for the precipitation
of azithromycin dihydrate from acetone and water, the optimal temperature
for addition of the water is from about 20.degree. C. to about 25.degree.
C.; and that prior to precipitation of azithromycin dihydrate, about
0.4 to about 0.5 volumes of water to about 1 volume of acetone are
added to the acetone solution over a time period of at least 2 hours.
Additional water should be added only after definite crystals of
azithromycin dihydrate are observed. The addition profile for water
includes two separate sequential additions of water, a first addition
of water, and a second addition of water. The final ratio of acetone:water
should about 0.5 to about 1.5, preferably, not less than 1:1.
[0017] By the process of the present invention, azithromycin is
dissolved in acetone. The temperature of the azithromycin solution
is maintained at a range of about 20.degree. C. to about 25.degree.
C. Preferably, the temperature is maintained at about 20.degree.
C. In the first addition of water to the acithromycin solution,
water is added to the azithromycin solution with stirring such that
crystallization of the azithromycin begins and a suspension is formed.
The azithromycin solution formed following the first addition of
water is stirred for at least two hours, preferably the reaction
is stirred for about 2 to about 3 hours. Preferably, during the
first addition of water, about 0.4 to about 0.5 volumes of water
are added per volume of acetone to induce formation of a suspension.
The resulting suspension is stirred until definite crystals of azithromycin
dihydrate are observed and before any additional water is added.
Preferably, the suspension which forms after the first addition
of water is stirred for about 4 hours before additional water is
added. After the suspension is formed, there is a second addition
of water wherein water is added to complete the formation of azithromycin
dihydrate crystals at a rate of up to 0.2 volumes of water per volume
of acetone per hour after the suspension is formed. Azithromycin
dihydrate is isolated by filtration followed by drying. The present
method provides for high isolated yields of azithromycin dihydrate
of greater than 90%.
[0018] The addition profile of water of the present invention provides
for the formation of pure azithromycin dihydrate substantially free
of azithromycin monohydrate. The unique temperature range maintained
by the present invention prevents formation of azithromycin monohydrate
which would occur at temperatures of greater than 35.degree. C.
Additionally, the unique addition rate of water of the present invention
ensures the formation of azithromycin dihydrate in contrast to where
the addition rate is less than 2 hours, which yields azithromycin
monohydrate. Further, the methods of the present invention provides
for a final ratio of acetone to water of not less than 1:1 which
provides for high yields of azithromycin dihydrate crystals.
[0019] Azithromycin used as the starting material for the present
invention may contain isomers of azithromycin in the amount of about
0.5% to about 1%. The methods of the present invention for making
azithromycin dihydrate further purify the azithromycin by reducing
the present of isomers of azithromycin in the isolated azithromycin
dihydrate. Preferably, the isomers of azithromycin in the isolated
azithromycin dihydrate are present in less than about 0.1%. More
preferably, the isomers of azithromycin in the isolated azithromycin
dihydrate are present in less than about 0.05% to about 0.02%. Most
preferably, the isolated azithromycin dihydrate is substantially
free of isomers of azithromycin dihydrate.
[0020] The present invention provides new processes for the manufacture
of azithromycin from desmethyl-azithromycin. Desmethyl-azithromycin
is also referred to in the art as 11-aza-10-deoxo-dihydroerythromycin
A. Desmethyl-azithromycin for use as a starting material in the
presently claimed method may be prepared according to the methods
set forth in U.S. Pat. No. 4,517,359, the contents of which are
incorporated herein by reference.
[0021] It has been discovered that azithromycin may contain an
impurity which is a derivative of azithromycin. The present invention
provides methods for the manufacture of azithromycin from desmethyl-azithromycin
in which the resulting azithromycin is substantially free of impurities
which are azithromycin derivatives.
[0022] By the methods of the present invention, desmethyl-azithromycin
is dissolved in acetone. Formaldehyde and formic acid are added
to the solution and the clear solution is heated to reflux (.about.58.degree.
C.). The mixture is maintained under reflux for about 3 hours then
cooled to less than about 40.degree. C. Water is added and the acetone
is separated from the reaction mixture by distillation under low
vacuum (.about.300 mbar). The distillation is stopped when the temperature
of the liquid phase reaches .about.40.degree. C./300 mbar. Activated
carbon SXI is added and the suspension is mixed for about 1 hour.
The activated carbon is then separated from the solution by filtration
on a Buchner filter containing Hyflow. The filter cake is washed
with water. The pH is adjusted with an NaOH to about 10-10.5 to
induce precipitation of azithromycin. The azithromycin suspension
is stirred for about 1 hour. The crude azithromycin crude is separated
by filtration and washed. Azithromycin is isolated upon drying the
filtrate 40.degree. C. in a vacuum oven. Preferably the azithromycin
is dried for at least 24 hours. No impurities were detected that
were derivatives of azithromycin in the isolated azithromycin Azithromycin
dihydrate prepared in accordance with the present invention is suitable
formulation and administration for the treatment of susceptible
bacterial infections in humans according to the methods and in the
amounts set forth in U.S. Pat. No. 4,474,768, cited above.
[0023] This invention will be better understood from the Example
that follows. However, the example illustrates, but does not limit,
the invention. Those skilled in the art will readily appreciate
that the specific methods and results discussed are merely illustrative
of the invention as described more fully in the claims that follow
thereafter.
EXAMPLES
Example 1Preparation of azithromycin dihydrate
[0024] Crude azithromycin, 50 g, was dissolved in 250 mL of acetone
at 20.degree. C. Water (100 mL) was added at 20.degree. C. over
a period of 3 hours. The addition of water was stopped and the solution
was mixed for 4 hours. During this time interval the initial turbidity
of the solution is transformed into a clear defined suspension.
Water (150 mL) was added at 20.degree. C. over a period of 3 hours.
After drying, 45.65 g of azithromycin dihydrate was obtained with
a yield of 91.3% based on weight.
Example 2Preparation of azithromycin from Desmethyl-azithromycin
[0025] In a 0.25 L three-necked round bottom flask equipped with
a mechanical stirrer, a condenser and thermometer, 25 g of desmethyl-azithromycin
was dissolved in 102 mL of acetone. Formaldehyde (5.3 mL) and formic
acid (2.6 mL) were added and the clear solution was heated to reflux
(.about.58.degree. C.). The mixture was maintained under reflux
for 3 hours then cooled to less than 40.degree. C. and 102 mL of
water was added. The acetone was separated from the reaction mixture
by distillation under low vacuum (.about.300 mbar). The distillation
was stopped when the temperature of the liquid phase reaches .about.40.degree.
C./300 mbar. Activated carbon SXI (1.25 g) was added and the suspension
was mixed for 1 hour. Then the activated carbon was separated from
the solution by filtration on a Buchner filter containing Hyflow.
The filter cake was washed with 102 mL of water. The pH was adjusted
with an NaOH solution of 47% to 10-10.5 (.about.3.14 g). A massive
precipitation of Azithromycin was observed. After stirring the suspension
for 1 hour, the crude azithromycin was separated by filtration,
washed twice with 25 mL of water and dried at 40.degree. C. in a
vacuum oven for>24 hours. After drying, 19.7 g of crude azithromycin
was obtained (yield 77% based on weight). No impurities that were
derivatives of azithromycin were detected.
Example 3Preparation of azithromycin monohydrate
[0026] Crude azithromycin (10 g) was dissolved in 50 mL of acetone
at 20.degree. C. Water (10 ml) was added at 20.degree. C. over 1
hour. The addition of water was stopped and the solution was heated
to 40.degree. C. and maintained at 40.degree. C. for about a half
hour. Over a 2 hour time period, 20 mL of water was added at 40.degree.
C. During the addition of water the precipitation of azithromycin
monohydrate started. An additional 20 mL of water was added during
the next half-hour. The suspension was cooled over 11/2 hours to
20.degree. C. After filtration and drying, 9.38 g of azithromycin
monohydrate was obtained. No azithromycin dihydrate was observed.
[0027] Although certain presently preferred embodiments of the
invention have been described herein, it will be apparent to those
skilled in the art to which the invention pertains that variations
and modifications of the described embodiments may be made without
departing from the spirit and scope of the invention. Accordingly,
it is intended that the invention be limited only to the extent
required by the appended claims and the applicable rules of law. |