CA1057661A - Pharmaceutical compositions comprising substituted 4,6-dihydroxy-2h-pyran-2-ones - Google Patents
Pharmaceutical compositions comprising substituted 4,6-dihydroxy-2h-pyran-2-onesInfo
- Publication number
- CA1057661A CA1057661A CA239,152A CA239152A CA1057661A CA 1057661 A CA1057661 A CA 1057661A CA 239152 A CA239152 A CA 239152A CA 1057661 A CA1057661 A CA 1057661A
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- CA
- Canada
- Prior art keywords
- pharmaceutical composition
- composition according
- pyran
- dihydroxy
- pharmaceutical
- Prior art date
- Legal status (The legal status is an assumption and is not a legal conclusion. Google has not performed a legal analysis and makes no representation as to the accuracy of the status listed.)
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Classifications
-
- C—CHEMISTRY; METALLURGY
- C07—ORGANIC CHEMISTRY
- C07D—HETEROCYCLIC COMPOUNDS
- C07D309/00—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only ring hetero atom, not condensed with other rings
- C07D309/34—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only ring hetero atom, not condensed with other rings having three or more double bonds between ring members or between ring members and non-ring members
- C07D309/36—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only ring hetero atom, not condensed with other rings having three or more double bonds between ring members or between ring members and non-ring members with oxygen atoms directly attached to ring carbon atoms
- C07D309/38—Heterocyclic compounds containing six-membered rings having one oxygen atom as the only ring hetero atom, not condensed with other rings having three or more double bonds between ring members or between ring members and non-ring members with oxygen atoms directly attached to ring carbon atoms one oxygen atom in position 2 or 4, e.g. pyrones
Abstract
ABSTRACT OF THE DISCLOSURE
Pharmaceutical compositions comprising a substituted 4,6-dihydroxy-2H-pyran-2-one and methods of inhibiting the antigen-antibody reaction by administering said compositions.
Pharmaceutical compositions comprising a substituted 4,6-dihydroxy-2H-pyran-2-one and methods of inhibiting the antigen-antibody reaction by administering said compositions.
Description
~ ~57~
l Thi~ invention relates to novel pharmaceutical compositions which inhibit certain antigen-antibody re-actions and to methods of inhibiting such antigen-antibody reactions by administering ~aid compositions. More ~pecifi-S cally3 the compositions of this invention comprise a sub stituted 496-dihydroxy-2H-pyran-2-one as the active , medlcamentO
: The novel pharmaceutlcal compositions of this in~
, .
; vention comprise a nontoxic pharmaceutical carrier or : ;.
diluent and a substituted 4,6-dihydroxy-2H-pyran-2-one of the following general structural formula: `:
. HO O ~` ;
1 5 ' '' "~~ FORMULA I ~ `
`i wherein R represents lo~er alkyl9 straight or branched :~
chaing of from l to 6 carbon atoms9 the R9s being identical. ~ :~
: Advantageously the compositions of this inventlon comprise a compound of ~ormula I above when R is methyl.
The compounds of formula I are generally prepared by the reaction of acetonedicarboxylic acid and an appro- ` :
i1 priate acid anhydride of the formula ~RCO)209 where R is as defined above. The reacta~ts are usually heated in . ~I
i, 25 sulfuric acid at an elevated temperat~re up to about 90C.
~¦ The compositions of thls invention inhibit thP.
release 2nd/or formation of pharmacologically active media- ;
tors from effector cells triggered by the ~nteraction of :
;.1 an~igen and a specific antibody fixed to the cell surface~
:~ 30 Thus the compositions are valuable in the treatment of '~ ~
:~ allergic diseases ~uch as asthma9 rhinitis and urticaria. :~
l Thi~ invention relates to novel pharmaceutical compositions which inhibit certain antigen-antibody re-actions and to methods of inhibiting such antigen-antibody reactions by administering ~aid compositions. More ~pecifi-S cally3 the compositions of this invention comprise a sub stituted 496-dihydroxy-2H-pyran-2-one as the active , medlcamentO
: The novel pharmaceutlcal compositions of this in~
, .
; vention comprise a nontoxic pharmaceutical carrier or : ;.
diluent and a substituted 4,6-dihydroxy-2H-pyran-2-one of the following general structural formula: `:
. HO O ~` ;
1 5 ' '' "~~ FORMULA I ~ `
`i wherein R represents lo~er alkyl9 straight or branched :~
chaing of from l to 6 carbon atoms9 the R9s being identical. ~ :~
: Advantageously the compositions of this inventlon comprise a compound of ~ormula I above when R is methyl.
The compounds of formula I are generally prepared by the reaction of acetonedicarboxylic acid and an appro- ` :
i1 priate acid anhydride of the formula ~RCO)209 where R is as defined above. The reacta~ts are usually heated in . ~I
i, 25 sulfuric acid at an elevated temperat~re up to about 90C.
~¦ The compositions of thls invention inhibit thP.
release 2nd/or formation of pharmacologically active media- ;
tors from effector cells triggered by the ~nteraction of :
;.1 an~igen and a specific antibody fixed to the cell surface~
:~ 30 Thus the compositions are valuable in the treatment of '~ ~
:~ allergic diseases ~uch as asthma9 rhinitis and urticaria. :~
2 -.
~ ~5'~
1 The inhibitory ac~ivity of the compositions oE
this invention on mediator release in sensitized tissues is measured by the ability of the active medicament to inhibît the passive cutaneous anaphylaxis (PCA`~ reaction S in rats. In this test system~ titered and approprlately ; diluted serum (from rats previously immunlzed by the intra~
-~ peritoneal injection of oval~umlnaluminum hydxo~ide or ovalbumin-i.m.-Bordatella pertussls ~SOPo i.p.~and N.
Brasiliensis i.p~ containing reagînic antibodies directed `~
against ovalbumin is injected intradermally at four sites on ~he shaved backs of normal adult male rats. Forty-eight .. .
hours later the anlmals are injected intravenously with 0.5 ml. of isotonic saline solution containing 5 mg. of the ovalbumin antigen and 5 mg. of Evans blue dye. Chemi~
15 cal mediators such as histamine and serotonin which are~
released at the sensitized sites as a result of a local cellular anaphylaxis9 cause an increase in capillary per~
li~ meability with resultant leakage of plasma and formation of a wheal~ The wheal is visualized by the plssma protein-~, 20 bound Evans blue dye. Under condition~ of the test~ the average control wheal is approximately 12x12 mmO Thirty ,;1 minutes following antigen challengeg the animalfq are Icilled~
l the dorsal skin i9 reflected and the diameter of the wheals 1l~ recor~ed. A test compound is administered intravenouslyg `1 25 initially at 0.5 min~tes prior to antigen challenge ~longer pretreatment times and other routes of drug administration9 i.e. oral or intraperitoneal 9 may be employed)O Percent ¦ inhibition is calculated from the dif~erence in mean aver-¦ age wheal diameter between a treated group and saline or :., 30 appropriate diluent controls. ;
~ ~ 3 ~
;'". ' ' .. . - . : :
~0576~
l The compounds o~ ormula I administered in~ra-venously to rats at doses of from S to 15 mg/kg produce marked inhibition of the PCA reaction. A preferred com-pound9 3~5-diacetyl-496-dihydroxy-2H-pyran-~-one~ produced ;
62% inhibitlon of the rat PCA wheal at 15 mg/kg l.v. ~n testing for mechanism of action9 the compounds of formula I
were found not to provide comparable inhibition of wheals of approximately equal ~everity produced in rats by the intracutaneous administration of hi~tamine and serotonin following i,v. administration o~ the test compound at the same dose an~ pretreatment time which exhibited slgnificant inhibition of the rat 48 hour PCA reaction.
Upon oral administration~ 395-diacetyl~496-dihy-droxy-2H~pyran-2-one produced 83% inhibition in the rat 48 hour PGA system at 150 mg/kg and a pretreatment time of .
15 minutes. This compound is also active in vitro for inhibition of antigen induced mediator release from monkey ~ , . . .
~ ~5'~
1 The inhibitory ac~ivity of the compositions oE
this invention on mediator release in sensitized tissues is measured by the ability of the active medicament to inhibît the passive cutaneous anaphylaxis (PCA`~ reaction S in rats. In this test system~ titered and approprlately ; diluted serum (from rats previously immunlzed by the intra~
-~ peritoneal injection of oval~umlnaluminum hydxo~ide or ovalbumin-i.m.-Bordatella pertussls ~SOPo i.p.~and N.
Brasiliensis i.p~ containing reagînic antibodies directed `~
against ovalbumin is injected intradermally at four sites on ~he shaved backs of normal adult male rats. Forty-eight .. .
hours later the anlmals are injected intravenously with 0.5 ml. of isotonic saline solution containing 5 mg. of the ovalbumin antigen and 5 mg. of Evans blue dye. Chemi~
15 cal mediators such as histamine and serotonin which are~
released at the sensitized sites as a result of a local cellular anaphylaxis9 cause an increase in capillary per~
li~ meability with resultant leakage of plasma and formation of a wheal~ The wheal is visualized by the plssma protein-~, 20 bound Evans blue dye. Under condition~ of the test~ the average control wheal is approximately 12x12 mmO Thirty ,;1 minutes following antigen challengeg the animalfq are Icilled~
l the dorsal skin i9 reflected and the diameter of the wheals 1l~ recor~ed. A test compound is administered intravenouslyg `1 25 initially at 0.5 min~tes prior to antigen challenge ~longer pretreatment times and other routes of drug administration9 i.e. oral or intraperitoneal 9 may be employed)O Percent ¦ inhibition is calculated from the dif~erence in mean aver-¦ age wheal diameter between a treated group and saline or :., 30 appropriate diluent controls. ;
~ ~ 3 ~
;'". ' ' .. . - . : :
~0576~
l The compounds o~ ormula I administered in~ra-venously to rats at doses of from S to 15 mg/kg produce marked inhibition of the PCA reaction. A preferred com-pound9 3~5-diacetyl-496-dihydroxy-2H-pyran-~-one~ produced ;
62% inhibitlon of the rat PCA wheal at 15 mg/kg l.v. ~n testing for mechanism of action9 the compounds of formula I
were found not to provide comparable inhibition of wheals of approximately equal ~everity produced in rats by the intracutaneous administration of hi~tamine and serotonin following i,v. administration o~ the test compound at the same dose an~ pretreatment time which exhibited slgnificant inhibition of the rat 48 hour PCA reaction.
Upon oral administration~ 395-diacetyl~496-dihy-droxy-2H~pyran-2-one produced 83% inhibition in the rat 48 hour PGA system at 150 mg/kg and a pretreatment time of .
15 minutes. This compound is also active in vitro for inhibition of antigen induced mediator release from monkey ~ , . . .
-3~ lung and skin and rat lung sys~ems at concentrations of - ;
1.2 x lV 3M to 5.9 x 10 4M.
,~ 20 The pharmaceutical compositions of this invention ~ ~`
, comprise an appropriate amount of a substituted 4~6-dihydroxy-¦ 2H-pyran-2-one as set forth in formula I in as~ociation with a pharm~ceutical carrier or diluent. ~le nature of 3 the composition and the pharmaceutical carrier or diluent will o course depend upon the intended rnute of adminis '1 tratio~9 L.e. orally~ parenterally or by inhalation. Pre-l, ferably the active medicament is administered to an animal i in a compo~ition comprising an amount sufficien~ to produce an inhibition of the antigen antibody reaction. When em~
ployed in ~his manner~ the dosage o~ compoæitivn is such ~ .
: I
~ ~7 6 ~ ~
l that from 25 mg. to 750 mg. of active ingredient are administered ~t each adminis~ration Advan~ageous1~ ~ual doses will be administered l to 4 times daily wlth the daily dosage regimen belng about ~5 mg. to about 3000 mg.
In generalg particularly for the prophylactic `~ treatment of asthma9 the compositions wll~ be in a form suitable for administration by ~nhalation. Thus the compo-sitions will comprise a suspenslon or solution of the active ingredient in water for administration ~y means of a CO''l-ventional nebulizer. Alternatively the compositions will comprise a suspension or solution of the active ingredient in a conventional liqui~ied propellant such as dichlorodi-fluoromethane or chlorotrifluoroethane to be administered from a pressurized container. The compositions may also ; .
lS comprise the solid active ingredient diluted with a solid diluent, e.g. lactose, for administration from a powder -inhalatio~ device. In the above compositions 9 the amount of carrier or dLluent will vary but preferably will be the major proportion of a suspension or solution o the active ingredient. When the diluent is a solid9 it may be present in less~ equal or greater amoun~s than the solid active ingredient.
A wide variety of other pharmaceutical forms can be employedO Thus9 if a solid carrier is used the ;l 25 preparation ca~ be tableted9 placed in a hard gelatin cap~
I sule in powder or pellet form9 or in the form o a troche ;~
.~ , . ~.
-i or lozenge for oral administration. The amoun~ o~ solid ~ carrier will vary t~idely but preferably will be about 25 mg.
;~ to about l g. If a liquid carrier is u~ed9 ~he preparation ~ 30 will be in the form of a syrup9 emulsion, so~t gelatin cap-.~ ! .
' ' '` ~'' ~"
.' ' .
l sule, sterile injectable liquid such as an ampul~ or an :~
aqueous or nonaqueous liquid suspension. ~ ~
Exemplary of solid carriers are lactose~ terra ~ :
alba~ sucrose~ talc3 gelatin9 agar~ pectln~ acacia9 magnes~
ium stearate9 stearic acid and the like. Exemplary o~
liquid carriers are syrup9 peanut oilg olive oil9 water :.
. and the likei. Similarly the carrier or diluent can include any time delay material well known to the art 9 such as glyceryl monDstearate or glyceryl distearate ala~e or with 0 a wax. ~ ~
`~ The method in accordance with this invention also ..
includes inhibiting the efects of the antigen-antibody reaction which comprises the prior application ~o the area l of ~he iantigen-antibody mechanism a therapeu~ically ~, 15 effective amount of a substituted 4,6-dihydroxy-2H-pyran- ;
:l 2-one as defined in foxmula I. A particular application is I a method or relieving or preventing allergic airway ~ :
¦: obætruction which comprises administering to an animal a the~apeutically ~ectiv~i amount at suitable i~tervals.
~ The pharmaceutical preparations are made follow- ~;
~,~ ing the conventional techniques o the pharmaceutical chem-I ist involving mixi~g~ granulating and compressing when necessary, or variously mixing and disso~ving the ingredi-~, enits as appropriate to the desired end produc~
~ $ The accompanying examples illustrate the prepara~
:~ tion of compounds of ormula I and their incorporation into 1 pharmaceutical compoæitions o~ this:invention and as such ~, ~: are not ~o be considered as limiting the invention set :
; forth in the claims appended here~o.
, - 6 - ~
,,'i: :.
~0S76~
1 Kiang~ A. K. et al. J. Chem. Soc. ~c3 pp. 2721-6 (1971) have questioned the structure assigned by previous authors such as Wiley~ R. H. et al. ~ 21:686-688 (1956) to the reaction product of acetonedicarboxylic acid and acetic anhydride.9 designated 5-carboxydehydro-acetic acid. Thusg Kiang et al. supra reported that the reaction of acetonedicarboxylic acid with acetic anhydride gave the compound of structure IIo -OH ` ;~
CH3CO ~ X 3 FORMULA II
M. Mamike et al.g J. Org _5~ Japan 25:472-6 (1951) and C. A. Salemink~ Rec. Trav. Chim. 80 422-30 (1961) have also reported "2-pyrone-5-carboxylic acids".
Upon investigation which has included l3C nucl~a~
ma~netic resonance spectral studies~ we have concluded that the reaction of acetonedicarboxylic acid with acetic anhydrlde gives a product having the ~automeric structure as shown b~low:
CH3~ ~ C~,H CH3/C ~ c\c CH /C ~ C~C
~5 HO O ~o O OH
For convenience this product~ designated herein as 3~5-diacetyl-4,6-dihydroxy-2H-pyran-2-one~ and the analogous , . products from reaction with other acid anhydrides are , ~
j represented by formula I above. ThiS agrees with Kiang ~l 30 e~ al's gross structure indicated by form~la II~ The :
) .~ .
. 7 :.
~L~)5'76~
l rate of tautomerization represented by ~ is afected~
among other factors~ by ~he sol~ent used in the 13C spectral study.
~EXA~LE 1 To a mixture o~ 12050 g~ ~116 ml~g 1~2 mO~ of ~, acetic anhydride and 5 mlO of concentra~ed sulfuric acidat 10-20Co is added slowly 36,5 gO ~0025 m.~ o~ acetonedi~
carboxylic acid. The resulting mix~ure is heated on a ~team bath at 90-95C. for 30 m~nutes and then poured into about 500 ml. of ice-water. The solid removed by filtration and r recrystallized from benzene to give 39S-dlacetyl-496-dihy-droxy-2H~pyran-2~one9 mJpu 153~155Co Acetonedicarboxylic acid ~703 gO 9 0005 m.) i9 added 510wly to 32.1 ml. (3205 g.g 0025 m,) of propionic . j .
j anhydride with 1 mlO of concentrated sulfuric acid at 10-20C.~ me resulting mi~:ture is heated on a Bteam bath at 90~95~C0 or~ 45~minutes and then poured into about 100 ml. of ice-waterO The solld is ~iltered and recry~
.1 ~
~ 20 stall~zed from methanol to yield 3D5-bis~propionyl)~4D6-.1 dihydroxy-2H pyran-2~oneD m~pO 114-115Co ~ ~, i, To a mixture of 39,55 g, (0.25 m.) of n-butyric ;!: anhydride with 1 ml, o concentrated sulfuri:c acid at , 25 10-20C. is added 910wly 7~3 gO ~0005 m.) of acetonedicax~
.. ~.
! boxylic acid and the resulting mixture i~ heated on a steam ~1 - , . . : . , '~ ' bath at 90-95C0 ~or one~hour. The reaction mix~ure is poured into ice-water9 the solid is fileered and recry-stallized from methanol to ~urnish 395-bis(butyryL)~496-dihydroxy-2H-pyran-2-one9 mOp~ 80~82C~
. : , , ~ - 8 ~ ~
.
~5'7~
}~`
~X~*PLE 4 Following the procedure of Example 1~ acetonedi~
carboxyllc acid ~703 gO 9 0~05 mO 3 i5 addP.d s13wly to 46c6 gO
~0.25 mO ) o n~valeric anhydri.de with 1 mlO of concentrated sul~uric acid at 10~20~C~ The resultlng mixture i~ heated -on a ~team ba~h at 90-95Co ~or one hour and then po~red into ice~water. The fil~red solid is recrystallized ~rom methanol to give 395-bis~valer~1~-4~6~dihydro~y;2H~pyran-2 one~ m.pO 84-85G~
EY~ E 5 To a mixture of 53~6 gO ~00~5 ~.~ of n~heganoic anhydride with 1 mlO of concen~rated sulfuric acld at 10-20Co i~ added slowly 703 gO (0005 m. ) of acetonedicar-~: 15 boxylic acid and the resulting mixture is heated on a ~team `~
bath for 30 minutes. The reac~ion mixture is poured in~o ice~water9 filtered and the ~olid recrystallized from : methanol to yield 3~5 bis~hexanoyl)-4 9 6~dihydroxy-2H;-pyran~ 2~0ne9 m~p~ 87~88C.
!: 20 : Simi-larly9 reaction of 65.5 g~ (7004 ml.9 0025 mO~
of n-hep~anoic anhydride with acetonedicarboxylic acid as described above gives the corresponding product 3~5~;bis~
eptanoyl)-496-dihydroxy-2H~pyran~2~one9 m.p~ 88~90Co `~;
~i As a specific embodiment o~ a useful composition of thi~ inventionD an active i~gredient such as 395~bis~
(hexanoyl~ 496-dihydroxy-2H~pyran-2~one i8 dissolved in :
~i sterile water at a concentra~ion of 0~5% aerosolized from ~ a nebulizer operating a~ an aîr ~low adjusted to deliver ;~
`j the desir2d aerosolized weight of drug.
For oral administra~ion9 composi~ions such as those in the following examples can be preparedO ~
~ :
~57~1~61 let 35,5-diacetyl~45,6-dihydroxy~2H~ 25 pyran-2~one Calcium sulfate9 dihydra~e 12S
S
Sucrose ~5 Starch 15 ' Talc 5 Stearic acid 3 ~ ~
10The sucrose~ calcium sulfate and the active ingredient are: ~;
~, thoroughly mi~ed and granulated wi~h hot ~0% gelatin solu--tion~ The wetted mass is passed through a ~6 mesh screen ~ :
directly onto dryi~g trays. me granules are dried at ~::
'! 120F, and passed through a #20 me~h screen9 mixed with i 15the starch~ talc and stearic acid9 and compressed into :' tablets~
.~
l ~ , il~ 3 9 5:-diacetyl-4 9 6-dihydroxy-2~I~ 100 pyran~2-one : 20 Magnesium stearate ~ 5 Lactose 300 The above ingredients are screened through a ~40 mesh ~ screen9 mixed and illed into ~tO hard gelatin cap~ulesO
;1 , ' -~ :.
.' . .
', .
~ - 10 ~
~, ~
, :
1.2 x lV 3M to 5.9 x 10 4M.
,~ 20 The pharmaceutical compositions of this invention ~ ~`
, comprise an appropriate amount of a substituted 4~6-dihydroxy-¦ 2H-pyran-2-one as set forth in formula I in as~ociation with a pharm~ceutical carrier or diluent. ~le nature of 3 the composition and the pharmaceutical carrier or diluent will o course depend upon the intended rnute of adminis '1 tratio~9 L.e. orally~ parenterally or by inhalation. Pre-l, ferably the active medicament is administered to an animal i in a compo~ition comprising an amount sufficien~ to produce an inhibition of the antigen antibody reaction. When em~
ployed in ~his manner~ the dosage o~ compoæitivn is such ~ .
: I
~ ~7 6 ~ ~
l that from 25 mg. to 750 mg. of active ingredient are administered ~t each adminis~ration Advan~ageous1~ ~ual doses will be administered l to 4 times daily wlth the daily dosage regimen belng about ~5 mg. to about 3000 mg.
In generalg particularly for the prophylactic `~ treatment of asthma9 the compositions wll~ be in a form suitable for administration by ~nhalation. Thus the compo-sitions will comprise a suspenslon or solution of the active ingredient in water for administration ~y means of a CO''l-ventional nebulizer. Alternatively the compositions will comprise a suspension or solution of the active ingredient in a conventional liqui~ied propellant such as dichlorodi-fluoromethane or chlorotrifluoroethane to be administered from a pressurized container. The compositions may also ; .
lS comprise the solid active ingredient diluted with a solid diluent, e.g. lactose, for administration from a powder -inhalatio~ device. In the above compositions 9 the amount of carrier or dLluent will vary but preferably will be the major proportion of a suspension or solution o the active ingredient. When the diluent is a solid9 it may be present in less~ equal or greater amoun~s than the solid active ingredient.
A wide variety of other pharmaceutical forms can be employedO Thus9 if a solid carrier is used the ;l 25 preparation ca~ be tableted9 placed in a hard gelatin cap~
I sule in powder or pellet form9 or in the form o a troche ;~
.~ , . ~.
-i or lozenge for oral administration. The amoun~ o~ solid ~ carrier will vary t~idely but preferably will be about 25 mg.
;~ to about l g. If a liquid carrier is u~ed9 ~he preparation ~ 30 will be in the form of a syrup9 emulsion, so~t gelatin cap-.~ ! .
' ' '` ~'' ~"
.' ' .
l sule, sterile injectable liquid such as an ampul~ or an :~
aqueous or nonaqueous liquid suspension. ~ ~
Exemplary of solid carriers are lactose~ terra ~ :
alba~ sucrose~ talc3 gelatin9 agar~ pectln~ acacia9 magnes~
ium stearate9 stearic acid and the like. Exemplary o~
liquid carriers are syrup9 peanut oilg olive oil9 water :.
. and the likei. Similarly the carrier or diluent can include any time delay material well known to the art 9 such as glyceryl monDstearate or glyceryl distearate ala~e or with 0 a wax. ~ ~
`~ The method in accordance with this invention also ..
includes inhibiting the efects of the antigen-antibody reaction which comprises the prior application ~o the area l of ~he iantigen-antibody mechanism a therapeu~ically ~, 15 effective amount of a substituted 4,6-dihydroxy-2H-pyran- ;
:l 2-one as defined in foxmula I. A particular application is I a method or relieving or preventing allergic airway ~ :
¦: obætruction which comprises administering to an animal a the~apeutically ~ectiv~i amount at suitable i~tervals.
~ The pharmaceutical preparations are made follow- ~;
~,~ ing the conventional techniques o the pharmaceutical chem-I ist involving mixi~g~ granulating and compressing when necessary, or variously mixing and disso~ving the ingredi-~, enits as appropriate to the desired end produc~
~ $ The accompanying examples illustrate the prepara~
:~ tion of compounds of ormula I and their incorporation into 1 pharmaceutical compoæitions o~ this:invention and as such ~, ~: are not ~o be considered as limiting the invention set :
; forth in the claims appended here~o.
, - 6 - ~
,,'i: :.
~0S76~
1 Kiang~ A. K. et al. J. Chem. Soc. ~c3 pp. 2721-6 (1971) have questioned the structure assigned by previous authors such as Wiley~ R. H. et al. ~ 21:686-688 (1956) to the reaction product of acetonedicarboxylic acid and acetic anhydride.9 designated 5-carboxydehydro-acetic acid. Thusg Kiang et al. supra reported that the reaction of acetonedicarboxylic acid with acetic anhydride gave the compound of structure IIo -OH ` ;~
CH3CO ~ X 3 FORMULA II
M. Mamike et al.g J. Org _5~ Japan 25:472-6 (1951) and C. A. Salemink~ Rec. Trav. Chim. 80 422-30 (1961) have also reported "2-pyrone-5-carboxylic acids".
Upon investigation which has included l3C nucl~a~
ma~netic resonance spectral studies~ we have concluded that the reaction of acetonedicarboxylic acid with acetic anhydrlde gives a product having the ~automeric structure as shown b~low:
CH3~ ~ C~,H CH3/C ~ c\c CH /C ~ C~C
~5 HO O ~o O OH
For convenience this product~ designated herein as 3~5-diacetyl-4,6-dihydroxy-2H-pyran-2-one~ and the analogous , . products from reaction with other acid anhydrides are , ~
j represented by formula I above. ThiS agrees with Kiang ~l 30 e~ al's gross structure indicated by form~la II~ The :
) .~ .
. 7 :.
~L~)5'76~
l rate of tautomerization represented by ~ is afected~
among other factors~ by ~he sol~ent used in the 13C spectral study.
~EXA~LE 1 To a mixture o~ 12050 g~ ~116 ml~g 1~2 mO~ of ~, acetic anhydride and 5 mlO of concentra~ed sulfuric acidat 10-20Co is added slowly 36,5 gO ~0025 m.~ o~ acetonedi~
carboxylic acid. The resulting mix~ure is heated on a ~team bath at 90-95C. for 30 m~nutes and then poured into about 500 ml. of ice-water. The solid removed by filtration and r recrystallized from benzene to give 39S-dlacetyl-496-dihy-droxy-2H~pyran-2~one9 mJpu 153~155Co Acetonedicarboxylic acid ~703 gO 9 0005 m.) i9 added 510wly to 32.1 ml. (3205 g.g 0025 m,) of propionic . j .
j anhydride with 1 mlO of concentrated sulfuric acid at 10-20C.~ me resulting mi~:ture is heated on a Bteam bath at 90~95~C0 or~ 45~minutes and then poured into about 100 ml. of ice-waterO The solld is ~iltered and recry~
.1 ~
~ 20 stall~zed from methanol to yield 3D5-bis~propionyl)~4D6-.1 dihydroxy-2H pyran-2~oneD m~pO 114-115Co ~ ~, i, To a mixture of 39,55 g, (0.25 m.) of n-butyric ;!: anhydride with 1 ml, o concentrated sulfuri:c acid at , 25 10-20C. is added 910wly 7~3 gO ~0005 m.) of acetonedicax~
.. ~.
! boxylic acid and the resulting mixture i~ heated on a steam ~1 - , . . : . , '~ ' bath at 90-95C0 ~or one~hour. The reaction mix~ure is poured into ice-water9 the solid is fileered and recry-stallized from methanol to ~urnish 395-bis(butyryL)~496-dihydroxy-2H-pyran-2-one9 mOp~ 80~82C~
. : , , ~ - 8 ~ ~
.
~5'7~
}~`
~X~*PLE 4 Following the procedure of Example 1~ acetonedi~
carboxyllc acid ~703 gO 9 0~05 mO 3 i5 addP.d s13wly to 46c6 gO
~0.25 mO ) o n~valeric anhydri.de with 1 mlO of concentrated sul~uric acid at 10~20~C~ The resultlng mixture i~ heated -on a ~team ba~h at 90-95Co ~or one hour and then po~red into ice~water. The fil~red solid is recrystallized ~rom methanol to give 395-bis~valer~1~-4~6~dihydro~y;2H~pyran-2 one~ m.pO 84-85G~
EY~ E 5 To a mixture of 53~6 gO ~00~5 ~.~ of n~heganoic anhydride with 1 mlO of concen~rated sulfuric acld at 10-20Co i~ added slowly 703 gO (0005 m. ) of acetonedicar-~: 15 boxylic acid and the resulting mixture is heated on a ~team `~
bath for 30 minutes. The reac~ion mixture is poured in~o ice~water9 filtered and the ~olid recrystallized from : methanol to yield 3~5 bis~hexanoyl)-4 9 6~dihydroxy-2H;-pyran~ 2~0ne9 m~p~ 87~88C.
!: 20 : Simi-larly9 reaction of 65.5 g~ (7004 ml.9 0025 mO~
of n-hep~anoic anhydride with acetonedicarboxylic acid as described above gives the corresponding product 3~5~;bis~
eptanoyl)-496-dihydroxy-2H~pyran~2~one9 m.p~ 88~90Co `~;
~i As a specific embodiment o~ a useful composition of thi~ inventionD an active i~gredient such as 395~bis~
(hexanoyl~ 496-dihydroxy-2H~pyran-2~one i8 dissolved in :
~i sterile water at a concentra~ion of 0~5% aerosolized from ~ a nebulizer operating a~ an aîr ~low adjusted to deliver ;~
`j the desir2d aerosolized weight of drug.
For oral administra~ion9 composi~ions such as those in the following examples can be preparedO ~
~ :
~57~1~61 let 35,5-diacetyl~45,6-dihydroxy~2H~ 25 pyran-2~one Calcium sulfate9 dihydra~e 12S
S
Sucrose ~5 Starch 15 ' Talc 5 Stearic acid 3 ~ ~
10The sucrose~ calcium sulfate and the active ingredient are: ~;
~, thoroughly mi~ed and granulated wi~h hot ~0% gelatin solu--tion~ The wetted mass is passed through a ~6 mesh screen ~ :
directly onto dryi~g trays. me granules are dried at ~::
'! 120F, and passed through a #20 me~h screen9 mixed with i 15the starch~ talc and stearic acid9 and compressed into :' tablets~
.~
l ~ , il~ 3 9 5:-diacetyl-4 9 6-dihydroxy-2~I~ 100 pyran~2-one : 20 Magnesium stearate ~ 5 Lactose 300 The above ingredients are screened through a ~40 mesh ~ screen9 mixed and illed into ~tO hard gelatin cap~ulesO
;1 , ' -~ :.
.' . .
', .
~ - 10 ~
~, ~
, :
Claims (10)
1. A pharmaceutical composition which inhibits the antigen-antibody reaction comprising a pharmaceutical carrier and an effective amount of a chemical compound of the formula:
wherein R is lower alkyl, straight or branched chain, of from 1 to 6 carbon atoms, the R's being identical.
wherein R is lower alkyl, straight or branched chain, of from 1 to 6 carbon atoms, the R's being identical.
2. A pharmaceutical composition according to claim 1 in a form suitable for administration by inhalation.
3. A pharmaceutical composition according to claim 1 comprising a solution or suspension of the active ingredient in sterile water.
4. A pharmaceutical composition according to claim 1 in the form of an aerosol formulation.
5. A pharmaceutical composition according to claim 1 comprising the solid active ingredient diluted with a solid diluent.
6. A pharmaceutical composition according to claim 1 in which R is methyl.
7. A pharmaceutical composition according to claim 1 in which R is n-pentyl.
8. A pharmaceutical composition in dosage unit form comprising a pharmaceutical carrier and a chemical compound of the formula:
wherein R is lower alkyl, straight or branched chain, of from 1 to 6 carbon atoms, the R's being identical, said compound being present in an amount of about 25 mg. to about 750 mg. per dosage unit.
wherein R is lower alkyl, straight or branched chain, of from 1 to 6 carbon atoms, the R's being identical, said compound being present in an amount of about 25 mg. to about 750 mg. per dosage unit.
9, A pharmaceutical composition according to claim 8 in which R is methyl.
10. A pharmaceutical composition according to claim 8 in which R is n-pentyl.
Applications Claiming Priority (1)
| Application Number | Priority Date | Filing Date | Title |
|---|---|---|---|
| US52283774A | 1974-11-11 | 1974-11-11 |
Publications (1)
| Publication Number | Publication Date |
|---|---|
| CA1057661A true CA1057661A (en) | 1979-07-03 |
Family
ID=24082586
Family Applications (1)
| Application Number | Title | Priority Date | Filing Date |
|---|---|---|---|
| CA239,152A Expired CA1057661A (en) | 1974-11-11 | 1975-11-07 | Pharmaceutical compositions comprising substituted 4,6-dihydroxy-2h-pyran-2-ones |
Country Status (8)
| Country | Link |
|---|---|
| AU (1) | AU498774B2 (en) |
| BE (1) | BE835266A (en) |
| CA (1) | CA1057661A (en) |
| DE (1) | DE2550647A1 (en) |
| FR (1) | FR2290197A1 (en) |
| GB (1) | GB1529463A (en) |
| IE (1) | IE43594B1 (en) |
| ZA (1) | ZA757067B (en) |
Families Citing this family (2)
| Publication number | Priority date | Publication date | Assignee | Title |
|---|---|---|---|---|
| US4153720A (en) * | 1978-01-19 | 1979-05-08 | Smithkline Corporation | 3-Acyl-5-alkyl-2H-pyran-2,4,6-(3H,5H)-triones and their 4-hydroxy tautomers |
| DK277585A (en) * | 1984-07-06 | 1986-01-07 | Lonza Ag | STABILIZER MIXTURES FOR VINYL CHLORIDE POLYME MASSES |
-
1975
- 1975-10-13 GB GB41844/75A patent/GB1529463A/en not_active Expired
- 1975-11-04 AU AU86312/75A patent/AU498774B2/en not_active Expired
- 1975-11-05 BE BE161598A patent/BE835266A/en not_active IP Right Cessation
- 1975-11-06 IE IE2423/75A patent/IE43594B1/en unknown
- 1975-11-07 CA CA239,152A patent/CA1057661A/en not_active Expired
- 1975-11-10 ZA ZA757067A patent/ZA757067B/en unknown
- 1975-11-10 FR FR7534306A patent/FR2290197A1/en active Granted
- 1975-11-11 DE DE19752550647 patent/DE2550647A1/en not_active Ceased
Also Published As
| Publication number | Publication date |
|---|---|
| DE2550647A1 (en) | 1976-05-20 |
| AU498774B2 (en) | 1979-03-22 |
| BE835266A (en) | 1976-05-05 |
| FR2290197A1 (en) | 1976-06-04 |
| FR2290197B1 (en) | 1978-07-28 |
| AU8631275A (en) | 1977-05-12 |
| ZA757067B (en) | 1976-11-24 |
| IE43594L (en) | 1976-05-11 |
| IE43594B1 (en) | 1981-04-08 |
| GB1529463A (en) | 1978-10-18 |
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