US3285935A - Indolyl glucuronides - Google Patents

Indolyl glucuronides Download PDF

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US3285935A
US3285935A US296111A US29611163A US3285935A US 3285935 A US3285935 A US 3285935A US 296111 A US296111 A US 296111A US 29611163 A US29611163 A US 29611163A US 3285935 A US3285935 A US 3285935A
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indomethacin
glucuronide
indolyl
glucuronides
methyl
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US296111A
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Robert E Harman
Jr Frederick A Kuehl
Robert G Strachan
Ralph F Hirschmann
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Merck and Co Inc
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Merck and Co Inc
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Priority to US296111A priority Critical patent/US3285935A/en
Priority to GB26807/64A priority patent/GB1061778A/en
Priority to DE19641470072 priority patent/DE1470072A1/en
Priority to DE19641695474 priority patent/DE1695474A1/en
Priority to BE650447D priority patent/BE650447A/xx
Priority to FR1565303D priority patent/FR1565303A/fr
Priority to CH1667767A priority patent/CH451147A/en
Priority to CH941064A priority patent/CH451145A/en
Priority to FR991578A priority patent/FR3930M/fr
Priority to US510999A priority patent/US3375166A/en
Application granted granted Critical
Publication of US3285935A publication Critical patent/US3285935A/en
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    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07DHETEROCYCLIC COMPOUNDS
    • C07D209/00Heterocyclic compounds containing five-membered rings, condensed with other rings, with one nitrogen atom as the only ring hetero atom
    • C07D209/02Heterocyclic compounds containing five-membered rings, condensed with other rings, with one nitrogen atom as the only ring hetero atom condensed with one carbocyclic ring
    • C07D209/04Indoles; Hydrogenated indoles
    • C07D209/10Indoles; Hydrogenated indoles with substituted hydrocarbon radicals attached to carbon atoms of the hetero ring
    • C07D209/18Radicals substituted by carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals
    • C07D209/26Radicals substituted by carbon atoms having three bonds to hetero atoms with at the most one bond to halogen, e.g. ester or nitrile radicals with an acyl radical attached to the ring nitrogen atom
    • C07D209/281-(4-Chlorobenzoyl)-2-methyl-indolyl-3-acetic acid, substituted in position 5 by an oxygen or nitrogen atom; Esters thereof

Definitions

  • This invention relates to new indolyl acid derivatives and to a method for the prolonged localized treatment of inflammation. More specifically, this invention relates to the glucuronides of 1-pchlorobenzoyl-2-methyl-5-rnethoxy-3-indolyl acetic acid and to the lower alkyl esters of per-lower alkanoylated glucuronides of the said indolyl acid. More specifically also, it relatesto a method for the prolonged localized treatment of inflammation which comprises the localized administration of these compounds.
  • carbohydrate derivatives of Indomethacin which are inactive systemically, are transformed in situ by metabolic processes very slowly into Indomethacin with the result that prolonged local treatment of inflammation is possible.
  • carbohydrate derivatives comprise the glucuronide of Indomethacin which is itself the deactivating metabolic product by which Indomethacin is excreted from feces of some species and the alkyl esters of the trialkanoylated glucuronide of Indomethacin, which are preparable either synthetically or from the metabolic product itself.
  • the glucuronide of Indomethacin is the metabolite by which Indomethacin is excreted from some species of animal (other species excrete other derivatives).
  • the glucuronide is treated with diazomethane to produce the corresponding methyl ester and then acetylated there is formed the methyl ester of the triacetylglucuronide of Indomethacin.
  • This same compound can be obtained from bromo triacetylglucuronic acid and the potassium salt of Indomethacin in acetone.
  • diazopropane or diazobutane are used, the corresponding other lower alkyl esters such as the ethyl, propyl and butyl esters are obtained.
  • acylation can be carried out with propionic anhydride, butyric anhydride or the like to produce When diazoethane, I
  • the key to this invention is the presence of an enzyme known as ,B-glucuronidase in mammalian tissue (Bollet, Goodwin, and Brown, J. Clin. Invest, 38, 451, 1959) as well as the presence of other esterases in synovial fluid.
  • an enzyme known as ,B-glucuronidase in mammalian tissue (Bollet, Goodwin, and Brown, J. Clin. Invest, 38, 451, 1958) as well as the presence of other esterases in synovial fluid.
  • systemic administration of the glucuronides alkanoylated alkyl esters causes elimination through the kidneys, over a relatively short period of time, local application of the glucuronide or its derivative permits a slow release of free Indomethacin through the action of these esterases.
  • the drug is thus used very etficiently and its effifect is felt over a prolonged period.
  • the glucuronide of Indomethacin or its acylated esters can be applied, either topically or by injection.
  • the glucuronide itself is especially useful in an aqueous carrier, whereas the acylated esters are useful in fat or oily carriers.
  • Example 1-Irzd0methacin glucuronide A rabbit is dosed orally (stomach tube) with 518.5 mg. of Indomethacin (l-p-chlorobenzoyl 2 methyl 5- methoxy-3-indolyl acetic acid) containing 11 o. of Indomethacin-2C.
  • Indomethacin l-p-chlorobenzoyl 2 methyl 5- methoxy-3-indolyl acetic acid
  • One g. of ammonium chloride is administered intraperitoneally in order to maintain the urine pH near 7.
  • Drug and ammonium chloride are given in two equal doses at times 0 and 12 hours.
  • One-half (108 ml., 5.2x l0 c.p.m.) of the first 24-hour urine is adjusted to pH 5.0 and extracted with four IOU-ml.
  • the residual urine is then adjusted to pH 2.0 and extracted with ethyl acetate. Water (50 ml.) is added to the combined extracts and the organic solvent removed in vacuo on a rota-ting concentrator. The residual aqueous solution is adjusted to pH 6.6 and lyophilized to give 318.5 mg. of brown gum which contains 80% of the radioactivity in the original urine.
  • Paper chromatography in a system comprising 2 methanol: 1 water: 1 n-butylalcohol: 1 benzene revealed the presence of 5- methoxy-Z-methylindole-3-acetic acid and the glucuronides of Indomethacin and 5-methoxy-2-methylindole-3-acetic acid.
  • a 60-tube countercurrent distribution apparatus with lower phase capacity 3 ml. per tube is prepared.
  • the solvent system is made by equilibration of 400 ml. of 0.5 M phosphate buffer (pH 6.6; equal volumes of 0.5 M Na HPO and 0.5 M NaH PO 328 ml. of ethyl acetate and 72 ml. of sec. butyl alcohol.
  • the upper phase proportioning device is adjusted to deliver 3 ml. per cycle.
  • the entire 318.5 mg. of crude glucuronide is dissolved in 6 ml. of lower phase, introduced into the first two tubes and a total of 75 transfers carried out. Scintillation counting of selected fractions shows that the distribution has yielded three radioactive zones.
  • Paper chromatographic analysis and ultraviolet spectra serves to identify the metabolites.
  • Material near the organic solvent end of the system contains 2-methyl-5-methoxy-3-indolyl acetic acid, and the polar material (tubes O-3) is the crude glucuronide of this compound which is reserved for isolation of that substance.
  • Indomethacin glucuronide has concentrated at about tube 29.
  • Tubes 16-34 are combined on the basis of radioactivity.
  • the phases are separated and the aqueous layer adjusted to pH 2.2 wit-h hydrochloric acid.
  • the phases are then recombined and three extractions with 15 ml. portions of ethyl acetate carried out.
  • Solvent is removed from the extract in vacuo and the residue is dissolved in water, adjusted to pH 6.0 and lyophilized. There results 45.5 mg. of White granular material that shows the ultraviolet max- 1 irnum at 320 m characteristic of Indomethacin.
  • the fraction contains 1.2 l c.p.m. and thus represented 28% of the original label.
  • a single peak at R 0.75 is observed on chromatography in a system comprising 2 methanolzl waterzl-n-but-anol-l benzene, and chromatographic analysis using a system comprising 8 isopropanol: 15 N NH OH: 1 water in combination with the above system after treatment with fl-glu-curonidase shows complete conversion to Indomethacin.
  • Final proof of structure is secured by conversion of the crude glucuronide to the crystalline triacetyl methyl ester, which is identified by comparison with a synthetic sample of the triacetyl methyl ester of Indomethacin glucuronide.
  • Example 2 Five grams (0.014 mole) of 1-p-chlorobenzoyl-2- me-thyl-S-meth0xy-3-indolyl acetic acid is suspended in 15 ml. of anhydrous methanol and 32.8 ml. of a solution of 0.427 N (0.014 eq.) of potassium-t-butoxide in t-butyl alcohol is added dropwise. The solid slowly dissolves and at the end of the addition the solution is clear and the pH is neutral. The yellow solution is concentrated to dryness in vacuo, dissolved in the minimum amount of refluxing acetone, cooled to room temperature and placed in the refrigerator overnight.
  • the resultant crystals are filtered, washed with a small amount of cold acetone and dried yielding 4.2 grams of the potassium salt of Indomethacin.
  • a four gram aliquot (0.0101 mole) of this salt is dissolved in the minimum amount of refluxing acetone and the resulting solution is treated with 4.1 grams (0.0103 mole) of methyl-(tri-O-acetyl-u-D-glucopyranosylbromide)-uronate dissolved in acetone.
  • the solution is refluxed for two hours in a nitrogen atmosphere. The color of the solution changes from yellow to maroon. After standing at room temperature overnight, the solution is concentrated to dryness and the residue is dissolved in methylene chloride.
  • the solution is filtered, extracted 3 times with an equal volume of a saturated solution of sodium bicarbonate, with H 0 and then is dried over MgSO
  • the dried methylene chloride solution is concentrated to yield a viscous yellow colored oil.
  • the oil is crystallized from ether-n-hexane to yield 2.0 grams of Indomethacin glucuronide triacetyl methyl ester, M.P. 150-151" C.
  • Example 3.Ind0methacin glucuronide triacetyl methyl ester A 16.4 mg. sample of crude Indomethacin glucuronide sodium salt, isolated from urine as described above in Example 1, is dissolved in 3.0 ml. of water and the pH is adjusted to 2.1 with hydrochloric acid. The resulting suspension is extracted with four 5 ml. portions of ethyl acetate and the extracts combined to yield 13.5 mg. of the free acid as an amorphous yellow solid. This material is dissolved in 1 ml. of methanol and treated with excess ethereal diazomethane. After one hour at 25, the solvent is removed in a stream of nitrogen and the amorphous crude methyl ester dried in vacuum.
  • the crude ester is chromatographed on silica gel by the thin layer technique, the plate being developed with ethyl acetate.
  • Example 4 Topical ointment No. 1 Percent Indomethacin glucuronide 1 White beeswax 5 W001 fat, anhydrous 20 Mineral oil, heavy 5 White petroleum, q.s 100 Levigate the Indomethacin glucuronide with a portion of the mineral oil. Melt the remaining ingredients separately on a steam bath and combine with the remaining mineral oil, which also has been heated, and stir until cool. Incorporate the levigated solid into the cooled base and pass through a roller mill several times.
  • Example 5 Topical ointment No. 2 Percent Indomethacin glucuronide 1 Mineral oil 30 Petrolatum, white, q.s. 100
  • Example 6 Topical cream: Percent Indomethacin glucuronide 1 Heat the stearyl alcohol, cetyl alcohol, mineral oil, Myrj 52, and anti-foam emulsion AP to 7580 C. Dissolve the remaining ingredients (except the Indomethacin glucuronide) in the water and heat to -85 C. Add the aqueous phase to the oil phase with stirring. Stir until cool. Levigate the solid with a portion of the base. Incorporate the remainder of the base and pass through a roller mill several times.

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  • Chemical & Material Sciences (AREA)
  • Organic Chemistry (AREA)
  • Pharmaceuticals Containing Other Organic And Inorganic Compounds (AREA)
  • Indole Compounds (AREA)

Description

United States Patent Ofitice 3,285,935 Patented Nov. 15, 1966 3,285,935 INDOLYL GLUCURONIDES Robert E. Harman, Avenel, Frederick A. Kuehl, Jr., Rumson, Robert G. Strachan, Summit, and Ralph F. Hirschmaun, Scotch Plains, N.J., assignors to Merck & Co., Inc., a corporation of New Jersey No Drawing. Filed July 18, 1963, Ser. No. 296,111
3 Claims. (Cl. 260-32613) This invention relates to new indolyl acid derivatives and to a method for the prolonged localized treatment of inflammation. More specifically, this invention relates to the glucuronides of 1-pchlorobenzoyl-2-methyl-5-rnethoxy-3-indolyl acetic acid and to the lower alkyl esters of per-lower alkanoylated glucuronides of the said indolyl acid. More specifically also, it relatesto a method for the prolonged localized treatment of inflammation which comprises the localized administration of these compounds.
The treatment of inflammation by chemotherapeutic agents has advanced a great distance in the last decade and a half, with the development of many new chemotherapeutic agents such as the steroids and the like. Recently, a new and very powerful drug has been added to the list known as Indomethacin, chemically 1-pschlorobenzoyl-2- methyl-5-methoxy-3-indolyl acetic acid. Like many other drugs this is a systemic medicine which is administered orally and passes into the blood stream for general distribution in the body. This presents certain disadvantages, under some circumstances. One such disadvantage is that a large amount of the drug becomes inactivated by metabolic processes over a period of time and passes out through the body excretions. Another disadvantage to this method of administering Indomethacin, is that the duration of the drugs effect is not too long and repeated periodic administrations are necessary. Furthermore, it is at times desirable to get a localized treatment with the drug applied only to the inflamed area, rather than waste it over the entire body.
We have found that certain carbohydrate derivatives of Indomethacin which are inactive systemically, are transformed in situ by metabolic processes very slowly into Indomethacin with the result that prolonged local treatment of inflammation is possible. These carbohydrate derivatives comprise the glucuronide of Indomethacin which is itself the deactivating metabolic product by which Indomethacin is excreted from feces of some species and the alkyl esters of the trialkanoylated glucuronide of Indomethacin, which are preparable either synthetically or from the metabolic product itself.
It is an advantage of these above products that, with their use, the method of our' invention permits localized treatment of inflammation. Such localized treatment puts the drug where it is needed and not systemically throughout the whole body and is thus far less wasteful of this drug. It is a further advantage of our invention that slow prolonged treatment is possible, again permitting economies in the use of the drug.
The glucuronide of Indomethacin is the metabolite by which Indomethacin is excreted from some species of animal (other species excrete other derivatives). When the glucuronide is treated with diazomethane to produce the corresponding methyl ester and then acetylated there is formed the methyl ester of the triacetylglucuronide of Indomethacin. This same compound can be obtained from bromo triacetylglucuronic acid and the potassium salt of Indomethacin in acetone. diazopropane or diazobutane are used, the corresponding other lower alkyl esters such as the ethyl, propyl and butyl esters are obtained. Similarly, instead of using acetice anhydride, acylation can be carried out with propionic anhydride, butyric anhydride or the like to produce When diazoethane, I
the corresponding lower alkanoylated glucuronic acid derivatives. These equivalent derivatives are similarly usable in our invention.
The key to this invention is the presence of an enzyme known as ,B-glucuronidase in mammalian tissue (Bollet, Goodwin, and Brown, J. Clin. Invest, 38, 451, 1959) as well as the presence of other esterases in synovial fluid. Although systemic administration of the glucuronides alkanoylated alkyl esters causes elimination through the kidneys, over a relatively short period of time, local application of the glucuronide or its derivative permits a slow release of free Indomethacin through the action of these esterases. The drug is thus used very etficiently and its effifect is felt over a prolonged period.
The glucuronide of Indomethacin or its acylated esters can be applied, either topically or by injection. The glucuronide itself is especially useful in an aqueous carrier, whereas the acylated esters are useful in fat or oily carriers.
Our invention can be illustrated by the following examples:
Example 1.-Irzd0methacin glucuronide A rabbit is dosed orally (stomach tube) with 518.5 mg. of Indomethacin (l-p-chlorobenzoyl 2 methyl 5- methoxy-3-indolyl acetic acid) containing 11 o. of Indomethacin-2C. One g. of ammonium chloride is administered intraperitoneally in order to maintain the urine pH near 7. Drug and ammonium chloride are given in two equal doses at times 0 and 12 hours. One-half (108 ml., 5.2x l0 c.p.m.) of the first 24-hour urine is adjusted to pH 5.0 and extracted with four IOU-ml. volumes of henzene to remove much of the unconjugated metabolites. The residual urine is then adjusted to pH 2.0 and extracted with ethyl acetate. Water (50 ml.) is added to the combined extracts and the organic solvent removed in vacuo on a rota-ting concentrator. The residual aqueous solution is adjusted to pH 6.6 and lyophilized to give 318.5 mg. of brown gum which contains 80% of the radioactivity in the original urine. Paper chromatography in a system comprising 2 methanol: 1 water: 1 n-butylalcohol: 1 benzene revealed the presence of 5- methoxy-Z-methylindole-3-acetic acid and the glucuronides of Indomethacin and 5-methoxy-2-methylindole-3-acetic acid.
A 60-tube countercurrent distribution apparatus with lower phase capacity 3 ml. per tube is prepared. The solvent system is made by equilibration of 400 ml. of 0.5 M phosphate buffer (pH 6.6; equal volumes of 0.5 M Na HPO and 0.5 M NaH PO 328 ml. of ethyl acetate and 72 ml. of sec. butyl alcohol. The upper phase proportioning device is adjusted to deliver 3 ml. per cycle. The entire 318.5 mg. of crude glucuronide is dissolved in 6 ml. of lower phase, introduced into the first two tubes and a total of 75 transfers carried out. Scintillation counting of selected fractions shows that the distribution has yielded three radioactive zones. Paper chromatographic analysis and ultraviolet spectra serves to identify the metabolites. Material near the organic solvent end of the system contains 2-methyl-5-methoxy-3-indolyl acetic acid, and the polar material (tubes O-3) is the crude glucuronide of this compound which is reserved for isolation of that substance. Indomethacin glucuronide has concentrated at about tube 29.
Tubes 16-34 are combined on the basis of radioactivity. The phases are separated and the aqueous layer adjusted to pH 2.2 wit-h hydrochloric acid. The phases are then recombined and three extractions with 15 ml. portions of ethyl acetate carried out. Solvent is removed from the extract in vacuo and the residue is dissolved in water, adjusted to pH 6.0 and lyophilized. There results 45.5 mg. of White granular material that shows the ultraviolet max- 1 irnum at 320 m characteristic of Indomethacin. The fraction contains 1.2 l c.p.m. and thus represented 28% of the original label. A single peak at R 0.75 is observed on chromatography in a system comprising 2 methanolzl waterzl-n-but-anol-l benzene, and chromatographic analysis using a system comprising 8 isopropanol: 15 N NH OH: 1 water in combination with the above system after treatment with fl-glu-curonidase shows complete conversion to Indomethacin. Final proof of structure is secured by conversion of the crude glucuronide to the crystalline triacetyl methyl ester, which is identified by comparison with a synthetic sample of the triacetyl methyl ester of Indomethacin glucuronide.
Example 2 Five grams (0.014 mole) of 1-p-chlorobenzoyl-2- me-thyl-S-meth0xy-3-indolyl acetic acid is suspended in 15 ml. of anhydrous methanol and 32.8 ml. of a solution of 0.427 N (0.014 eq.) of potassium-t-butoxide in t-butyl alcohol is added dropwise. The solid slowly dissolves and at the end of the addition the solution is clear and the pH is neutral. The yellow solution is concentrated to dryness in vacuo, dissolved in the minimum amount of refluxing acetone, cooled to room temperature and placed in the refrigerator overnight. The resultant crystals are filtered, washed with a small amount of cold acetone and dried yielding 4.2 grams of the potassium salt of Indomethacin. A four gram aliquot (0.0101 mole) of this salt is dissolved in the minimum amount of refluxing acetone and the resulting solution is treated with 4.1 grams (0.0103 mole) of methyl-(tri-O-acetyl-u-D-glucopyranosylbromide)-uronate dissolved in acetone. The solution is refluxed for two hours in a nitrogen atmosphere. The color of the solution changes from yellow to maroon. After standing at room temperature overnight, the solution is concentrated to dryness and the residue is dissolved in methylene chloride. The solution is filtered, extracted 3 times with an equal volume of a saturated solution of sodium bicarbonate, with H 0 and then is dried over MgSO The dried methylene chloride solution is concentrated to yield a viscous yellow colored oil. The oil is crystallized from ether-n-hexane to yield 2.0 grams of Indomethacin glucuronide triacetyl methyl ester, M.P. 150-151" C.
xgfiP 1755 cmf 1673 cm. 0.:0). 1585 cm.- (aromatic) and 12001285 cm.
Analysis-Calculated for C H O NCl: C, 57.79; H, 4.85; N, 2.11; Cl, 5.33 Found: C, 57.71; H, 4.59; N, 2.06; Cl, 5.12.
Example 3.Ind0methacin glucuronide triacetyl methyl ester A 16.4 mg. sample of crude Indomethacin glucuronide sodium salt, isolated from urine as described above in Example 1, is dissolved in 3.0 ml. of water and the pH is adjusted to 2.1 with hydrochloric acid. The resulting suspension is extracted with four 5 ml. portions of ethyl acetate and the extracts combined to yield 13.5 mg. of the free acid as an amorphous yellow solid. This material is dissolved in 1 ml. of methanol and treated with excess ethereal diazomethane. After one hour at 25, the solvent is removed in a stream of nitrogen and the amorphous crude methyl ester dried in vacuum. One-half ml. of pyridine and /2 ml. of acetic anhydride are added to the crude ester and the solution is held at 25 overnight. The acetylation mixture is then poured into 5 ml. of water, allowed to stand at 25 a further hour, and the acetylated ester of Indomethacin glucuronide filtered off and dried in vacuum.
The crude ester is chromatographed on silica gel by the thin layer technique, the plate being developed with ethyl acetate. Partially purified ester (R; 0.83), recovered by elution with ethyl acetate, is re chromatographed using chloroform as the developer. The ester, R 0.05, is
eluted with ethyl acetate and crystallized from etherhexane. It has a MI. 1445, unchanged upon admixture with authentic Indomethacin glucuronide triacetyl methyl ester prepared in Example 2 and the infrared spectra of the two samples are identical.
Example 4 Topical ointment No. 1: Percent Indomethacin glucuronide 1 White beeswax 5 W001 fat, anhydrous 20 Mineral oil, heavy 5 White petroleum, q.s 100 Levigate the Indomethacin glucuronide with a portion of the mineral oil. Melt the remaining ingredients separately on a steam bath and combine with the remaining mineral oil, which also has been heated, and stir until cool. Incorporate the levigated solid into the cooled base and pass through a roller mill several times.
Example 5 Topical ointment No. 2: Percent Indomethacin glucuronide 1 Mineral oil 30 Petrolatum, white, q.s. 100
Melt the petrolatum on a steam bath, add the mineral oil, and stir until cool. Levigate the Indomethacin glucuronide with a portion of the base. Incorporate the remainder of the base and pass the entire formulation through a roller mill several times.
Example 6 Topical cream: Percent Indomethacin glucuronide 1 Heat the stearyl alcohol, cetyl alcohol, mineral oil, Myrj 52, and anti-foam emulsion AP to 7580 C. Dissolve the remaining ingredients (except the Indomethacin glucuronide) in the water and heat to -85 C. Add the aqueous phase to the oil phase with stirring. Stir until cool. Levigate the solid with a portion of the base. Incorporate the remainder of the base and pass through a roller mill several times.
We claim:
1. A compound selected from the group consisting of the glucuronide of 1-p-chl-orobenzoyl-Z-methyl-S methoxy-3-indolyl acetic acid and the lower alkyl esters of thed'per-lower alkanoylated glucuronide of the said indolyl aci 2. The glucuronide of 1-p-chlorobenzoyl-2-methyl-5- methoxy-3-indolyl acetic acid.
3. The methyl ester of the triacetylglucuronide of l-pchlorobenzoyl-2-methyl-5-methoxy-3-indolyl acetic acid.
References Cited by the Examiner UNITED STATES PATENTS 3,127,413 3/1964 Gray 260319 3,133,083 5/1964 Hester 260319 3,143,465 8/1964 Keating 167-65 3,156,619 11/1964 Bertin et al. 167-65 ALEX MAZEL, Primary Examiner.
HENRY R. JILES, JULIAN S. LEVITT, Examiners.
M. I. COHEN, M. E. OBRIEN, Assistant Examiners.

Claims (1)

1. A COMPOUND SELECTED FROM THE GROUP CONSISTING OF THE GLUCURONIDE OF 1-P-CHLOROBENZOYL-2-METHYL-5-METHOXY-3-INDOLYL ACETIC ACID AND THE LOWER ALKYL ESTERS OF THE PER-LOWER ALKANOYLATED GLUCURONIDE OF THE SAID INDOLYL ACID.
US296111A 1963-07-18 1963-07-18 Indolyl glucuronides Expired - Lifetime US3285935A (en)

Priority Applications (10)

Application Number Priority Date Filing Date Title
US296111A US3285935A (en) 1963-07-18 1963-07-18 Indolyl glucuronides
GB26807/64A GB1061778A (en) 1963-07-18 1964-06-29 Indolyl acetic acid glucuronides
DE19641695474 DE1695474A1 (en) 1963-07-18 1964-06-30 Lower alkyl esters of per-lower alkanoylated glucuronides and process for their preparation
DE19641470072 DE1470072A1 (en) 1963-07-18 1964-06-30 1-p-chlorobenzoyl-2-methyl-5-methoxy-3-indolyl-acetic acid glucuronide and process for its preparation
BE650447D BE650447A (en) 1963-07-18 1964-07-10
FR1565303D FR1565303A (en) 1963-07-18 1964-07-16
CH1667767A CH451147A (en) 1963-07-18 1964-07-17 Process for the preparation of the lower alkyl esters of the per-lower-alkanoylated glucuronides of 3-indolylacetic acid
CH941064A CH451145A (en) 1963-07-18 1964-07-17 Process for the preparation of new indolyl acid derivatives
FR991578A FR3930M (en) 1963-07-18 1964-10-15
US510999A US3375166A (en) 1963-07-18 1965-09-14 Methods of prolonged inflammatory treatment

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Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3127413A (en) * 1960-11-22 1964-03-31 Neisler Lab Inc Octahydroisoindoles
US3133083A (en) * 1962-05-25 1964-05-12 Upjohn Co Derivatives of 6-fluorotryptamine
US3143465A (en) * 1961-06-19 1964-08-04 Wallace & Tiernan Inc Pharmaceutical preparations comprising phosphorus containing cation exchange resins having a basic drug adsorbed thereon; and treatment therewith
US3156619A (en) * 1962-06-25 1964-11-10 Roussel Uclaf 20alpha (beta-[nu, nu-dimethyl-amino]-ethylamino)-19-nor-delta1, 3, 5 (10)-pregnatrienes, process for preparation thereof and method of treatment

Patent Citations (4)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US3127413A (en) * 1960-11-22 1964-03-31 Neisler Lab Inc Octahydroisoindoles
US3143465A (en) * 1961-06-19 1964-08-04 Wallace & Tiernan Inc Pharmaceutical preparations comprising phosphorus containing cation exchange resins having a basic drug adsorbed thereon; and treatment therewith
US3133083A (en) * 1962-05-25 1964-05-12 Upjohn Co Derivatives of 6-fluorotryptamine
US3156619A (en) * 1962-06-25 1964-11-10 Roussel Uclaf 20alpha (beta-[nu, nu-dimethyl-amino]-ethylamino)-19-nor-delta1, 3, 5 (10)-pregnatrienes, process for preparation thereof and method of treatment

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