US2586154A - Racemization of amino acid - Google Patents

Racemization of amino acid Download PDF

Info

Publication number
US2586154A
US2586154A US171245A US17124550A US2586154A US 2586154 A US2586154 A US 2586154A US 171245 A US171245 A US 171245A US 17124550 A US17124550 A US 17124550A US 2586154 A US2586154 A US 2586154A
Authority
US
United States
Prior art keywords
lysine
racemization
acid
phosphoric acid
mixture
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.)
Expired - Lifetime
Application number
US171245A
Inventor
Robert D Emmick
Current Assignee (The listed assignees may be inaccurate. Google has not performed a legal analysis and makes no representation or warranty as to the accuracy of the list.)
EIDP Inc
Original Assignee
EI Du Pont de Nemours and Co
Priority date (The priority date 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 date listed.)
Filing date
Publication date
Application filed by EI Du Pont de Nemours and Co filed Critical EI Du Pont de Nemours and Co
Priority to US171245A priority Critical patent/US2586154A/en
Application granted granted Critical
Publication of US2586154A publication Critical patent/US2586154A/en
Anticipated expiration legal-status Critical
Expired - Lifetime legal-status Critical Current

Links

Classifications

    • CCHEMISTRY; METALLURGY
    • C07ORGANIC CHEMISTRY
    • C07CACYCLIC OR CARBOCYCLIC COMPOUNDS
    • C07C51/00Preparation of carboxylic acids or their salts, halides or anhydrides
    • C07C51/42Separation; Purification; Stabilisation; Use of additives
    • C07C51/487Separation; Purification; Stabilisation; Use of additives by treatment giving rise to chemical modification
    • CCHEMISTRY; METALLURGY
    • C12BIOCHEMISTRY; BEER; SPIRITS; WINE; VINEGAR; MICROBIOLOGY; ENZYMOLOGY; MUTATION OR GENETIC ENGINEERING
    • C12PFERMENTATION OR ENZYME-USING PROCESSES TO SYNTHESISE A DESIRED CHEMICAL COMPOUND OR COMPOSITION OR TO SEPARATE OPTICAL ISOMERS FROM A RACEMIC MIXTURE
    • C12P13/00Preparation of nitrogen-containing organic compounds
    • C12P13/04Alpha- or beta- amino acids
    • C12P13/08Lysine; Diaminopimelic acid; Threonine; Valine

Definitions

  • enantiomorphic d() -1ysine has no known nutritional value.
  • Lysine which has been synthesized from optically inactive materials, for example, by the process of Eck and Marvel, Organic Syntheses Collecl5,
  • its nutritional value can be doubled by con verting its d()-lysine content into the l'('+) form while retaining the quantity of the latter initially present.
  • Resolution of dl-lysine is usually effected by combining the material to be resolved with an optically active compound known as the resolving agent and fractionally crystallizing the product. This may be accomplished by known methods. For example, in a method disclosed by C. P. Berg in the Journal of Biological Chemistry, vol.
  • d-camphoric acid is used Y as a resolving agent to obtain l(+) -lysine.
  • This author also shows the use of l-camphoric acid to obtain d() -lysine.
  • the racemization of lysine, or conversion of the optically active material to the racemic mix- I ture, has previously been accomplished by heating the isomer with hydrochloric" acid. This method is disclosed in Ber. 35, 3778, (1902). Although good recoveries of lysine are obtainableby this method, the mixture of hydrochloric acid 66 The lysine 5 racemization at a practical rate. sive corrosion resistant equipment is necessary if this method is to be used.
  • a further object is to provide a new and improved process by which a mixture of l(+) and d() -isomers of lysine may easily be recovered from the reaction medium.
  • Still another object is to provide a rapid process for the, racemization of lysine which may be operated at atmospheric pressure.
  • phosphoric acid is added to an aqueous solution of optically active lysine or lysine hydrochloride and the resulting solution is "boiled to remove water until the desired temperature of operation is reached.
  • a reflux condenser is then attached and heating is continued until racemization is substantially complete.
  • the racemized lysine may be recovered by diluting the racemization mixture and passing the resulting solution into contact with a cation-exchange material which adsorbs the lysine.
  • 'Lysine may then be displaced from the cation-exchange material by elution with a base, for example, ammonia, and free lysine obtained by evaporation to remove the ammonia.
  • An acid for example, hydrochloric acid, may be utilized if desired to remove the lysine from the cation-exchange material in which case thelysine may be recovered as the hydrochloride.
  • Racemization in accordance with this invention may be carried out by heating either free lysine or lysine monohydrochloride in combination with phosphoric acid.
  • the racemization is carried out using the hydrochloride a somewhat longer time is required but better recovery of lysine is obtained and higher yields of optically active lysine are obtained in the subsequent resolution step.
  • the time required for complete racemization 5 will vary with the temperature as well as the ratio of optical isomers :-present in 'therlysine" treated.
  • complete'racemizat-ion of l(+)-lysine has been obtained by heating with sorbs the lysine and allows the phosphoric acid to phosphoric acid during 1 hour at about 170 td lo material for eluting the cation-exchange material 175?
  • Racemization of -l(+)-'-lysine-mono-'- hydrochloride required 4 hoursat 160"'to162*C.” 1'5" tures the racemization is "slower while at higher temperatures?although the ratepf racemization is incrjeased j si'dereactionsand. decompositioni of lysi'rie maypccur *vv-ith 're'sultii'ig low recoveries of lysine-5 Although rac'emizationmay'be'carried to com U.'S5-P;'2,366,007.1 Otheri-examplesiinclude p'oly u. phenolsulfonic acids, sulfonated hydrocarbon" Sulfonated coals and natural. and'..synthetic zeolites: having:
  • Th'us th cationtezexchanget material whenzusedin desired point -tHe Iysine :may" bei'sepa1:ated-ircrnii the phos horic acid-Tand ther'latter 'iS-ZSllil78.b18ffdf"' reuseintheraeemiiationiorocessiz variou'soneth ods maysbe utilized rfor::theiseparationi-oflysine Various :formstofthe zcation'i ex'change material.
  • Ezcample' 1' A soluti'on of 12.80' g.- (0.07 mole) of -l -1yslne droxides are examples of materials"suitable-"for Emon hydfgchloride--a,nd "10 35% phosphoric
  • Example 3 Toa water solution of 0.14 mole free lysine con-j I taining about 70% d( -isomer, was added 20 ml.
  • Example 4 To 68 g. of l(+) -lysine monohydrochloride was added 53.5 ml. 85% phosphoric acid and about 20 ml. water. The mixtures was boiled until the temperature reached 160 C. A reflux condenser was then attached and the mixture heated at 160 to 162 C. for 4 hours. Samples (5 ml.) were taken atvarious intervals, diluted to 25 ml., and the rotation observed. The results are summarized in the table below:
  • Example 5 The sameprocedure as in Example 4 was used. The racemization was run at 150 to 153 C. The results are summarized in the table below.
  • Example 6 A water solution of 1.055 mole free lysine co'ntaining-about 70% d()-isomer was mixed with 143 ml. 85% phosphoric acid and the solution l(+)-lysine d-camphorate; 94% optically pure.
  • Example 7 A series of runs similar to Example 6 was made in which lysine monohydrochloride was treated j with phosphoric acid and racemized at C.
  • the process of this invention is superior to the prior art process utilizing hydrochloric acid in the surprising and unexpected speed with which racemization is accomplished. It has been found that racemization of lysine with hydrochloric acid at 185 C. requires about 12 hours as compared with only about 1 hour for the process of this invention at a temperature of to C. Thus the racemization with phosphoric acid may be carried out at a much lower temperature and still require only a fraction of the time required by the prior art method. In addition racemiza-, tion with phosphoric acid may be carried out at atmospheric pressure.
  • the process of this invention is useful in racemizing optically active lysine from any source, it is of particular utility as a part of the resolution-racemization cycle involved in converting dl-lysine or, other mixture of l(+) and d()-lysine to a pure optical isomer.
  • This procedure which may vary in detail consists essentially in resolving lysine by known methods, for example, the method described by Berg, separating the desired isomer,” heating the remaining undesired isomer in combination with phosphoric acid to effect racemization, recovering a mixture of l(+) and d() -lysine and returning the latter to the resolution step.
  • lysine to be racemized in accordance with this invention is in the form of its compound with a resolving agent such as optically active camphoric acid
  • the latter may be recovered from solution upon the addition of phosphoric acid followed by filtration and extraction with ether and racemization is then carried out 7' by heating the-remaining solution of lysine in combination with? phosphoric :acid. "as described above.
  • Process which comprises heating; optically active lysinein'combination with phosphoric'a'cidin the presence of water, passing an aqueous solutionof the racemized lysine obtained thereby into contact with'a cation-exchange materialgrecovering phosphoric acid, eluting said cation-exchange material with a material capable of displacing lysine from said cation-exchange material and recovering lysine, from the elutriate.

Description

Patented Feb. 19, 1952 UNITED STATES PATENT OFFICE RACEMIZATION or AMINO ACID Robert D. Emmick, Niagara Falls, N. Y., assignor to E. I. du Pont de Nemours. and Company, Wilmington, Del., a corporation of Delaware No Drawing. Application June 29, 1950, Serial No. 171,245
8 Claims. (Cl. 260-534) essential component of animal diets whereas the 10:
enantiomorphic d() -1ysine has no known nutritional value.
Lysine which has been synthesized from optically inactive materials, for example, by the process of Eck and Marvel, Organic Syntheses Collecl5,
tive vol. II, page 374, or by the process described in U. S. P. 2,498,300 is optically inactive and consists of equal parts of the biologically active l(+) isomer and the biologically inactive d() -isomer.
Thus, its nutritional value can be doubled by con verting its d()-lysine content into the l'('+) form while retaining the quantity of the latter initially present.
It is possible to convert synthetic lysine completely to the biologically active form by first 5 separating the isomers (resolution) and then converting the inactive d()-lysine back to the dl-mixture (racemization). By a repetition of these operations, the lysine is eventually converted entirely into the l(+)-form. As a practical matter it is unnecessary and usually impossible to effect a complete separation of the l'(+) -lysine and the d()-isomer. The requirements for an economically feasible process are that a substantial portion of the l(+) -lysine be isolated in pure form in the resolution step and that no serious loss of total lysine occur in either step.
Resolution of dl-lysine is usually effected by combining the material to be resolved with an optically active compound known as the resolving agent and fractionally crystallizing the product. This may be accomplished by known methods. For example, in a method disclosed by C. P. Berg in the Journal of Biological Chemistry, vol.
115, pages 9-15, (1936), d-camphoric acid is used Y as a resolving agent to obtain l(+) -lysine. This author also shows the use of l-camphoric acid to obtain d() -lysine The racemization of lysine, or conversion of the optically active material to the racemic mix- I ture, has previously been accomplished by heating the isomer with hydrochloric" acid. This method is disclosed in Ber. 35, 3778, (1902). Although good recoveries of lysine are obtainableby this method, the mixture of hydrochloric acid 66 The lysine 5 racemization at a practical rate. sive corrosion resistant equipment is necessary if this method is to be used. Furthermore, the use of hydrochloric acid requires equipment capable of withstanding elevated pressures. Attempts to use this method by reducing the proportion of hydrochloric acid to that stoichiometrically equivalent to the lysine present have failed to obviate this serious disadvantage. Another method for the racemization of lysine which is disclosed in U. S. P. 2,071,327 consists in heating the aminoacid with acetyl chloride in the presence of acetic acid. Obviously, this method is even less desir able than the one described above.
It is an object of this invention to provide a simple, practical and economical process for the racemization of lysine. A further object is to provide a new and improved process by which a mixture of l(+) and d() -isomers of lysine may easily be recovered from the reaction medium.
Still another object is to provide a rapid process for the, racemization of lysine which may be operated at atmospheric pressure. These and other'objects will be apparent from the following description of the invention.
The above objects are attained in accordance with this invention by heating optically active lysine in combination with phosphoric acid.
In one mode of operating the process of this invention phosphoric acid is added to an aqueous solution of optically active lysine or lysine hydrochloride and the resulting solution is "boiled to remove water until the desired temperature of operation is reached. A reflux condenser is then attached and heating is continued until racemization is substantially complete. The racemized lysine may be recovered by diluting the racemization mixture and passing the resulting solution into contact with a cation-exchange material which adsorbs the lysine. 'Lysine may then be displaced from the cation-exchange material by elution with a base, for example, ammonia, and free lysine obtained by evaporation to remove the ammonia. An acid, for example, hydrochloric acid, may be utilized if desired to remove the lysine from the cation-exchange material in which case thelysine may be recovered as the hydrochloride.
Racemization in accordance with this invention may be carried out by heating either free lysine or lysine monohydrochloride in combination with phosphoric acid. When the racemization is carried out using the hydrochloride a somewhat longer time is required but better recovery of lysine is obtained and higher yields of optically active lysine are obtained in the subsequent resolution step.
The time required for complete racemization 5 will vary with the temperature as well as the ratio of optical isomers :-present in 'therlysine" treated. For'example, complete'racemizat-ion of l(+)-lysine has been obtained by heating with sorbs the lysine and allows the phosphoric acid to phosphoric acid during 1 hour at about 170 td lo material for eluting the cation-exchange material 175? C. Lysine containing about:'70%.-of=--thet d(-) -isomer was completely racemized by heating with phosphoric acid during l hour-M 155 to 165 C. Racemization of -l(+)-'-lysine-mono-'- hydrochloride required 4 hoursat 160"'to162*C." 1'5" tures the racemization is "slower while at higher temperatures?although the ratepf racemization is incrjeased j si'dereactionsand. decompositioni of lysi'rie maypccur *vv-ith 're'sultii'ig =low recoveries of lysine-5 Although rac'emizationmay'be'carried to com U.'S5-P;'2,366,007.1 Otheri-examplesiinclude p'oly u. phenolsulfonic acids, sulfonated hydrocarbon" Sulfonated coals and natural. and'..synthetic zeolites: having:
pletion-in accordance =withthis invention it is unnecessary =and may-sometiines' be undesirable in-- practical -operation'=- to-"racemize completely:
Sincemixtures containing l varying proportions of"l(-"+ )-lysine and"'d ly'sine may' be -resoIved": L the practice of this invention. The selection of a particular: cation-exchange --ma-terialz'willt. depend upon such considerations as capacity., exchange without difiiculty it is entirely s atisf actory to stop-i: the racemization at 'anydesired point. However; it is-of course" desirable iii-increasesubstantially the proportion ofithedesirediisomer inatlieimixe tare-5 Although lysine mavbe racemiz'eziby heatinginf combination-with-phosphoric acid in the -absence of-water it* is preferable to' move present-at least Fr 2% by weight 'of wat'er-based upon the'wei'ghtof solubleipolymeric materials which-contain acidic groups capable of combining 'i withv a :variety: of cations;tolfo'rm insoluble 'saits::. A typical example of" a catiom exchange;- material is: describe'dz' in polymersrand': polycarboxylic" acids:
cation-exchange: properties. are zal'so suitable :in
rateymechanical ruggedness andz'ch'emicalz stabilitysi'as :welluasxcost; Any. off':tlie.'.icommercially' availableicatiorr exchangelmaterials are suitable. Fortexample;z-satisfactoryi results may be; obtained '3 with catiomexchangeirmaterials sold. under the:
the mixture in order tomir'iimize 'del'iydration:of"40 :Di1olite (II-3;." "Amberlite:i[RC-'-50 and: Permu:-.
the lysine:-- The racernization may also -b"'eaccom= plish'ed in the presence of large" amounted water;:- for example: *7i by weight; but sucli large amounts of water will involve a longer" time: for
racemization because-of tn'mowertemperatureor" 5 drocarbonipolymerszx These cation exchange-ma+ terials areiparificularly'valuable; in the practicaof 2 this? inventiohtsincwthey 'possessiexcell'ent .chemi'-' cal and Lphysical stability -Iunder? the conditions:
operation or pressureequipment -in' ordr 'to ob tain the preferred temperatur'e' of operatibn. Ifi general it i's desirable to adjizstiitlie amount of water utili'zed -in accordance with 'tlie-temperm A'rpreferred class-of cationteexchangeimaterials" are those in which the acidic glOllpSSaIBlSlflfOniC."
aci'd igroups asexemplified bythe; sulfonated: hy-
utilized; arelreadilyravailabl,"and have highrcature at wliich -tlie operation to be carriedt: out-. 501 pacit'y: and exchange rate.-
phosphoric acid to rmole of lysines hascbeen used withfexcelInt results A greater? excess mav be utiliaed if' des'iredbut n' inost' cases-no advan ta'ge' is bbtairied th'ereb :3"
when thefracemizatibflih&befiical'riditd the: uo teri'aitistused kthet cationi exchange material must be-.-la"st1tong:acid:.:type; for :example,=- a: material in'" WhiC-BI'ITTthETaOidlJCI group: are sulfonic' 'acidfgroups.
Th'us th cationtezexchanget material; whenzusedin desired point -tHe Iysine :may" bei'sepa1:ated-ircrnii the phos horic acid-Tand ther'latter 'iS-ZSllil78.b18ffdf"' reuseintheraeemiiationiorocessiz variou'soneth ods maysbe utilized rfor::theiseparationi-oflysine Various :formstofthe zcation'i ex'change material. maysbe' utili'Zedbut :the acid form or ammonium formarezmost suitablerand the acid form 'is'usual'e necessity ':of fconvertingzthe ammonium; or other form to the free acid for reuse in' the racemization Step;
when: the? acid: form of aication exchan'ge-mathe'acidzformshould 'be-suiiiciently: strong to libfrom:thenhosphoricracida: For example: a'-'conr-'- ermimphosphoflc c d The following examples villustratethe invention;
Ezcample' 1' A soluti'on of 12.80' g.- (0.07 mole) of -l -1yslne droxides are examples of materials"suitable-"for Emon hydfgchloride--a,nd "10 35% phosphoric A preferredemethodiofrisolatingt thezlysirre fol'a lowi'r'i'g racemizatibn' ospassitneiunutedfrace mi'zation '-m-iictiire into contact with a :cadJon acid in 3U mlrwater was boileduntil the temperatu're reached 185 0. and! 'was then 'heated under reflux at"-185 to'192'C. for L hour. The solution;- & v after diliition with water, showed zero rotationexchange ma'terial in tlie' acid form whiclf ad indicatingi completeracemization. The-solution" was diluted to 1 liter and the lysine adsorbed on a column of cation-exchange resin. The resin was C1- (theory 32.4) and a water solution showed zero rotation. Example 2 To a water solution containing 0.07 mole free l(+)-lysine was added ml. 85% phosphoric acid. The mixture was heated until the temperature reached 170 C. and was then heated under reflux at 170-175 C. for 1 hour. The mixture;
after dilution with water, showed zero rotation.
boiled until the temperature reached 160 C. The
solution was then heated under reflux at 160 C. for 1 hour, diluted with water, and boiled minutes. It was found to be completely racemized.
2 Free lysine was recovered by adsorbing the lysine.
on a cation-exchange resin and eluting it with ammonia; the recovery'was 92.5 percent. Reso-.
lution of the lysine with d-camphoric 'acid in aqueous methanol gave a 40 percent yield 01' The lysine dihydrochloride, recovered as described in Example 1, weighed 14.44 g., 94 percent 0! the theoretical.
: Example 3 Toa water solution of 0.14 mole free lysine con-j I taining about 70% d( -isomer, was added 20 ml.
85% phosphoric acid. The mixture was boiled until the temperature reached 155 C. and was then heated under reflux at 155-165 C. for 1 hour.
The mixture, after dilution with water, showed zero rotation; The lysine dihydrochloride recov ered as described in Example 1, weighed 30.64 g.,
99.9 percent of the theoretical.
Example 4 To 68 g. of l(+) -lysine monohydrochloride was added 53.5 ml. 85% phosphoric acid and about 20 ml. water. The mixtures was boiled until the temperature reached 160 C. A reflux condenser was then attached and the mixture heated at 160 to 162 C. for 4 hours. Samples (5 ml.) were taken atvarious intervals, diluted to 25 ml., and the rotation observed. The results are summarized in the table below:
Time of Heating Observed Rom" at 160 to 162 C.
(Hmus) tion (Degrees) Example 5 The sameprocedure as in Example 4 was used. The racemization was run at 150 to 153 C. The results are summarized in the table below.
Observed Rota- Time of Heating 53 tion (Degrees) at 150-1 C.
Example 6 A water solution of 1.055 mole free lysine co'ntaining-about 70% d()-isomer was mixed with 143 ml. 85% phosphoric acid and the solution l(+)-lysine d-camphorate; 94% optically pure.
The methanol was stripped from the mother liquor which was then treated with 114 ml. phosphoric acid. The theoretical quantity of .d-camphoric acid was recovered by filtration and extraction with ether. The racemization and reconversion to free lysine was repeated with an' 89 percent recovery of lysine. This was resolved with d-camphoric acid and gave a 43 percent yield of optically pure -l(+)-lysine d-camphorate.
The resolution mother'liquor was again converted to lysine phosphate, racemized and reconverted tofree lysine. The recovery of lysinewas 87 percent.
Example 7 A series of runs similar to Example 6 was made in which lysine monohydrochloride was treated j with phosphoric acid and racemized at C.
The results are shown in thetable below.
Per Cent l(+)-lysine d-Oamphorate Recovery Free Lysine Racemization Per Cent cal Purity In the first run 97.5% optically pure l(+)-lysine monohydrochloride was used as the starting material.
The process of this invention is superior to the prior art process utilizing hydrochloric acid in the surprising and unexpected speed with which racemization is accomplished. It has been found that racemization of lysine with hydrochloric acid at 185 C. requires about 12 hours as compared with only about 1 hour for the process of this invention at a temperature of to C. Thus the racemization with phosphoric acid may be carried out at a much lower temperature and still require only a fraction of the time required by the prior art method. In addition racemiza-, tion with phosphoric acid may be carried out at atmospheric pressure.
Although the process of this invention is useful in racemizing optically active lysine from any source, it is of particular utility as a part of the resolution-racemization cycle involved in converting dl-lysine or, other mixture of l(+) and d()-lysine to a pure optical isomer. This procedure which may vary in detail consists essentially in resolving lysine by known methods, for example, the method described by Berg, separating the desired isomer," heating the remaining undesired isomer in combination with phosphoric acid to effect racemization, recovering a mixture of l(+) and d() -lysine and returning the latter to the resolution step.
When the lysine to be racemized in accordance with this invention is in the form of its compound with a resolving agent such as optically active camphoric acid, the latter may be recovered from solution upon the addition of phosphoric acid followed by filtration and extraction with ether and racemization is then carried out 7' by heating the-remaining solution of lysine in combination with? phosphoric :acid. "as described above.
'Throughout'this-specification and. in the appended claims the term lysine, unless :otherwise indicated, is'intended to include'within itsrscope bothufreelysineand alysine hydrochloride orrother salt oil-lysine.
I claim:
:1. Process for the racemization 'of'lysine-which comprises heating optically active lysineiin combination with phosphoric'acid.
2. Processfcr the racemiza'tion of lysine which comprisesxheating optically active lysine in combination with'p'hosphoric acidin the presence of water.
3. "The process of claim 2 wherein'the'temperaturetismaintainedat 11 0" to210 C.
:4. The process-of claim 2 wherein the concentration of phosphoric acid is at least equimolar;
15'; .Process which:comprises: resolving a mixture 0f-"'1(+)and'd( ).-lysine, separating a desired optically active isomer, heating the remaining undesired optically active isomer in combination with phosphoric acid and recovering a mixture of l(-|--) and d(- )--.lysine.
6. .Process which comprises resolving 'a .mixture of 1'(+) and d'( )--lysine into 1(+) -lysine and d()-lysine', separating :l(-|-.).-lysine, heating the remaining d( -lysine in combination with ph0sphoric acid in thepresenceioi'water andrecovering a mixture of l(+) and'd,(-) -lysine.
7. Process which comprises heating; optically active lysinein'combination with phosphoric'a'cidin the presence of water, passing an aqueous solutionof the racemized lysine obtained thereby into contact with'a cation-exchange materialgrecovering phosphoric acid, eluting said cation-exchange material with a material capable of displacing lysine from said cation-exchange material and recovering lysine, from the elutriate.
8. Process which comprises heating optically active lysine in combination with phosphoric acid,
in the presence of water, passing an aqueous solution of the racemized lysine obtained'thereby into contact with a cation-exchange material, re-
REFERENCES CITED The following references are of record in the file of this patent:
Neuberger: "Advances in Protein Chemistry,.
vol. 4, edited by Anson et al. v(Academic Press) p. 339 (1948.).
Block et. al.: The Amino Acid Composition 01. Proteins and Foods, .(Thomas) -.pp. 292-293

Claims (1)

1. PROCESS FOR THE RACEMIZATION OF LYSINE WHICH COMPRISES HEATING OPTICALLY ACTIVE LYSINE IN COMBINATION WITH PHOSPHORIC ACID.
US171245A 1950-06-29 1950-06-29 Racemization of amino acid Expired - Lifetime US2586154A (en)

Priority Applications (1)

Application Number Priority Date Filing Date Title
US171245A US2586154A (en) 1950-06-29 1950-06-29 Racemization of amino acid

Applications Claiming Priority (1)

Application Number Priority Date Filing Date Title
US171245A US2586154A (en) 1950-06-29 1950-06-29 Racemization of amino acid

Publications (1)

Publication Number Publication Date
US2586154A true US2586154A (en) 1952-02-19

Family

ID=22623076

Family Applications (1)

Application Number Title Priority Date Filing Date
US171245A Expired - Lifetime US2586154A (en) 1950-06-29 1950-06-29 Racemization of amino acid

Country Status (1)

Country Link
US (1) US2586154A (en)

Cited By (12)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
US2859244A (en) * 1956-09-28 1958-11-04 Dow Chemical Co Resolution of dl-lysine with d-camphoric acid
US2878282A (en) * 1957-02-19 1959-03-17 Du Pont Purification of lysine
US2894027A (en) * 1956-08-01 1959-07-07 Du Pont Purification of lysine
US2894026A (en) * 1956-08-01 1959-07-07 Du Pont Purification of lysine
DE1092923B (en) * 1956-05-22 1960-11-17 Dr Miroslav Semonsky Process for converting L-propanolamide- (2) or (+) - butanolamide- (2) of l-lysergic acid or l-isolysergic acid into the same amides of d-lysergic acid or d-isolysergic acid
US3213106A (en) * 1961-11-16 1965-10-19 Ajinomoto Kk Process of racemizing optically active alpha acids
US3231388A (en) * 1962-12-03 1966-01-25 Dow Chemical Co Cereal products fortified with l-lysine h3po4
US4169207A (en) * 1977-06-30 1979-09-25 Sumitomo Chemical Company, Limited Racemization of an optically active lysine alkyl ester
EP0214572A2 (en) * 1985-08-30 1987-03-18 Stauffer Chemical Company Racemization of optically active compounds having a chlorine substituted chiral carbon atom
EP0216196A2 (en) * 1985-08-30 1987-04-01 Stauffer Chemical Company Racemization of optically active compounds having a bromine substituted chiral carbon atom
WO2011001889A1 (en) 2009-06-29 2011-01-06 三菱瓦斯化学株式会社 METHOD FOR RACEMIZING OPTICALLY ACTIVE α-AMINO ACIDS
US9598353B2 (en) 2013-08-23 2017-03-21 Aminologics Co., Ltd. Process for the racemization of α-amino acids

Non-Patent Citations (1)

* Cited by examiner, † Cited by third party
Title
None *

Cited By (14)

* Cited by examiner, † Cited by third party
Publication number Priority date Publication date Assignee Title
DE1092923B (en) * 1956-05-22 1960-11-17 Dr Miroslav Semonsky Process for converting L-propanolamide- (2) or (+) - butanolamide- (2) of l-lysergic acid or l-isolysergic acid into the same amides of d-lysergic acid or d-isolysergic acid
US2894027A (en) * 1956-08-01 1959-07-07 Du Pont Purification of lysine
US2894026A (en) * 1956-08-01 1959-07-07 Du Pont Purification of lysine
US2859244A (en) * 1956-09-28 1958-11-04 Dow Chemical Co Resolution of dl-lysine with d-camphoric acid
US2878282A (en) * 1957-02-19 1959-03-17 Du Pont Purification of lysine
US3213106A (en) * 1961-11-16 1965-10-19 Ajinomoto Kk Process of racemizing optically active alpha acids
US3231388A (en) * 1962-12-03 1966-01-25 Dow Chemical Co Cereal products fortified with l-lysine h3po4
US4169207A (en) * 1977-06-30 1979-09-25 Sumitomo Chemical Company, Limited Racemization of an optically active lysine alkyl ester
EP0214572A2 (en) * 1985-08-30 1987-03-18 Stauffer Chemical Company Racemization of optically active compounds having a chlorine substituted chiral carbon atom
EP0216196A2 (en) * 1985-08-30 1987-04-01 Stauffer Chemical Company Racemization of optically active compounds having a bromine substituted chiral carbon atom
EP0216196A3 (en) * 1985-08-30 1988-09-21 Stauffer Chemical Company Racemization of optically active compounds having a bromine substituted chiral carbon atom
EP0214572A3 (en) * 1985-08-30 1988-09-28 Stauffer Chemical Company Racemization of optically active compounds having a chlorine substituted chiral carbon atom
WO2011001889A1 (en) 2009-06-29 2011-01-06 三菱瓦斯化学株式会社 METHOD FOR RACEMIZING OPTICALLY ACTIVE α-AMINO ACIDS
US9598353B2 (en) 2013-08-23 2017-03-21 Aminologics Co., Ltd. Process for the racemization of α-amino acids

Similar Documents

Publication Publication Date Title
US2586154A (en) Racemization of amino acid
WO1995016662A1 (en) Enantiomeric resolution
US2556907A (en) Resolution of lysine
US3213106A (en) Process of racemizing optically active alpha acids
EP0119804B1 (en) Novel method for optical resolution of dl-alpha-amino acid or (+)-alpha-phenylethanesulfonic acid
EP0664784B1 (en) Enantiomeric resolution
US2536360A (en) Racemization of lysine
JPS63500942A (en) How to obtain vanillin
US3994962A (en) Method of manufacturing optically active p-hydroxyphenylglycine
US4330484A (en) Diastereomeric salts of malic acid and 2-aminobutanol, and process for the resolution of rademis maic acid
EP0664781B1 (en) Enantiomeric resolution
US3190914A (en) Process for the preparation of amino acids
US4617155A (en) Novel lysine salt crystals and process for production thereof
IE47236B1 (en) Optical resolution of amino acids into optical antipodes
EP0036265A1 (en) Method of optical resolution of (+/-)-2-amino-1-butanol and/or (+/-) -mandelic acid
US2859244A (en) Resolution of dl-lysine with d-camphoric acid
US2934561A (en) Optically active salts of lysine and butane-2-sulfonic acid
US3683002A (en) Optical separation of methionine nitrile
US3862985A (en) Resolution of lysineamide
US5936118A (en) Process for chiral enrichment of optically active carboxylic acids or salts or esters thereof
EP0009722B1 (en) Optically active complex, alanine.ring-substituted mandelic acid, and the method for producing the same
US3409667A (en) Method for separating monochlorocarboxylic acids from dichlorocarboxylic acids
US3772364A (en) Method of obtaining the optical antipodes d(-)-and l(+)-alpha-azidophenylacetic acid
US2833823A (en) Method for the separation of optically active isomers of amphetamine
US2878282A (en) Purification of lysine