Enantiomers Separation. Method 1.1. R,R-Tartaric Acid
Literature Information
Optical rotation at λ=589 nm of Na D-lines, cuvette 1 dm (100 mm)
Substance | Optical rotation [α]D20 | Concentration c (g/100 ml) | Solvent |
D-(-)-Tartaric acid CAS 147-71-7 | -11.5 – (-13.5) -11 – (-13) -11.9 -12.2 | 10 20 20 20 | H2O H2O H2O H2O |
L-(+)-Tartaric acid CAS 87-69-4 | +11.5 to +13.5 +13.0±1.0 +12.2 | 10 20 20 | H2O H2O H2O |
S-(+)-Methamphetamine | +14.0 - +20.0 +16 to +19 +17.9 | 1 (FB) 2 (hydrochloride) 3 (hydrochloride) | 1М HCl H2O H2O |
R-(-)-Methamphetamine | −14 – (-15) −24.7 −18.2 -17.4 | 1 (FB) 5 (hydrochloride) 0.115 (hydrochloride) 3 (hydrochloride) | 1M HCl H2O H2O H2O |
L-Ephedrine | -33 – (-33.5) -29.5 – (-32) | 5 (hydrochloride) 5 (sulphate) | H2O H2O |
D-Pseudoephedrine | +51 +62 +61 - +62.5 | 0.6 (FB) 0.8 (hydrochloride) 5 (hydrochloride) | EtOH EtOH H2O |
S-(+)-Amphetamine | +24.2 | 5 (hydrochloride) | H2O |
R-(-)-Amphetamine | -24.7 | 5 (hydrochloride) | H2O |
(R)-(-)-Methamphetamine (R,R)-tartrate | +4.77 | 5 | H2O |
(S)-(+)-Methamphetamine (R,R)-tartrate | +22.1 | 5 | H2O |
References
- Thermo Fisher Scientific Data https://www.thermofisher.com/order/catalog/product/137862500?SID=srch-srp-137862500
- Merck Index, 15th ed., O’Neil, M.J., Royal Society of Chemistry, Cambridge, UK, 2013
- European Pharmacopoeia, 10th ed., Monograph, 2019
- Dobšíková K.; Michal, P.; Spálovská, D.; Kuchař, M.; Paškanová, N.; Jurok, R.; Kapitán, J.; Setnička V. Conformational analysis of amphetamine and methamphetamine: a comprehensive approach by vibrational and chiroptical spectroscopy. Analyst 2023, 148, 1337–1348. https://pubs.rsc.org/en/content/articlelanding/2023/an/d2an02014a DOI https://doi.org/10.1039/D2AN02014A
- The Japanese Pharmacopoeia, 17th ed.; Ministry of Health, Labour and Welfare: Tokyo, Japan, 2016
- O'Neil M.J., Smith A., Heckelman P.E. The Merck Index An Encyclopedia of Chemicals, Drugs, and Biologicals. 1996
- European Pharmacopoeia v8.0 (2014)
- Elemer Fogassy, Maria Acs, Ferenc Faigl. Pseudosymmetry and Chiral Discrimination in Optical Resolution via Diastereoisomeric Salt Formation. The Crystal Structures of (R)- and (S)-N-Methylamphetamine Bitartrates (RMERTA and SMERTA). J. CHEM. SOC., PERKIN TRANS. II, pp. 1881-1886, 1986. doi:10.1039/P29860001881
537-46-2 CAS MSDS (D-METHAMPHETAMINE) Melting Point Boiling Point Density CAS Chemical Properties
ChemicalBook Provide 537-46-2(D-METHAMPHETAMINE)Melting Point Boiling Point Density,537-46-2(D-METHAMPHETAMINE) CAS Chemical Properties MSDS.www.chemicalbook.com(S)-(+)-Methamphetamine
ChemSpider record containing structure, synonyms, properties, vendors and database links for (S)-(+)-Methamphetamine, 537-46-2, Metamfetamine, MYWUZJCMWCOHBA-VIFPVBQESA-N
www.chemspider.com
Main Calculation Formulas
Calculation of the standard rotation angle:
Calculation of the observed angle of rotation:
Were:
[α]D20 – angle of rotation at temperature 20℃ and at λ=589 nm of Na D-lines
[α] – observed rotation angle on a polarimeter
l – length of the cuvette, 20 мм = 0.2 дм
с – Concentration, g/100 ml
FB Obtaining
The process of FB separation is shown in Scheme 1
Scheme 1
Starting Reagents and Materials
- 120 g Methamphetamine hydrochloride
- 1300-1500 ml H2O
- 30 g NaOH
- 60 g NaCl
- 250-300 ml DCM
- 2 g molecular sieves 3A
- Separations funnel 2000 ml
- Beakers
- Funnel
- Paper filter
- Indicator strips рН 0-14
Synthesis
120 g of Methamphetamine hydrochloride is dissolved in 400-500 ml of water.
Fig 1
Stir until the Methamphetamine hydrochloride is completely dissolved.
Fig 2
A sodium hydroxide solution is prepared: 30 g NaOH in 200 ml water
Fig 3
The alkali solution is cooled to room temperature.
Fig 4
A solution of sodium chloride is prepared: 60 g and 200 ml of water.
Fig 5
The mixture is stirred until NaCl completely dissolved.
Fig 6
The Methamphetamine hydrochloride solution is transferred into a separatory funnel
Fig 7
A solution of Methamphetamine hydrochloride (especially after long-term storage) is purified with 4 portions of 50-70 ml of DCM.
Fig 8
The mixture is shaken well.
Fig 9
The mixtures are given time for the layers to separate. The DCM layer is discarded.
Fig 10
Purification is carried out until a colorless layer of DCM is obtained.
Fig 11
After purification of DCM, the Methamphetamine hydrochloride solution is filtered through a paper filter. The funnel and filter are rinsed with new portions of water.
Fig 12
Filtration of Methamphetamine hydrochloride solution
Fig 13
Filtered solution of Methamphetamine hydrochloride
Fig 14
The filtered solution of Methamphetamine hydrochloride is transferred to a clean separatory funnel.
Fig 15
A prepared solution of sodium hydroxide at a temperature not higher than room temperature is added to the solution of Methamphetamine hydrochloride.
Fig 16
For better separation of Methamphetamine FB, a sodium chloride solution is added.
Fig 17
The mixture is kept for 30-60 minutes.
Fig 18
The lower alkaline layer is separated and discarded or subjected to extraction.
Fig 19
The FB layer is kept for 20-30 minutes.
Fig 20
FB layer
Fig 21
The FB layer is drained into a sealed bottle for further storage.
Fig 22
2g of 3A molecular sieves are added to the FB
Fig 23
Separated FB and dried with 3A molecular sieves. FB weight 94.2 g (yield 97%)
Fig 24
EXPERIMENT 1
Method 1.1. Resolution with Using R,R-Tartaric Acid
The separation process proceeds according to Scheme 2Scheme 2
Starting Reagents and Materials
- 10 g FB + 20 ml EtOH(abs)
- 10 g L-(+)-Tartaric acid + 60 ml EtOH(abs) full dissolution by stirring on a magnetic stirrer
- 3 days of stirring at 5-10℃
Synthesis
R,R-tartaric acid (L-(+)-Tartaric acid) CAS 87-69-4
Fig 25
R,R-tartaric acid (L-(+)-Tartaric acid) (10 g) was dissolved in absolute ethanol (60 ml)
Fig 26
Full dissolution is carried out by using a magnetic stirrer
Fig 27
10 g of Methamphetamine free base is collected and placed into a flask.
Fig 28
Fig 29
Racemic Methamphetamine free base (10 g) was dissolved in absolute ethanol (20 ml)
Fig 30
Fig 31
A solution of R,R-tartaric acid (L-(+)-Tartaric acid) is added to a solution of Methamphetamine FB in ethanol.
Fig 32
Fig 33
Then the RM is stirred for 72 hours at T = 5-10℃
Fig 34
After some time, a sediment precipitation in the RM
Fig 35
After 72 hours of stirring, the precipitate is filtered off using a porous filter.
Fig 36
The residue in the flask is washed off with a small portion of alcohol 15-20 ml
Fig 37
The filtered precipitate is dried directly in a vacuum and then for 48 hours in a desiccator over alkali.
Fig 38
Fig 39
The dried Methamphetamine tartrate (precipitate). Yield 11.82 g (59.1%)
Fig 40
The mother liquor is evaporated.
Fig 41
Fig 42
Fig 43
Fig 44
The mother liquor does not crystallize after evaporation. This can occur for several reasons: alcohol-soluble impurities (including resins) migrate into the mother liquor, as well as excess tartaric acid.
Fig 45
Fig 46
Since tartrate is very difficult to convert into dry residue, Methamphetamine tartrate was converted to Methamphetamine hydrochloride. 100-150 ml of 20% sodium hydroxide is prepared.
Fig 47
An alkali solution is added to the Methamphetamine tartrate syrup.
Fig 48
Fig 49
The resulting homogeneous RM is transferred to a separatory funnel.
Fig 50
Extraction of FB is carried out with 3-4 portions of DCM, 30-50 ml each.
Fig 51
Fig 52
The mixture is shaken well and left to stand to separate the layers.
Fig 53
The DСM layer is separated (total volume 150-200 ml).
Fig 54
Hydrochloric acid is added to the separated DCM layer and stirred for 20-30 minutes. The aqueous layer should have an acidic or slightly acidic pH.
Fig 55
The mixture is transferred to a separatory funnel. The DCM layer is separated and discarded.
Fig 56
The aqueous acidic layer is evaporated until crystallization occurs. It is dried in a desiccator over alkali under vacuum for 24-48 hours. It is washed with petroleum ether if further purification is necessary.
Fig 57
Fig 58
Methamphetamine hydrochloride. Yield 6.7 g (33.5%)
Fig 59
Determination of Optical Rotation of the Obtained Substances
To determine the optical rotation, a polarimeter with a cuvette length of 20 mm was used.
For the separated M tartrate precipitate ((R)-(-)-N-methylamphetamine (R,R)-tartrate (RMERTA)), a standard solution of 0.5 g in 10 ml of water is prepared. A certified Class A volumetric flask is used.
For the separated M tartrate precipitate ((R)-(-)-N-methylamphetamine (R,R)-tartrate (RMERTA)), a standard solution of 0.5 g in 10 ml of water is prepared. A certified Class A volumetric flask is used.
Fig 60
The values of the observed rotation angle in 3 measurements on a polarimeter showed 0.12, which corresponds to the rotation angle [α]D20 = +12 (literature data is +4.77), which approximately corresponds to the optical enantiomer (R)-(-)-N-methylamphetamine (R,R)-tartrate
Fig 61
For the mother liquor, which was converted into M hydrochloride, a solution of 0.3 g in 10 ml of water was prepared.
Fig 62
The values of the observed rotation angle on the polarimeter showed 0.11 in 3 measurements, which corresponds to the rotation angle [α]D20=+18.3 (literature data is +17.9) and the optical enantiomer (S)-(+)-N-methylamphetamine hydrochloride.
Fig 63
Conclusions
- The method allows to separate racemic Methamphetamine into levo- and dextro-Methamphetamine with a yield of 59.1% and 33.5%, respectively.
- (R)-(-)-N-methylamphetamine (levo-) remains in the precipitate in the form of (R,R)-tartrate. (S)-(+)-N-methylamphetamine (dextro-) also remains in the mother liquor in the form of the more soluble (R,R)-tartrate. This creates further problems in separating the dextro-isomer, since impurities (pollutants, resins, etc.), as well as excess of (R,R)-tartaric acid, pass into the mother liquor.
- According to obtained optical rotation values, it is show that the precipitated (R)-(-)-N-methylamphetamine (R,R)-tartrate contains a significant portion of (S)-(+)-N-methylamphetamine (R,R)-tartrate. Recrystallization is required for more complete separation.
- Using the separated levo-M, it is possible to regenerate enantiomerically pure tartaric acid and use (R)-(-)-N-methylamphetamine FB for further separation of racemic tartaric acid and for generating a quantity of enantiomeric separation reagents.
Last edited:
