Lysergic Acid Amide
LSA.png

Lysergic Acid Amide (LSA) is a compound of natural origin that structurally resembles the potent artificial psychedelic compound LSD. LSA itself is classified as a sedative.

LSA occurs in the seeds of morning glories and similar plants as a decomposition product of lysergic acid hydroxyethylamide (LSH).

LSH is believed by some to have psychedelic properties similar to LSD. Animal tests have shown LSH produces stimulant effects similar to LSD, while LSA produces sedation.

LSA can be prepared by decomposing ergotoxine or ergotinine in alcoholic potassium hydroxide.[1] It's theoretically possible that LSH can also be decomposed to LSA in alcoholic potassium hydroxide.


Adducts of LSA

LSA Acetaldehyde LSH
LSA.png Acetaldehyde.png LSH.png

Lysergic Acid Hydroxyethylamide (LSH) is an adduct of lysergic acid amide and acetaldehyde.

The LSA adducts ergotoxine and ergotinine can be decomposed in alcoholic potassium hydroxide.[1] It's theoretically possible that LSH can also be decomposed to LSA in alcoholic potassium hydroxide.


Adducts of LSA (Anecdotal)


LSA Extraction

Groger's Method

Groger's method of obtaining a crude alkaloid extract of Heavenly Blue seeds was outlined by Marderosian, Guarin and Youngken in 1964 and includes the following steps:[4]

  1. Defat the ground seeds with petroleum ether.
  2. Extract with an acetone-tartaric acid solution.
  3. Evaporated off the acetone on a water bath.
  4. Neutralized the resulting tartaric acid solution.
  5. Extract with methylene chloride to obtain the alkaloids.

Chemical Properties

LSA Freebase

Synonyms: LSA; lysergamide; Ergine; (+)-Lysergamide; D-Lysergic acid amide
PubChem Compound ID: 442072
Molecular Weight: 267.32568 [g/mol]
Molecular Formula: C16H17N3O
XLogP3: 1.6
IUPAC Name: (6aR,9R)-7-methyl-6,6a,8,9-tetrahydro-4H-indolo[4,3-fg]quinoline-9-carboxamide
InChI: InChI=1S/C16H17N3O/c1-19-8-10(16(17)20)5-12-11-3-2-4-13-15(11)9(7-18-13)6-14(12)19/h2-5,7,10,14,18H,6,8H2,1H3,(H2,17,20)/t10-,14-/m1/s1
InChIKey: GENAHGKEFJLNJB-QMTHXVAHSA-N
Canonical SMILES: CN1CC(C=C2C1CC3=CNC4=CC=CC2=C34)C(=O)N
Isomeric SMILES: CN1C[C@@H](C=C2[C@H]1CC3=CNC4=CC=CC2=C34)C(=O)N
Appearance: Solutions of the base give a bluish-violet fluorescence in UV light, which is particularly evident in acetone as the solvent.[1] It gives an alkaline reaction with moist litmus paper.[1]
Solubility: soluble in methylene chloride.[4] Readily soluble in acetone, soluble in chloroform and ethyl acetate. Sparingly soluble in methyl alcohol, ethyl alcohol, ether, benzene, and almost insoluble in light petroleum and water.[1]
Crystallization in acetone: crystallizes readily from aqueous acetone in long colorless plates. Crystals from aqueous acetone are hydrates, stable in air but completely loses its water when kept over sulfuric acid in a vacuum desiccator.[1]
Crystallization in methyl alcohol: LSA is sparingly soluble in methyl alcohol and is conveniently separated from more soluble impurities by this solvent. It crystallizes in colorless prisms which contain one molecular proportion of methyl alcohol, which is retained with remarkable tenacity and is not completely removed after many hours of heating at 90 C in a vacuum.[1]
Decomposition: LSA is decomposed by alkali into the carboxylic acid lysergic acid.[2][3] LSA crystals from acetone decompose with frothing at 115 C and on further heating blacken and undergo further decomposition at about 230 C.[1] Crystals from methyl alcohol decompose with frothing at about 135 C; blackening with evolution of gas occurs at about 230 C.[1]

LSA Hydrochloride

Preparation: LSA hydrochloride can be prepared by treating a solution of LSA freebase in alcohol with dilute hydrochloric acid and adding ether.[1]
Appearance: colorless plates, crystallized from methyl alcohol by addition of ether or from water.[1]
Decomposition: on heating, LSA hydrochloride gradually becomes grey at approximately 200 C and decomposes with frothing and formation of a black tar at 255-260 C.[1]

LSA Hydrobromide

Preparation: LSA hydrobromide can be prepared by treating a solution of the LSA freebase in acetone with hydrobromic acid, and crystallized by the addition of ether.[1]
Appearance: It crystallizes in colorless prisms.[1]
Decomposition: contracts at about 200 C, and gradually darkens and at 260 C, and decomposes with evolution of gas and the formation of a black tar.[1]

LSA Nitrate

Preparation: LSA nitrate can be prepared by treating a solution of LSA freebase in acetone and alcohol with dilute nitric acid and adding ether.[1]
Appearance: It crystallizes in long colorless plates.[1]
Decomposition: become grey at approximately 200 C and decomposes with the evolution of gas and blackening at 225-230 C.[1]

LSA Picrolonate

Preparation: LSA picrolonate can be prepared in acetone solution, from which its separated.[1]
Appearance: pale yellow plates.[1]
Decomposition: darkens at 210 C and decomposes at 215 C, giving a black tar.[1]

LSA Perchlorate

Preparation: LSA perchlorate can be prepared by adding a solution of sodium perchlorate in water to a solution of LSA freebase in water containing a little acetic acid.[1]
Appearance: fine needles.[1]
Crystallization: can be recrystallized from alcohol.
Decomposition: gradually darkens at about 200 C and decomposes at 225 C, giving a black tar.[1]
Solubility: sparingly soluble in alcohol.[1]


See Also


Bibliography
1. The alkaloids of ergot. Part III. Ergine, a new base obtained by the degradation of ergotoxine and ergotinine
Sydney Smith and Geoffrey Millward Timmis J. Chem. Soc., 1932, Pages 763-766. DOI: 10.1039/JR9320000763
2. The alkaloids of ergot. Part V. The nature of ergine
Sydney Smith and Geoffrey Millward Timmis J. Chem. Soc., 1934, Pages 674-675. DOI: 10.1039/JR9340000674
3. The alkaloids of ergot. Part VII. isoErgine and isolysergic acids
Sydney Smith and Geoffrey Millward Timmis J. Chem. Soc., 1936, Pages 1440-1444. DOI: 10.1039/JR9360001440
4. A uterine stimulant effect of extracts of morning glory seeds
der Marderosian AH, Guarin A, de Feo J, Youngken W. Psychedelic Review, 1964, Pages 317-323, web link: 013317der.pdf
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