Isoergine

Isoergine

Clinical data
Other names	Isolysergic acid amide; D-Isolysergic acid amide; Erginine; Isolysergamide; (+)-Isolysergic acid amide; Iso-LA; Iso-LA-819; Iso-LSA; d-Isolysergamide; 6-Methyl-9,10-didehydroergoline-8α-carboxamide
Routes of administration	Oral^[1]
Drug class	Serotonin receptor modulator; Serotonergic psychedelic; Hallucinogen
ATC code	None
Identifiers
IUPAC name (6aR,9S)-7-methyl-6,6a,8,9-tetrahydro-4H-indolo[4,3-fg]quinoline-9-carboxamide
CAS Number	2889-26-1
PubChem CID	12309749
ChemSpider	32698654
UNII	90DGH6Y8E9
CompTox Dashboard (EPA)	DTXSID80183082
Chemical and physical data
Formula	C₁₆H₁₇N₃O
Molar mass	267.332 g·mol⁻¹
3D model (JSmol)	Interactive image
SMILES CN1C[C@H](C=C2[C@H]1CC3=CNC4=CC=CC2=C34)C(=O)N
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+/m0/s1 Key:GENAHGKEFJLNJB-IINYFYTJSA-N

Use and effects

Summarize

Perspective

Isoergine occurs naturally in morning glory species, including Ipomoea tricolor (tlitliltzin), Ipomoea corymbosa (ololiuhqui), and Argyreia nervosa (Hawaiian baby woodrose).^[3]^[4]^[6] It has been found to constitute 8 to 35% of total alkaloid content relative to 5 to 58% for ergine.^[4]^[6]

Albert Hofmann, the discoverer of LSD's psychedelic effects, tried 2 mg isoergine orally and experienced feelings of unreality, detachment from the outside world, feelings of mental emptiness, tiredness, and apathy, though no specific sensory distortions were mentioned.^[4]^[5]^[1]^[8]^[10] He described its effects as similar to those of ergine, which he had tested at doses of up to 2 mg.^[10] Subsequently Heim and colleagues assessed ergine at higher doses of 3 to 6 mg orally and observed toxic-like effects, while isoergine at 2 to 5 mg orally produced notable hallucinogenic effects.^[2]^[3]^[1]^[9] The psychedelic effects of isoergine observed in this study included some euphoria, synaesthesia, and altered time perception.^[3]^[1]^[9] However, although hallucinogenic, isoergine's effects have been described as not LSD-like.^[2]^[11] The presence of hallucinogenic effects of isoergine have also been described as quite unusual for an isolysergamide derivative.^[11]

It is thought that ergine and isoergine together may account for most or all of the effects of morning glory seeds, with ergine producing intoxication, sedation, and autonomic side effects and isoergine producing hallucinogenic effects.^[3]^[1]^[2]^[4]^[6]^[9]^[12] Conversely, other notable constituents, including elymoclavine, lysergol, and chanoclavine, produced no psychoactive or hallucinogenic effects in humans.^[1]^[2]^[13]^[14]^[15]^[16]^[8]^[9] Ergometrine, which is a minor constituent representing up to 8% of total alkaloids, is known to produce psychedelic effects only in higher amounts (2–10 mg) than those in typical doses of morning glory seeds and hence is thought to not contribute to the effects of the seeds either.^[16]^[1]^[3]^[17]^[18]^[4] Moreover, ergometrine is present in Ipomoea tricolor and Argyreia nervosa but not in Ipomoea corymbosa.^[1]^[3] Isoergine being responsible for the hallucinogenic effects of morning glory seeds is also supported by animal studies.^[3]^[1]^[12] However, the poorly-stable lysergic acid hydroxyethylamides (LSHs) might still alternatively be involved in the psychedelic effects of morning glory seeds per Alexander Shulgin.^[7]

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Pharmacology

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Perspective

Pharmacodynamics

Isoergine shows affinity for serotonin receptors labeled with serotonin or LSD in rat brain membranes.^[19]^[20]^[21] It has about 10- to 25-fold lower affinity for these receptors than serotonin or LSD and has the same affinity as ergine and iso-LSD (IC₅₀Tooltip half-maximal inhibitory concentration = 100–200 nM for isoergine, 200 nM for ergine and iso-LSD, and 8–10 nM for LSD).^[19]^[20]^[21] No other receptor interaction data are available for isoergine as of 2020.^[3] However, computer-predicted receptor affinities are available for ergine/isoergine (stereochemistry not taken into account).^[22] The drug is said to have about 4.3% of LSD's antiserotonergic potency in vitro.^[23]^[24] It is 5- to 33-fold less potent than LSD in producing behavioral changes in the conditioned avoidance test in rodents.^[3]^[4]^[25]^[12]

Pharmacokinetics

The pharmacokinetics of isoergine in rodents have been studied.^[3]^[12] Isoergine is much less lipophilic than LSD, with log P values of 0.95 and 2.95, respectively.^[21] This might influence its pharmacological properties, for instance reducing its blood–brain barrier permeability.^[21] However, isoergine showed a similar ratio of brain-to-plasma levels as LSD in rodents.^[12]

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Chemistry

Derivatives

Derivatives of isoergine include isolysergic acid diethylamide (iso-LSD), isolysergic acid hydroxyethylamide (iso-LSH), and ergometrinine (isoergometrine; isolysergic acid propanolamide), among others.^[2]^[26]^[4]^[27] With the apparent exception of isoergine, isolysergamides, such as iso-LSD, have been found to be inactive as psychedelics in humans.^[28]^[29]^[30]^[31]^[32]^[11]

History

Isoergine was first identified by Sidney Smith and Geoffrey Timmis in 1936 via hydrolysis of ergot alkaloids.^[1]^[33] This followed the identification of ergine in the same way in 1932.^[1]^[34] Isoergine was first synthesized by Albert Hofmann and colleagues by 1949.^[1]^[35] Subsequently, it was isolated by Hofmann and colleagues in morning glory seeds in 1960.^[36]^[8]^[37] The psychoactive effects of isoergine were first described by Hofmann in 1963.^[4]^[1]^[8] Heim and colleagues more clearly substantiated the hallucinogenic effects of isoergine and its role in producing the psychedelic effects of morning glory seeds in 1968.^[3]^[1]^[9]

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Use and effects

Pharmacology

Pharmacodynamics

Pharmacokinetics

Chemistry

Derivatives

History

See also

References

External links

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