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minus-squaredai@lemmy.worldlinkfedilinkEnglisharrow-up2arrow-down1·15 hours agoBerman et al., Sci. Adv. 12, eaeb3034 (2026) 1 April 2026 S c i e n c e A d v A n c e S | R e S e A R c h A R t i c l e 1 of 18 P L A N T S C I E N C E S Complete biosynthesis of psychedelic tryptamines from three kingdoms in plants Paula Berman1,2 *†, Janka Höfer 1 †, Herschel Mehlman1 , Efrat Almekias-Siegl1 , Olga Khersonsky 3 , Younghui Dong 4 ‡, Uwe Heinig4 , Liron Sulimani5 , Let Kho Hao1,2 , Shahar Cohen2 , Yoav Peleg4 , Sagit Meir1 , Ilana Rogachev 1 , David Meiri5 , Sarel J. Fleishman3 , Asaph Aharoni1 * Psychedelic indolethylamines with therapeutic potential are naturally produced in plants, fungi, and animals. Here, we elucidated the complete N,N-dimethyltryptamine (DMT) biosynthetic pathway in hallucinogenic plant species traditionally used in shamanic rituals for spiritual healing. Leveraging the similarities in their chemical structures, we reconstructed in one plant assay the full biosynthetic pathways of five renowned natural psyche- delics; psilocin and psilocybin found in mushrooms, DMT from plants, and bufotenin and 5-methoxy-DMT secret- ed by the Sonoran Desert toad. We further engineered halogenated analogs of these molecules, which do not naturally occur in plants and exhibit prospective therapeutic potential for psychiatric conditions. Blending cata- lytic functions across the tree of life, coupled with metabolic engineering guided by rational protein design of mutant enzymes, enabled substantially more efficient in planta production of the indolethylamine components. This work establishes a versatile platform for concurrent biosynthesis and diversification of psychoactive indole- thylamines, paving the way for their production in plants. INTRODUCTION For thousands of years, psychedelic substances have been used by indigenous cultures as entheogens in rituals intended to induce al- tered states of consciousness for spiritual and therapeutic purposes. Psilocybin-containing mushrooms were central to ancient Aztec ceremonies (1), while N,N-dimethyltryptamine (DMT), the pri- mary psychoactive component of ayahuasca, has long been used in traditional Amazonian rituals. This ceremonial brew combines Psychotria viridis (a natural source of DMT) with Banisteriopsis caapi, which provides β-carboline monoamine oxidase (MAO) inhibi- tors that render DMT orally active (1, 2). Similarly, 5-methoxy-N,N- dimethyltryptamine (5-MeO-DMT), found in the secretion of the Sonoran Desert toad (Incilius alvarius) and in several plant spe- cies, is thought to have been used ceremonially by indigenous groups in northern Mexico (3). 5-MeO-DMT has been described as the most potent DMT analog, being about 4- to 10-fold more po- tent than DMT in humans and is known to induce psychedelic ex- periences that are distinct from those of DMT (4). Knowledge of the traditional use of these molecules has fueled contemporary therapeutic interest in psychedelics as treatments for neuropsychiat- ric conditions. Recent studies have shown that classical indolethylamine psy- chedelics promote neuroplasticity and modulate serotonergic cir- cuits, primarily through 5-HT 2A receptor activation (5–7). These compounds have demonstrated therapeutic potential for depression, anxiety, posttraumatic stress disorder, and addiction (5–8), with psi- locybin receiving Food and Drug Administration Breakthrough Therapy designation for major depressive disorder in 2019 (6, 7). Although widely considered hallucinogenic, psilocybin itself func- tions as a prodrug, undergoing enzymatic dephosphorylation in the digestive tract and liver to produce psilocin, the active compound responsible for its psychoactive effects. DMT is produced by a broad range of plant species and, in low abundance, by certain animals (2). When administered via smoking or intravenous injection, it pro- duces rapid and intense psychoactive effects that typically peak with- in 5 min and subside within 30 min, due to rapid metabolism by MAO enzymes in the liver. Coadministration with MAO inhibitors can extend the half-life of DMT in vivo (2). The traditional use of ayahuasca exemplifies how combining compounds from different sources can enable oral activity; however, such combinations require carefully balanced dosing to mitigate adverse effects associated with MAO inhibition (9). The expanding clinical interest in psychedelics as therapeutics has sparked the need for scalable and versatile production platforms and structural diversification (10, 11). Traditionally, the supply of psychedelics relies on natural producers, mainly plants, fungi, and the Sonoran Desert toad. Harvesting these organisms for their psy- choactive compounds raises ecological and ethical concerns, being increasingly threatened by habitat loss and overexploitation (12). While synthetic routes for these compounds are available and, in some cases, relatively straightforward, they still require compound- specific reactants, can lead to unwanted intermediates and prod- ucts, and require several processing steps (2, 13, 14). Biocatalys
Berman et al., Sci. Adv. 12, eaeb3034 (2026) 1 April 2026
S c i e n c e A d v
A
n c e
S
| R e
S
e
A R
c h A
R
t i c l e
1 of 18
P L A N T S C I E N C E S
Complete biosynthesis of psychedelic tryptamines from
three kingdoms in plants
Paula Berman1,2
*†, Janka Höfer 1
†, Herschel Mehlman1
, Efrat Almekias-Siegl1
, Olga Khersonsky 3
,
Younghui Dong 4
‡, Uwe Heinig4
, Liron Sulimani5
, Let Kho Hao1,2
, Shahar Cohen2
, Yoav Peleg4
,
Sagit Meir1
, Ilana Rogachev 1
, David Meiri5
, Sarel J. Fleishman3
, Asaph Aharoni1
*
Psychedelic indolethylamines with therapeutic potential are naturally produced in plants, fungi, and animals.
Here, we elucidated the complete N,N-dimethyltryptamine (DMT) biosynthetic pathway in hallucinogenic plant
species traditionally used in shamanic rituals for spiritual healing. Leveraging the similarities in their chemical
structures, we reconstructed in one plant assay the full biosynthetic pathways of five renowned natural psyche-
delics; psilocin and psilocybin found in mushrooms, DMT from plants, and bufotenin and 5-methoxy-DMT secret-
ed by the Sonoran Desert toad. We further engineered halogenated analogs of these molecules, which do not
naturally occur in plants and exhibit prospective therapeutic potential for psychiatric conditions. Blending cata-
lytic functions across the tree of life, coupled with metabolic engineering guided by rational protein design of
mutant enzymes, enabled substantially more efficient in planta production of the indolethylamine components.
This work establishes a versatile platform for concurrent biosynthesis and diversification of psychoactive indole-
thylamines, paving the way for their production in plants.
INTRODUCTION
For thousands of years, psychedelic substances have been used by
indigenous cultures as entheogens in rituals intended to induce al-
tered states of consciousness for spiritual and therapeutic purposes.
Psilocybin-containing mushrooms were central to ancient Aztec
ceremonies (1), while N,N-dimethyltryptamine (DMT), the pri-
mary psychoactive component of ayahuasca, has long been used
in traditional Amazonian rituals. This ceremonial brew combines
Psychotria viridis (a natural source of DMT) with Banisteriopsis caapi,
which provides β-carboline monoamine oxidase (MAO) inhibi-
tors that render DMT orally active (1, 2). Similarly, 5-methoxy-N,N-
dimethyltryptamine (5-MeO-DMT), found in the secretion of
the Sonoran Desert toad (Incilius alvarius) and in several plant spe-
cies, is thought to have been used ceremonially by indigenous
groups in northern Mexico (3). 5-MeO-DMT has been described
as the most potent DMT analog, being about 4- to 10-fold more po-
tent than DMT in humans and is known to induce psychedelic ex-
periences that are distinct from those of DMT (4). Knowledge of
the traditional use of these molecules has fueled contemporary
therapeutic interest in psychedelics as treatments for neuropsychiat-
ric conditions.
Recent studies have shown that classical indolethylamine psy-
chedelics promote neuroplasticity and modulate serotonergic cir-
cuits, primarily through 5-HT 2A receptor activation (5–7). These
compounds have demonstrated therapeutic potential for depression,
anxiety, posttraumatic stress disorder, and addiction (5–8), with psi-
locybin receiving Food and Drug Administration Breakthrough
Therapy designation for major depressive disorder in 2019 (6, 7).
Although widely considered hallucinogenic, psilocybin itself func-
tions as a prodrug, undergoing enzymatic dephosphorylation in the
digestive tract and liver to produce psilocin, the active compound
responsible for its psychoactive effects. DMT is produced by a broad
range of plant species and, in low abundance, by certain animals (2).
When administered via smoking or intravenous injection, it pro-
duces rapid and intense psychoactive effects that typically peak with-
in 5 min and subside within 30 min, due to rapid metabolism by
MAO enzymes in the liver. Coadministration with MAO inhibitors
can extend the half-life of DMT in vivo (2). The traditional use of
ayahuasca exemplifies how combining compounds from different
sources can enable oral activity; however, such combinations require
carefully balanced dosing to mitigate adverse effects associated with
MAO inhibition (9).
The expanding clinical interest in psychedelics as therapeutics
has sparked the need for scalable and versatile production platforms
and structural diversification (10, 11). Traditionally, the supply of
psychedelics relies on natural producers, mainly plants, fungi, and
the Sonoran Desert toad. Harvesting these organisms for their psy-
choactive compounds raises ecological and ethical concerns, being
increasingly threatened by habitat loss and overexploitation (12).
While synthetic routes for these compounds are available and, in
some cases, relatively straightforward, they still require compound-
specific reactants, can lead to unwanted intermediates and prod-
ucts, and require several processing steps (2, 13, 14). Biocatalys