Active constituents: Forskolin, a chemical found in coleus,
activates the enzyme adenylate cyclase.2 This enzyme is a turnkey compound that
initiates a cascade of critical events within every cell of the body. Adenylate cyclase and
the chemicals it activates comprise a “second messenger” system that is
responsible for carrying out the complex and powerful effects of hormones in the body.
Stimulation of the second messenger system by forskolin leads to blood vessel
dilation,3 inhibition of allergic reactions,4 and an increase in thyroid
hormone secretion.5 Forskolin has other properties as well, including inhibition of
the pro-inflammatory substance known as platelet-activating factor (PAF)6 and
inhibition of the spread of cancer cells.7
Studies in healthy humans, including at least one double-blind trial, have shown that
direct application of an ophthalmic preparation of forskolin to the eyes lowers eye
pressure,8 9 thus reducing the risk of glaucoma. Direct application of the whole herb to the eyes has
not been studied and is not recommended.
Forskolin may help dilate blood vessels and improve the forcefulness with which the heart
pumps blood. A preliminary trial found that forskolin reduced blood pressure and improved heart function in people with cardiomyopathy.10 It is unknown if oral
coleus extracts would have the same effect. A small double-blind trial found that inhaled
forskolin could decrease lung spasms in
asthmatics.11 It is unclear if oral ingestion of coleus extracts will provide
similar benefits.
References:
1. Dubey MP, Srimal RC, Nityanand S, Dhawan BN. Pharmacological studies
on coleonol, a hypotensive diterpene from Coleus forskohlii. J Ethnopharmacol
1981;3:1–13.
2. Seamon KB, Daly JW. Forskolin: A unique diterpene activator of
cAMP-generating systems. J Cyclic Nucleotide Res 1981;7:201–24 [review].
3. Wysham DG, Brotherton AF, Heistad DD. Effects of forskolin on cerebral
blood flow: Implications for the role of adenylate cyclase. Stroke
1986;17:1299–303.
4. Marone G, Columbo M, Triggiani M, et al. Forskolin inhibits the
release of histamine from human basophils and mast cells. Agents Actions
1986;18:96–9.
5. Roger PP, Servais P, Dumont JE. Regulation of dog thyroid epithelial
cell cycle by forskolin, an adenylate cyclase activator. Exp Cell Res
1990;172:282–92.
6. Wong S, Mok W, Phaneuf S, et al. Forskolin inhibits
platelet-activating factor binding to platelet receptors independently of adenylyl cyclase
activation. Eur J Pharmacol 1993;245:55–61.
7. Agarwal KC, Parks RE. Forskolin: A potential antimetastatic agent.
Int J Cancer 1983;32:801–4.
8. Caprioli J, Sears M. Forskolin lowers intraocular pressure in rabbits,
monkeys and man. Lancet 1983;1:958–60.
9. Badian M, Dabrowski J, Grigoleit HG, et al. Effect of forskolin eye
drops on intraocular pressure in healthy males. Klin Monatsbl Augenheilkd
1984;185:522–6 [in German].
10. Kramer W, Thormann J, Kindler M, Schlepper M. Effects of forskolin on
left ventricular function in dilated cardiomyopathy. Arzneim Forsch
1987;37:364–7.
11. Bauer K, Dietersdorfer F, Sertl K, et al. Pharmacodynamic effects of
inhaled dry powder formulations of fenoterol and colforsin in asthma. Clin Pharmacol
Ther 1993;43:76–83.
12. Bone K, Morgan M. Clinical Applications of Ayurvedic and Chinese
Herbs: Monographs for the Western Herbal Practitioner. Queensland, Australia:
Phytotherapy Press, 1996.
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purposes only. It is based on scientific studies (human, animal, or in vitro),
clinical experience, or traditional usage as cited in each article. The results reported may
not necessarily occur in all individuals. For many of the conditions discussed, treatment with
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before making any changes in prescribed medications. Information expires December 2003.