Research links chili compound to lower blood pressure

By Nathan Gray

- Last updated on GMT

Related tags Blood pressure Blood vessel Nitric oxide

A new study has linked frequent intake of capsaicin to a reduction in blood pressure, the first time that the effect has been observed for long-term use.

The study provides fresh evidence to support the theory that capsaicin can improve blood vessel function and lower blood pressure, which lends support to it use as a dietary supplement or functional ingredient in foods.

Published in the journal Cell Metabolism​, it suggests that the blood vessel receptor TRPV1 is stimulated by capsaicin, mediating a beneficial effect in the cardiovascular system by promoting nitric oxide release and lowering blood pressure.

The researchers, led by Zhiming Zhu from Third Military Medical University in China, wrote: “TRPV1 activation through dietary capsaicin may represent a promising intervention of lifestyle in high-risk populations with hypertension and related vascular disorders.”

Health Benefits

Capsaicin is found in the white pulp of chili peppers and is the compound that gives them their ‘heat’, causing a burning sensation in any tissue it comes into contact with. The burning pain caused by capsaicin is down to its selective binding of capsaicin to the receptor TRPV1.

Transient receptor potential channels (TRPs), including TRPV1, have been linked with the development of several diseases, including cardiovascular and neurological diseases, asthma, cancer, and renal disease.

​The new study is not the first to look for a molecular link between capsaicin and lower blood pressure, but earlier studies were based on short-term exposure to the compound.

Experimental Evidence

The research assigned transgenic mice and rats to one of two groups (control or capsaicin), and assessed various cardiovascular risk factors (such as blood pressure and nitric oxide levels) over a six month period.

The results of the study provide experimental evidence for the beneficial effects of dietary capsaicin in reducing high blood pressure, via direct stimulation TRPV1 channels.

The researchers’ observations suggest that TRPV1 activation may increase the activity of endothelial nitric oxide synthase (eNOS) in arteries, and increase nitric oxide (NO) production in endothelial cells.

The study’s findings suggest that TRPV1 activation is required to enhance eNOS activity, however the researchers also state that there is no way to exclude the possibility that other mechanisms may also contribute to the up-regulation of eNOS activity during prolonged capsaicin consumption.

The researchers stated: “Present results agree with other reports showing that TRPV1 activation causes relaxation of isolated arteries.”

Further Questions

In a preview in Cell Metabolism​, William Sessa from Yale University School of Medicine wrote: “Although these data are provocative, there are several outstanding questions that need to be addressed; namely, what are the mechanisms of capsaicin up-regulation of TRPV1 protein levels”

Sessa suggests further research is needed to confirm these mechanisms, adding: “Deleting TRPV1 in sensory nerves versus vasculature in mice would be highly informative to discriminate the role of sensory nerve input versus direct vascular effects of capsaicin.”

Zhu added that the study’s findings in rats should be confirmed in humans through epidemiological analysis.

Zhu also suggests that a split in the prevalence of hypertension in different areas of China may be down to differences in capsaicin intake, and could provide evidence that the chilli compound has protective effects.

“People in these [low prevalence] regions like to eat hot and spicy foods with a lot of chili peppers,"​ Zhu says.

Source: Cell Metabolism

doi: 10.1016/j.cmet.2010.05.015

“Activation of TRPV1 by Dietary Capsaicin Improves Endothelium-Dependent Vasorelaxation and Prevents Hypertension”

Authors: D.Yang, Z. Luo, S. Ma, WT Wong, L. Ma, J. Zhong, H. He, Z. Zhao, T. Cao, Z. Yan, D. Liu, W.J. Arendshorst, Y. Huang, M. Tepel, Z. Zhu,

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