Ginseng and Blood Pressure

Long-Term Intake of North American Ginseng Has No Effect on 24-Hour Blood
Pressure and Renal Function
P. Mark Stavro, Minna Woo, Lawrence A. Leiter, Tibor F. Heim, John L. Sievenpiper and Vladimir Vuksan
Hypertension 2006;47;791-796; originally published online Mar 6, 2006;
DOI: 10.1161/01.HYP.0000205150.43169.2c
Hypertension is published by the American Heart Association. 7272 Greenville Avenue, Dallas, TX
72514
Copyright © 2006 American Heart Association. All rights reserved. Print ISSN: 0194-911X. Online
ISSN: 1524-4563

The online version of this article, along with updated information and services, is located on the World Wide Web at: http://hyper.ahajournals.org/cgi/content/full/47/4/791 Subscriptions: Information about subscribing to Hypertension is online at http://hyper.ahajournals.org/subscriptions/ Permissions: Permissions & Rights Desk, Lippincott Williams & Wilkins, a division of Wolters
Kluwer Health, 351 West Camden Street, Baltimore, MD 21202-2436. Phone: 410-528-4050. Fax:
410-528-8550. E-mail: journalpermissions@lww.com Reprints: Information about reprints can be found online at http://www.lww.com/reprints Downloaded from hyper.ahajournals.org by on July 28, 2009

Long-Term Intake of North American Ginseng Has No
Effect on 24-Hour Blood Pressure and Renal Function
P. Mark Stavro, Minna Woo, Lawrence A. Leiter, Tibor F. Heim,
John L. Sievenpiper, Vladimir Vuksan
Abstract—Ginseng is consumed by 10% to 20% of adults in Asia and by up to 5% in Western countries. Despite observational evidence suggesting a link between its intake and the development of hypertension, there remains no long-term scrutiny for its effect on blood pressure (BP). We therefore undertook a randomized, placebo-controlled, double-blinded, crossover trial in 52 hypertensive individuals to determine the effect of 12-week North American ginseng intake on 24-hour BP; we also measured serum cystatin C as a marker of renal function. After a 4-week placebo run-in, we randomly assigned 52 participants to 3 g/day of ginseng or placebo for 12 weeks. This was followed by an
8-week washout and a subsequent 12-week period in which the opposite treatment was administered. At run-in and at weeks 0 and 12 of each treatment period, participants were fitted with an ambulatory BP monitor to assess 24-hour BP.
The primary outcome was the treatment difference at week 12 in mean 24-hour systolic BP. Secondary outcomes were treatment differences at week 12 in other ambulatory BP parameters and serum cystatin C. Forty participants (77%) completed the trial, with 3 removed from main analysis (nϭ2, antihypertensive drug changes; nϭ1, incomplete ambulatory monitoring). In the remaining 37, 12-week ginseng treatment was associated with a neutral effect on all ambulatory BP parameters compared with placebo; an intention-to-treat analysis supported this. Ginseng did not affect serum cystatin C level. Overall, long-term ginseng use had no effect on 24-hour BP and renal function in hypertensive individuals. (Hypertension. 2006;47:791-796.)
Key Words: clinical trials Ⅲ blood pressure Ⅲ hypertension, essential

G

inseng is an herb that populations have valued as a tonic since 25 A.D.1 It is also shown through randomized, controlled trials (RCTs) to improve glycemic control2 and cognitive function.3 In contrast, however, there is repeated mention in the medical literature that ginseng can elevate blood pressure (BP).4 – 6 This stems from an early observational study by Siegel7 that connected the self-reported use of ginseng to the development of hypertension in 14 individuals after 3 months of use. This possibility could have widespread impact, because ginseng is used by 10% to 20% of adults in
Asia8 –10 and by up to 5% in the United States,11 Australia,12 and parts of Europe.13 Furthermore, given that 20% to 40% of adults in these regions are estimated to have hypertension,14 there is potential for overlap between the prevalence of ginseng use and hypertension. Still, there remains no longterm RCT investigation of the effect of ginseng on BP, and until such evaluations are undertaken, physicians will remain greatly limited in the advice they can provide to hypertensive individuals regarding ginseng use.
Although many species of ginseng exist, Panax quinquefolius, or North American ginseng (NAG), and Panax gin-

seng together account for the majority of ginseng consumed worldwide. Recently, we demonstrated that single 3-g doses of NAG15 and P ginseng16 exert neutral and lowering effects on BP, respectively, for 160 minutes after intake. In the former study,15 the neutral effect on BP was comprehensively shown with 6 batches of NAG in hypertensive individuals. To add to this finding now, the long-term effect of NAG on BP would be of even greater significance, because long-term BP outcomes are associated with cardiovascular disease events.17,18
Also, because long-term BP outcomes might not necessarily be inferable from acute outcomes,19 we proceeded to address the effect of NAG on BP after 12 weeks of intake (defined as long-term relative to our acute studies). We measured 24hour ambulatory BP (ABP), because it is a better determinant of cardiovascular disease risk than office BP, and it allows for an assessment of circadian BP changes.20,21 As well, for safety reasons, serum cystatin C was measured as a marker of glomerular filtration rate and an indicator of the effect of
NAG on renal function.22
We determined here, through a single-center, randomized, controlled, double-blinded, crossover trial, the effect of 12-

Received November 1, 2005; first decision November 5, 2005; revision accepted January 13, 2006.
From the Risk Factor Modification Centre (P.M.S., L.A.L., J.L.S., V.V.) and Division of Endocrinology and Metabolism (M.W., L.A.L.), St Michael’s
Hospital, Toronto, Ontario, Canada; and Departments of Medicine (M.W., L.A.L, V.V.) and Nutritional Sciences (P.M.S., L.A.L., T.F.H., V.V.), Faculty of Medicine, University of Toronto, Toronto, Ontario, Canada.
Correspondence to Vladimir Vuksan, Risk Factor Modification Centre, St Michael’s Hospital, #6-136 61 Queen St East, Toronto, Ontario, Canada M5C
2T2. E-mail v.vuksan@utoronto.ca
© 2006 American Heart Association, Inc.
Hypertension is available at http://www.hypertensionaha.org

DOI: 10.1161/01.HYP.0000205150.43169.2c

791
Downloaded from hyper.ahajournals.org by on July 28, 2009

792

Hypertension

April 2006

week NAG intake on 24-hour ABP and renal function in hypertensive individuals. We used a single batch of NAG, which was representative of NAG on the world market and which was shown previously to exert a neutral effect on BP for 160 minutes after intake.15 Thus, this study provided, for the first time, insight into how long-term ginseng intake could affect both BP and renal function in humans.

Methods
Participants
The research ethics board at St Michael’s Hospital approved the study, and the procedures used were in accordance with institutional guidelines. Individuals were recruited through newspaper advertisements in Toronto and provided written informed consent to participate. Inclusion was an age of 18 to 85 years and hypertension as defined by the use of antihypertensive drugs or a seated office systolic BP Ն140 mm Hg or diastolic BP Ն90 mm Hg at each of 3 prestudy visits. Exclusion was secondary hypertension, white-coat hypertension, diabetes, kidney/liver disease, unstable angina, ginseng use for 2 months before or during the study, or any changes in the type/dose of antihypertensive drugs 1 month before or during the study.
Overall, 37 (30 men and 7 women) hypertensive individuals were included in the main analysis. Their ethnicities included European-white
(nϭ26), East-Asian (nϭ5), South-Asian (nϭ4), African-Caribbean
(nϭ2), and Native-Canadian (nϭ1) individuals. At run-in they had a meanϮSEM age of 58.4Ϯ1.6 years, body mass index of 28.6Ϯ0.9 kg/m2, serum cystatin C of 0.97Ϯ0.03 mg/L, office systolic/diastolic
BP of 130.2Ϯ2.4/85.8Ϯ1.6 mm Hg, and 24-hour systolic/diastolic
BP of 131.6Ϯ1.9/81.1Ϯ1.5 mm Hg. Of the 37 individuals, 32 were taking antihypertensive agents (monotherapy, nϭ20; Ն2 agents, nϭ12), including angiotensin-converting enzyme inhibitors (nϭ16), angiotensin receptor blockers (nϭ5), ␤-blockers (nϭ7), calcium channel blockers (nϭ12), diuretics (nϭ8), and ␣-blockers (nϭ1). The run-in characteristics of the 37 individuals included in the main analysis did not significantly differ from those who withdrew or were removed from main analysis (nϭ15; data not shown).

participants to consume a 3-g daily dose as 3 capsules between 7:00
AM and 9:00 AM and 3 between 7:00 PM and 9:00 PM, because preliminary evidence has suggested that ginsenosides remain in human plasma for Ϸ12 hours.25 All of the study personnel (including those administering the treatments and those assessing the outcomes) and participants were blinded to treatment assignment for the duration of the study.
After screening, 52 individuals were deemed eligible, and 28 were randomly assigned to the NAG-then-placebo treatment sequence and
24 to the placebo-then-NAG treatment sequence. The protocol included: (1) a 4-week open-label placebo run-in, (2) a 12-week treatment period in which the first treatment of the assigned sequence was consumed, (3) an 8-week washout period with no treatment, and
(4) a 12-week treatment period in which the second treatment of the assigned sequence was consumed. At the start of run-in, and at the start (week 0) and end (week 12) of each treatment period, participants arrived at our clinic between 8:00 AM and 9:00 AM fasted (10 to 12 hours prior) and off their antihypertensives (8 hours prior).
Initially, they had body weight assessed, blood samples drawn, and were fitted with an ABP monitor (ABPM) that was activated between 9:00 AM and 10:00 AM. Immediately after ABPM activation, each participant began his/her typical antihypertensive drug routine
(we were, thus, able to ensure that antihypertensive drugs were taken according to the same schedule each time the ABPM was worn).
Participants refrained from taking NAG or placebo capsules for the period that the ABPM was worn (Ն24 hours). Participants were instructed to retire between 10:00 PM and 12:00 AM and to awaken between 6:00 AM and 8:00 AM. They also prepared a 24-hour diary detailing activity, sleep, and drug schedules.

Primary and Secondary Outcomes
The primary outcome was mean 24-hour ambulatory systolic BP at week 12. Secondary outcomes included mean 24-hour diastolic BP and pulse pressure (PP), as well as mean daytime and night systolic
BP, diastolic BP, and PP at week 12, with daytime defined as 8:00
AM to 8:00 AM and nighttime as 12:00 AM to 6:00 AM.21,26,27
Additional secondary outcomes were serum cystatin C (marker of kidney function)22 and body weight at week 12. To avoid multiplicity, no subgroup analyses or adjusted analyses were performed.

BP Measurement

Treatments and Protocol
In this single-center, randomized, placebo-controlled, doubleblinded trial conducted between April 2001 and October 2003
(recruitment: April 2001 to May 2002; follow-up: May 2002 to
October 2003), we sought to determine the effect of 12-week NAG intake on 24-hour BP. To do so, we used an AB/BA 2-treatment,
2-period crossover design with the treatment sequences being NAGthen-placebo and placebo-then-NAG.23
We tested a 3-g dose of cornstarch placebo and a single batch of
3-year-old dried NAG root from an Ontario farm. Its acute BP effects and ginsenoside profile have been described previously (where it was designated as NAG from Farm B).15 Briefly, the total ginsenoside content of NAG was 62.8 mg/g; as well, its authenticity was indicated by the lack of ginsenoside Rf, which is absent from NAG but found in other ginseng species, such as P ginseng.24 We administered NAG and cornstarch as powders in identical blue-white
500 mg #00 capsules (with vanilla extract added to mask smell and taste), which were prepared by Sunny Crunch Foods Ltd (Markham,
Ontario, Canada).
Capsules were packaged in identical bottles, with their contents known by 1 person independent of the conduct of the study. This person coded the treatment bottles, performed the blinding, and prepared a concealed allocation schedule that randomly assigned 2 treatment sequences (NAG-then-placebo and placebo-then-NAG) to a consecutive series of numbers in an order generated by a randomnumber table. The treatments were sealed in sequentially numbered bottles according to the allocation schedule. On enrollment, each participant was assigned to the next consecutive number, and at the start of each study period, a second person dispensed the participant’s corresponding bottles of treatment capsules. We instructed

Office BP (at recruitment and run-in) was measured as described previously.15 Briefly, 3 readings were obtained from the right arm of seated participants while their arm was supported at heart level; 1 trained observer took all of the measures and used a mercury sphygmomanometer (Baumanometer, W.A. Baum). For ABP measurements, participants were fitted with a SpaceLabs 90207 ABPM
(SpaceLabs), with the cuff secured on the nondominant arm for the entire Ն24-hour period (worn on the same arm for all of the visits).
ABPM measurements occurred every 15 minutes from 7:00 AM to
9:00 PM inclusive and every 20 minutes from 10:00 PM to 6:00 AM inclusive, with a maximum of 87 successful readings for the 24-hour period. Measurements were automatically repeated if an error occurred. The adult and large adults cuffs were used for arm circumferences of 24 to 31 cm and 32 to 42 cm, respectively.

Cystatin C
All of the assays were performed in serum obtained from fasted participants. Specimens were stored at Ϫ70°C. Cystatin C was measured by a particle-enhanced immunonephelometric assay (N
Latex Cystatin C, Dade Behring) with a nephelometer (BNII, Dade
Behring).

Statistical Analyses
Based on previous findings,16 we speculated that the maximum difference in mean 24-hour systolic BP at week 12 between NAG and placebo would be 4.4 mm Hg. Accordingly, with an estimated
SD of the between-treatment difference being 7.1 mm Hg and assuming a correlation coefficient of 0.80 between-treatment values at week 12, at a significance level (␣) of 0.05 we calculated that 36

Downloaded from hyper.ahajournals.org by on July 28, 2009

Stavro et al individuals were required to achieve the noted difference in mean
24-hour systolic BP compared with placebo with 80% power. Based on previous withdrawal rates of Ϸ10% during study periods of 12 weeks,28 we calculated that the enrollment of 52 participants would yield 36 participants to a 36-week study period.
We conducted a main analysis, a secondary analysis, and an intention-to-treat analysis. The main analysis included participants who: (1) finished both treatment periods, (2) completed 24-hours of
ABP monitoring for all of the visits, and (3) adhered to the study protocol and exclusion criteria (ie, no medication changes). Data from these participants underwent crossover analysis.23 According to the assumptions of this analysis, each parameter was first tested for a period and carryover effect. Then, for the 24-hour, 8:00 AM to 8:00
PM, and 12:00 AM to 6:00 AM periods, the independent and interactive effects of treatment (NAG and placebo), week (0 and 12), and time of day (hour) on ambulatory systolic BP, diastolic BP, and PP were assessed by a repeated measures, general linear model (GLM), and
3-way ANOVA. Significant treatment effects were additionally explored at weeks 0 and 12 with repeated-measures GLM-ANOVA.
For cystatin C, the independent and interactive effects of treatment and week were assessed by repeated-measures GLM 2-way ANOVA.
Significant treatment effects were additionally explored at weeks 0 and
12 with repeated-measures GLM-ANOVA. We assessed body weight by the same procedure.
The secondary analysis included participants who finished the first treatment period with complete 24-hour ABPM at weeks 0 and 12.
This analysis followed a parallel design test in which a GLM 2-way
ANOVA tested the independent and interactive effects of treatment
(NAG versus placebo) and week (0 versus 12) on ABP during the first treatment period. Significant treatment effects were explored at these weeks with a GLM-ANOVA. The intention-to-treat analysis included all of the participants who finished both treatment periods with complete 24-hour ABPM, and their data underwent crossover analysis (as described for main analysis).23

Ginseng and 24-Hour Blood Pressure

All of the analyses were run with sex and age as covariates and were performed with the Number Cruncher Statistical Software
2000. Significance was set at ␣ of 0.05 and was 2-sided. Values are expressed as meanϮSEM.

Adequacy of Blinding
The adequacy of blinding was assessed according to participant responses when asked which treatment they believed they were taking (NAG, placebo, or uncertain). This question was asked after each treatment period by an individual independent of the conduct of the study.

Results
Subjects
Of the screened individuals (nϭ67), 52 proceeded through run-in and randomization. Among them, 12 (23%) withdrew:
8 from the NAG-then-placebo sequence (nϭ3, period 1; nϭ1, washout; nϭ4, period 2) and 4 from the placebo-then-NAG sequence (nϭ2, period 1; nϭ2, washout). Accordingly, 3 withdrew while taking NAG (nϭ1, diarrhea; nϭ1, headache; nϭ1, antihypertensive drug change), 6 while taking placebo
(nϭ6, work schedule), and 4 during washout (nϭ3, work schedule; nϭ1, antihypertensive drug change). Also, 3 from the placebo-then-NAG sequence were not included in main analysis because of antihypertensive drug changes (nϭ2) and unsuccessful ABPM (nϭ1). Overall, 37 participants (71%) proceeded to main analysis.

Compliance and Blinding
Compliance was estimated by pill count (NAG: 91.7Ϯ2.3%; placebo: 93.6Ϯ1.9%; Pϭ0.50). Evaluation of blinding re-

Mean 24-Hour, Daytime, and Night Ambulatory Systolic BP, Diastolic BP, and PP Before (Week 0) and After
(Week 12) NAG and Placebo Intake in 37 Hypertensive Participants

24-Hour systolic BP
Daytime systolic BP†

Week 0
(nϭ37),
mm Hg

P
Value*

Week 12
(nϭ37),
mm Hg

P
Value*

Difference at Week 12
(NAG–Placebo 95% CI), mm Hg

NAG

129.6Ϯ1.8

0.56

130.9Ϯ2.0

0.99

(Ϫ2.4 to 2.4)

Placebo

Parameter

130.4Ϯ1.9

0.64

(Ϫ2.0 to 3.3)

0.59

(Ϫ3.9 to 2.2)

0.99

(Ϫ1.6 to 1.7)

0.79

(Ϫ1.6 to 2.0)

0.94

(Ϫ2.3 to 2.2)

0.94

(Ϫ1.5 to 1.4)

0.60

(Ϫ1.2 to 1.9)

0.35

(Ϫ2.5 to 0.9)

Treatment

Night systolic BP‡

NAG

135.1Ϯ2.0

Placebo

24-Hour diastolic BP

NAG

118.3Ϯ1.7

NAG

79.7Ϯ1.3
84.6Ϯ1.5

NAG

71.4Ϯ1.3

NAG

49.8Ϯ1.6

Night PP‡

0.91

NAG

51.1Ϯ1.7

0.93

NAG

46.9Ϯ1.6
48.1Ϯ1.6

84.9Ϯ1.5
84.7Ϯ1.5

0.63

73.4Ϯ1.6
73.4Ϯ1.3

0.27

50.3Ϯ1.6
50.4Ϯ1.5

51.5Ϯ1.6

Placebo

80.6Ϯ1.5
80.5Ϯ1.4

50.4Ϯ1.5

Placebo

120.8Ϯ1.9
121.6Ϯ1.8

72.4Ϯ1.4

Placebo
Daytime PP†

0.25

84.6Ϯ1.5

Placebo
24-Hour PP

NAG

136.6Ϯ2.1
136.0Ϯ2.0

79.9Ϯ1.3

Placebo
Night diastolic BP‡

0.83

120.1Ϯ2.1

Placebo
Daytime diastolic BP†

130.9Ϯ1.8

135.9Ϯ2.0

Placebo

793

0.61

51.6Ϯ1.8
51.3Ϯ1.6

0.21

47.4Ϯ1.5
48.2Ϯ1.5

Also shown are the 95% CIs for the treatment differences at week 12. Values are presented as meanϮSEM.
*P values are for between-treatment comparisons at week 0 and at week 12.
†Daytime indicates the mean of the period 8:00 AM to 8:00 PM inclusive.
‡Night indicates the mean of the period 12:00 AM to 6:00 AM inclusive.

Downloaded from hyper.ahajournals.org by on July 28, 2009

794

Hypertension

April 2006

vealed that of the 40 participants who completed both treatment periods, only 16 expressed certainty of when (ie, indicated what period) they consumed NAG. Accordingly, 9 of 40 (22.5%) correctly predicted when they were on NAG, whereas 7 of 40 (17.5%) indicated they were on NAG when on placebo (Pϭ0.58 for ␹2 analysis).

Main Analysis of BP, Cystatin C, and
Body Weight
There were no significant period or carryover effects on any of the measured parameters (BP, bodyweight, or cystatin C).
For the BP parameters at week 0, mean values did not differ between NAG and placebo (Table). However, at 6:00 AM on week 0, the PP was significantly lower for NAG compared with placebo (PϽ0.05; Figure); there were no other mean hourly differences.
There was no significant effect of treatment on the primary outcome, mean 24-hour systolic BP, or on any secondary outcomes (ie, mean values at week 12 did not differ between
NAG and placebo; Table); and there was no significant interaction among treatment, week, and/or hour. At 1:00 PM

(13:00 hours), however, diastolic BP was significantly higher at week 12 for NAG compared with placebo (Figure). There were no other mean hourly differences.
Body weight did not differ between NAG and placebo at week 0 (82.8Ϯ2.3 versus 82.7Ϯ2.3 kg, respectively; Pϭ0.86; nϭ37) and at week 12 (82.6Ϯ2.3 versus 82.8Ϯ2.3 kg, respectively; Pϭ0.47; nϭ37). The serum level of cystatin C did not differ between NAG and placebo at week 0 (0.97Ϯ0.03 versus 0.98Ϯ0.03 mg/L, respectively; Pϭ0.40; nϭ34) and at week 12 (1.00Ϯ0.03 versus 0.90Ϯ0.03 mg/L, respectively;
Pϭ0.32; nϭ34). A sufficient number of blood samples were obtained from only 34 participants for the measurement of serum cystatin C.

Secondary Analysis
The secondary analysis included the 39 participants who completed the entire study plus those who withdrew but completed the first treatment period (nϭ7). When their data were analyzed together in a parallel-design comparison of
NAG (nϭ25) versus placebo (nϭ21) on all of the ABP parameters from treatment period 1, NAG showed no signif-

The meanϮSEM hourly ambulatory systolic BP, diastolic BP, and PP values before (at week 0) and after (at week 12) treatment with 3 g/day of North American ginseng (f) and placebo (Ⅺ) in 37 hypertensive individuals. *North American ginseng vs placebo, PϽ0.05.

Downloaded from hyper.ahajournals.org by on July 28, 2009

Stavro et al icant effect versus placebo on any parameter (results not shown). Intention-to-Treat Analysis
Because 12 of the 52 randomized participants were lost to follow-up, and 1 had incomplete ABPM, the intention-to-treat analysis included 39 individuals. It was only performed for ABP and showed no significant effect of period, carryover, or treatment on any ABP parameter (results not shown).

Discussion
We showed here, for the first time in a long-term RCT, the effect of ginseng on BP and renal function. The ginseng used was
NAG, which is a species native to North America that is used predominantly in Canada, the United States, and China.29 We found that its intake at 3 g/day for 12 weeks relative to placebo was associated with a neutral effect on BP in hypertensive individuals. This was shown in the main analysis by a lack of difference between NAG and placebo at 12 weeks for each of the mean 24-hour, daytime and night ABP parameters (Table), which was supported by an intention-to-treat analysis. Also, although there was an increase in diastolic BP for NAG relative to placebo at the 1:00 PM (13:00 hours) time point of week 12 (Figure), this was considered clinically insignificant, because mean daytime and 24-hour diastolic BP did not differ between treatments. As for cystatin C, NAG intake did not affect its serum level relative to placebo, indicating no influence on renal function. Thus, this study showed that 12-week consumption of NAG had no effect on
ABP or renal status in hypertensive individuals.
The BP outcomes here added to our previous finding,15 which showed an acute neutral effect on BP with 6 batches of
NAG differing in quality and profile of ginsenosides, pharmacologically active components of NAG.30 Importantly, the
6 batches were chosen by the Ginseng Growers Association of Ontario to represent the total crop of NAG from Ontario, which supplies Ͼ60% of NAG worldwide.15 Here, we tested
1 of these batches, and because it was phytochemically similar to the other 5 batches, we speculated that our current findings could be extrapolated to these other 5 and, thus, to a majority of NAG on the world market.
With respect to the form of NAG tested, we administered the whole dried root in its natural form, which is the most consumed form, and the form that cultivators sell to supplement manufacturers. Accordingly, we were able to assess all of the components of NAG within their native matrix. In particular, we avoided using aqueous-alcohol extracts, because they would have contained only the NAG components soluble within the base of the extract,31 thus precluding a comprehensive investigation of the efficacy of NAG.
As for dosage, in keeping with our acute efficacy trial,15 we administered 3 g, which is the recommended dose of ginseng in traditional Chinese medicine,32 and the average intake reported in the study by Siegel,7 where ginseng intake was associated with elevated BP. As well, the 12-week treatment period represented the time span in which hypertension developed in Siegel’s report.7
Although this was the first long-term RCT on ginseng root and BP, it should be emphasized that it evaluated the species of

Ginseng and 24-Hour Blood Pressure

795

ginseng known as P quinquefolius, or NAG. NAG is unique from P ginseng, which is the species that has been tested in other clinical interventions on ginseng and BP.16,33–35 After harvest, the root portion of NAG is dried, whereas the root portion of
P ginseng is either dried or steamed,1 with the steamed form being marketed as Korean red ginseng (KRG). Importantly,
NAG contains a 3- to 5-times higher content of ginsenosides and different profile of ginsenosides than both forms of P ginseng.2,15,16,24,28 As well, KRG is the only marketed ginseng to contain ginsenoside Rg3, the most potent vasodilating ginsenoside.36 To date, 4 clinical interventions have tested the effect of P ginseng root on BP.16,33–35 Of these, 1 tested the dried root and showed that an aqueous-ethanol extract of it at 200 mg/day had no effect on BP in a 4-week RCT with young, normotensive adults.33 In the case of steamed root, KRG, our group found that 3 g of the natural root could lower BP for
160 minutes relative to placebo in an RCT with hypertensive individuals.16 As well, an 8-week nonrandomized trial demonstrated that 4.5 g/day of the natural KRG root significantly decreased BP in hypertensive individuals.35 Furthermore, in a nonrandomized trial with young, normotensive adults, an aqueous extract of KRG root at a mean dose of 610 mg significantly decreased BP at 45, 60, and 75 minutes after intake.34 Thus, although studies on ginseng and BP exist, the use of extracts and nonrandomized designs was common, which precluded an accurate assessment of efficacy. Still, evidence to date indicates that NAG has no effect on BP and that P ginseng, if steamed, could be antihypertensive. Future
RCTs will have to determine whether the ginseng species, the steaming process, and the ginsenoside content and/or profile are important factors affecting BP. Importantly, though, contrary to
Siegel’s7 observational finding, no clinical intervention has shown ginseng to elevate BP.
In the current study, 2 participants reported adverse events
(headache and diarrhea), and withdrew, and both were taking
NAG at the time. Whereas clinical documentation of the adverse events of NAG is lacking, Coon and Ernst37 systematically reviewed 146 clinical trials representing Ͼ8500 individual exposures to P ginseng and found it to have the same adverse event profile as placebo.
The current study had 3 limitations. First, 25% of the participants withdrew, and another 5% had their data removed from main analysis. We did, however, conduct a secondary analysis and intention-to-treat analysis to rectify this, and both showed identical outcomes to the main analysis. Second, whereas the antihypertensive-treated participants in the main analysis (nϭ32) held their antihypertensive type(s) and dose(s) constant for the entire study, their use of antihypertensives could have prevented an accurate interpretation of the effect of NAG on BP because of possible
NAG– drug interactions. However, an objective here was to determine the effect of NAG on BP in a representative population of hypertensive individuals so that the findings could be extrapolated to such individuals. To add to the current findings, future studies should determine the effect of
NAG on BP in untreated hypertensive or prehypertensive individuals to better understand the influence of NAG on BP in the absence of antihypertensive drugs.

Downloaded from hyper.ahajournals.org by on July 28, 2009

796

Hypertension

April 2006

Perspectives

The topic of ginseng and BP in humans commenced Ͼ25 years ago with an observational study that suggested a link between ginseng use and hypertension.7 Since then, 2 acute-duration
RCTs found that NAG15 and P ginseng16 have neutral and lowering effects on BP, respectively. We showed here that
12-week intake of NAG is associated with a neutral effect on
24-hour BP relative to placebo in a multiethnic, middle-toolder aged, hypertensive population. NAG also had no effect on the serum level of cystatin C, a marker of renal function and cardiovascular mortality.38 Overall, these findings widen the perspective on ginseng and BP and provide initial insight into the effect of ginseng on renal function. Future RCTs should evaluate additional doses of NAG that represent its range of intake in the general population. As well, the effect of P ginseng on BP should be determined through similar long-term RCTs, because it shows the potential to lower
BP.16

Acknowledgments
Funding for this study was provided by the Ontario Ministry of
Agriculture and Food, as well as by the Ontario Ginseng Growers
Association, who also provided the ginseng.

References
1. Yun TK. Brief introduction of panax ginseng. J Korean Med Sci. 2001;
16(Suppl):S3–S5.
2. Vuksan V, Sievenpiper JL, Koo VY, Francis T, Beljan-Zdravkovic U, Xu
Z, Vidgen E. Am ginseng (panax quinquefolius l) reduces postprandial glycemia in nondiabetic subjects and subjects with type 2 diabetes mellitus. Arch Intern Med. 2000;160:1009 –1013.
3. Kennedy DO, Scholey AB. Ginseng: Potential for the enhancement of cognitive performance and mood. Pharmacol Biochem Behav. 2003;75:
687–700.
4. Klepser TB, Klepser ME. Unsafe and potentially safe herbal therapies.
Am J Health Syst Pharm. 1999;56:125–141.
5. Baldwin CA, Anderson LA, Phillipson JA. What pharmacists should know about ginseng. Pharm J. 1986;237:583–586.
6. Miller LG. Herbal medicinals: Selected clinical considerations focusing on known or potential drug-herb interactions. Arch Intern Med. 1998;
158:2200 –2211.
7. Siegel RK. Ginseng abuse syndrome. Problems with the panacea. JAMA.
1979;241:1614 –1615.
8. Lim MK, Sadarangani P, Chan HL, Heng JY. Complementary and alternative medicine use in multiracial Singapore. Complement Ther Med.
2005;13:16 –24.
9. Kim MJ, Lee SD, Kim DR, Kong YH, Sohn WS, Ki SS, Kim J, Kim YC,
Han CJ, Lee JO, Nam HS, Park YH, Kim CH, Yi KH, Lee YY, Jeong SH.
Use of complementary and alternative medicine among Korean cancer patients. Korean J Intern Med. 2004;19:250 –256.
10. Shin KR, Jho MY, Lee GS, Park SY, Shin SJ. Study of the patterns of alternative therapy by the elderly (abstract). Nurs Health Sci. 2002;4:A8.
11. Barnes PM, Powell-Griner E, McFann K, Nahin RL. Complementary and alternative medicine use among adults: United States, 2002. Adv Data.
2004;1–19.
12. MacLennan AH, Wilson DH, Taylor AW. The escalating cost and prevalence of alternative medicine. Prev Med. 2002;35:166 –173.
13. Nilsson M, Trehn G, Asplund K. Use of complementary and alternative medicine remedies in Sweden. A population-based longitudinal study within the northern Sweden MONICA project. Multinational monitoring of trends and determinants of cardiovascular disease. J Intern Med.
2001;250:225–233.
14. Kearney PM, Whelton M, Reynolds K, Muntner P, Whelton PK, He J.
Global burden of hypertension: Analysis of worldwide data. Lancet.
2005;365:217–223.
15. Stavro PM, Woo M, Heim TF, Leiter LA, Vuksan V. North American ginseng exerts a neutral effect on blood pressure in individuals with hypertension. Hypertension. 2005;46:406 – 411.

16. Stavro PM, Woo M, Vuksan V. Korean red ginseng lowers blood pressure in individuals with hypertension (abstract). Am J Hypertens. 2004;17:S33.
17. Neal B, MacMahon S, Chapman N. Effects of ace inhibitors, calcium antagonists, and other blood-pressure-lowering drugs: Results of prospectively designed overviews of randomised trials. Blood pressure lowering treatment trialists’ collaboration. Lancet. 2000;356:1955–1964.
18. Julius S, Kjeldsen SE, Weber M, Brunner HR, Ekman S, Hansson L, Hua
T, Laragh J, McInnes GT, Mitchell L, Plat F, Schork A, Smith B,
Zanchetti A. Outcomes in hypertensive patients at high cardiovascular risk treated with regimens based on valsartan or amlodipine: The value randomised trial. Lancet. 2004;363:2022–2031.
19. Guyton AC. Blood pressure control–special role of the kidneys and body fluids. Science. 1991;252:1813–1816.
20. Staessen JA, Thijs L, Fagard R, O’Brien ET, Clement D, de Leeuw PW,
Mancia G, Nachev C, Palatini P, Parati G, Tuomilehto J, Webster J.
Predicting cardiovascular risk using conventional vs ambulatory blood pressure in older patients with systolic hypertension. Systolic hypertension in Europe trial investigators. JAMA. 1999;282:539 –546.
21. Clement DL, De Buyzere ML, De Bacquer DA, de Leeuw PW, Duprez
DA, Fagard RH, Gheeraert PJ, Missault LH, Braun JJ, Six RO, Van Der
Niepen P, O’Brien E. Prognostic value of ambulatory blood-pressure recordings in patients with treated hypertension. N Engl J Med. 2003;
348:2407–2415.
22. Mussap M, Plebani M. Biochemistry and clinical role of human cystatin c.
Crit Rev Clin Lab Sci. 2004;41:467–550.
23. Senn S. Cross-Over Trials in Clinical Research. 2nd ed. West Sussex,
England: John Wiley and Sons Ltd; 2002.
24. Wang X, Sakuma T, Asafu-Adjaye E, Shiu GK. Determination of ginsenosides in plant extracts from panax ginseng and panax quinquefolius
l. By lc/ms/ms. Anal Chem. 1999;71:1579 –1584.
25. Tawab MA, Bahr U, Karas M, Wurglics M, Schubert-Zsilavecz M.
Degradation of ginsenosides in humans after oral administration. Drug
Metab Dispos. 2003;31:1065–1071.
26. Fagard R, Brguljan J, Thijs L, Staessen J. Prediction of the actual awake and asleep blood pressures by various methods of 24 h pressure analysis.
J Hypertens. 1996;14:557–563.
27. Fagard RH, Staessen JA, Thijs L. Optimal definition of daytime and night-time blood pressure. Blood Press Monit. 1997;2:315–321.
28. Vuksan V, Sievenpiper JL, Sung MK, Di Buono M, Jenkins AL, Stavro
PM, Leiter LA, Nam KY. Safety and efficacy of korean red ginseng intervention (Saeki): Results of a double-blind, placebo-controlled, crossover trial in type 2 diabetes (abstract). Diabetes. 2003;52:A137.
29. Novelli S. Ginseng from Canada. Bi-Weekly Bulletin of Market Analysis
Division Agriculture and Agri-Food Canada. 2003;16:1– 4.
30. Attele AS, Wu JA, Yuan CS. Ginseng pharmacology: Multiple constituents and multiple actions. Biochem Pharmacol. 1999;58:1685–1693.
31. Gafner S, Bergeron C, McCollom MM, Cooper LM, McPhail KL, Gerwick
WH, Angerhofer CK. Evaluation of the efficiency of three different solvent systems to extract triterpene saponins from roots of panax quinquefolius using high-performance liquid chromatography. J Agric Food Chem. 2004;
52:1546 –1550.
32. Dharmananda S. The nature of ginseng. Traditional use, modern research, and the question of dosage. HerbalGram. 2002;54:34 –51.
33. Caron MF, Hotsko AL, Robertson S, Mandybur L, Kluger J, White CM.
Electrocardiographic and hemodynamic effects of panax ginseng. Ann
Pharmacother. 2002;36:758 –763.
34. Han K, Shin IC, Choi KJ, Yun YP, Hong JT, Oh KW. Korea red ginseng water extract increases nitric oxide concentrations in exhaled breath.
Nitric Oxide. 2005;12:159 –162.
35. Han KH, Choe SC, Kim HS, Sohn DW, Nam KY, Oh BH, Lee MM, Park
YB, Choi YS, Seo JD, Lee YW. Effect of red ginseng on blood pressure in patients with essential hypertension and white coat hypertension. Am J
Chin Med. 1998;26:199 –209.
36. Kim ND, Kang SY, Park JH, Schini-Kerth VB. Ginsenoside rg3 mediates endothelium-dependent relaxation in response to ginsenosides in rat aorta: Role of kϩ channels. Eur J Pharmacol. 1999;367:41– 49.
37. Coon JT, Ernst E. Panax ginseng: A systematic review of adverse effects and drug interactions. Drug Saf. 2002;25:323–344.
38. Shlipak MG, Sarnak MJ, Katz R, Fried LF, Seliger SL, Newman AB,
Siscovick DS, Stehman-Breen C. Cystatin c and the risk of death and cardiovascular events among elderly persons. N Engl J Med. 2005;352:
2049 –2060.

Downloaded from hyper.ahajournals.org by on July 28, 2009

References: 1. Yun TK. Brief introduction of panax ginseng. J Korean Med Sci. 2001; 16(Suppl):S3–S5. Am J Health Syst Pharm. 1999;56:125–141. 11. Barnes PM, Powell-Griner E, McFann K, Nahin RL. Complementary and alternative medicine use among adults: United States, 2002 12. MacLennan AH, Wilson DH, Taylor AW. The escalating cost and prevalence of alternative medicine. Prev Med. 2002;35:166 –173. hypertension. Hypertension. 2005;46:406 – 411. treatment trialists’ collaboration. Lancet. 2000;356:1955–1964. randomised trial. Lancet. 2004;363:2022–2031. Crit Rev Clin Lab Sci. 2004;41:467–550. J Hypertens. 1996;14:557–563. 30. Attele AS, Wu JA, Yuan CS. Ginseng pharmacology: Multiple constituents and multiple actions. Biochem Pharmacol. 1999;58:1685–1693. Nitric Oxide. 2005;12:159 –162.