Review and Assessment of Medicinal Safety Data of Orally Used Echinacea Preparations

• Introduction
• Pharmacodynamic interactions
• Pharmacokinetic interactions
• Special warnings and precautions for use
• Undesirable effects
• Allergic reactions
• Thrombocytopenia
• Leucopenia and eosinophilia
• Erythema nodosum
• Sjögren syndrome
• Exanthema
• Acute cholestatic autoimmune hepatitis
• Effects on Reproduction and Development
• Use in children
• Duration of use
• Discussion
• References

Abstract

Echinacea purpurea, Echinacea angustifoli and Echinacea pallida are frequently used as medicinal plants. Besides asking for evidence on their efficacy, there is an increasing interest for safety data. This review systematically presents the available literature on drug interactions, contraindications, adverse events, duration of use, and safety of use in pregnant and nursing women, and assesses the safety profile of corresponding Echinacea preparations. It is noteworthy that all safety data reported are as product specific as the pharmacological or efficacy data are. In pharmacokinetic herb-drug interaction studies performed in vivo, no significant inhibitions of human CYP2D6 and CYP3A4 isoforms have been found after the administration of standardized E. purpurea preparations. However, contradictory results exist in studies using liver microsomes. Adverse events reported during clinical trials following administration of Echinacea spp. mono-preparations were generally mild and mostly without causality. Due to published long term studies with continuous ingestion of different Echinacea preparations up to 6 month with no reported toxicological concerns, Echinacea can be recommended also for long-term use. Moreover, the contraindications in cases of autoimmune diseases and immune-suppression are questionable, since lipophilic Echinacea preparations containing alkamides suppress cellular immune responses, and beneficial effects in autoimmunity were reported. The same applies for the use during pregnancy. Although there has been some impact reported on embryonic angiogenesis in mice, no association with an increased risk for major or minor malformations during organogenesis was found in a literature review. Altogether, the different evaluated Echinacea preparations are well-tolerated herbal medicines in the management in children and adults alike.

Introduction

Echinacea purpurea (L.) Moench, Echinacea angustifolia DC., and Echinacea pallida (Nutt.) Nutt. (Asteraceae) are frequently used as medicinal plants for the prevention and treatment of the common cold, influenza, and upper respiratory tract infection. The aerial parts of E. purpurea are used, as well as the whole plant including the roots from all three species. Polysaccharides, glycoproteins, caffeic acid derivatives and alkamides have been considered as the constituents being most relevant for activity [1]. Polysaccharides, glycoproteins and caffeic acid derivatives have been shown to have immunomodulatory effects. However, the question of bioavailability is still not solved. Recent investigations have demonstrated that at least alkamides are detectable in human blood in reasonable concentrations after oral application of Echinacea preparations. Alkamides possess a structural similarity with anandamide, an endogenous ligand of cannabinoid receptors, and in fact it was shown that they also bind to cannabinoid receptors and trigger effects on cytokines [2]. Besides asking for evidence on their efficacy, there is an increasing interest for safety of these preparations. Therefore we have systematically reviewed the available literature for evidence on drug interactions, contraindications, adverse events, duration of safe use, and data on safety of use in pregnant and nursing women and have assessed the safety and tolerability profile of corresponding Echinacea preparations.

Cautions from the Committee on Herbal Medicinal Products (HMPC) [3], [4], [5], [6], [7] have been critically evaluated, especially the use in children below 12 years of age, duration of use, contraindications like allergic diathesis or in case of immunosuppression and hematologic systemic diseases and special warnings that autoimmune diseases can be triggered. Many of these warnings are based only on the theoretical possibility that the immune-mediated inflammatory mechanism of diseases like autoimmune disease, tuberculosis, multiple sclerosis and human immunodeficiency virus infection, can be exacerbated by the immunostimulatory properties of Echinacea [3], [4], [5], [6], [7], [8].

Therefore, this review shall help to make evidence based decisions about the advice safe use of Echinacea preparations.

Pharmacodynamic interactions

One study in healthy mice reported that a commercially prepared powder extract of the root of E. purpurea (0.45 mg/mouse/day) and melatonin (0.0142 mg/mouse/day) administered together, but not alone, had a detrimental effect on the levels of mature granulocytes in both, bone marrow and spleen [9], [10]. A potentially positive interaction between E purpurea and the anticonvulsant medication phenytoin (Epanutin®, Phenhydan®, Zentropil®, Dilantin®) has been reported in mice. Phenytoin has a documented teratogenic activity. Most notably, phenytoin is known to increase the risk of cleft palate development if taken in pregnancy. Its use in pregnancy has also been reported to be associated with an increased risk of heart malformations. The increased incidence of cleft palate reportedly can be reduced by the stimulation of the maternal immune system. These led researchers to investigate the use of ethanolic (70 %) extract of E. purpurea dried aerial parts with phenytoin in relationship to the incidence of cleft palate in mice. The incidence of cleft palate with phenytoin alone, phenytoin with the immune modulator levamisole, or phenytoin plus E. purpurea extract (360 mg i. p.) was 16 %, 5.3 % and 3.2 %, respectively, showing that both levamisole and Echinacea decreased the incidence of cleft palate [11]. It is unknown whether the observed effects have any clinical relevance.

In a recently published clinical study by Abdul et al., the pharmacodynamic and pharmacokinetic interactions of either Echinacea (1275 mg four times daily containing a mixture of 600 mg of E. angustifolia roots and 675 mg of E. purpurea root; standardized to contain 5.75 mg of total alkamides per tablet) or policosanol (10 mg tablet twice daily) with warfarin in healthy subjects have been investigated. The apparent clearance of (S)-warfarin was significantly higher during a concomitant treatment with Echinacea, but this did not lead to a clinically significant change in an INR (International Normalised Ratio) measurement. No evidence of any apparent effect of CYP2C9 interaction has been found. Neither Echinacea nor policosanol significantly affected warafarin pharmacodynamics, platelet aggregation or baseline clotting status in healthy subjects [12].

Although details of drug administration, species, and type of extract are not stated, it is worth to mention a first report on a possible interaction between Echinacea and etoposide, a CYP3A4 substrate [13]. A 61-year-old man newly diagnosed with cell lung cancer began concurrent chemoradiation with cisplatin and etoposide. He was admitted to the hospital on day 8 of his first cycle and found to be thrombocytopenic. His platelet count reached a nadir of 16 × 10(3)/L, requiring platelet transfusion support. Upon admission, it was discovered that he was taking vitamin B12, vitamin E, vitamin D, vitamin C, Echinacea (not characterized) and “vitamin B17” (laetrile-apricots kernel), which were discontinued. He received his next cycle of chemotherapy without taking herbal products and vitamins and with the addition of pegfilgrastim. As the patient also stopped taking laetrile and his other vitamins after cycle 1, a potential interaction between laetrile and etoposide or cisplatin cannot be fully excluded. The authors of the report concluded that since the exact preparation of Echinacea and corresponding plant extract constituents was unkown, the interaction remains equivocal. However, it has been written that cautions should be exercised in patients receiving chemotherapy including CYP3A4 substrates (antracyclines, etoposide, vinca alcaloids, taxanes) while taking Echinacea [3], [13].

Pharmacokinetic interactions

The vast majority of reported interactions are of pharmacokinetic nature, resulting in changes in biotransformation of the affected drug through inhibition or induction of drug metabolizing enzymes. A number of in vitro and in vivo studies suggest a potential for herb-drug interaction between different uncharacterized Echinacea extracts and the cytochrome P450 family of drug metabolizing enzymes (CYP 3A4, 2D6, 1 A2 and 2C9) [14], [15], [16], [17]. But only the recently published pharmacokinetic drug interaction studies determined the influence of chemically characterized Echinacea preparations on CYP3A and CYP2D6, with four conducted in human [18], [19], [20], [21] and seven in vitro studies [22], [23], [24], [25], [26], [27].

In a recently performed clinical study on the activity of human CYP2D6, no significant inhibition was detected after the application of E. purpurea softgel capsules (Gaia Herbs, Inc., Brevard, NC, USA, 267 mg extract, three times daily) standardized to contain 2.2 mg alkamides per capsule [18]. Penzak et al. investigated the influence of standardized E. purpurea fresh plant liquid extract 8 : 1 (250 mg) softgel capsules with 500 mg (two 250 mg capsules) 3 times/day for 28 days on the pharmacokinetics of lopinavir (400 mg)/ritonavir (100 mg) twice/day and on CYP3A and p-glycoprotein activity by using the probe substrates midazolam (8 mg) and fexofenadine (120 mg) as single doses, respectively. The concentrated extract from freshly harvested E. purpurea plants contained standardized amounts of alkamides 0.25 mg/mL, polysaccharides 25.5 mg/mL and cichoric acid 2.5 mg/mL. The 13 volunteers received for 14 days E. purpurea in combination with lopinavir-ritonavir and for 14 days E. purpurea alone. Neither lopinavir nor ritonavir pharmacokinetics were significantly altered by 14 days of E. purpurea co-administration [21]. More recently, interactions between etravirine (a nonnucleoside reverse transcriptase inhibitor of HIV) and darunavir (protease inhibitor) with capsules containing E. purpurea root extract at a dosage of 500 mg every 6 h from days 1 to 14 has been investigated in HIV infected patients. Etravirine and darunavir undergo extensive metabolism by the hepatic CYP3A4 isoform. Similar to lopinavir studied by Penzak et al., no significant interaction has been found with darunavir [19]. Also no significant treatment effects were observed for any of the primary pharmacokinetic parameters after administration of etravirine with or without E. purpurea [20].

Already in 2007, Raner et al. evaluated the potential of 11 isolated alkamides and a 33 % and 95 % ethanolic E. purpurea root extract to inhibit cytochrome P450 2E1 in human liver microsomes and from an in vitro expression system. Extracts of E. purpurea root in 95 % ethanol (2.0 µL of extract in 500 µL reaction) significantly inhibited the activity (30 %) of cytochrome P450 2E1 in human liver microsomes. No inhibition was seen when 2 µL of the 33 % ethanolic extract of the E. purpurea roots was used in a 500 µL reaction using human liver microsomes or expressed P450. The alkamides present in E. purpurea root preparations (undeca-2E/Z,4E-diene-8,10-diynoic acid isobutylamides and dodeca-2E,4E,8Z,10E/Z-tetraenoic acid isobutylamides) showed significant inhibition at concentrations as low as 25 µM, which corresponds to roughly 6 µg/mL, whereas the caffeic acid derivatives had no effect [27]. Compared to the measured plasma levels in humans (~ 10 ng/mL) the concentration needed for in vitro CYP450 2E1 inhibition was about 600 times higher and therefore the relevance of these results for the in vivo-situation is questionable.

A standardized E. purpurea preparation (Echinaforce®) induced mild inhibition of CYP isoforms, with CYP3A4 being the most, and CYP2D6 the least sensitive enzyme. In further studies, the Echinacea alkamides were suspected to be responsible for CYP3A4 inhibitory activity [24]. In a more recent approach, a detailed analysis of six commercial Echinacea liquid preparations with emphasis on the metabolomics characterisation of the Echinacea compounds responsible for inhibiting CYP3A4 has been reported by Modarai et al. 2010. The used preparations were a pressed juice from the aerial parts of E. purpurea (Madaus AG), a tincture from the roots of E. pallida (Salus), and three different tinctures from E. purpurea (with 22 % ethanol from Viridian, with 65 % ethanol from Holland & Barrett, Echinagold® with 50 % ethanol from a Health Food Shop in Denmark), and a herb/root preparation from E. purpurea (Echinaforce®, Bioforce). After the separation of each preparation into their ethanol and water-soluble components, the results directly confirmed the role of alkamides in the inhibition of CYP3A4. Levels of the alkamides (dodeca-2E,4E,8Z,10E/Z-tetraenoic acid isobutylamides and undeca-2E,4E/Z-diene-8,10-diynoic acid isobutylamides) correlated well with CYP3A4 inhibition [25]. Due to variable and conflicting results in CYP3A4 inhibition between laboratories, it is now suggested to use multiple CYP3A4 probes in the assessment of CYP3A4 interaction potentials. Hansen and colleagues compared the CYP3A4 inhibition profiles of E. purpurea (Echinagard®, with final concentrations between 0.24–6360 µg/mL) measured by three different CYP3A4 substrates and different methodologies. Testosterone metabolism showed a much lower CYP3A4 inhibition (IC₅₀ 5394 µg/mL) compared to the fluorescent substrates BFC (7-benzyloxy-trifluoromethylcoumarin) and BQ (7-benzyloxyquinoline) (IC₅₀ 354 and 452 µg/mL, respectively). The choice of substrate might thus be essential for the evaluation of the inhibition of CYP3A4 metabolism for some herbs when performing in vitro studies. The previously described inhibition potential of E. purpurea towards CYP3A4-mediated metabolism was confirmed by the use of three different substrates [28]. Aside from direct enzymatic inhibition also the transcriptional activity can be altered by different herbal medicinal products (e.g. induction or inhibition of CYP expression). Hellum and colleagues found that a commercial pressed juice from the aerial parts of E. purpurea (Echinagard® – Madaus AG) moderately suppressed CYP3A4 expression in primary human hepatocytes [22]. In addition, Gorski et al. found that an 8-day course of 400 mg of E. purpurea root preparation administered 4 times daily could cause an induction of CYP3A4 in intestinal cells, but suppressed hepatic CYP3A4 expression. However, the bioavailability of midazolam, a CYP3A4 substrate, increased by the same amount, leading to no overall change in AUC [15]. Kortenkamp et al. (2011) carried out an analysis of the CYP3A4 induction in human hepatocellular carcinoma HepG2 cells by an E. purpurea herb and root preparation (Echinaforce®, Bioforce), using real-time reverse transcription polymerase chain reaction (RT-PCR) to determine steady-state mRNA levels. HepG2 cells were exposed for 96 h to clinically relevant concentrations of the E. purpurea preparation (22, 11.6 and 1.16 µg/mL), or of four Echinacea alkamides (1.62 and 44 nM). Neither Echinaforce® nor the pure alkamides produced any significant change in the steady-state CYP3A4 mRNA levels [29]. A further study on the rat cytochrome P450 expression level has been carried out only recently by Mrozikiewicz and colleagues. The potential influence of a standardized E. purpurea 60 % ethanolic extract of the aerial parts containing 3.7 % m/m polyphenolic compounds expressed as caffeic acid on the mRNA expression level of major CYP450 enzymes using an animal model has been investigated. The male Wistar rats were randomly divided into four groups from A to D (n = 10). Group A was treated once a day with 50 mg/kg p. o. of E. purpurea ethanolic extract for 3 days, and group B received a standard diet. Group C was treated with the same extract like group A, 50 mg/kg p. o. once a day, but for 10 days, whereas group D was used as control for group C. Total RNA was isolated from the rat liver tissue sixteen hours after the last administration. The authors concluded that the obtained in vivo data indicated a potent inhibition of the expression of CYP3A1 (41 %, p < 0.05) and CYP3A2 (25 %, p = 0.001), and an induction of CYP1A1 (80 %, p = 0.01) and CYP2D1 (40 %, p = 0.007) after the administration of an E. purpurea ethanolic extract [26]. However, nothing has been reported about the important isoform CYP3A4.

In a pharmacokinetic herb-drug interaction study in rats, the effects of different phytochemically characterized preparations of E. angustifolia, E. purpurea and E. pallida were assessed for its cytochrome P450 (CYP) interaction potential. A total of 216 rats were assigned to the different experimental groups (n = 12) with various dosages, positive/negative controls (ketoconazole, quinidine, rifampicin) and dodeca-2E,4E,8Z,10E/Z-tetraenoic acid isobutylamides (“tetraenes”). Echinacea preparations were administered for two consecutive weeks. On the last day a CYP cocktail consisting of theophylline (CYP1A2), tolbutamide (CYP2C), dextromethorphan (CYP2D), and midazolam (CYP3A) was orally administered before blood sampling. Plasma levels of substrates and their metabolites were quantified using a validated LC-MS/MS method [30]. Pharmacokinetic parameters (C_max and AUC_last) were calculated and compared with the blank control group using geometric mean ratios (GMRs) and its 90 % confidence interval (CI). E. purpurea, E. angustifolia and E. pallida preparations showed significant interactions mainly on CYP1A2 substrate activities. Co-administration of E. purpurea preparations (60 % ethanolic root extract p < 0.001; CO₂-extract p < 0.01; Echinaforce® p < 0.001 and pressed juice p < 0.01) with theophylline led to a significant increase in the AUC_last of the metabolite, 1,3-dimethyluric acid. In addition, the main alkamides of Echinacea (tetraenes) inhibited CYP1A2 with a GMR of 8.65 (7.72–9.68) for the AUC_last and 2.96 (2.59–3.39) for C_max. The pharmacokinetics of dextrorphan (rat CYP2D2 metabolite) were moderately affected. However, Echinacea formulations showed no significant inhibition on CYP3A and CYP2C activities [3], [31].

Preclinical studies conducted since 2004 indicate that Echinacea constituents modulate immune mechanisms and there is increasing evidence that lipophilic Echinacea preparations containing alkamides can suppress stress-related cellular immune responses [2], [8], [32], [33], [34], [35], [36], [37], in contrast to older literature published, which described only “immunostimulatory” effects [38], [39], [40], [41], [42], [43]. Therefore, the activity of Echinacea may better be described as “immunomodulatory” rather than immunostimulatory [44]. Warnings against the concomitant use of Echinacea spp. together with immunosuppressive drugs because of the theoretical possibility of diminished effectiveness and the ingestion in people with inflammatory conditions, such as asthma, and HIV, therefore remain questionable [45], [46].

The Eclectics, a group of practitioners, who were prominent around the late 19th and early 20th centuries in the U. S., used Echinacea (especially the root of E. angustifolia) for an extensive range of conditions, including tuberculosis [47]. The use for tuberculosis and disorders related to autoimmunity such as diabetes, exophthalmic goiter, psoriasis, and renal haemorrhages contrasts with the contraindications suggested by some recent authors.

Although it is recommended by the authorities that “Echinacea” should be avoided in patients with autoimmune diseases, very few published case reports exist in this context, moreover they have a limited causal association [48], [49]. The suggestion that Echinacea preparations are contraindicated in autoimmune diseases assumes that the modulation of any aspect of immune function is deleterious. However, immune function is extraordinarily complex and a substance that acts largely on phagocytic activity may be safe or even beneficial in autoimmunity [50], [51], [52], [53], [54]. There were no clinical or laboratory alterations (blood count, electrolytes, liver and kidney functions) reported after the ingestion of E. angustifolia whole plant dry extract (undefined extraction solvent) over 12 weeks by HIV positive subjects.

Special warnings and precautions for use

Since the possibility of immune-related adverse consequences has not been ruled out in atopic individuals, especially this group of patients should use Echinacea spp. with caution and under the supervision of a health care practitioner. The Community Herbal Monograph stated that atopic patients should consult their doctor before using Echinacea [4], [5], [6]. The potential allergenicity of Echinacea has received a fair amount of attention, although some may have not been definitively associated with the ingested Echinacea preparations [55].

Undesirable effects

Reports of adverse effects within clinical trials, comparing mono-preparations of Echinacea with placebo since 1996 are summarized in [Table 1]. Most of the adverse events were specified as mild to moderate. However a causal relationship between Echinacea and the adverse events could not be established. Headache, one of the predominant mentioned adverse effects, may not accurately reflect adverse events because it is also a frequent symptom of the common cold.

Allergic reactions

E. angustifolia (3825 mg whole plant extract) and E. purpurea (150 mg dry root) have been associated with allergic reactions, including one reported case of anaphylaxis [56], [57]. Skin allergy testing of 84 patients with asthma or allergic rhinitis demonstrated reactivity to those Echinacea extracts in 16 subjects (19 %) [57].

Huntley et al. analysed a total of 8 case reports of allergic reactions to Echinacea with such typical signs as generalized urticaria, itchy and watery eyes, gastrointestinal upset, respiratory obstruction, asthma, and a positive reaction to skin prick test (skin allergy test, SPT), which may or may not resolve with time [45]. A 19-year-old female suffered an acute asthma attack and severely itchy and watery eyes and a runny nose within 10 minutes of her first ever exposure to an Echinacea-containing tea, with no further characterization of the species and the plant part. It is necessary to mention that combination products and homeopathic preparations were excluded from this safety reviwe.

Jeschke et al. [58] published the results of a prospective pharmacovigilance study of Asteraceae extracts, including Echinacea. The aim of this study was to analyze prescribing patterns and adverse drug reactions (ADRs) for Asteraceae-containing remedies in Germany. Altogether, 18 830 patients (58.0 % female, 60.3 % children) received 42 378 Asteraceae-containing remedies. This included 2672 patients receiving 4605 Echinacea-containing prescriptions with 69 different medications (30 % phytotherapeutic, 60 % < D4, 10 % > D4). No serious adverse drug reactions were reported. In a subgroup analysis, considering also non severe adverse drug reactions in 6961 prescriptions for Asteraceae, 11 non-serious adverse reactions were detected (all for homeopathic preparations and none for phytotherapeutic preparations). This supports the observation that allergic reactions due to Echinacea products are rather rare and mostly not serious [3], [58].

There is no literature available for the Stevens-Johnson Syndrome, which is mentioned in the HMPC Monograph as an hypersensitive reaction. But obviously there have been 4 cases reported in the Eudra vigilance database [3].

Thrombocytopenia

Only one adverse event report with thrombocytopenia was identified specifically for E. pallida. Liatsos et al. [59] reported a case of severe thrombotic thrombocytopenic purpura (TTP) in an otherwise healthy 32-year-old Caucasian man. Examination revealed hypotension, sinus tachycardia, mild elevation in temperature, and few diffused petechiae, anemia (Hb = 6.0 g/dL), severe thrombocytopenia (platelets = 20 000/µL), and microangiopathic-type haemolytic anemia with fragmented red blood cells, increased indirect bilirubin, and markedly elevated LDH levels. Bacterial and viral antibodies were negative. The patient was transfused with red blood cells and fresh frozen plasmas (FFPs) but had a syncope episode followed by seizures and finally entered status epilepticus which was controlled with general anesthesia and ventilator assistance. He was treated with large-volume plasmapheresis twice a day, and administration of FFPs. He finally had an uneventful outcome [59]. Causality has not been evidenced.

Leucopenia and eosinophilia

Kemp and Franco published a case report of leucopenia associated with the long-term use of an uncharacterized Echinacea product (450 mg tid). A 51-year old woman appeared healthy from all aspects with the exception that her white cell count had decreased from 5800/µL the preceding year to 3300/µL (normal range 4000 to 11 000). For the past 8 weeks she had been taking the undefined Echinacea product (1350 mg of Echinacea per day), Ginkgo biloba L. (Ginkgoaceae; dosage not given), bupropion for depression (300 mg daily), as well as vitamins-C, -E, -B, and calcium. She suffered from hayfever, but did not take medication for it. One month after the discontinuation of therapy with Echinacea, her white cell count had increased to 3700/µL. The next year she resumed taking Echinacea and after two months her white cell count was 2880/µL. Two months after discontinuing taking Echinacea, her white cell count was 3440/µL and 7 months later arose to 4320/µL. Due to the fact, that the authors could not find another reason for the leucopenia, they assumed a relationship to the intake of Echinacea [60]. Although it is known that the concomitant ingested product, bupropion (Wellbutrin SR®), releases changes in hematology. While in a study performed by Goel et al., no significant differences between groups taking E. purpurea (ethanol extraction of various freshly harvested parts) or a placebo after white blood cell differential count were observed [61]. Furthermore, a case of a patient with eosinophilia of unclear aetiology whose condition resolved after the discontinuation of “Echinacea” has been reported. The authors felt that this represents an IgE-mediated allergic process to an uncharacterized used Echinacea preparation [62].

Erythema nodosum

One isolated report describes the case of a 41-year-old man who experienced four episodes of erythema nodosum after using an undefined Echinacea preparation at each onset of an influenza-like illness. The man had been using Echinacea intermittently for 18 months, as well as loratadine on a basis as required, and St. Johnʼs wort for the previous 6 months. Each episode of erythema nodosum responded to conventional treatment, including prednisone. The man was advised to discontinue the treatment with Echinacea and, after 1 year, he had not experienced any further recurrences. However, the report does not provide any details (species, plant part, formulation, dosage regimen) of the Echinacea (or the St. Johnʼs wort) preparation involved and therefore is difficult to interpret. Causality has not been established [63].

Sjögren syndrome

Logan and Ahmed reported on a 36 year old woman, who ingested St. Johnʼs wort, undefined Echinacea, and Kava for 2 weeks, a development of severe general muscle weakness, which resolved under supplementation of NaHCO₃ and KCl. The report did not provide any further details of the Echinacea species that was contained in the product, or of the types of preparations, formulations, dosages and routes of administration of any of the herbal medicines listed. Complaints of joint stiffness, fatigue, dry mouth and eyes surfaced 6 weeks later. Sjögren syndrome was diagnosed and a Plaquenil (hydroxychloroquine 200 mg daily) treatment begun. The abnormalities renal tubular function resulting in hypokalimea and acidification with muscle weakness, are reported because of the Sjögren syndrome. Problems resolved under therapy with prednisone and cyclophosphamide, which unterlines the autoimmunogenesis. This case may represent one example where an autoimmune disease was exacerbated. The connection between the Echinacea therapy and the undesirable effect has been estimated as possible, but is not conclusive [49].

Exanthema

An autoimmune disease supposedly triggered by an unspecified Echinacea supplement has been reported by Lee and Werth. A patient with pre-existing chronic inflammatory condition started taking Echinacea for the first time in his life at the onset of an upper respiratory tract infection. Within days the patient developed blisters on body, head and oral mucosa. The authors also mentioned that the temporal relationship of the patient disease flare with ingestion of Echinacea is strongly suggestive of a causal relationship. However, the practitioners could not rule out the possibility that the patient experienced an exacerbation as part of the natural course of his condition, nor could they dismiss the possibility that the upper respiratory tract infection contributed to his flare [48]. Furthermore, no further details of the product, including species of Echinacea, plant part, excipients, type of preparation, and dosage were provided. Without verification that the product implicated did contain Echinacea material and was free of other ingredients or adulterants, this report adds little to the debate on the safety of use of Echinacea by individuals with autoimmune disorders [48].

Among a total of 64 493 reported adverse reactions submitted to the Swedish Medical Products Agency, only 778 reports concerned adverse reactions related to the use of complementary and alternative medicine (CAM) products. 63 (8.1 %) reports concerned E. purpurea, among them mostly urticaria (11) and exanthema (13) were reported [64].

Acute cholestatic autoimmune hepatitis

In a case report by Kocaman et al. (2008) a 45-year old male patient complained of fatigue and jaundice of 1-week duration. He told that he had started taking “Echinacea root” (1500 mg/day) after catching a common cold. Physical examination revealed an icteric patient. Markers for viral hepatitis, ceruloplasmin, iron and ferritin levels, and alpha 1 antitrypsin level were not remarkable for acute hepatitis. Liver biopsy revealed an interface hepatitis, prominent cholestasis, and a portal lymphoplasmocytic and eosinophilic granulocyte infiltration. After admission, the patient stopped taking the “Echinacea”. One month later, all laboratory values were normalized, except for the anti-smooth muscle antibody positivity. The authors concluded this first report of an Echinacea-induced acute cholestatic autoimmune hepatitis (ACAH) as a result in a breakdown of autoimmunity self-control in the liver. Due to the undefined Echinacea preparation used (species, formulation) it is difficult to interpret the connection between Echinacea and the severe acute hepatitis [65]. In the same year, a case communication reported a patient with autoimmune hepatitis and hypergammaglobulinemic purpura related to an uncharacterized herbal medicine including “Echinacea, Combucha, Chinese herbal mixtures, and Kava Kava”. The 57 year old woman, a practitioner of alternative medicine, was hospitalized with jaundice and weakness. Viral serology for hepatitis B and C were negative. A liver biopsy demonstrated cirrhosis with severe piecemeal necrosis, severe intra-acinar necrosis, focal necrosis and cholestasis. The patient was started on prednisone 60 mg per day with a prompt laboratory improvement and complete normalization of her liver function. It remains speculative whether the association between the herbal preparation and the autoimmune hepatitis is causative or only coincidental. Above all, the connection between the uncharacterized “Echinacea” preparation and the autoimmune hepatitis is questionable [66].

Concerns of potential hepatotoxicity have been raised, although documented cases are lacking. Miller published that all Echinacea preparations, if used beyond 8 weeks, could cause hepatotoxicity and therefore should not be used with other known hepatotoxic drugs, such as anabolic steroids, amiodarone, methotrexate, and ketoconazole [46]. However, the magnitude of this hepatoxicity has been questioned since Echinacea lacks pyrrolizidine alkaloids with a 1,2 unsaturated necine ring associated with hepatotoxicity. There have also been hepatoprotective effects of Echinacea reported in male rats [67]. Therefore, there is no clear evidence for hepatotoxicity.

Autoimmune diseases like encephalitis disseminate and the Evans Syndrome are undesirable effects cited in the HMPC monographs with unclear background. There is no literature available in connection with Echinacea. In the recent update of the European Medicines Agency monograph on E. purpurea, herba recens [4] Evans Syndrome has already been deleted.

Effects on Reproduction and Development

Preclinical data indicate that E. purpurea aerial part or root preparations are unlikely to cause negative reproductive or developmental effects in laboratory animals. Oral doses up to 2700 mg/kg of Echinacin® did not cause embryotoxicity in rats or rabbits or affect postnatal development in rats. Studies looking for gene mutations, malignant transformation, or chromosome aberrations in bacteria, mouse lymphoma cells, cultured hamster cells, or human lymphocytes have found no evidence of mutagenicity of Echinacin® [68]. However, Ondrizek et al. reported that very high concentrations of E. purpurea (0.6 mg/mL, plant part undisclosed) applied directly to sperm impaired sperm motility and they suggested that this may have a negative effect on male fertility. Motility was inhibited at 24 and 48 h after incubation. They reported similar in vitro results using hamster sperm and oocytes [69], [70]. It is questionable whether these findings are relevant in an in vivo situation.

In 2007, the first study was conducted to evaluate whether pharmaceuticals containing alcoholic extracts of E. purpurea given to pregnant mice (n = 8) influence angiogenic activity and may then lead to severe developmental disturbances. They found an increase in the angiogenic activity of tissue homogenates in the Esberitox® group, containing 3.2 mg of a native dry extract (30 % ethanol) from Baptisia tinctoria (L.) Vent. (Fabaceae) root, E. purpurea root, E. pallida root and Thuja occidentalis L. (Cupressaceae) herba, and a diminution in case of Immunal forte (1 tablet contains 80 mg dry E. purpurea pressed juice 31–60 : 1). The growth factor concentration was lower in all groups compared to the control. They concluded that there is some possibility that pharmaceuticals containing E. purpurea might influence the fetal development in humans also, because they may interfere with embryonic angiogenesis, and should not be recommended for pregnant women [71].

The vascular endothelial growth factor (VEGF) known as the most powerful angiogenesis promoter plays a crucial role in organogenesis, liver and pancreas induction, kidney glomerulus, bone and nervous system development. Moreover, VEGF contributes to the placentation and cytotrophoblast proliferation during pregnancy. Wasiutynski et al. (2009) evaluated the effect of the following E. purpurea containing drugs on the angiogenic activity and VEGF concentration of murine sarcoma L-1 tumors: Immunal forte tablets (1 tablet contains 80 mg dry E. purpurea pressed juice 31–60 : 1; LEK, Slovenia) and Echinapur tablets (no detailed characterization; Herbapol Poznan). They found that both drugs significantly diminished the VEGF concentration in L1 sarcoma tumor tissue and they speculated that therefore they may affect the placenta formation in pregnant women [72], [73].

Perri et al. (2006) conducted a literature review with no specification of Echinacea (species, plant part and extraction method used) of seven electronic databases from their inception through 2005 and compiled data according to the degree of evidence for the use, safety, and pharmacology of Echinacea pertaining to pregnancy and lactation [74]. No association with an increased risk for major or minor malformations with a reported gestational use of Echinacea during organogenesis was found [75], [76], [77]. Capsule and/or tablet formulations of undefined Echinacea were used by 114 (58 %) of the 198 respondents, while 76 (38 %) of the respondents used tinctures. The dosage of capsules and/or tablets used varied from 250 to 1000 mg/day. Tincture dose varied from a minimum of 5 to 10 to a maximum of 30 drops per day. Duration of use also varied but was normally continuous for 5 to 7 days. The different brands used covered the two species E. angustifolia and E. purpurea without detailed characterization. 112 women (54 %) reported taking the herb in the first trimester of pregnancy, and 17 (8 %) used Echinacea throughout their pregnancies. No significant differences were noted between the Echinacea and the control groups in the rate of major or minor birth defects, nor were there any differences in pregnancy outcome, delivery method, maternal weight gain, gestational age, infant birth weight, or foetal distress. Thirteen miscarriages were documented in the Echinacea group, compared with seven in the control group [76]. The study has several limitations. The most important is that participants used a range of different preparations of Echinacea at different dosage regimens. So the study does not provide adequate evidence for a specific preparation.

Use in children

Götte and Roschke [78] made an observation in children with recurring infections of the upper respiratory tract to assess the tolerability and efficacy of an alcohol free pressed juice from the aerial parts of E. purpurea. The children had to be at least 2 years of age, and the juice was administered over a period of 11 days with doses adjusted according to age. In more than 95 % of cases (n = 1322), the physician and parents globally assessed the tolerability as good or very good [78]. It has been reported in a recently published study by Du et al. that the use of herbal medicinal products in general is closely associated with younger age between 0 and 17 years, and that two thirds of the preparations used are for the treatment of coughs and colds [79]. Taylor et al. found an increased risk of rash when children of 2 to 11 years (mean 5.5 years, standard deviation 2.7 years) received an alcohol-free preparation of dried pressed E. purpurea juice of the aerial parts, compared with those who received a placebo [80]. In this study adverse events were found in 45.1 % of patients receiving Echinacea (and in 39.5 % of patients receiving placebo). The most frequent adverse events were: stomach ache, diarrhoea, drowsiness, headache, “hyper” behaviour, rash and vomiting. Rash was the only side effect that was significantly more frequent in the Echinacea group compared to the placebo group (7.1 % versus 2.7 %, respectively). Therefore, caution is recommended when using this E. purpurea juice preparation in children who have atopy and asthma because they are likely to be at higher risk for a rash. In a subgroup analysis of the Taylor et al. data it has been found that children taking Echinacin® juice were significantly less likely to have another URI compared to children receiving placebo. Use of Echinacea was associated with a 28 % decreased risk of subsequent URI (p = 0.01) [81]. Moreover, in a study performed by Saunders and colleagues, the safety and tolerability of an open-label E. purpurea product prepared from the dried, pressed juice of aerial parts (Echinagard®) has been examined in children. The dose was based on age (2.5 mL three times q day for children aged 2–5 years, and 5 mL two times per day for children aged 6–12 years) and administered for 10 days in an open-label trial. No allergic or adverse reaction occurred and no safety issues arose during this study [82].

Four observational studies regarding the safety of the oral administration of preparations of the aerial parts of E. purpurea in different dosages for children below the age of 18 were submitted by the German authority [3]. From the in total 1184 children, two cases of nausea and two generalized exanthema have been reported, which could be due to an infection as well. Three children dropped out due to the bad taste of the preparation. Otherwise there were no reports concerning adverse events even when used more than 10 days [3].

Duration of use

Several authoritative sources (e.g. EMA/HMPC/48 704/2014) have suggested that Echinacea should be used only for limited periods of time (not longer than one week or 10 days), without giving reasons and references to verify the scientific background. The World Health Organization (1999) and the European Scientific Cooperative on Phytotherapy (ESCOP) monographs [83], citing the German Commission E monographs on Echinacea, cautions that internal and external administration of E. pallida and E. purpurea should not exceed 8 weeks, again without rationale. There was no data found supporting a treatment duration limit for Echinacea [84]. When addressing the issue of a duration limit for Echinacea preparations, Bone (2004) emphasized the importance of reviewing the traditional use of Echinacea by the U. S. Eclectic physicians that were active in the late 19th and early 20th century. Authoritative works published by these physicians, based upon their extensive clinical experience, indicate that Echinacea was used over a long-term in chronic conditions without side effects [47].

Several studies of long-term (10–24 weeks) oral use of different Echinacea preparations without occurrence of serious adverse effects have been reported [85], [86], [87]. The longest intervention of E. purpurea whole plant dry extract (undefined extraction solvent) studied to date was 800 mg twice per day for 6 months. The only adverse events reported by these subjects were nausea without vomiting (n = 4) and diarrhoea (n = 5) [87]. Melchart et al. studied the oral use of an E. purpurea root liquid extract and E. angustifolia root extract for 12 weeks (100 drops daily of a 1 : 11, 30 % ethanolic extract for 5 days a week). No toxicological concerns were reported [86]. Parnham published that no adverse reactions other than aversion to the taste have been reported after oral administration of Echinacin® (E. purpurea pressed juice) for up to 12 weeks [88]. Recently, Jawad et al. tested the safety and efficacy of E. purpurea (57.3 % m/m alcoholic extraction from freshly harvested 95 % herba and 5 % roots, Echinaforce®) in a large clinical trial (755 healthy subjects) and investigated its risk/benefit in a long-term treatment (4 month). In the haematological or biochemical measures no significant or clinically relevant changes from before to after Echinacea treatment and in comparison to placebo were detected. No abnormalities were found after the 4-month exposure to Echinacea [89]. Schapowal reported that a standardized extract of Echinacea purpurea (Echinaforce®) can be recommended for long-term use, also in children, the elderly as well as those suffering from COPD, asthma patients or smokers, people in whom the consequences of cold and flu can be severe [90].

Discussion

After review of the available literature, all medicinal species of „Echinacea“, including E. purpurea, E. angustifolia, and E. pallida appear to be quite safe. While the absence of severe drug-related adverse events does not conclusively prove safety, it is an indication that significant acute toxicological events are lacking. In a toxicity study by Mengs et al. it has been concluded that even a lethal dose could not be found [68]. Except for in vitro studies, which claim some cytotoxic effects [70], [91], studies in humans and with experimental animals are reassuring and suggesting a wide therapeutic window of safety. Oral treatment of rats for 4 weeks at doses up to 8 g/kg daily of the fresh juice of E. purpurea aerial parts failed to cause any toxicology. Moreover, oral doses up to 2700 mg/kg of the same preparation did not cause embryotoxicity in rats or rabbits or affect postnatal development in rats [68]. While Echinacea ingestion during human pregnancy is touted to be safe [74], [76], [77] others are more sceptical, indicating that other members of the family Asteraceae have distinctly negative effects on human pregnancy [56], [92]. However, the Asteraceae family is very big and plants are quite different in constituents. Echinacea for example is lacking sesquiterpene lactones. Some caution exists regarding the use of an E. purpurea extract (0.6 mg/day within Esberitox®, Immunal® or Echinapur®) in the first trimester of pregnancy based upon testing in mice. The growth factor concentration was lower in all Echinacea groups compared to the control. Based on animal studies, there is some suspicion that pharmaceuticals containing alcoholic extracts of E. purpurea and pressed juice of E. purpurea might influence fetal development in humans, because they may interfere with embryonic angiogenesis, and should therefore only be taken during pregnancy and lactation after consulting a physician [71], [72], [73], [93]. However, there is no evidence on the possibility that consuming Echinacea may promote spontaneous abortions. This hypothesis arose from only one report. Gallo et al. found a virtual doubling in the number of spontaneous abortions, i.e., in 13 women consuming two species, E. angustifolia and E. purpurea without a detailed characterization (total: 206), versus 7 in 206 women not consuming the herb [76]. It is known that, in vivo, Echinacea, given to either normal, healthy adult mice, or to adult leukemic mice, significantly increases the numbers of natural killer cells [94], [95]. Since, natural killer cells have been implicated in foetus rejection, manifesting in humans as spontaneous abortion [96], [97], [98], [99] it was speculated that Echinacea may influence abortion. Actually, the results from the human and animal studies of Echinacea spp. are not sufficient to conclude on the safety in pregnancy [100]. No firm conclusions on the risk of spontaneous abortions and angiogenesis can be drawn from the animal studies [71], [93]. The small number of test animals and the dubious relation to human conditions make the results questionable. Furthermore, Perri et al. conducted a literature review and found no significant differences between the Echinacea group (E. angustifolia and E. purpurea, without detailed characterization) and the control groups in the rate of major or minor birth defects, nor were there any differences in pregnancy outcome, delivery method, maternal weight gain, gestational age, infant birth weight, or foetal distress. For clarification and rational evaluation more studies are needed, however, pregnancy is not necessarily a contraindication and application of Echinacea preparations during pregnancy should be subjected to medical supervision.

Cautions from several authoritative sources (Community Herbal Monographs) are available and concern especially hypersensitive persons like atopic or immunosuppressed patients, the duration of use, and children. However, many trademark products containing Echinacea sp. will be defined as dietary supplements and thus not be legally bound to follow the recommendations in the official plant monographs. E. g., in the latest Monographs stated from the official European Medicines Agency (EMEA) [3], [4], [5], [6], [7], it has been suggested that the medicinally used Echinacea species should not be used for more than 10 days, but there were no pharmacological, toxicological and clinical data found supporting a limit of treatment duration for any “Echinacea” species used in either modern or traditional medical literature. The primary concerns for these temporal limits appear to be theoretical, including over-stimulation of the immune system and possible immune depression and immune habituation following long-term use. However, up to now the limitations are not justified and no substance classes can be hold responsible for the temporal limits. Long-term use of the pressed juice of Echinacea purpurea has not shown evidence of a deleterious effect on immune cells. One study reported that the immune reactivity in mice was greater after 10 weeks of continuous oral doses of an expressed juice of the aerial parts of Echinacea purpurea than after 2 weeks [85]. Miller et al. reported in a study that the chronic administration of an Echinacea purpurea root extract (0.45 mg daily for 14 months) from puberty until old age in mice resulted in the preservation of NK cell activity. Natural killer cell activity normally decreases with age and contributes to an increased mortality. The use of Echinacea purpurea preparations increased the life span of most of the mice and no toxicological concerns were noted [52]. Moreover, three further long term studies (12–24 weeks) with continuous ingestion of ethanolic Echinacea purpurea root or whole plant extracts reported no toxicological concerns [86], [87], [88], [89]. Moreover, no significant or clinically relevant changes from before to after the Echinacea treatment and in comparison to the placebo were detected in haematological or biochemical measures, after 4-month exposure to an E. purpurea preparation (alcoholic extraction from freshly harvested 95 % herba and 5 % roots) [89]. There is no firm evidence to conclude the debate on duration limits.

Application of “Echinacea” species and preparations in those taking immunosuppressive drugs has been assumed as with any immune stimulant. Similarly, those with allergic sensitivities to members of the plant family Asteraceae, as well as atopic individuals and patients with asthma, should use Echinacea species with cautions and after consulting a physician. Regardless, very few published reports exist in this context, and those have limited causal association [48], [49]. The cautions in taking “Echinacea” from atopic patients arise from the common known allergenicity to the pollen proteins from plants of the sunflower family (Asteraceae). E. purpurea aerial parts products have more potential to elicit allergic reactions in atopic individuals than do root products. Considering the fact that proteins are very poorly extracted in ethanol-water mixtures it is also unlikely that an allergy would result from the fluid extracts and tinctures of Echinacea, even if the aerial parts were used. Proteins that are potentially contained may be denaturized by alcohol and are unlikely to cause an allergic cross-reactivity [52]. This indicates that the general risk for an allergic reaction to Echinacea is low. However, atopic patients and those with asthma should be informed about such a possibility before intake of preparations containing Echinacea. The suggestion that “Echinacea” preparations are contraindicated in autoimmune disease assumes that the modulation of any aspect of immune function is deleterious. However, immune function is extraordinarily complex and a substance that acts largely on the phagocytic activity may be safe or even beneficial in autoimmunity [50], [51], [52], [53], [54]. It is known that a stimulation of cytokines may lead to an exacerbation of autoimmune related inflammation and a majority of autoimmune diseases are thought to be due to a loss of tolerance to self-antigens and a dysregulation of Th1T-helper cells. Th1 cells produce cytokines IL-2, TNF-α, and IFN-γ. There has been one report indicating that both Th1 cytokine and IFN-γ and T-cell proliferation can be stimulated by E. angustifolia [101]. Haemolytic anemia (thrombocytopenia, leucopenia and eosinophilia) have been published only in single cases, mostly with uncharacterized Echinacea preparations and concomitant intake of other drugs or herbal medicinal products, so that the relevance is not clear. The published data on leucopenia have to be considered as not relevant for the safety of Echinacea due to reports concerning the occurrence of changes in hematology, like anemia and pancytopenia after a concomitant ingestion of bupropion (product information Wellbutrin, PDR, USA). Moreover, the patient showed also low respectively borderline levels of the white cell counts without Echinacea [60].

A specific risk in children is not documented and adverse events are very rare, with no causality. Rash was the only side effect that occured significantly more frequent after the ingestion of an alcohol-free preparation of the dried pressed juice of the aerial parts of E. purpurea compared to a placebo (Taylor et al. 2003). Moreover, it has been found that those children taking the pressed juice from E. purpurea were significantly less likely to have another upper respiratory infection [81]. Risk/benefit results suggest that the use in children can be recommended, but an intake of any Echinacea preparation in children less than 1 year of age should be discussed with a physician, because their immune system is not fully developed.

Concerning pharmacokinetic herb-drug interactions, which can result in tremendous variability (over 10-fold changes) in pharmacokinetics of concomitantly administered drugs, only the studies published since 2007, present reasonable data. The studies before have been performed with different and phytochemically insufficient characterized Echinacea preparations. With the in vivo studies published no significant inhibitions of human CYP2D6 and CYP3A4 isoforms have been found after the application of standardized E. purpurea preparations (softgel capsules with 267 mg, 3 times daily or fresh plant liquid extract again in softgel capsules with 500 mg, 3 times daily) [18], [21]. No significant interaction has been found with etravirine, darunavir, and lopinavir-ritonavir, which undergoes extensive metabolism by the hepatic CYP3A4 isoform [19], [20], [21]. Only a cautious conclusion can been drawn that Echinacea alkamides inhibit CYP2E1 and CYP3A4 in human liver microsomes or enzyme substrates (supersome assay) [27]. After separating each characterized Echinacea preparation (pressed juices or alcoholic tinctures from E. purpurea and E. pallida) into its ethanol- and water-soluble components, the results directly confirmed the role of alkamides in the inhibition of CYP3A4 [24], [25]. Controversial results exist on the transcriptional/translational activities with, e.g., induction or inhibition of CYP3A4 expression. A pressed juice from the aerial parts of E. purpurea and an E. purpurea root preparation suppressed hepatic CYP3A4 expression [15], [22]. Whereas, Kortenkamp et al. found no significant changes in the steady-state CYP3A4 mRNA levels neither for Echinaforce® nor the pure alkamides [29]. However, herbal products are often marketed as dietary supplements, which have fewer requirements for testing of pharmacokinetic interaction potential before marketing compared to registered drugs. Recently the U. S. Department of Health and Human Services, Food and Drug Administration (FDA) and the European Medicines Agency (EMA) released “Guidelines on the Investigation of Drug Interactions” [102], [103]. Two pharmacodynamic interaction studies in mice exist about the administration of an E. purpurea root extract or an ethanolic extract of E. purpurea dried aerial parts. One study found a negative effect on levels of mature granulocytes after a concomitant ingestion of melatonin [9], [10]. However, a positive interaction has been reported after taking phenytoin at the same time, with a decrease in the incidence of cleft palate [11]. No evidence of any apparent effect on warfarin pharmacodynamics with platelet aggregation or baseline clotting status in healthy subjects has been found after concomitant administration of Echinacea (600 mg E. angustifolia roots and 675 mg E. purpurea roots, four times a day) with (S)-warfarin [12].

A declaration of pharmacodynamic and pharmacokinetic interactions with homeopathic preparations is not needed.

In conclusion, these data suggest that medicinally used Echinacea spp. have a very good safety profile.

Conflict of Interest

The authors declare that they have performed consulting work and analytical investigations for companies producing Echinacea products.

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