| Literature DB >> 23818934 |
Julino Assunção Rodrigues Soares Neto1, Edna Myiake Kato, Adriana Bugno, José Carlos F Galduróz, Luis Carlos Marques, Thiago Macrini, Eliana Rodrigues.
Abstract
The present study aimed to assess the quality and risks involved in the consumption of psychoactive herbal products (PHs) that are available through informal commerce in the city of Diadema, SP, Brazil. Methods of ethnography were used to conduct the fieldwork during which four dealers were selected to record the collection, handling, packaging, types of PHs marketed, and their therapeutic purposes. In addition, lots of the PHs selected were purchased from the dealers and analyzed using microbiology and pharmacognosy techniques. 217 PHs were recorded and categorized into two main groups: stimulants (67%) and depressants (27%) of the central nervous system; sixteen of them were selected, and their 52 lots were acquired. The deficiencies observed in handling and packaging these lots by dealers were confirmed by microbiological analysis; 80.8% of them presented risk according to the indicators defined by the Brazilian Pharmacopoeia. The pharmacognostic analysis confirmed the authenticity of only 9 to 16 PHs analyzed. In addition, descriptions of contraindications, adverse reactions, and drug interactions were found in the literature for the PHs. The results of this study allow the observation of the priorities for the sanitary adequacy of the popular trade of herbs.Entities:
Year: 2013 PMID: 23818934 PMCID: PMC3684123 DOI: 10.1155/2013/894834
Source DB: PubMed Journal: Evid Based Complement Alternat Med ISSN: 1741-427X Impact factor: 2.629
16 PHs investigated in this study and their ethnopharmacological, microbiological, and pharmacognostic data and published reports indicating their possible risks of use.
| 16 PHDs (52 lots) | Ethnopharmacology Psychoactive use | Microbiology (no. of lots containing the following microorganisms) | Pharmacognosy authenticity (no. of lots containing foreign material) | Literature data indicating risk of use |
|---|---|---|---|---|
| Star anise (2 lots analyzed) | Depressant and stimulant (seeds) | Not detected | (+) | Toxicity: neurotoxicity has been associated with the use of star anise infusions in infants. The toxicity is attributed to adulteration or contamination of Chinese star anise ( |
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| Depressant and stimulant (flowers) |
| (+) | Contraindications: hypersensitivity to matricaria flower or other members of the Asteraceae family, atopic high fever or asthma, and pregnancy. Pregnancy category: internal consumption of the whole plant should be avoided during early pregnancy. Adverse effects: anaphylaxis, emesis in high doses, conjunctivitis, eye-lid angioedema, contact dermatitis, eczema, and rhinitis. Interactions: anticoagulants [ |
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| Catuaba | Stimulant (stem barks) |
| (−) | Interactions: front of antidepressant effects experimentally verified with mechanisms of inhibition of the reuptake of serotonin and dopamine; catuaba |
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| Clove vine | Stimulant (stalks) |
| (+) | Interactions: checking for the presence of coumarin in parts of the plant allows to relate theory, its potential interaction with drugs and herbal anticoagulants [ |
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| St. John wort | Depressant and Stimulant (leaves) |
| (−) | ** |
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| Stimulant (leaves) |
| (+) | Adverse events: dermatitis is likely to occur following contact with the plant. It can be irritating to mucous membranes and, if ingested or placed in the eye, it might cause periorbital edema, cheilitis, eye irritation, stomatitis, and rectal irritation. In sensitized patients, it can produce pruritus ani. Nausea and vomiting may occur after ingesting the leaf extract or the seeds. Contraindications: hypersensitivity to ginkgo; concomitant use of aspirin or other antiplatelet medication. Interactions: drugs such as anticonvulsants, anticoagulants, low molecular weight heparins, selective serotonin reuptake inhibitors, monoamine oxidase inhibitors, and thiazide diuretics. Pregnancy: pregnancy risk category C; not recommended during lactation [ |
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| Ginseng | Stimulant (roots) |
| (−) | For the roots of |
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| Guarana | Stimulant (seeds) |
| (+) | Contraindications: hypersensitivity to guarana, arrhythmia, pregnancy, breastfeeding, and severe signs of toxicity have not been reported but the usual cautions regarding caffeine apply; guarana should not be used or used with caution in patients with cardiovascular disease, chronic headache, diabetes, gastric ulcer, and in those taking theophylline, not recommended for excessive long-term use. Pregnancy: do not use during pregnancy; do not use during lactation. Interactions: drugs such as clonazepam, diazepam, alendronate, cimetidine, theophylline, and pantoprazole. Adverse effects: agitation, insomnia, nervousness, restlessness, gastrointestinal irritation, serious: arrhythmias (at high doses), palpitations (at high doses), tachycardia (at high doses), and excessive central nervous system stimulation [ |
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| Jatob | Stimulant (barks) |
| (−) | ** |
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| Passion fruit | Depressant (leaves) |
| (+) | Adverse effects: Information is limited concerning toxicity of |
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| Marapuama | Stimulant (stem barks) |
| (+) | Interactions: although there is little information available, it was found that crude ethanolic extract of marapuama increases the amphetamine-induced toxicity in animal models (amphetamine stereotypy test, lethality of yohimbine and by reversal of reserpine ptosis). There was occurrence of convulsions, cyanosis, and increased mortality of animals used in testing [ |
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| Lemon balm | Depressant (leaves) | Enterobacter | (−) | ** |
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| Mulungu | Depressant (barks) |
| (−) | ** |
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| Node of dog | Stimulant (roots) |
| (−) | Little information is available for both |
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| Lime flower | Depressant (leaves) |
| (+) | Contraindications: it topically can cause hives; frequent use of flowers in the form of tea is associated with rare cardiac damage and should be used with caution in patients with heart problems. A case of a pollinic patient sensitized to lime flower pollen ( |
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| Valerian | Depressant (roots) |
| (+) | Adverse effect: chronic ingestion of valerian has been associated with headache, insomnia, agitation, and hepatotoxicity. Cardiac complications and delirium have been reported following abrupt withdrawal. Symptoms of overdose have included fatigue, lightheadedness, abdominal pain, tremor, hypotension, and mydriasis. Interactions: barbiturates, benzodiazepines, ethanol, hepatotoxic agents, loperamide, and opioid analgesics [ |
(+) Plants that have their authenticity confirmed by the Pharmacopoeia and (−) plants that had no confirmation of their authenticity.
**Data on the adverse effects were not collected due to the absence of their botanical identification.