Published: 27 November 2018
Revised: 29 August 2023

Safety Information

Alert Communication

Artemisia annua (Sweet wormwood, Sweet Annie, Qing hao) extract marketed as Arthrem: risk of harm to the liver – statement under section 98 of the Medicines Act 1981

Products Affected
Information for consumers and caregivers
Information for healthcare professionals
Data Summary
What actions are Medsafe taking?
How to report adverse events
Further information

This alert communication updates a previous alert published on 15 February 2018: ‘Arthrem – potential risk of harm to the liver – statement under section 98 of the Medicines Act 1981’.

The Centre for Adverse Reactions Monitoring (CARM) has received a total of 25 reports of liver toxicity associated with the use of Artemisia annua extract marketed as Arthrem (as at 30 September 2018). CARM received 11 of these reports following publication of the previous alert.

Artemisia annua extract (also known as Sweet Wormwood, Sweet Annie or Qing hao) is marketed as a natural dietary supplement for maintaining and supporting joint health and mobility. Several products containing Artemisia annua extract are available in New Zealand.

Consumers should be aware that there is a potential risk of harm to the liver when taking products containing Artemisia annua extract.

Products Affected

The cases reported to CARM indicate use of Arthrem soft gel capsules (Promisia). Two cases also report use of GO Arthri-Remedy 1-A-Day soft gel capsules (GO Healthy).

GO Arthri-Remedy 1-A-Day was withdrawn after publication of the previous alert.

There are other products in New Zealand that contain Artemesia annua extract.


 

Information for consumers and caregivers

  • Medsafe has received information that strongly suggests Artemisia annua extract may harm the liver in some people.
  • If you develop any of the following problems: nausea (feeling sick), stomach pain, pale stools, dark urine, itching all-over, the whites of the eyes have turned yellow or the skin is yellow (jaundice), stop taking Artemisia annua extract and contact your doctor as soon as possible.
  • Medsafe has not approved any products containing Artemisia annua extract. The quality, safety and efficacy of products containing Artemisia annua extract have not been formally assessed by Medsafe.
  • Always tell your healthcare professional if you are taking any dietary supplements or herbal products. Talk to your healthcare professional if you have any concerns.
  • If you suspect you have had an adverse reaction to a product containing Artemisia annua extract or any other natural health product, report it to the Centre for Adverse Reactions Monitoring (CARM). Please see below for how to report.

 

Information for healthcare professionals

  • Liver toxicity, including hepatitis, abnormal liver function and jaundice, has been reported in patients taking products containing Artemisia annua extract.
  • Consider products containing Artemisia annua extract as a possible cause of abnormal liver function.
  • Advise patients/consumers experiencing liver problems while taking Artemisia annua extract or other natural health products to stop taking the product and to contact their GP.
  • Report any suspected adverse reactions to Artemisia annua extract, or any other natural health products, to the Centre for Adverse Reactions Monitoring (CARM). Please see below for how to report.

Data Summary

CARM has received 25 reports of liver toxicity associated with the use of products containing Artemisia annua extract, up until 30 September 2018 (Table 1).

All of the reports identified Arthrem as the medicine suspected of causing the liver reaction. GO Arthri-Remedy 1-A-Day was co-suspected in two of the 25 reports.

The number of reports received by CARM suggests that the risk of liver toxicity associated with the use of this product is approximately 0.5 to 6.3 cases per 10 000 consumers.

The pattern of liver toxicity reported in the cases varied. A hepatocellular pattern was reported in 6 cases, a cholestatic pattern in 7 cases, and a mixed pattern in 3 cases. One case of hepatic cirrhosis was also reported. No information on the pattern of liver toxicity was available for the remaining 8 cases.

All of the patients stopped taking the product containing Artemisia annua extract when signs of liver toxicity developed. At the time the information was reported to CARM, most patients had already recovered from the hepatotoxicity, or were improving.

Arthrem has been studied in a 12-week pilot study1 . During the study, one of 14 patients who took Arthrem 300 mg twice per day developed hepatitis, which was considered by the study investigators to be possibly related to Arthrem.

What actions are Medsafe taking?

Medsafe will continue to monitor the safety of Arthrem.

How to report adverse events

Online Submit a CARM report
Prescribers can also submit a report using the online reporting tool available in patient management software.
Paper Download a consumer reporting form (Word Document, 61KB, 1 page)
Download a healthcare professional reporting form (PDF, 292 KB, 2 pages)
Submit completed forms by emailing CARMreport@health.govt.nz or mail (Medsafe, Ministry of Health, 133 Molesworth Street, Thorndon, Wellington, 6011).
Email CARMreport@health.govt.nz


Medsafe cannot give advice about an individual’s medical condition. If you have any concerns about a medicine you are taking Medsafe encourages you to talk to your healthcare professional.

Further information

CARM has received 25 reports of patients who have experienced an adverse reaction to the liver after while taking a product containing Artemisia annua extract.

Table 1: Summary of Cases reported to CARM linking Arthrem with harm to the liver
CARM Report ID Age & Sex Medicines reported Reactions Reported
119615 71 M Arthrem *
Pantoprazole
Atorvastatin
Cilazapril/ hydrochlorothiazide
Fluoxetine
Terazosin
Finasteride
Ibuprofen
Febuxostat
Lesinuride
Hepatic enzymes increased
120445 48 F Arthrem *
Diltiazem
Cilazapril
Nortriptyline
Paracetamol
Magnesium
Abdominal pain
Fever
Hepatic enzymes increased
Nausea
122052 54 F Arthrem * Hepatitis
Jaundice
Pruritus
123150 76 F Arthrem *
Fish oil
Glucosamine
Turmeric
Ibuprofen
Hepatitis
Jaundice
Pruritus
124405 67 F Arthrem * Hepatic function abnormal
Jaundice
Pruritus
124539 72 F Arthrem * Hepatic enzymes increased
Jaundice
124873 55 F Arthrem *
Felodipine
Fever
Hepatitis
Jaundice
Nausea
125378 62 M Arthrem *
Atorvastatin
Omeprazole
Candesartan
Hepatitis
125847 66 F Arthrem * Hepatic function abnormal
Jaundice
125947 64 F Arthrem * Hepatic enzymes increased
Nausea
Vomiting
125969 76 F Arthrem *
Melatonin
Hepatic function abnormal
Jaundice
125970 77 M Arthrem * Hepatic function abnormal
Jaundice
126905 55 M Arthrem *
Metoprolol *
Hepatic enzymes increased
Jaundice
126933 71 F Arthrem *
GO Arthri-Remedy *
Hepatic enzymes increased
Jaundice
127445 65 M Arthrem * Anorexia
Faeces pale
Hepatic function abnormal
Jaundice
Pruritus
127447 60 M Arthrem *
Paracetamol/codeine
Diclofenac
Abdominal pain
Anorexia
Jaundice
Hepatic enzymes increased
Vomiting
127451 58 F Arthrem *
GO Arthri-Remedy *
Hepatic function abnormal
127475 64 F Arthrem * Haematuria
Hepatic enzymes increased
Jaundice
Pruritus
Purpura
127492 69 F Arthrem * Jaundice
Hepatic enzymes increased
Pruritus
Tiredness
127632 93 F Arthrem
Metoprolol
Donepezil
Pantoprazole
Atorvastatin
Isosorbide mononitrate
Aspirin
Timolol eye drops
Levothyroxine
Hepatic enzymes increased
127841 71 M Arthrem * Hepatic function abnormal
128001 69 M Arthrem * Hepatic function abnormal
128048 81 M Arthrem *
Cilazapril
Metoprolol
Allopurinol
Levothyroxine
Hepatic cirrhosis
128413 83 F Arthrem * Hepatic enzymes increased
128422 86 F Arthrem * Jaundice
Hepatitis cholestatic
Pruritus

* Medicine suspected to have caused the adverse reaction, as indicated by the reporter.

References
  1. Stebbings S, Beattie E, McNamara D, et al. 2016. A pilot randomized, placebo-controlled clinical trial to investigate the efficacy and safety of an extract of Artemisia annua administered over 12 weeks, for managing pain, stiffness, and functional limitation associated with osteoarthritis of the hip and knee. Clinical Rheumatology 35: 1829-36
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