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Milk thistle

Also listed as: Silybum marianum; St. Mary's thistle

• Overview
• Plant Description
• What's It Made Of?
• Available Forms
• How to Take It
• Precautions
• Possible Interactions
• Supporting Research

Overview

Milk thistle ( Silybum marianum ) has been used since Greco-Roman times as an herbal remedy for a variety of ailments, particularly liver problems. In the late 19th and early 20th centuries physicians in the United States used milk thistle seeds to relieve congestion of the liver, spleen, and kidneys. Today, several scientific studies suggest that active substances in milk thistle (particularly silymarin) protect the liver from damage caused by viruses, toxins, alcohol, and certain drugs such as acetaminophen (a common over the counter medication used for headaches and pain; acetaminophen, also called paracetamol, can cause liver damage if taken in large quantities or by people who drink alcohol regularly.)

Many professional herbalists recommend milk thistle extract for the prevention and/or treatment of various liver disorders including viral hepatitis, fatty liver associated with long term alcohol use, and liver damage from drugs and industrial toxins such as carbon tetrachloride.

Mushroom Poisoning Milk thistle has also been used as a preventive and/or antidote to poisoning by deathcap mushroom (Amanita phalloides). Animal studies have found that milk thistle extract completely counteracts the toxic effects of the mushroom when given within 10 minutes of ingestion. If given within 24 hours of ingestion, the herb significantly reduces the risk of liver damage and death.

Liver disease from alcohol A comprehensive review by the U.S. Agency for Healthcare Research and Quality (AHRQ) recently identified 16 scientific studies on the use of milk thistle for the treatment of various forms of liver disease. A European standardized extract of milk thistle was used in most of the trials.

Problems in study design (such as small numbers of participants, variations in the causes of liver disease, and differences in dosing and duration of milk thistle therapy) made it difficult to draw any definitive conclusions. However, five of seven studies evaluating milk thistle for alcoholic liver disease found significant improvements in liver function. Those with the mildest form of the disease appeared to improve the most. Milk thistle was less effective for those with severe liver disease such as cirrhosis. Cirrhosis is characterized by scarring and permanent, non-reversible damage to the liver. It is often referred to as end-stage liver disease.

Viral hepatitis Despite the fact that milk thistle is widely used in the treatment of hepatitis (particularly hepatitis C), results from four viral hepatitis studies were contradictory. Some found improvements in liver enzyme activity while others failed to detect these benefits. None of the studies compared milk thistle with interferon or other medications for viral hepatitis.

Cancer Preliminary laboratory studies also suggest that active substances in milk thistle may have anti-cancer effects. One active substance known as silymarin has strong antioxidant properties and has been shown to inhibit the growth of human prostate, breast, and cervical cancer cells in test tubes. Further studies are needed to determine whether milk thistle is safe or effective for people with these forms of cancer.

Plant Description

Milk thistle is native to the Mediterranean, but is now widespread throughout the world. This stout thistle usually grows in dry, sunny areas. The stem branches at the top, and reaches a height of 4 to 10 feet. The leaves are wide, with white blotches or veins. The flowers are red-purple. The small, hard-skinned fruit is brown, spotted, and shiny. Milk thistle is easy to grow, and it matures quickly, in less than a year.

What's It Made Of?

The active ingredient, or liver-protecting compound in milk thistle is known as silymarin. This substance, which actually consists of a group of compounds called flavonolignands, helps repair liver cells damaged by alcohol and other toxic substances. Silymarin also keeps new liver cells from being destroyed by these same substances, reduces inflammation (important for people with liver inflammation or hepatitis), and has potent antioxidant effects.

Most milk thistle products are standardized preparations extracted from the fruits (seeds) of the plant. Most preparations are standardized to contain 70% to 80% of flavonolignans (silibinin, silychristin, and silydianin), collectively known as silymarin.

Available Forms

• Capsules of standardized dried herb (each capsule contains about 120 to 140 mg silymarin)
• Liquid extract
• Tincture
• Silymarin phosphatidyl choline complex

The silymarin in milk thistle seeds is difficult to absorb. The more concentrated the solution of silymarin, the more easily it is absorbed and the more readily it enters the bloodstream. Standardized capsules are the most concentrated form and, therefore, should be used whenever possible. Silymarin-phosphatidylcholine complex may be absorbed even more easily than regular standardized milk thistle. In clinical trials, the silymarin-phosphatidylcholine complex has worked better than silymarin by itself for treating liver disorders. A key element in cell membranes, phosphatidylcholine helps the silymarin attach easily to the cell membranes. This may keep toxins from getting inside liver cells. Alcohol extracts may be less effective and, therefore, should likely be avoided.

How to Take It

Pediatric

Adjust the recommended adult dose to account for the child's weight. Most herbal dosages for adults are calculated on the basis of a 150 lb (70 kg) adult. Therefore, if the child weighs 50 lb (20 to 25 kg), the appropriate dose of milk thistle for this child would be 1/3 of the adult dosage.

Adult

• Recommended dose: Generally 12 to 15 g dried herb (200 to 400 mg silymarin) per day or silymarin-phosphatidylcholine complex 100 to 200 mg two times per day.
• For liver protection: 120 mg silymarin (about 2 capsules), two times daily
• To treat liver damage (from alcohol, drugs, or chemicals): 120 mg (about 3 capsules), three times per day

Precautions

The use of herbs is a time-honored approach to strengthening the body and treating disease. Herbs, however, contain active substances that can trigger side effects and interact with other herbs, supplements, or medications. For these reasons, herbs should be taken with care, under the supervision of a practitioner knowledgeable in the field of botanical medicine.

Side effects from milk thistle happen only rarely, but may include stomach pain, nausea, vomiting, diarrhea, headache, rash or other skin reactions, joint pain, impotence, and anaphylaxis (a life-threatening allergic reaction that causes throat tightness, shortness of breath, and, possibly, loss of consciousness.) The last two reactions listed are extremely rare.

Milk thistle should not be used by pregnant or breastfeeding women.

Possible Interactions

If you are currently being treated with any of the following medications, you should not use milk thistle without first talking to your healthcare provider.

Similar to its ability to protect against damage to the liver from alcohol and acetominophen, as discussed in the Overview, milk thistle may also protect against liver damage from the following medications:

• Antipsychotics : This group of medications used for schizophrenia includes butyrophenones (such as haloperidol) and phenothiazines (such as chlorpromazine, fluphenazine, and promethazine)
• Phenytoin : a medication used for seizures
• Halothane : a medication used during general anesthesia

Other medications that may interact with milk thistle include:

Aspirin
One animal study found that milk thistle may enhance the effectiveness of aspirin in rats with liver cirrhosis. Whether this herb-drug combination has the same effect in people is not known at this time.

Chemotherapy medications
Preliminary research suggests that silybin may enhance the tumor fighting effects of cisplatin and doxorubicin when tested against breast and ovarian cancer cells.

In addition, milk thistle may protect the kidneys against toxic side effects associated with cisplatin and cyclosporine, two medications that are commonly used to treat cancer.

On the other hand, a different laboratory study revealed that the anticancer effect of cisplatin and ifosfamide was diminished in the presence of milk thistle. More research needs to be done to assess how milk thistle and cancer-fighting agents interact.

Supporting Research

Agency for Healthcare Research and Quality. Milk thistle: effects on liver disease and cirrhosis and clinical adverse effects. Summary, evidence report/technology assessment: number 21, September 2000. Accessed at: http://www.ahrq.gov/clinic/milktsum.htm on April 15, 2002.

Bhatia N, Zhao J, Wolf DM, Agarwal R. Inhibition of human carcinoma cell growth and DNA synthesis by silibinin, an active constituent of milk thistle: comparison with silymarin. Cancer Lett . 1999;147(1-2):77-84.

Blumenthal M, Goldberg A, Brinckmann J. Herbal Medicine: Expanded Commission E Monographs . Newton, MA: Integrative Medicine Communications; 2000:257-263.

Bokemeyer C, Fels LM, DunnT, et al. Silibinin protects against cisplatin-induced nephrotoxicity without compromising cisplatin on isosfamide anti-tumor activity. Br J Cancer . 1996;74:2036–2041.

Brinker F. Herb Contraindications and Drug Interactions . 2nd ed. Sandy, OR: Eclectic Medical Publications; 1998:103-104.

Campos R, Garrido A, Guerra R, et al. Silybin dihemisuccinate protects against glutathione depletion and lipid peroxidation induced by acetaminophen on rat liver. Planta Med . 1989;55:417–419.

Feher J, Deak G, Muzes G, Lang I, Neiderland V, Nekan K, et al. Hepatoprotective activity of silymarin therapy in patients with chronic alcoholic liver disease. Orv Hetil . 1990;130:51.

Ferenci P, Dragosics B, Dittrich H, Frank H., Benda L, Lochs H, et al. Randomized controlled trial of silymarin treatment in patients with cirrhosis of the liver. J Hepatol . 1989;9:105-113.

Fintelmann V. Modern phytotherapy and its uses in gastrointestinal conditions. [Review]. Planta Med. 1991;57(7):S48-52.

Flora K, Hahn M, Rosen H, Benner K. Milk thistle ( Silybum marianum ) for the therapy of liver disease. Am J Gastroenterol . 1998;93:139–43.

Gaedeke J, Fels LM, Bokemeyer C, et al. Cisplatin nephrotoxicity and protection by silibinin. Nephrol Dial Transplant . 1996;11:55–62.

Giese LA. A study of alternative health care use for gastrointestinal disorders. Gastroenterol Nurs . 2000;23(1):19-27.

Jiang C, Agarwal R, Lu J. Anti-angiogenic potential of a cancer chemopreventive flavonoid antioxidant, Silymairn: inhibition of key attributes of vascular endothelial cells and angiogenic cytokine secretion by cancer epithelial cells. Biochem Biophys Res Commun . 2000;276:371-378.

Krecman V, Skottova N, Walterova D, Ulrichova J, Simanek V. Silymarin inhibits the development of diet-induced hypercholesterolemia in rats. Planta Med . 1998;64(2):138-142.

Low Dog T. Traditional and alternative therapies for breast cancer. A ltern Ther Health Med . 2001;7(3):36-47.

Luper S. A review of plants used in the treatment of liver disease: part 1. [Review].

Altern Med Rev . 1998;3(6):410-421.

Mourelle M, Favari L. Silymarin improves metabolism and disposition of aspirin in cirrhotic rats. Life Sci. 1988;43:201–207.

Palasciano G, Portincasa P, Palmieri V, Ciani D, Vendemiale G, Altomare E. The effect of silymarin on plasma levels of malon-dialdehyde in patients receiving long-term treatment with psychotropic drugs. Curr Therapeut Res . 1994;55(5):537-545.

Rotblatt M, Ziment I. Evidence-Based Herbal Medicine . Philadelphia, PA: Hanley & Belfus, Inc; 2002:266-271.

Scanbia G, De Vincenzo RD, Ranelletti FO, et al. Antiproliferative effect of Silybin on gynaecological malignancies: synergism with cisplatin an doxorubicin. Eur J Cancer . 1996;32A(5):877-882.

Silybum marianum (Milk Thistle). Alt Med Rev . 1999;4(4):272-274.

Valenzuela A, Lagos C, Schmidt K, et al. Silymarin protection against hepatic lipid peroxidation induced by acute ethanol intoxication in the rat. Biochem Pharmacol . 1985;34(12):2209–2212.

von Schonfeld J, Weisbrod B, Muller MK. Silibinin, a plant extract with antioxidant and membrane stabilizing properties, protects exocrine pancreas from cyclosporin A toxicity. Cell Mol Life Sci. 1997;53(11–12):917–920.

White L, Mavor S. Kids, Herbs, Health . Loveland, Colo: Interweave Press; 1998:22, 36.

Zi X, Feyes DK, Agarwal R. Anticarcinogenic effect of a flavonoid antioxidant, silymarin, in human breast cancer cells MDA-MB 468: induction of G1 arrest through an increase in Cip1/p21 concomitant with a decrease in kinase activity of cyclin-dependent kinases and associated cyclins. Clin Cancer Res . 1998;4(4):1055-1064.

Zi X, Mukhtar H, Agarwal R. Novel cancer chemopreventive effects of a flavonoid antioxidant silymarin: inhibition of mRNA expression of an endogenous tumor promoter TNF-alpha. Biochem Biophys Res Commun . 1997;239(1):334–339.

• Review Date: 4/1/2002
• Reviewed By: Participants in the review process include: Jacqueline A. Hart, MD, Department of Internal Medicine, Newton-Wellesley Hospital, Harvard University and Senior Medical Editor Integrative Medicine, Boston, MA; Gary Kracoff, RPh (Pediatric Dosing section February 2001), Johnson Drugs, Natick, MA; Steven Ottariono, RPh, Veteran's Administrative Hospital, Londonderry, NH; David Winston, Herbalist (April 1999), Herbalist and Alchemist, Inc., Washington, NJ; Tom Wolfe, P.AHG (April 1999), Smile Herb Shop, College Park, MD. All interaction sections have also been reviewed by a team of experts including Joseph Lamb, MD (July 2000), The Integrative Medicine Works, Alexandria, VA;Enrico Liva, ND, RPh (August 2000), Vital Nutrients, Middletown, CT; Brian T Sanderoff, PD, BS in Pharmacy (March 2000), Clinical Assistant Professor, University of Maryland School of Pharmacy; President, Your Prescription for Health, Owings Mills, MD; R. Lynn Shumake, PD (March 2000), Director, Alternative Medicine Apothecary, Blue Mountain Apothecary & Healing Arts, University of Maryland Medical Center, Glenwood, MD; Ira Zunin, MD, MPH, MBA (July 2000), President and Chairman, Hawaii State Consortium for Integrative Medicine, Honolulu, HI.

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