Related Terms

• Acetadote®, acetiscisteína, acetylcistein natrium, acetylcysteine, CAS 616-91-1, cysteine, dacistein, Fabrol(, Fluimucil(, Flumacil®, Hidonac®, L-cysteine, L-cysteine HCl, Lysomucil®, Mucomyst®, N-acetil cysteine, N-acetyl-B-cysteine, N-acetylcysteine.

Background

• N-acetyl cysteine (NAC) is made from the amino acid L-cysteine. It is a source of sulfhydryl (-SH) groups and, thus, may act as a strong antioxidant.

• Because it has the ability to thin mucus, NAC has been used traditionally as a decongestant. It has also been used to reduce poisoning associated with compounds such as acetaminophen and heavy metals.

• NAC has been used clinically for approximately 40 years and has shown benefit for treating bronchiolitis and chronic bronchitis. Recent study has investigated its role as an antioxidant with the potential to treat HIV infection, cancer, and heart conditions. There is a lack of evidence of benefit in using NAC to prevent kidney impairment or to treat hepatitis, cystic fibrosis, or erythropoietic protoporphyria (a disorder caused by a defect in making heme).

• NAC is generally well tolerated. The most frequent side effects are diarrhea, nausea, and vomiting. NAC is also well known for its unpleasant taste.

Scientific Evidence

Tradition/Theory

The below uses are based on tradition or scientific theories. They often have not been thoroughly tested in humans, and safety and effectiveness have not always been proven. Some of these conditions are potentially serious and should be evaluated by a qualified health care professional.

• Abdominal pain, adjunct in surgery, aging, alcoholic liver disease, allergy, anti-inflammatory, antioxidant, arthritis, ataxia, attention-deficit hyperactivity disorder (ADHD), autism, autoimmune diseases, blood disorders, bile duct disorders, brain damage, burns, chronic fatigue syndrome, circulation improvement, common cold, congestive heart failure, diabetes, diabetic retinopathy, dialysis, ear infections, emphysema, epilepsy (Unverricht-Lundborg disease), fatigue, fibromyalgia, gallstones, hay fever, headaches, hearing loss, heart disease, heavy metal/lead toxicity, hepatitis B, immune function, infant development / neonatal care (meconium obstruction, intestinal obstruction), intestinal blockage (meconium ileus), kidney or bladder stones, kidney toxicity, liver disease, liver protection, lung cancer, lung problems, memory, meningitis, mental illness, metabolic disorders (glutathione synthetase deficiency, lysosomal storage disorders), mucilage, muscle pain, muscle weakness, nasal congestion, neuropathy, obesity, Parkinson's disease, pneumonia, poisoning, premature labor prevention, radiation skin protection, Raynaud's disease, retinitis pigmentosa, scleroderma, sinusitis, skin problems, smoking cessation, sports injuries, stroke, toxin/alcohol elimination from the body, urinary tract health (mucolysis).

Dosing

The below doses are based on scientific research, publications, traditional use, or expert opinion. Many herbs and supplements have not been thoroughly tested, and safety and effectiveness may not be proven. Brands may be made differently, with variable ingredients, even within the same brand. The below doses may not apply to all products. You should read product labels, and discuss doses with a qualified healthcare provider before starting therapy.

Adults (18 years and older)

• Note: Intravenous or inhaled N-acetyl cysteine (NAC) should be used only under the supervision of a health care provider. All patients should consult a healthcare provider before starting any treatment.

• For acetaminophen toxicity, an initial dose of 140 milligrams per kilogram NAC has been taken by mouth, followed by 70 milligrams per kilogram every four hours for 72 hours or until serum levels of acetaminophen were undetectable. A loading dose of 140-150 milligrams per kilogram body weight of NAC, followed by 50-70 milligrams per kilogram over four hours, with or without 100 milligrams per kilogram over 8-16 hours (or until serum acetaminophen levels were undetectable), has been used parenterally.

• For acute respiratory distress syndrome, 150 milligrams per kilogram body weight of NAC has been delivered intravenously over 20 minutes the first day, followed by 50 milligrams per kilogram daily for three days.

• For acute respiratory infections, 200-230 milligrams of NAC has been taken by mouth two to three times daily for 6-15 days.

• For addiction to gambling, 600 milligrams of NAC, increasing every two weeks to a dose of 1,800 milligrams, has been taken by mouth for up to 14 weeks.

• For angina, 2 grams of NAC in 100 milliliters of saline has been delivered intravenously over 15 minutes, followed by 5 milligrams per kilogram body weight per hour over 30 hours, as has 5 grams of NAC in 200 milliliters of 5% dextrose infused over 15 minutes, every six hours over a period of 24 hours.

• For asthma, 0.5% nebulized NAC has been inhaled.

• For exercise performance enhancement,125 milligrams per kilogram body weight of NAC per hour has been infused intravenously for 15 minutes, followed by 25 milligrams per kilogram body weight per hour for 20 minutes prior to and throughout exercise.

• For sulfur mustard-induced bronchiolitis (swelling in the small air passages of the lungs), 1,200-1,800 milligrams of NAC has been taken by mouth in two or three divided doses daily for four months.

• For chemotherapy adverse events, 5.5 grams per square meter body mass of NAC has been taken by mouth one hour before doxorubicin therapy every four weeks until the doxorubicin dose reached 300-350 milligrams per square meter or 500-550 milligrams per square meter. NAC at a dose of 1,200 milligrams has been taken by mouth 1.5 hours prior to oxaliplatin for 12 treatment cycles, with fluorouracil and leucovorin.

• For chronic bronchitis, 200-600 milligrams of NAC has been taken by mouth twice daily for up to six months, as well as 300 milligrams of NAC in controlled-release tablets twice daily for six months.

• For chronic obstructive pulmonary disease, 600 milligrams of NAC has been taken by mouth daily for six months.

• For cocaine withdrawal, 600 milligrams of NAC has been taken by mouth every 12 hours for a total of four doses.

• For depression, 1 gram of NAC has been taken by mouth twice daily for 24 weeks.

• For diminished appetite (high-altitude anorexia), 400 milligrams of NAC has been taken by mouth daily with breakfast.

• For dry eye syndrome, 20% NAC ophthalmic solution every two hours has been applied to the affected eye.

• For female infertility, 1,200 milligrams of NAC has been taken by mouth daily for five days starting at day two or three of the menstrual cycle. Patients were also using clomiphene citrate.

• For heart protection during coronary artery bypass grafting (CABG), an induction cardioplegia solution containing 4 millimoles per liter of NAC, and a maintenance cardioplegia solution containing 2 millimoles per liter of NAC has been delivered through a catheter. Also studied was a dose of 300 milligrams of NAC added to intermittent antegrade blood cardioplegia. Fifty milligrams per kilogram body weight NAC has been added to cold blood cardioplegia. For one hour before the procedure a dose of 50 milligrams per kilogram body weight has been intravenously infused, followed by intravenous infusion for 48 hours after the operation at a dose of 50 milligrams per kilogram body weight daily.

• For Helicobacter pylori infection, 10 milliliters (400 milligrams) of NAC has been taken by mouth three times daily for 10 days with clarithromycin and lansoprazole.

• For hyperhomocysteinemia (high blood levels of homocysteine), 600 milligrams of NAC has been taken by mouth daily for eight weeks. Five grams of NAC (Hidonac®) in 500 milliliters of 5% glucose has been intravenously infused for four hours in patients with end-stage kidney disease.

• For influenza prevention, 600 milligrams of NAC effervescent tablets have been taken by mouth twice daily for six months.

• For male infertility, 600 milligrams of NAC has been taken by mouth daily for 26 weeks.

• For miscarriage prevention, 600 milligrams of NAC plus folic acid has been taken by mouth daily up to week 20 of gestation or miscarriage.

• For myocardial ischemia (decreased blood flow to the heart), 100 milligrams per kilogram body weight NAC with streptokinase has been used intravenously six times daily. A loading dose of 20 milligrams per minute of NAC for one hour, followed by 10 milligrams per minute for 23 hours with streptokinase and nitroglycerine, has been delivered parenterally. A dose of 150 milligrams per kilogram body weight of NAC in 250 milliliters of 5% dextrose over 30 minutes or 15 grams over 24 hours with streptokinase has also been used.

• For nosebleed, 600 milligrams of NAC has been taken by mouth three times daily for 12 weeks.

• For organ transplantation, a 20% NAC solution in 0.9% saline (150 milligrams per kilogram body weight) 15 minutes prior to cardiac arrest has been intravenously infused, followed by 75 milligrams per kilogram body weight of NAC via portal vein in perfusion solution during cold phase dissection (1 gram per liter for 3 liters of citrate solution).

• For pancreatitis, 600 milligrams of NAC has been given by mouth at 12 and 24 hours prior to endoscopic retrograde cholangiopancreatography, followed by 600 milligrams given intravenously twice daily for two days following the procedure. Six hundred milligrams of NAC has been administered intravenously 12 and 24 hours prior to endoscopic retrograde cholangiopancreatography, followed by 600 milligrams twice daily for two days after the procedure.

• For plaque formation, 4 milliters of a 10% aqueous solution has been used in the mouth.

• For polycystic ovarian syndrome, 1.2 grams of NAC has been taken by mouth daily, starting on day three of the menstrual cycle, for five days with clomiphene citrate. Another dose taken by mouth was 1.8-3 grams of NAC daily for 5-6 weeks.

• For recovery after heart surgery, 600 milligrams has been taken by mouth the day before surgery, followed by a bolus of 150 milligrams per kilogram body weight delivered intravenously before skin incision, followed by perfusion at 12.5 milligrams per kilogram per hour for 24 hours.

• For pregnancy support, 600 milligrams of NAC plus 17-hydroxyprogesterone caproate has been taken by mouth daily until 36 weeks of pregnancy or active labor.

• For schizophrenia, two 500-milligram capsules of NAC have been taken by mouth twice daily for 24 weeks.

• For sepsis, 150 milligrams per kilogram body weight NAC has been infused over 15 minutes, followed by a continuous infusion of 50 milligrams per kilogram body weight over four hours.

• For Sjögren's syndrome, 200 milligrams of NAC has been taken by mouth three times daily for four weeks.

• For ulcerative colitis, 800 milligrams has been taken by mouth daily for four weeks, in addition to mesalamine.

Children (under 18 years old)

• Note: Intravenous N-acetyl cysteine (NAC) should be used only under the supervision of a health care provider. All patients should consult a healthcare provider before starting any treatment.

• For acetaminophen toxicity, a loading dose of 140 milligrams per kilogram body weight of NAC, followed by 70 milligrams per kilogram body weight every four hours for 72 hours or until serum levels of acetaminophen were undetectable, has been taken by mouth. A loading dose of 150 milligrams per kilogram body weight of NAC over 15 minutes, followed by 50 milligrams per kilogram body weight over four hours, and then 100 milligrams per kilogram body weight for 16 hours (total duration varies) has been used parenterally.

• For acute respiratory infection, 300-600 milligrams (depending on age) has been taken by mouth for eight days. A dose of 100-300 milligrams (depending on age) has been taken by mouth for six days.

Safety

The U.S. Food and Drug Administration does not strictly regulate herbs and supplements. There is no guarantee of strength, purity or safety of products, and effects may vary. You should always read product labels. If you have a medical condition, or are taking other drugs, herbs, or supplements, you should speak with a qualified healthcare provider before starting a new therapy. Consult a healthcare provider immediately if you experience side effects.

Allergies

• Avoid with known allergy or hypersensitivity to N-acetyl cysteine (NAC) and related substances.

• There have been reports of patients developing an anaphylactic-like reaction to NAC. Features of the anaphylactic-like reaction include rash, swelling under the skin, low blood pressure, and bronchospasm. Hives have also been reported.

Side Effects and Warnings

• NAC is generally well tolerated and regarded as safe. Most side effects of NAC resulted at single doses of greater than 9 grams when part of a daily regime of greater than 30 grams daily. The most common side effects in humans include diarrhea, nausea, vomiting, and headache.

• Patients treated for acetaminophen toxicity with NAC have died secondarily to questionable NAC overdose. Intravenous or inhaled NAC should only be used under a physician's care. All patients should consult with a healthcare provider before starting any treatment.

• There have been reports of patients developing an anaphylactic-like reaction to NAC. Features of the anaphylactic-like reaction include rash, swelling under the skin, low blood pressure, and bronchospasm. Hives have also been reported.

• Other potential side effects include abnormally slow or fast heartbeat, angina, appetite loss, asthmatic reaction, bad taste, blurred vision, brain disorder, burning at the infusion site, chest pain, chest tightness, cold symptoms, constipation, cough, coughing up blood, decreased peak flow and exercise tolerance, sore throat, diarrhea, disorientation and inability to concentrate, dizziness, dry mouth, facial swelling, feeling of warmth without flushing, fever, flushing, gas, headache, heartburn, hemorrhage, hives, increase in resistance when inhalation NAC is administered undiluted in patients with "low-resistance" chronic obstructive pulmonary disease (COPD), increased deterioration in bulbar function in patients with amyotrophic lateral sclerosis, increased frequency of cyanosis in premature infants, increased phlegm, indigestion, inflammation, intolerance to taste and odor, itching, pain, joint pain, leg pain, lightheadedness, magnesium deficiency, metallic taste, muscle contraction disorder, nausea, pain in the upper abdomen, painful urination, palpitations, pooling of blood and multiple hemorrhages of the bowel mucosa, rash, respiratory arrest (during treatment for acetaminophen toxicity with intravenous NAC), shortness of breath, seizure followed by cortical blindness (during intravenous NAC therapy for acetaminophen ingestion), skin abrasion, skin redness, stomach damage, sweating, throat irritation, tiredness, unpleasant mood, vein inflammation at the site of injection, vomiting, wheezing.

• NAC may increase the risk of bleeding. Caution is advised in patients with bleeding disorders or taking drugs that may increase the risk of bleeding. Dosing adjustments may be necessary.

• NAC may increase blood pressure. Caution is advised in patients with blood pressure disorders or in those taking drugs, herbs or supplements that affect blood pressure.

• NAC may increase blood sugar levels. Caution is advised in patients with diabetes, hyperglycemia or hypoglycemia, and in those taking drugs, herbs, or supplements that affect blood sugar. Blood glucose levels may need to be monitored by a qualified healthcare professional, including a pharmacist, and medication adjustments may be necessary.

• Use with caution in patients with heart disease, due to increased risk of changes in heart function, such as palpitations and rapid heartbeat.

• Use with caution in patients with gastrointestinal disorders, due to the risk of increased gastrointestinal symptoms.

• Use with caution in patients with respiratory disorders, due to a potential for increased respiratory symptoms such as wheezing, shortness of breath, cough, and sputum (phlegm) production.

• Use with caution in patients using antibiotics, due to theoretical negative interactions.

• Use with caution in patients needing charcoal treatment, as charcoal may reduce NAC absorption and efficacy.

• Use with caution in patients using nitroglycerin, due to a potential for increased headaches and coronary dilation.

• Use with caution in zinc-deficient patients, due to possible decreased zinc absorption with high doses of NAC.

• Use with caution in patients with unpleasant mood, due to a potential for increased symptoms.

• Use with caution in patients complaining of dizziness, lightheadedness, or with visual complaints, due to a potential for increased symptoms.

• Avoid in patients with allergy or hypersensitivity to NAC. NAC should be used in allergic patients only when medical personnel consider it necessary.

• Avoid use of doses greater than 30 grams daily.

• Avoid in pregnant or breastfeeding women due to a lack of safety data. NAC has been used for acetaminophen toxicity in pregnant women.

Pregnancy and Breastfeeding

• Avoid in pregnant or breastfeeding women due to a lack of safety data. NAC has been used for acetaminophen toxicity in pregnant women.

Interactions

Most herbs and supplements have not been thoroughly tested for interactions with other herbs, supplements, drugs, or foods. The interactions listed below are based on reports in scientific publications, laboratory experiments, or traditional use. You should always read product labels. If you have a medical condition, or are taking other drugs, herbs, or supplements, you should speak with a qualified healthcare provider before starting a new therapy.

Interactions with Drugs

• NAC may increase the risk of bleeding when taken with drugs that increase the risk of bleeding. Some examples include aspirin, anticoagulants ("blood thinners") such as warfarin (Coumadin®) or heparin, anti-platelet drugs such as clopidogrel (Plavix®), and non-steroidal anti-inflammatory drugs such as ibuprofen (Motrin®, Advil®) or naproxen (Naprosyn®, Aleve®).

• NAC may increase blood sugar levels. Caution is advised when using medications that affect blood sugar. Patients taking drugs for diabetes by mouth or insulin should be monitored closely by a qualified healthcare professional, including a pharmacist. Medication adjustments may be necessary.

• NAC may increase blood pressure. Caution is advised in patients taking drugs, herbs or supplements that affect blood pressure.

• NAC may also interact with acetaminophen, acetylcholine, allopurinol, antibiotics, anti-inflammatory agents, antivirals, bleomycin, cardiovascular agents, cefuroxime, charcoal, chemotherapeutic agents, chloroquine, cimetidine, contrast agents used in angiography, cyclophosphamide, cystic fibrosis agents, doxorubicin, exercise performance enhancement agents, fenoldopam, gentamicin, agents that affect the immune system, interferon, interleukin-2, ifosfamide, liver-protective agents, mesalamine, meso-2,3-dimercaptosuccinic acid (DMSA), mucoactive agents, neurologic agents, nitrates, nitroglycerin (NTG), nitroprusside, osteoporosis agents, phenazopyridine, radiotherapy, thyroid hormone, tigecycline, trimethoprim-sulfamethoxazole, tuaminoheptane sulphate, or zidovudine.

Interactions with Herbs and Dietary Supplements

• NAC may increase the risk of bleeding when taken with herbs and supplements that are believed to increase the risk of bleeding. Multiple cases of bleeding have been reported with the use of Ginkgo biloba, and fewer cases with garlic and saw palmetto. Numerous other agents may theoretically increase the risk of bleeding, although this has not been proven in most cases.

• NAC may increase blood sugar levels. Caution is advised when using herbs or supplements that affect blood sugar levels. Blood glucose levels may require monitoring, and doses may need adjustment.

• NAC may increase blood pressure. Caution is advised in patients taking herbs or supplements that lower blood pressure.

• NAC may also interact with alpha-lipoic acid, Amanita smithiana, anti-inflammatory herbs or supplements, antioxidants, antivirals, cardiovascular herbs or supplements, chemotherapeutic herbs or supplements, curcumin, epigallocatechin-3-gallate (EGCG), exercise performance enhancement herbs or supplements, hyperbaric oxygen therapy, herbs or supplements that affect the immune system, L-arginine, liver-protective herbs or supplements, magnesium, mucoactive herbs or supplements, mushrooms, osteoporosis herbs or supplements, vitamins (such as vitamin C), and zinc.

Author Information

• This information is based on a systematic review of scientific literature edited and peer-reviewed by contributors to the Natural Standard Research Collaboration (www.naturalstandard.com).

References

Natural Standard developed the above evidence-based information based on a thorough systematic review of the available scientific articles. For comprehensive information about alternative and complementary therapies on the professional level, go to www.naturalstandard.com. Selected references are listed below.

1. Baker WL, Anglade MW, Baker EL, et al. Use of N-acetylcysteine to reduce post-cardiothoracic surgery complications: a meta-analysis. Eur J Cardiothorac Surg 2009;35(3):521-527. View Abstract

2. Brok J, Buckley N, Gluud C. Interventions for paracetamol (acetaminophen) overdose. Cochrane Database Syst Rev 2006;(2):CD003328. View Abstract

3. Charunwatthana P, Abul Faiz M, Ruangveerayut R, et al. N-acetylcysteine as adjunctive treatment in severe malaria: a randomized, double-blinded placebo-controlled clinical trial. Crit Care Med 2009;37(2):516-522. View Abstract

4. Ghanei M, Shohrati M, Jafari M, et al. N-acetylcysteine improves the clinical conditions of mustard gas-exposed patients with normal pulmonary function test. Basic Clin Pharmacol Toxicol 2008;103(5):428-432. View Abstract

5. Grandjean EM, Berthet P, Ruffmann R, et al. Efficacy of oral long-term N-acetylcysteine in chronic bronchopulmonary disease: a meta-analysis of published double-blind, placebo-controlled clinical trials. Clin Ther 2000;22(2):209-221. View Abstract

6. Guijarro LG, Mate J, Gisbert JP, et al. N-acetyl-L-cysteine combined with mesalamine in the treatment of ulcerative colitis: randomized, placebo-controlled pilot study. World J Gastroenterol 2008;14(18):2851-2857. View Abstract

7. Ho KM, Morgan DJ. Meta-analysis of N-acetylcysteine to prevent acute renal failure after major surgery. Am J Kidney Dis 2009;53(1):33-40. View Abstract

8. Keays R, Harrison PM, Wendon JA, et al. Intravenous acetylcysteine in paracetamol induced fulminant hepatic failure: a prospective controlled trial. BMJ 1991;303(6809):1026-1029. View Abstract

9. Minder EI, Schneider-Yin X, Steurer J, et al. A systematic review of treatment options for dermal photosensitivity in erythropoietic protoporphyria. Cell Mol Biol (Noisy-le-grand) 2009;55(1):84-97. View Abstract

10. Moradi M, Mojtahedzadeh M, Mandegari A, et al. The role of glutathione-S-transferase polymorphisms on clinical outcome of ALI/ARDS patient treated with N-acetylcysteine. Respir Med 2009;103(3):434-441. View Abstract

11. Nash EF, Stephenson A, Ratjen F, et al. Nebulized and oral thiol derivatives for pulmonary disease in cystic fibrosis. Cochrane Database Syst Rev 2009;(1):CD007168. View Abstract

12. Nigwekar SU, Kandula P. N-acetylcysteine in cardiovascular-surgery-associated renal failure: a meta-analysis. Ann Thorac Surg 2009;87(1):139-147. View Abstract

13. Shohrati M, Aslani J, Eshraghi M, et al. Therapeutics effect of N-acetyl cysteine on mustard gas exposed patients: evaluating clinical aspect in patients with impaired pulmonary function test. Respir Med 2008;102(3):443-448. View Abstract

14. Stey C, Steurer J, Bachmann S, et al. The effect of oral N-acetylcysteine in chronic bronchitis: a quantitative systematic review. Eur Respir J 2000;16(2):253-262. View Abstract

15. Sutherland ER, Crapo JD, Bowler, RP. N-acetylcysteine and exacerbations of chronic obstructive pulmonary disease. COPD 2006;3(4):195-202. View Abstract