Savings Program


Eligible* patients pay as little as $5 for their CUPRIMINE® prescription

The WD Rx Access program helps make it easier for patients who are prescribed CUPRIMINE® to have affordable access to the medication they need with:

Copay Assistance: A $5 copay for qualified patients with commercial insurance
 
Prescription management: WD Rx Access representatives will connect patients to a specialty pharmacy that will coordinate fulfillment of their prescription


For patients facing financial challenges in filling their CUPRIMINE® prescription, Valeant Pharmaceuticals has a Patient Assistance Program (PAP). PAP is subject to eligibility requirements. Documents needed to determine eligibility are listed on the Enrollment Form.

How to Enroll

 
1. Download the WD Rx Access Enrollment Form here
 
2. Patients complete the enrollment form with their doctor
 
3. The completed enrollment form, along with the CUPRIMINE® prescription and supporting documentation, if applicable, should be mailed or faxed to:

WD Rx Access
PO Box 220667
Charlotte, NC 28222-0667

Fax: (855) 735-4624
4. WD Rx Access will research the patient's coverage and contact them to discuss their assistance options

Questions? Call us at
(888) 607-7267
Monday-Friday, 8:00 AM - 6:00 PM Eastern Time.
 
*This offer is not valid for any person eligible for reimbursement of prescriptions, in whole or in part, by any federal, state, or other governmental programs, including, but not limited to, Medicare (including Medicare Advantage and Part A, B, and D plans), Medicaid, TRICARE, Veterans Administration or Department of Defense health coverage, CHAMPUS, the Puerto Rico Government Health Insurance Plan or any other federal or state health care programs. These patients may qualify for alternative financial assistance. These offers are only good for use with Cuprimine®. No other purchase necessary. These offers are not health insurance. These offers are not transferable. These offers are not valid with other offers. These offers have no cash value. The patient understands and agrees to comply with the terms and conditions of these offers. Program term eligibility expires December 31, 2018. Valeant Pharmaceuticals reserves the right to rescind, revoke, terminate, or amend these offers at any time, with or without notice. For more information, call a WD Rx Access representative at 888-607-7267.

Patients who are eligible for the Valeant Pharmaceuticals PAP will be contacted with information on how to enroll. If you have questions about eligibility or alternate funding options, please call the Valeant Patient Assistance Program at 833-862-VPAP (833-862-8727), 8 AM to 5 PM Eastern Time. Eligibility requirements, terms and conditions are online here: https://www.valeantpap.com.
 


Physicians planning to use penicillamine should thoroughly familiarize themselves with its toxicity, special dosage considerations, and therapeutic benefits. Penicillamine should never be used casually. Each patient should remain constantly under the close supervision of the physician. Patients should be warned to report promptly any symptoms suggesting toxicity.

INDICATION

CUPRIMINE® (penicillamine) is indicated in the treatment of Wilson's disease, cystinuria, and in patients with severe, active rheumatoid arthritis who have failed to respond to an adequate trial of conventional therapy. Available evidence suggests that CUPRIMINE® is not of value in ankylosing spondylitis.

IMPORTANT SAFETY INFORMATION

  • Except for the treatment of Wilson's disease or certain patients with cystinuria, use of penicillamine during pregnancy is contraindicated. Mothers on therapy with penicillamine should not nurse their infants.
  • Patients with a history of penicillamine-related aplastic anemia or agranulocytosis should not be restarted on penicillamine. Because of its potential for causing renal damage, penicillamine should not be administered to rheumatoid arthritis patients with a history or other evidence of renal insufficiency.
  • The use of penicillamine has been associated with fatalities due to certain diseases such as aplastic anemia, agranulocytosis, thrombocytopenia, Goodpasture's syndrome, and myasthenia gravis.
  • Routine urinalysis, white and differential blood cell count, hemoglobin determination, direct platelet count, together with monitoring of the patient's skin, lymph nodes and body temperature, must be done twice weekly for five months and monthly thereafter. Patients should be instructed to report promptly the development of signs and symptoms of granulocytopenia and/or thrombocytopenia such as fever, sore throat, chills, bruising or bleeding.
  • A reduction in WBC count below 3500/mm3 requires discontinuation. Platelet count below 100,000/mm3 even in absence of clinical bleeding; or a progressive fall in either platelet or WBC count in three successive determinations requires at least temporary cessation of therapy.
  • Proteinuria and/or hematuria may develop during therapy and may be warning signs of membranous glomerulopathy which can progress to a nephrotic syndrome.
  • Because of rare reports of intrahepatic cholestasis and toxic hepatitis, liver function tests are recommended every six months for the duration of therapy. In Wilson's disease, these are recommended every three months, at least during the first year of treatment.
  • Onset of new or worsening of existing neurological symptoms has been reported during initiation of therapy with CUPRIMINE®.
  • When pemphigus is suspected, CUPRIMINE® should be discontinued.
  • Pregnancy Category D - Penicillamine can cause fetal harm when administered to a pregnant woman. Penicillamine should not be administered to pregnant women with cystinuria or rheumatoid arthritis and should be discontinued promptly in patients in whom pregnancy is suspected or diagnosed. Penicillamine has been shown to be teratogenic in rats when given doses 6 times higher than the highest dose recommended for humans.
  • Penicillamine for Wilson’s disease should be used in women of childbearing potential only when the expected benefits outweigh the possible hazards. Reported experience shows that continued treatment with penicillamine throughout pregnancy protects the mother against relapse of the Wilson's disease, and discontinuation of penicillamine has deleterious effects on the mother, which may be fatal.
  • Some patients may experience drug fever with or without macular cutaneous eruptions. Penicillamine should be temporarily discontinued in these patients if being treated for Wilson's disease or cystinuria until the reaction subsides. In the case of drug fever in rheumatoid arthritis patients, because other treatments are available, penicillamine should be discontinued.
  • The skin and mucous membranes should be observed for allergic reactions. Early and late rashes have occurred. Less commonly, a late rash may be seen, usually after six months or more of treatment, and requires discontinuation of penicillamine.
  • The appearance of a drug eruption accompanied by fever, arthralgia, lymphadenopathy or other allergic manifestations usually requires discontinuation of penicillamine.
  • Penicillamine should not be used in patients who are receiving concurrently gold therapy, antimalarial or cytotoxic drugs, oxyphenbutazone or phenylbutazone because these drugs are also associated with similar serious hematologic and renal adverse reactions. Patients who have had gold salt therapy discontinued due to a major toxic reaction may be at greater risk of serious adverse reactions with penicillamine but not necessarily of the same type.
  • Patients who are allergic to penicillin may theoretically have cross-sensitivity to penicillamine.
  • Patients with Wilson's disease or cystinuria should be given 25 mg/day of pyridoxine during therapy, since penicillamine increases the requirement for this vitamin. Patients also may receive benefit from a multivitamin preparation. In Wilson's disease, multivitamin preparations must be copper-free. Rheumatoid arthritis patients whose nutrition is impaired should also be given a daily supplement of pyridoxine. Mineral supplements should not be given, since they may block the response to penicillamine.
  • Penicillamine is a drug with a high incidence of untoward reactions, some of which are potentially fatal.
  • Reported incidences for the most commonly occurring adverse reactions in rheumatoid arthritis patients based on 17 representative clinical trials reported in the literature (1270 patients) include events related to Allergy: pruritis, rashes, pemphigus; Gastrointestinal: anorexia, epigastric pain, nausea, vomiting, or occasional diarrhea, hepatic dysfunction, effect on taste perception and oral ulcerations; Hematological: leukopenia, thrombocytopenia leading to fatalities; Renal: proteinuria and/or hematuria progressing to nephrotic syndrome, renal failure; Central Nervous System: tinnitus, optic neuritis, peripheral sensory and motor neuropathies, muscular weakness, visual and psychic disturbances, mental disorders, and agitation and anxiety; Neuromuscular: myasthenia gravis, dystonia. Other: Adverse reactions reported rarely include thrombophlebitis, hyperpyrexia, alopecia, lichen planus, polymyositis, dermatomyositis, mammary hyperplasia, elastosis perforans serpiginosa, toxic epidermal necrolysis, anetoderma, and Goodpasture's syndrome. Vasculitis, including fatal renal vasculitis, allergic alveolitis, obliterative bronchiolitis, interstitial pneumonitis, pulmonary fibrosis, and bronchial asthma also has been reported.
Please click here to see full Prescribing Information for CUPRIMINE® capsules.

WD RX Access is sponsored by Valeant Pharmaceuticals North America LLC.
©2018 Valeant Pharmaceuticals North America LLC. All Rights Reserved. CUP.0017.USA.18

 

INDICATIONS

Cuprimine® (penicillamine) is indicated in the treatment of Wilson's disease, cystinuria, and in patients with severe, active rheumatoid arthritis who have failed to respond to an adequate trial of conventional therapy. Available evidence suggests that Cuprimine is not of value in ankylosing spondylitis.

IMPORTANT SAFETY INFORMATION

Physicians planning to use penicillamine should thoroughly familiarize themselves with its toxicity, special dosage considerations, and therapeutic benefits. Penicillamine should never be used casually. Each patient should remain constantly under the close supervision of the physician. Patients should be warned to report promptly any symptoms suggesting toxicity.

  • Except for the treatment of Wilson's disease or certain patients with cystinuria, use of penicillamine during pregnancy is contraindicated. Mothers on therapy with penicillamine should not nurse their infants.
  • Patients with a history of penicillamine-related aplastic anemia or agranulocytosis should not be restarted on penicillamine. Because of its potential for causing renal damage, penicillamine should not be administered to rheumatoid arthritis patients with a history or other evidence of renal insufficiency.
  • The use of penicillamine has been associated with fatalities due to certain diseases such as aplastic anemia, agranulocytosis, thrombocytopenia, Goodpasture's syndrome, and myasthenia gravis.
  • Routine urinalysis, white and differential blood cell count, hemoglobin determination, direct platelet count, together with monitoring of the patient's skin, lymph nodes and body temperature, must be done twice weekly for five months and monthly thereafter. Patients should be instructed to report promptly the development of signs and symptoms of granulocytopenia and/or thrombocytopenia such as fever, sore throat, chills, bruising or bleeding.
  • A reduction in WBC count below 3500/mm3 requires discontinuation. Platelet count below 100,000/mm3 even in absence of clinical bleeding; or a progressive fall in either platelet or WBC count in three successive determinations requires at least temporary cessation of therapy.
  • Proteinuria and/or hematuria may develop during therapy and may be warning signs of membranous glomerulopathy which can progress to a nephrotic syndrome.
  • Because of rare reports of intrahepatic cholestasis and toxic hepatitis, liver function tests are recommended every six months for the duration of therapy. In Wilson's disease, these are recommended every three months, at least during the first year of treatment.
  • Onset of new or worsening of existing neurological symptoms has been reported during initiation of therapy with Cuprimine.
  • When pemphigus is suspected, Cuprimine should be discontinued.
  • Pregnancy Category D - Penicillamine can cause fetal harm when administered to a pregnant woman. Penicillamine should not be administered to pregnant women with cystinuria or rheumatoid arthritis and should be discontinued promptly in patients in whom pregnancy is suspected or diagnosed. Penicillamine has been shown to be teratogenic in rats when given doses 6 times higher than the highest dose recommended for humans. enicillamine for Wilson’s disease should be used in women of childbearing potential only when the expected benefits outweigh the possible hazards. Reported experience shows that continued treatment with penicillamine throughout pregnancy protects the mother against relapse of the Wilson's disease, and discontinuation of penicillamine has deleterious effects on the mother, which may be fatal.
  • Some patients may experience drug fever with or without macular cutaneous eruptions. Penicillamine should be temporarily discontinued in these patients if being treated for Wilson's disease or cystinuria until the reaction subsides. In the case of drug fever in rheumatoid arthritis patients, because other treatments are available, penicillamine should be discontinued.
  • The skin and mucous membranes should be observed for allergic reactions. Early and late rashes have occurred. Less commonly, a late rash may be seen, usually after six months or more of treatment, and requires discontinuation of penicillamine.
  • The appearance of a drug eruption accompanied by fever, arthralgia, lymphadenopathy or other allergic manifestations usually requires discontinuation of penicillamine.
  • Penicillamine should not be used in patients who are receiving concurrently gold therapy, antimalarial or cytotoxic drugs, oxyphenbutazone or phenylbutazone because these drugs are also associated with similar serious hematologic and renal adverse reactions. Patients who have had gold salt therapy discontinued due to a major toxic reaction may be at greater risk of serious adverse reactions with penicillamine but not necessarily of the same type.
  • Patients who are allergic to penicillin may theoretically have cross-sensitivity to penicillamine.
  • Patients with Wilson's disease or cystinuria should be given 25 mg/day of pyridoxine during therapy, since penicillamine increases the requirement for this vitamin. Patients also may receive benefit from a multivitamin preparation. In Wilson's disease, multivitamin preparations must be copper-free. Rheumatoid arthritis patients whose nutrition is impaired should also be given a daily supplement of pyridoxine. Mineral supplements should not be given, since they may block the response to penicillamine.
  • Penicillamine is a drug with a high incidence of untoward reactions, some of which are potentially fatal.
  • Reported incidences for the most commonly occurring adverse reactions in rheumatoid arthritis patients based on 17 representative clinical trials reported in the literature (1270 patients) include events related to Allergy: pruritis, rashes, pemphigus; Gastrointestinal: anorexia, epigastric pain, nausea, vomiting, or occasional diarrhea, hepatic dysfunction, effect on taste perception and oral ulcerations; Hematological: leukopenia, thrombocytopenia leading to fatalities; Renal: proteinuria and/or hematuria progressing to nephrotic syndrome, renal failure; Central Nervous System: tinnitus, optic neuritis, peripheral sensory and motor neuropathies, muscular weakness, visual and psychic disturbances, mental disorders, and agitation and anxiety; Neuromuscular: myasthenia gravis, dystonia. Other: Adverse reactions reported rarely include thrombophlebitis, hyperpyrexia, alopecia, lichen planus, polymyositis, dermatomyositis, mammary hyperplasia, elastosis perforans serpiginosa, toxic epidermal necrolysis, anetoderma, and Goodpasture's syndrome. Vasculitis, including fatal renal vasculitis, allergic alveolitis, obliterative bronchiolitis, interstitial pneumonitis, pulmonary fibrosis, and bronchial asthma also has been reported.
Please click here to see full Prescribing Information for Cuprimine capsules.
 

INDICATIONS

Cuprimine® (Penicillamine) is indicated in the treatment of Wilson's disease, cystinuria, and in patients with severe, active rheumatoid arthritis who have failed to respond to an adequate trial of conventional therapy. Available evidence suggests that Cuprimine is not of value in ankylosing spondylitis.

IMPORTANT SAFETY INFORMATION

Physicians planning to use penicillamine should thoroughly familiarize themselves with its toxicity, special dosage considerations, and therapeutic benefits. Penicillamine should never be used casually. Each patient should remain constantly under the close supervision of the physician. Patients should be warned to report promptly any symptoms suggesting toxicity.

  • Except for the treatment of Wilson's disease or certain patients with cystinuria, use of penicillamine during pregnancy is contraindicated. Mothers on therapy with penicillamine should not nurse their infants.
  • Patients with a history of penicillamine-related aplastic anemia or agranulocytosis should not be restarted on penicillamine. Because of its potential for causing renal damage, penicillamine should not be administered to rheumatoid arthritis patients with a history or other evidence of renal insufficiency.
  • The use of penicillamine has been associated with fatalities due to certain diseases such as aplastic anemia, agranulocytosis, thrombocytopenia, Goodpasture's syndrome, and myasthenia gravis.
  • Routine urinalysis, white and differential blood cell count, hemoglobin determination, direct platelet count, together with monitoring of the patient's skin, lymph nodes and body temperature, must be done twice weekly for five months and monthly thereafter. Patients should be instructed to report promptly the development of signs and symptoms of granulocytopenia and/or thrombocytopenia such as fever, sore throat, chills, bruising or bleeding.
  • A reduction in WBC count below 3500/mm3 requires discontinuation. Platelet count below 100,000/mm3 even in absence of clinical bleeding; or a progressive fall in either platelet or WBC count in three successive determinations requires at least temporary cessation of therapy.
  • Proteinuria and/or hematuria may develop during therapy and may be warning signs of membranous glomerulopathy which can progress to a nephrotic syndrome.
  • Because of rare reports of intrahepatic cholestasis and toxic hepatitis, liver function tests are recommended every six months for the duration of therapy. In Wilson's disease, these are recommended every three months, at least during the first year of treatment.
  • Onset of new or worsening of existing neurological symptoms has been reported during initiation of therapy with Cuprimine.
  • When pemphigus is suspected, Cuprimine should be discontinued.
  • Pregnancy Category D - Penicillamine can cause fetal harm when administered to a pregnant woman. Penicillamine should not be administered to pregnant women with cystinuria or rheumatoid arthritis and should be discontinued promptly in patients in whom pregnancy is suspected or diagnosed. Penicillamine has been shown to be teratogenic in rats when given doses 6 times higher than the highest dose recommended for humans. enicillamine for Wilson’s disease should be used in women of childbearing potential only when the expected benefits outweigh the possible hazards. Reported experience shows that continued treatment with penicillamine throughout pregnancy protects the mother against relapse of the Wilson's disease, and discontinuation of penicillamine has deleterious effects on the mother, which may be fatal.
  • Some patients may experience drug fever with or without macular cutaneous eruptions. Penicillamine should be temporarily discontinued in these patients if being treated for Wilson's disease or cystinuria until the reaction subsides. In the case of drug fever in rheumatoid arthritis patients, because other treatments are available, penicillamine should be discontinued.
  • The skin and mucous membranes should be observed for allergic reactions. Early and late rashes have occurred. Less commonly, a late rash may be seen, usually after six months or more of treatment, and requires discontinuation of penicillamine.
  • The appearance of a drug eruption accompanied by fever, arthralgia, lymphadenopathy or other allergic manifestations usually requires discontinuation of penicillamine.
  • Penicillamine should not be used in patients who are receiving concurrently gold therapy, antimalarial or cytotoxic drugs, oxyphenbutazone or phenylbutazone because these drugs are also associated with similar serious hematologic and renal adverse reactions. Patients who have had gold salt therapy discontinued due to a major toxic reaction may be at greater risk of serious adverse reactions with penicillamine but not necessarily of the same type.
  • Patients who are allergic to penicillin may theoretically have cross-sensitivity to penicillamine.
  • Patients with Wilson's disease or cystinuria should be given 25 mg/day of pyridoxine during therapy, since penicillamine increases the requirement for this vitamin. Patients also may receive benefit from a multivitamin preparation. In Wilson's disease, multivitamin preparations must be copper-free. Rheumatoid arthritis patients whose nutrition is impaired should also be given a daily supplement of pyridoxine. Mineral supplements should not be given, since they may block the response to penicillamine.
  • Penicillamine is a drug with a high incidence of untoward reactions, some of which are potentially fatal.
  • Reported incidences for the most commonly occurring adverse reactions in rheumatoid arthritis patients based on 17 representative clinical trials reported in the literature (1270 patients) include events related to Allergy: pruritis, rashes, pemphigus; Gastrointestinal: anorexia, epigastric pain, nausea, vomiting, or occasional diarrhea, hepatic dysfunction, effect on taste perception and oral ulcerations; Hematological: leukopenia, thrombocytopenia leading to fatalities; Renal: proteinuria and/or hematuria progressing to nephrotic syndrome, renal failure; Central Nervous System: tinnitus, optic neuritis, peripheral sensory and motor neuropathies, muscular weakness, visual and psychic disturbances, mental disorders, and agitation and anxiety; Neuromuscular: myasthenia gravis, dystonia. Other: Adverse reactions reported rarely include thrombophlebitis, hyperpyrexia, alopecia, lichen planus, polymyositis, dermatomyositis, mammary hyperplasia, elastosis perforans serpiginosa, toxic epidermal necrolysis, anetoderma, and Goodpasture's syndrome. Vasculitis, including fatal renal vasculitis, allergic alveolitis, obliterative bronchiolitis, interstitial pneumonitis, pulmonary fibrosis, and bronchial asthma also has been reported.
Please click here to see full Prescribing Information for Cuprimine capsules.