Study of Dose-Effect of COL-121 Ointment in Patients With Plaque-Type Psoriasis
NCT ID: NCT00625326
Last Updated: 2011-04-27
Study Results
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Basic Information
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COMPLETED
PHASE2
321 participants
INTERVENTIONAL
2008-01-31
2009-06-30
Brief Summary
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Detailed Description
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Although the exact cause of this skin disease is unknown, it is clear that immune-based inflammatory mechanisms initiate an accelerated growth of skin cells. This accelerated growth results in an agglomeration of skin cells on the surface of the epidermis that the body cannot shed. This agglomeration creates the thickened patches of scaly skin characteristic of the disease.
Clinical use of systemic vitamin D to treat psoriasis has been limited because of the induction of hypercalcemia. In contrast, low doses of topically administered vitamin D analogs have been shown to have an anti-psoriatic effect without the risk of hypercalcemia. Topical vitamin D analogs have the ability to inhibit the proliferation and promote the differentiation of keratinocytes in psoriatic skin. In addition, vitamin D analogs may also act by inhibiting cytokine production by keratinocytes or lymphocytes. Calcipotriol, the most thoroughly studied of the vitamin D analogs, was first approved in Europe in the early 1990s. It has been shown to be comparable or slightly more effective than class II corticosteroid ointments. In patients with extensive psoriasis, calcipotriol ointment was shown to be effective. However, patients had reduced levels of parathyroid hormone; mean serum and urine calcium were increased during treatment and hypercalciuria was recorded in 3 patients. These effects were reversible with discontinuation of therapy. In a review of the effects on calcium homeostasis, it was noted that calcipotriol (50 µg/g) had no effects on serum or urine calcium when administered at doses of 40-50 g/week and two reports of hypercalcemia at doses of 70-100 g/week. Thus, while calcipotriol ointment was shown to be effective, the potential for alterations in calcium homeostasis have limited its use to 100 g of ointment per week (0.5 mg calcipotriol/week). Subsequently, calcipotriol and tacalcitol, another vitamin D analog, have become first-line therapies in the management of "mild to moderate" psoriasis in several countries in Western Europe, Japan and the USA.
Work has continued on the creation of new vitamin D analogs, such as COL-121, with the intent of eliminating the adverse effects of hypercalcemia and hypercalciuria with a compound that is more stable and more easily administered.
Conditions
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Study Design
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RANDOMIZED
PARALLEL
TREATMENT
DOUBLE
Study Groups
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75 µg/g COL-121 Ointment
75 µg/g COL-121 Ointment
COL-121
75 µg/g COL-121 Ointment
150 µg/g COL-121 Ointment
150 µg/g COL-121 Ointment
COL-121
150 µg/g COL-121 Ointment
300 µg/g COL-121 Ointment
300 µg/g COL-121 Ointment
COL-121
300 µg/g COL-121 Ointment
50 µg/g Calcipotriene Ointment
50 µg/g Calcipotriene Ointment (active control)
50 µg/g Calcipotriene Ointment
50 µg/g Calcipotriene Ointment
Placebo Ointment
Placebo Ointment
Placebo
Placebo
Interventions
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COL-121
75 µg/g COL-121 Ointment
50 µg/g Calcipotriene Ointment
50 µg/g Calcipotriene Ointment
Placebo
Placebo
COL-121
150 µg/g COL-121 Ointment
COL-121
300 µg/g COL-121 Ointment
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Subject must have 2 to 4 target plaques on the area to be treated, excluding the face and scalp.
* Subjects who are women of childbearing potential must have a negative pregnancy test and be non-lactating.
* Subjects who are women of childbearing potential must utilize one of the following methods of birth control throughout the study: IUD, diaphragm, a condom, a spermicidal gel or foam, oral contraceptives (provided subject has been utilizing this method for at least 4 months prior to Visit 1 and has not changed the brand within this period). Subjects may also participate if they are surgically sterilized, in a monogamous relationship with a sterile partner, or abstain from sexual intercourse during the course of the study.
* Subjects must be in good general health and free of any disease state or physical condition that, in the investigator's opinion, may interfere with study evaluations or exposes the subject to unacceptable risk by study participation.
* Subject must be willing and able to apply the study medication as directed, comply with the study instructions, and commit to all the follow-up visits for the duration of the study.
* Subjects must sign an informed consent form.
Exclusion Criteria
* Subjects who have spontaneously improving or rapidly deteriorating plaque psoriasis.
* Subjects who have used systemic immunomodulatory therapy known to affect psoriasis and to typically decrease immune cell populations (e.g., alefacept) within the previous 40 weeks.
* Subjects who have used any systemic immunomodulatory therapy known to affect psoriasis and to NOT typically decrease immune cell populations (e.g., etanercept) within the previous 16 weeks.
* Subjects who have used any photo-therapy (including laser), photo-chemotherapy or systemic psoriasis therapy (e.g., systemic corticosteroids, methotrexate, retinoids, cyclosporine) within the previous 12 weeks.
* Subjects who have had prolonged exposure to natural or artificial sources of ultraviolet radiation within the previous 3 weeks or are intending to have such exposure during the study, thought by the investigator likely to modify the subject's plaque psoriasis.
* Subjects who have used topical anti-psoriatic therapy (including topical retinoids) on the areas to be evaluated within the previous 2 weeks.
* Subjects who have used emollients/moisturizers on the areas to be evaluated within the previous 1 day.
* Subjects who have untreated bacterial, tubercular, fungal or viral lesions of the skin on the areas to be evaluated.
* Subjects who have known sensitivity to a component of the study medication or to topical or systemic vitamin D.
* Subjects who have any significant condition such as diseases of the hepatic, renal, endocrine, musculoskeletal, or nervous system, or any gross physical impairment.
* Subjects who have taken a vitamin D supplement that exceeds 400 IU per day in the previous 30 days.
* Subjects who have taken a calcium supplement that exceeds 1200 mg per day in the previous 30 days.
* Subjects who are using lithium or Plaquenil.
* Subjects who are using beta-blocking medication or thiazide diuretics whose dose has not been stable for at least 12 weeks.
* Subjects who have a history of hypercalcemia or evidence of vitamin D toxicity.
* Subjects who are currently being treated for malignancy or have been diagnosed with melanoma within the past 5 years.
* Subjects who have received any investigational treatment(s) within the previous 30 days.
18 Years
ALL
No
Sponsors
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Deltanoid Pharmaceuticals
INDUSTRY
Responsible Party
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Galderma
Principal Investigators
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Michael Graeber, MD
Role: STUDY_DIRECTOR
Galderma R&D
Locations
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East Bay Dermatology Medical Group
Fremont, California, United States
Dermatology Research Associates
Los Angeles, California, United States
Skin Surgery Medical Group, Inc.
San Diego, California, United States
Dermatology Specialists, Inc.
Vista, California, United States
Cherry Creek Research, Inc.
Denver, Colorado, United States
Longmont Medical Research Network
Longmont, Colorado, United States
The Savin Center, PC
New Haven, Connecticut, United States
International Dermatology Research, Inc.
Miami, Florida, United States
MedaPhase, Inc.
Newnan, Georgia, United States
Dermatology Specialists
Louisville, Kentucky, United States
Michigan Center for Skin Care Research
Clinton Township, Michigan, United States
Grekin Skin Institute
Warren, Michigan, United States
Academic Dermatology Associates
Albuquerque, New Mexico, United States
Northwest Cutaneous Research Specialists
Portland, Oregon, United States
Philadelphia Institute of Dermatology
Flourtown, Pennsylvania, United States
DermResearch, Inc.
Austin, Texas, United States
Dermatology Associates of San Antonio
San Antonio, Texas, United States
Dermatology Research Center
Salt Lake City, Utah, United States
The Education & Research Foundation, Inc.
Lynchburg, Virginia, United States
Premier Clinical Research
Spokane, Washington, United States
Countries
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Other Identifiers
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COL-121-PSOR-201
Identifier Type: -
Identifier Source: org_study_id
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