Bioequivalence and Pharmacokinetic Study of Prurisol™ and Abacavir Sulfate in Healthy Volunteers
| Status: | Completed |
|---|---|
| Conditions: | Psoriasis |
| Therapuetic Areas: | Dermatology / Plastic Surgery |
| Healthy: | No |
| Age Range: | 18 - 65 |
| Updated: | 10/28/2018 |
| Start Date: | March 2014 |
| End Date: | October 2014 |
A Randomized, Open-Label, Single-Dose, 2 Period Crossover Pharmacokinetic and Bioequivalence Study, With a Lead-In Dose Period, Evaluating Oral Abacavir Acetate (Prurisol™) and Oral Abacavir Sulfate (Ziagen®) in Healthy Volunteers
Cellceutix Corporation has created a new chemical entity for the treatment of psoriasis,
termed Prurisol™, which is an ester of abacavir. This first-in-human study of Prurisol
(abacavir acetate) is being performed to evaluate the pharmacokinetics, safety and tolerance
of a single oral doses of Prurisol administered to healthy volunteers and the bioequivalence
to abacavir sulfate (Ziagen). This study will be followed by a 505(b)(2) Phase 2 trial in
patients with moderate to severe plaque psoriasis.
termed Prurisol™, which is an ester of abacavir. This first-in-human study of Prurisol
(abacavir acetate) is being performed to evaluate the pharmacokinetics, safety and tolerance
of a single oral doses of Prurisol administered to healthy volunteers and the bioequivalence
to abacavir sulfate (Ziagen). This study will be followed by a 505(b)(2) Phase 2 trial in
patients with moderate to severe plaque psoriasis.
Prurisol™, abacavir acetate, is an ester of abacavir. Prurisol is believed to act as an
immune response modifier in certain conditions, including psoriasis. Abacavir is a synthetic
nucleoside analogue. Ziagen, abacavir sulfate, was developed and marketed as a treatment for
HIV-1 infection for over a decade. Ziagen inhibits viral DNA synthesis. Consequently,
Prurisol is under consideration as a possible new therapy for moderate to severe plaque
psoriasis. The nonclinical efficacy of Prurisol has been demonstrated in the human psoriatic
skin xenograft model in irradiated severe combined immune deficient mice. Histologic as well
as visual observations confirmed a treatment benefit of Prurisol in this animal model.
Interleukin-20 (IL-20) is a recently discovered cytokine displaying increased levels in
psoriatic lesions, and levels of IL-20 have been shown to decrease with anti-psoriasis
treatment and correlate with clinical improvement. IL-20 has been suggested as a specific
target in psoriasis treatment. In comparison to vehicle-treated animals, the mice
transplanted with human psoriatic tissue and treated with Prurisol had significant reductions
in plasma IL-20 levels which were greater than those seen with methotrexate treatment. The
expression of PRINS (psoriasis susceptibility-related RNA gene induced by stress) was
significantly lower with twice daily Prurisol treatment compared to control.
This study is designed as an open-label, randomized, 2-period, 2-treatment, 2-sequence,
single-dose intensive pharmacokinetic (PK) study conducted in healthy volunteers. In
addition, a lead-in dosing period will allow the evaluation of the PK of abacavir from 3
escalating single doses of Prurisol (50mg, 100mg, 200mg). Completion of each dosing cohort
will be followed by a 24-hour safety evaluation period before moving to a higher dose.
Adverse Events, vital signs, physical examination, and safety laboratory tests (clinical
chemistry and hematology) from each dosed cohort will be reviewed prior to any dose
escalation for next cohort.
For each subject completing the first part, there will be a 5 to 21 day washout period before
the next dose of study drug. Subjects will be randomly assigned to receive either a single
dose of 350mg Prurisol or 300mg of Ziagen in the second dosing period. After a 5 to 21 day
washout period, subjects will receive the alternate treatment in the third dosing period.
Blood samples for PK analysis will be obtained over a 24 hour period for each dose. Safety
and tolerability will be assessed by ascertainment of adverse events, results of clinical
laboratory testing and physical examination.
immune response modifier in certain conditions, including psoriasis. Abacavir is a synthetic
nucleoside analogue. Ziagen, abacavir sulfate, was developed and marketed as a treatment for
HIV-1 infection for over a decade. Ziagen inhibits viral DNA synthesis. Consequently,
Prurisol is under consideration as a possible new therapy for moderate to severe plaque
psoriasis. The nonclinical efficacy of Prurisol has been demonstrated in the human psoriatic
skin xenograft model in irradiated severe combined immune deficient mice. Histologic as well
as visual observations confirmed a treatment benefit of Prurisol in this animal model.
Interleukin-20 (IL-20) is a recently discovered cytokine displaying increased levels in
psoriatic lesions, and levels of IL-20 have been shown to decrease with anti-psoriasis
treatment and correlate with clinical improvement. IL-20 has been suggested as a specific
target in psoriasis treatment. In comparison to vehicle-treated animals, the mice
transplanted with human psoriatic tissue and treated with Prurisol had significant reductions
in plasma IL-20 levels which were greater than those seen with methotrexate treatment. The
expression of PRINS (psoriasis susceptibility-related RNA gene induced by stress) was
significantly lower with twice daily Prurisol treatment compared to control.
This study is designed as an open-label, randomized, 2-period, 2-treatment, 2-sequence,
single-dose intensive pharmacokinetic (PK) study conducted in healthy volunteers. In
addition, a lead-in dosing period will allow the evaluation of the PK of abacavir from 3
escalating single doses of Prurisol (50mg, 100mg, 200mg). Completion of each dosing cohort
will be followed by a 24-hour safety evaluation period before moving to a higher dose.
Adverse Events, vital signs, physical examination, and safety laboratory tests (clinical
chemistry and hematology) from each dosed cohort will be reviewed prior to any dose
escalation for next cohort.
For each subject completing the first part, there will be a 5 to 21 day washout period before
the next dose of study drug. Subjects will be randomly assigned to receive either a single
dose of 350mg Prurisol or 300mg of Ziagen in the second dosing period. After a 5 to 21 day
washout period, subjects will receive the alternate treatment in the third dosing period.
Blood samples for PK analysis will be obtained over a 24 hour period for each dose. Safety
and tolerability will be assessed by ascertainment of adverse events, results of clinical
laboratory testing and physical examination.
Inclusion Criteria:
Individuals who meet ALL of the following criteria are eligible for participation in this
study:
- Provided written informed consent
- Male or female adult aged 18-65 years old (inclusive). At least 20% of enrolled
subjects will be aged 55-65 years, inclusive. Effort will be made to enroll equivalent
numbers of males and females
- BMI of 19-32 kg/m2
- Identified as a non-smoker at the Consent/Screening Visit. A urine cotinine test will
be performed at screening and during each clinic check-in before for each of the three
Treatment Visits
- Willing and able to comply with all aspects of the study protocol including avoiding
use of certain concomitant medications and attending the required clinic visits
Exclusion Criteria:
Subjects are not eligible for participation in the study if any of the following criteria
are met:
- Females of childbearing potential not using reliable contraception, (e.g., abstinence,
double barrier method, oral/implantable/transdermal contraception. Depo-provera,
intrauterine device)
- Female who is pregnant, lactating, has a positive serum pregnancy test drawn at the
Consent/Screening Visit, or has a positive urine pregnancy test at check-in performed
prior to any of the 3 Treatment Days
- Presence of any uncontrolled (in the Investigator's medical opinion) systemic disease,
including, but not limited to renal, hepatic, hematologic, gastrointestinal,
endocrine, pulmonary, cardiac, neurologic, or psychiatric disease
- History of any immune disorder, or disease/condition potentially affecting the immune
system
- Regular use of oral or parenteral corticosteroids (inhaled corticosteroids for stable
asthma or chronic obstructive pulmonary disease are permitted)
- ECG obtained at Consent/Screening Visit which shows medically significant
abnormalities (e.g. bundle branch block, frequent premature ventricular contractions,
corrected QT interval (QTc) prolongation >450 msec for males and >470 msec for
females)
- Presence of a condition that makes it unlikely that the requirements of the protocol
will be completed
- Urine screening test(s) positive for evidence of amphetamines, barbiturates,
benzodiazepines, cocaine, methamphetamine, opiates, phencyclidine, marijuana
- Positive urine cotinine test
- Positive breath alcohol test
- History of hypersensitivity to any formulation of abacavir
- Previous treatment with any abacavir-containing product
- Current participation or participation in a drug/device or biologic investigational
research study within 30 days prior to the Treatment A Visit
- An elective surgical or medical procedure is planned or scheduled to be performed
during the period of the study
- Past surgical history of any degree of gastric resection or gastric banding
- History of a clinically diagnosed upper respiratory tract infection or any acute
illness requiring antibiotic therapy within 14 days prior to the Treatment A Visit
- Systolic blood pressure >150 mmHg or diastolic blood pressure >90 mmHg or heart rate
<45 bpm in a subject under the age of 40 years and heart rate <50 bpm in a subject
aged ≥40 years or >100 bpm (any subject age) on repeat determinations at the
Consent/Screening Visit or at check-in on the day prior to each of the 3 Treatment
Days and at pre-dose if drug administered on different day than check-in
- Clinical laboratory results at the Consent/Screening Visit that show any one or more
of the following:
- Hemoglobin <11 Gm/dL, Hematocrit<30%
- Total white blood cell count <3000cells/mm3
- Absolute neutrophil count <1500cells/mm3
- Platelet count <100,000/mm3
- alanine aminotransferase or aspartate aminotransferase >1.5 x Upper Limit of
Normal (ULN)
- Serum amylase above ULN
- Serum creatinine >1.5 x ULN
- Positive serum human chorionic gonadotropin
- Positive serologic test for HBsAg, HIV, hepatitis C virus
- Positive test for HLA-B*5701 allele by certified laboratory
- Urinalysis showing medically significant abnormality
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