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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT00261833
Other study ID # CE1226_4001
Secondary ID 14492005-003459-
Status Completed
Phase Phase 4
First received December 2, 2005
Last updated January 11, 2015
Start date March 2006
Est. completion date September 2012

Study information

Verified date January 2015
Source CSL Behring
Contact n/a
Is FDA regulated No
Health authority United States: Food and Drug AdministrationAustralia: Department of Health and Ageing Therapeutic Goods AdministrationCanada: Ethics Review CommitteeCanada: Health CanadaCzech Republic: Ethics CommitteeCzech Republic: State Institute for Drug ControlDenmark: Danish Medicines AgencyDenmark: Ethics CommitteeDenmark: The Danish National Committee on Biomedical Research EthicsEstonia: The State Agency of MedicineFinland: Ethics CommitteeFinland: Finnish Medicines AgencyGermany: Ethics CommissionGermany: Paul-Ehrlich-InstitutIreland: Irish Medicines BoardIreland: Medical Ethics Research CommitteePoland: Office for Registration of Medicinal Products, Medical Devices and Biocidal ProductsRomania: National Medicines AgencySweden: Medical Products Agency
Study type Interventional

Clinical Trial Summary

This is a randomized, placebo-controlled, double-blind, multicenter phase III/IV study to compare the efficacy and safety of Zemaira® with placebo in subjects with emphysema due to alpha1-proteinase inhibitor deficiency. The effect of Zemaira® on the progression of emphysema will be assessed by the decline of lung density, measured by computed tomography (CT).


Recruitment information / eligibility

Status Completed
Enrollment 180
Est. completion date September 2012
Est. primary completion date September 2012
Accepts healthy volunteers No
Gender Both
Age group 18 Years to 65 Years
Eligibility Inclusion Criteria:

- 18 to 65 years of age and willing to sign informed consent.

- Males and non-pregnant, non-lactating females whose screening pregnancy test is negative and who are using contraceptives methods deemed reliable by the investigator.

- Diagnosis of alpha1-proteinase inhibitor (A1-PI) deficiency (serum A1-PI levels < 11 µM or < 80 mg/dL). This includes newly diagnosed subjects, previously untreated subjects, currently treated subjects, and subjects currently not on treatment therapy but on treatment in the past.

- Subjects with emphysema and forced expiratory volume in 1 second (FEV1) = 35% and = 70% (predicted).

- No signs of chronic or acute Hepatitis A, Hepatitis B, Hepatitis C or HIV infection (negative serologies for HIV and viral hepatitis). In case of positive serologies for viral hepatitis, vaccination status or negative IgM should be available.

Exclusion Criteria:

- Any relevant chronic diseases or history of relevant diseases (e.g., severe renal insufficiency) except respiratory or liver disease secondary to alpha1-proteinase inhibitor deficiency. Subjects with well-controlled, chronic diseases may be included after consultation with the treating physician and the sponsor.

- Current evidence of alcohol abuse or history of abuse of illegal and/or legally prescribed drugs such as barbiturates, benzodiazepines, amphetamines, cocaine, opioids, and cannabinoids.

- History of allergy, anaphylactic reaction, or severe systemic response to human plasma derived products, or known mannitol hypersensitivity, or history of prior adverse reaction to mannitol.

- History of transfusion reactions.

- Selective IgA deficiency.

- Acute illness within one week prior to the first administration of the investigational medicinal product (IMP). Start of treatment after recovery is possible.

- Current tobacco smoker (smoking has to be ceased at least 6 months prior study inclusion). Subjects with a positive cotinine test due to nicotine replacement therapy (e.g. patches, chewing gum) or snuff are eligible.

- Conditions or behaviors that interfere with attending scheduled study visits in the opinion of the investigator.

- History of non-compliance.

- Administration of any other experimental new drug or participation in an investigation of a marketed product within one month prior to the screening visit date.

- Inability to perform necessary study procedures.

- Lung transplantation, lung volume reduction surgery or lobectomy or being on a waiting list for any such surgeries.

Study Design

Allocation: Randomized, Endpoint Classification: Safety/Efficacy Study, Intervention Model: Parallel Assignment, Masking: Double Blind (Subject, Caregiver, Investigator, Outcomes Assessor), Primary Purpose: Treatment


Related Conditions & MeSH terms


Intervention

Biological:
Alpha1-proteinase inhibitor
60 mg/kg body weight/week intravenous
Other:
Placebo
Lyophilized preparation: 60 mg/kg body weight/week intravenous

Locations

Country Name City State
Australia Study Site Adelaide South Australia
Australia Study Site Brisbane Queensland
Australia Study Site Darlinghurst New South Wales
Australia Study Site Fitzroy
Australia Study Site Nedlands Western Australia
Australia Study Site New Lambton New South Wales
Canada Study Site Halifax Nova Scotia
Canada Study Site Toronto Ontario
Canada Study Site Vancouver British Columbia
Czech Republic Study Site Praha
Denmark Study Site Arhus
Denmark Study Site Hellerup
Estonia Study Site Tartu
Finland Study Site Oulu
Germany Study Site Berlin
Germany Study Site Essen
Germany Study Site Heidelberg
Germany Study Site Nürnberg
Ireland Study Site Dublin
Poland Study Site Krakow
Poland Study Site Warsaw
Romania Study Site Bucuresti
Russian Federation Study Site Barnaul
Sweden Study Site Malmo
United States Study Site Denver Colorado
United States Study Site Hershey Pennsylvania
United States Study Site Miami Florida
United States Study Site Tyler Texas

Sponsors (1)

Lead Sponsor Collaborator
CSL Behring

Countries where clinical trial is conducted

United States,  Australia,  Canada,  Czech Republic,  Denmark,  Estonia,  Finland,  Germany,  Ireland,  Poland,  Romania,  Russian Federation,  Sweden, 

Outcome

Type Measure Description Time frame Safety issue
Other Baseline Lung Density at Total Lung Capacity (TLC) and Forced Residual Capacity (FRC) Baseline No
Primary Annual Rate of Change in Lung Density As measured by centralized, standardized computer tomographic (CT) lung densitometry. CT scans were acquired at 2 inspiration states: TLC (ie, full inspiration) and FRC (ie, full expiration). Results were adjusted for total lung volume and are presented as point estimates for the average rate of decline in each treatment group. Over a 2-year period No
Secondary Annual Rate of Pulmonary Exacerbations Primary diagnostic criteria for exacerbations were increased dyspnea, increased sputum volume, and increased sputum purulence. Supporting diagnostic criteria were upper respiratory tract infection, fever without other apparent cause, increased wheezing, and increased cough. For diagnosis, participants had to meet 2 of the 3 primary criteria or 1 primary criterion and 1 supporting criterion. The annual rate was based on the total number of exacerbations and the total number of participant study days for all participants in the specified analysis population and adjusted to 365.25 days. Over a 2-year period No
Secondary Percent Change in FEV1 Percent change from baseline to Month 24. From baseline to 2 years No
Secondary Time to First Pulmonary Exacerbation Primary diagnostic criteria for exacerbations were increased dyspnea, increased sputum volume, and increased sputum purulence. Supporting diagnostic criteria were upper respiratory tract infection, fever without other apparent cause, increased wheezing, and increased cough. For diagnosis, participants had to meet 2 of the 3 primary criteria or 1 primary criterion and 1 supporting criterion. Over a 2-year period No
Secondary Change in Lung Density Change from baseline to Month 24 as measured by centralized, standardized CT lung densitometry. CT scans were acquired at 2 inspiration states: TLC (ie, full inspiration) and FRC (ie, full expiration). Results were adjusted for total lung volume. From baseline to 2 years No
Secondary Change in Exercise Capacity Exercise capacity was measured as distance walked, using the incremental shuttle walk test. Change from baseline to end of treatment (2 years) in exercise capacity was analysed using an analysis of covariance (ANCOVA). From baseline to 2 years No
Secondary Change in Patient-reported Symptoms Patient-reported symptoms were measured using the symptoms score component of the St George's Respiratory Questionnaire (SGRQ). SGRQ scores range from 0 to 100, with higher scores indicating more limitations and negative values for change indicating improvement. Change from baseline to end of treatment (2 years) in SGRQ was analysed using an ANCOVA. From baseline to 2 years No
Secondary Frequency and Intensity of Adverse Events (AEs) Number of participants with at least one AE, and the number of participants with mild, moderate or severe AEs. AE intensity was defined as mild (does not interfere with routine activities), moderate (interferes with routine activities), or severe (impossible to perform routine activities). Over a 2-year period Yes
Secondary Percent Change in Percent Predicted FEV1 Percent change from baseline to Month 24. From baseline to 2 years No
Secondary Percent Change in FEV1 Divided by Forced Vital Capacity Percent change from baseline to Month 24. From baseline to 2 years No
Secondary Percent Change in DLCO Percent change from baseline to Month 24. From baseline to 2 years No
Secondary Duration of Pulmonary Exacerbations Relative to Treatment Duration Defined as the percentage of total treatment duration across participants for 1) exacerbations overall, 2) antibiotic treatment for exacerbations, and 3) hospitalization for exacerbations. Primary diagnostic criteria for exacerbations were increased dyspnea, increased sputum volume, and increased sputum purulence. Supporting diagnostic criteria were upper respiratory tract infection, fever without other apparent cause, increased wheezing, and increased cough. For diagnosis, participants had to meet 2 of the 3 primary criteria or 1 primary criterion and 1 supporting criterion. Over a 2-year period No
Secondary Severity of Pulmonary Exacerbations Defined as the number of participants requiring 1) antibiotic treatment for exacerbations, and 2) hospitalization for exacerbations. Primary diagnostic criteria for exacerbations were increased dyspnea, increased sputum volume, and increased sputum purulence. Supporting diagnostic criteria were upper respiratory tract infection, fever without other apparent cause, increased wheezing, and increased cough. For diagnosis, participants had to meet 2 of the 3 primary criteria or 1 primary criterion and 1 supporting criterion.
Antibiotic treatment usage was reported by quarterly interval.
Over a 2-year period No
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