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MK0507A Clinical Study in Patients With Glaucoma and Ocular Hypertension

This study has been completed.
Sponsor:
Information provided by:
Merck
ClinicalTrials.gov Identifier:
NCT00449956
First received: March 19, 2007
Last updated: April 20, 2010
Last verified: April 2010
History of Changes
Results First Received: January 23, 2009  
Study Type: Interventional
Study Design: Allocation: Randomized;   Endpoint Classification: Safety/Efficacy Study;   Intervention Model: Parallel Assignment;   Masking: Double Blind (Subject, Investigator);   Primary Purpose: Treatment
Condition: Glaucoma
Interventions: Drug: dorzolamide hydrochloride (+) timolol maleate
Drug: Comparator: timolol maleate
Drug: Comparator: dorzolamide hydrochloride

  Participant Flow
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Recruitment Details
Key information relevant to the recruitment process for the overall study, such as dates of the recruitment period and locations
Phase III. Studied period: April 9, 2007 (date study therapy started for the first subject) to February 16, 2008 (the last subject’s last visit stipulated in study protocol). Study was conducted at 67 clinical sites.

Pre-Assignment Details
Significant events and approaches for the overall study following participant enrollment, but prior to group assignment
Outpatients with primary open angle glaucoma (broad definition) and/or ocular hypertension received 4-week timolol 0.5% monotherapy in the wash-out period before the study randomization.

Reporting Groups
  Description
MK0507A (Dorzolamide 1.0% / Timolol 0.5% Combination) MK0507A (Dorzolamide 1.0% / Timolol 0.5% combination), one drop per dose twice daily to the study eye.
Timolol 0.5% Timolol 0.5%, one drop per dose twice daily to the study eye.
Concomitant (Dorzolamide 1.0% / Timolol 0.5%) Concomitant (Dorzolamide 1.0%, one drop per dose three times daily to the study eye / Timolol 0.5%, one drop per dose twice daily to the study eye).

Participant Flow:   Overall Study
    MK0507A (Dorzolamide 1.0% / Timolol 0.5% Combination)     Timolol 0.5%     Concomitant (Dorzolamide 1.0% / Timolol 0.5%)  
STARTED     189     92     193  
COMPLETED     179     88     184  
NOT COMPLETED     10     4     9  
Adverse Event                 7                 1                 6  
Lack of Efficacy                 0                 0                 1  
Protocol Violation                 1                 1                 1  
Withdrawal by Subject                 0                 1                 0  
Physician Decision                 2                 1                 1  



  Baseline Characteristics
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Reporting Groups
  Description
MK0507A (Dorzolamide 1.0% / Timolol 0.5% Combination) MK0507A (Dorzolamide 1.0% / Timolol 0.5% combination), one drop per dose twice daily to the study eye.
Timolol 0.5% Timolol 0.5%, one drop per dose twice daily to the study eye.
Concomitant (Dorzolamide 1.0% / Timolol 0.5%) Concomitant (Dorzolamide 1.0%, one drop per dose three times daily to the study eye / Timolol 0.5%, one drop per dose twice daily to the study eye).
Total Total of all reporting groups

Baseline Measures
    MK0507A (Dorzolamide 1.0% / Timolol 0.5% Combination)     Timolol 0.5%     Concomitant (Dorzolamide 1.0% / Timolol 0.5%)     Total  
Number of Participants  
[units: participants]
 		  189     92     193     474  
Age  
[units: Years]
Mean ± Standard Deviation 		  63.2  ± 10.8     61.3  ± 11.6     62.3  ± 12.7     62.4  ± 11.7  
Age, Customized  
[units: participants]
 		       
<65 years     92     50     102     244  
>=65 years     97     42     91     230  
Gender  
[units: participants]
 		       
Female     104     43     98     245  
Male     85     49     95     229  
Diagnosis  
[units: participants]
 		       
Open-angle glaucoma     107     51     90     248  
Normal-tension glaucoma     8     6     4     18  
Ocular hypertension     74     35     99     208  
Intraocular pressure (IOP) at Hour 2  
[units: mmHg]
Mean ± Standard Deviation 		  20.54  ± 2.07     20.23  ± 1.85     20.38  ± 2.31     20.42  ± 2.13  



  Outcome Measures
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1.  Primary:   Change in Intraocular Pressure (IOP) From Baseline at 8 Weeks   [ Time Frame: 8 weeks ]
  Show Outcome Measure 1

2.  Secondary:   Percent Change From Baseline in Intraocular Pressure (IOP) at 8 Weeks   [ Time Frame: 8 Weeks ]
  Show Outcome Measure 2

3.  Secondary:   Percent Change From Baseline in Outflow Pressure Reduction Rate at 8 Weeks   [ Time Frame: 8 weeks ]
  Show Outcome Measure 3


  Serious Adverse Events
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  Other Adverse Events
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Time Frame No text entered.
Additional Description No text entered.

Frequency Threshold
Threshold above which other adverse events are reported   2%  

Reporting Groups
  Description
MK0507A (Dorzolamide 1.0% / Timolol 0.5% Combination) MK0507A (Dorzolamide 1.0% / Timolol 0.5% combination), one drop per dose twice daily to the study eye.
Timolol 0.5% Timolol 0.5%, one drop per dose twice daily to the study eye.
Concomitant (Dorzolamide 1.0% / Timolol 0.5%) Concomitant (Dorzolamide 1.0%, one drop per dose three times daily to the study eye / Timolol 0.5%, one drop per dose twice daily to the study eye).

Other Adverse Events
    MK0507A (Dorzolamide 1.0% / Timolol 0.5% Combination)     Timolol 0.5%     Concomitant (Dorzolamide 1.0% / Timolol 0.5%)  
Total, other (not including serious) adverse events        
# participants affected     36     12     40  
Eye disorders        
Conjunctival hyperaemia * 1      
# participants affected / at risk     3/189 (1.59%)     1/92 (1.09%)     4/193 (2.07%)  
Corneal epithelium defect * 1      
# participants affected / at risk     2/189 (1.06%)     2/92 (2.17%)     5/193 (2.59%)  
Punctate keratitis * 1      
# participants affected / at risk     3/189 (1.59%)     0/92 (0.00%)     6/193 (3.11%)  
General disorders        
Instillation site irritation * 1      
# participants affected / at risk     13/189 (6.88%)     0/92 (0.00%)     7/193 (3.63%)  
Infections and infestations        
Nasopharyngitis * 1      
# participants affected / at risk     5/189 (2.65%)     3/92 (3.26%)     8/193 (4.15%)  
Investigations        
Alanine aminotransferase increased * 1      
# participants affected / at risk     4/189 (2.12%)     2/91 (2.20%)     5/193 (2.59%)  
Glucose urine present * 1      
# participants affected / at risk     5/189 (2.65%)     1/91 (1.10%)     9/193 (4.66%)  
Blood urine present * 1      
# participants affected / at risk     3/198 (1.52%)     3/91 (3.30%)     0/193 (0.00%)  
Musculoskeletal and connective tissue disorders        
Osteoarthritis * 1      
# participants affected / at risk     1/189 (0.53%)     1/92 (1.09%)     4/193 (2.07%)  
Lumbar spinal stenosis * 1      
# participants affected / at risk     0/189 (0.00%)     2/92 (2.17%)     0/193 (0.00%)  
Nervous system disorders        
Headache * 1      
# participants affected / at risk     4/189 (2.12%)     0/92 (0.00%)     0/193 (0.00%)  
* Events were collected by non-systematic assessment
1 Term from vocabulary, MedDRA 10.1



  More Information
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Certain Agreements:  
Principal Investigators are NOT employed by the organization sponsoring the study.
There IS an agreement between Principal Investigators and the Sponsor (or its agents) that restricts the PI's rights to discuss or publish trial results after the trial is completed.
The agreement is:
unchecked The only disclosure restriction on the PI is that the sponsor can review results communications prior to public release and can embargo communications regarding trial results for a period that is less than or equal to 60 days. The sponsor cannot require changes to the communication and cannot extend the embargo.
unchecked The only disclosure restriction on the PI is that the sponsor can review results communications prior to public release and can embargo communications regarding trial results for a period that is more than 60 days but less than or equal to 180 days. The sponsor cannot require changes to the communication and cannot extend the embargo.


Limitations and Caveats
Limitations of the study, such as early termination leading to small numbers of participants analyzed and technical problems with measurement leading to unreliable or uninterpretable data
No text entered.  


Results Point of Contact:  
Name/Title: Senior Vice President, Clinical and Quantitative Sciences
Organization: Merck Sharp & Dohme Corp
phone: 1-800-672-6372


No publications provided


Responsible Party: Executive Vice President, Clinical and Quantitative Sciences, Merck Sharp & Dohme Corp
ClinicalTrials.gov Identifier: NCT00449956     History of Changes
Other Study ID Numbers: 2007_011, MK0507A-149
Study First Received: March 19, 2007
Results First Received: January 23, 2009
Last Updated: April 20, 2010
Health Authority: Japan: Pharmaceuticals and Medical Devices Agency