Macular Degeneration Clinical Trial
Official title:
Complement Factor H Haplotypes and Smoking in Age-related Macular Degeneration
Risk factors for Age-related Macular Degeneration (AMD) involves genetic variations in the alternative pathway of complement inhibitor factor H. The complement system is part of the innate and adaptive immune system. Smoking is the only environmental factor known to increase the risk of Age-related Macular Degeneration (AMD). Using serum samples of Age-related Macular Degeneration (AMD) patients and controls the investigators will test the hypothesis that smoking increases Age-related Macular Degeneration (AMD) by increasing complement activation; and that this is positively correlated with known disease variations in the complement factor H (CFH) gene.
RESEARCH DESIGN AND METHODS A) Study design This study is designed to determine whether
smoking increases complement activation and whether there are specific AMD genotypes that are
particularly sensitive to this elevated level of serum complement components.
B) Selection of subjects and controls Case subjects and age-matched (within 5 years) control
subjects will be recruited under a protocol approved by the Johnson and DeBakey VA Medical
Centers, and the Medical University of South Carolina (MUSC) Human Investigation Review
Board.
Inclusion Criteria
- Case subjects with a clear diagnosis of AMD and at least a 20/40 view of the fundus.
- Control subjects with <5 small hard drusen and at least a 20/40 view of the fundus.
- All subjects will have the ability to provide a blood sample, demonstrate the absence of
exclusion criteria listed below, provide their own consent, or have a legal
representative available to provide consent for them, able to complete all aspects of
testing, and be in generally good medical health in the opinion of the study physician.
Exclusion Criteria
- Individuals who are unable to provide consent and who lack a legal representative, whose
best corrected visual acuity for both eyes is worse than 20/40, who are taking a
medication known to cause retinopathy, unable to cooperate to complete testing, and who
present themselves with media opacity, who exhibit diseases that phenotypically overlap
with AMD such as drusen or pigmentary disturbance of the retinal pigment epithelium; or
provide insufficient evidence to diagnose AMD.
- Individuals who present themselves with macular dystrophies, toxoplasmosis,
histoplasmosis, degenerative myopia, central serous chorioretinopathy, or any disease or
treatment that would diminish the ability to recognize drusen such as laser
photocoagulation, prior retinal detachment surgery, posterior uveitis, and trauma.
Sample Size and Power Estimation A total of 150 case subjects and 150 control subjects will
be recruited. Sample size was determined by statistically simulating the study findings using
the following assumptions: an alpha level of 0.05; 2-sided hypothesis testing; and an
expected distribution across the CC, CT, and TT factor H genotypes of 8.1%, 52%, and 39.9%,
respectively, [1 and assuming ~35% of the subjects being current smokers. This sample size
would provide 85% power to detect a significant smoking by genotype interaction, the main
focus of this study.
Recruitment Case and age-matched (within 5 years) control subjects will be recruited.
Recruitment will take place in two ways: 1) they will be called or recruited after the
diagnosis in the doctor's office. Upon signed consent, these subjects will also be asked to
provide information about their smoking status, and a blood sample (two 3 mL tubes) will be
collected.
C) Outcome measures Incidence of AMD will have been determined in the prior clinical visit
based on Fundus photographs and accepted AMD definitions. Additional outcome measurements
that will help characterize the severity of AMD disease might include the visual field test,
OCT and fluorescein angiograms.
D) Data analyses
- Data assembled as normalized serum levels of complement factors Ba, C3d and fD and fH
activity levels will be initially evaluated with univariate statistics to assure that
the quality of the data is adequate for further analyses. The association between each
measured parameter (i.e., serum levels of complement factors), AMD diagnosis, genotype
and smoking will be assessed in a stratified bivariate fashion using Student t tests or
Wilcoxon rank sum tests, as appropriate, and standard measure assessments will be used
to check for normality, skewing, etc.
- Multivariate analyses will be conducted through the use of general linear mixed models
[5]. The models will include random subject effects to account for dependence among
repeated measurements of subjects. This type of model is ideal when there are multiple
measurements on subjects, such as when laboratory measurements are performed in
triplicate. The dependent variables of interest will be the complement level
measurements (log transformed, if necessary), while independent variables will include
AMD status (case/control), factor H genotype (CC, CT, TT), smoking (current, former,
never), and an interaction-term involving factor H genotype and smoking status. The
interaction-term will help us to determine whether the impact of factor H genotype and
smoking on serum complement levels is linear (additive), or non-linear (e.g.,
multiplicative). The model will also include adjustments for age, gender, and race,
which may all affect complement factors. Thus, any differences among haplotypes will be
adjusted (corrected) for effects that may be attributed to age, gender, or race.
Different correlation structures will be examined for the random subject effects, and
the investigators will use Akaike's Information Criterion to select the most appropriate
model. Secondary analyses will involve excluding never smokers, to assess the nature of
the association (if any) between pack/year histories. factor H genotypes. and their
complement levels. An additional analysis (using conditional logistic regression) will
be conducted to determine whether smoking interacts with a subject's factor H genotype
with respect to the risk of AMD. Again, this model will be adjusted for age, gender, and
race, and the results will be expressed as odds ratios associated with the risk of AMD.
E) Potential risks
- Subjects will have received a comprehensive eye examination that was not part of this
study. The potential risks cannot be described.
- Venipuncture for whole blood. The risks of venipuncture are pain or bruising at the site
of venipuncture; fainting or dizziness; or infection at the site of the needle stick.
None of these are permanent or substantial losses. Clinical staff are trained to deal
with these complications.
- Personal information. Sharing of personal information (blood specimens, personal
history, genetic information, etc.) is not without risk. Research to identify genes that
cause or contribute to a disease or trait is an increasingly important way to try to
understand the role of genes in human disease. The participants were given a consent
form because the Johnson and DeBakey VA Medical Centers investigators want to include
the participants' blood sample in a research project, or because they want to save such
biological specimens for future research.
There are several things participants should know before allowing the blood to be studied or
to be saved.
- Blood samples will be stored under an alphanumeric identifier which could eventually be
linked to the participants.
- In addition to name, other information about participants might be connected to blood
samples.
- Genetic information about the participants' will often apply to family members.
- The participants have the right to refuse to allow their blood to be studied or saved
for future research studies.
- South Carolina law mandates that genetic information, obtained from any tests or from
this research, be kept confidential.
- Genetic research raises difficult questions about informing participants and other
subjects of any results, or of future results.
- If the participants are concerned about a potential genetic disorder, the participant
and their doctor might choose to test specifically for it. This would require additional
blood or tissue samples and would not be part of this research project.
- The presence of a genetic marker for a disease does not necessarily mean that the
participants will develop that disease.
Unknown risks. The researchers will let the participants know if they learn of anything that
might make a change of mind about participating in this study.
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