Age-related Macular Degeneration Clinical Trial
Official title:
A Multicenter Study on the Investigation of Previously Verified Leading Gene Polymorphisms Related to Age-related Macular Degeneration in Turkish Population
The purpose of this study is to determine whether common genetic polymorphisms that have been verified to be related to age-related macular degeneration (AMD) in some populations are also associated with AMD in Turkish population
Age-related macular degeneration (AMD) remains as the most important cause of severe visual
impairment of elderly people in developed countries. It is one of the best-characterized
complex trait diseases. Multiple genetic and environmental factors play a role in the
pathogenesis. A number of different biological pathways and related gene polymorphisms are
strongly implicated in its etiology. A lot of chromosomal locations have been studied to
figure out genetic risk factors responsible from the development of AMD. Most genetic
variants that have been found to be related to AMD at least in one study have not been
verified in subsequent studies. However in recent years, single-nucleotide polymorphisms
related to the complement system and also chromosome 10q26 have strongly been elicited to
predispose individuals to the susceptibility to AMD. These polymorphisms have been verified
in subsequent studies. However, results from different geographic regions of the world can
represent discrepancies according to ethnic populations. Aforementioned genetic tests have
been commercially introduced to give the patients the risk of progression to advanced stage
of AMD, and rate of the risk can be given by the genetic results together with environmental
factors in USA.
Age related macular degeneration is consisted of dry and wet forms. Although wet form is
responsible from severe vision loss due to AMD, dry form can progress to wet form by passage
of time. The risk of AMD increases when age get older and it causes very severe central
vision loss; consequently reduces considerably the quality of life in senile population.
Available treatment of AMD is expensive and has economical burden. Early diagnosis of the
disease has favourable impact on post-treatment prognosis. Although the basis of treatment
is primarily based on the preservation of current visual acuity, it is possible to obtain
improvement in visual acuity with the agents inhibiting angiogenesis in recent years.
However, complete response to the treatment is not obtained approximately in one fifth of
the patients. Different responses to the treatment are obtained in the remaining group. The
reason for the differences at the treatment may be due to different morphological subgroups
and/or diversity of genetic variants in wet AMD. . We do not at the moment know whether gen
polymorphisms related to AMD established in some western population are also related to AMD
in our population or whether this relationship has similar risk or protective effect for
AMD. The gen variants mostly studied in relation to AMD are CFH (rs1061170 and rs1410996),
LOC387715/ARMS-2 (A69S /rs10490924), HTRA-1 (rs11200638), C3 (R102G/ rs2230199), C2 E318D
(rs9332739), and CFB R32Q (rs641153). A preliminary study which was published recently,
carried out by our team in a single center and in a small number of patients showed that CFH
and LOC387715 gen polymorphisms entertain a risk for late AMD and suggested a necessity to
perform a forward study with larger population to learn definite information about our
population. On the other hand, the entire eight genetic locus related to AMD will be studied
first time in our population. In the introduced projects study, the relationship of eight
different gen polymorphisms (CFH rs1061170 and rs1410996, LOC387715 / ARMS2 gene rs10490924,
C2 gene rs9332739, CFB gene rs641153, CFI rs10033900 , HTRA-1 gene rs11200638, C3 rs2230199)
will be studied in 2800 patients with high risk intermediate and late stage AMD and 2200
age-matched control subjects. Blood samples from brachial veins of the study subjects will
be collected in the 5 health centers composed of Bursa Retina Eye Center and Hospitals of
Afyon Kocatepe University, Dokuz Eylul University, Konya University and Uludag University
within the period of 32 months. After the collection of venous samples, polymorphisms will
be genotyped by "real-time PCR'' and ''pyrosequencing" genotyping systems in the genetic
laboratory of Afyon Kocatepe University Medical School. Within the last 3 months of the
project duration, having completed genotyping of all samples, evaluation of the study data
by clinically and statistically will be made, and preparation of final report will be
realized. . As a primary outcome, protective effects or the risk rate of developing the late
AMD for each genetic polymorphism will be calculated by statistical analysis following the
genotyping. Sub-analyses will be done to investigate any relationship between genetic
polymorphism and response to the treatment. Sub-analyses will be done to determine possible
differences in genetic variants between the late dry and wet AMD and also among the
morphological subtypes of the wet AMD. Main study and secondary sub-studies derived from
sub-analyses by further methodology will be submitted as different studies for publication.
The anticipated results of the study may have impact on the management and follow-up of the
patients with AMD. Because AMD is etiologically multi-factorial disease and has
environmental controllable risk factor outside the genotypic features, it may be possible to
early diagnosis and frequent follow-up in addition to recommending to avoid from modifiable
risk factors in patients with early AMD who are genetically under the high risk of the
development of late AMD according to findings obtained from our study results. It will also
be possible to establish the patients with wet AMD who are resistant or sensitive to the
treatment according to genotyping. Whether performing genetic tests in patients who are
candidate to the late AMD in the near future is significant and meaningful for our
population will be established. Our results evaluated together with the literature will make
substantial contribution to better understanding of pathogenesis of AMD as well as early
diagnosis and better classification or treatment choices.
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Observational Model: Case Control, Time Perspective: Prospective
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