Age-Related Macular Degeneration Clinical Trial
Official title:
Genetic Biomarkers for the Response to Anti-VEGF (Vascular Endothelial Growth Factor).Treatment in Wet Age-related Macular Degeneration (Wet ARMD)
Age-Related Macular Degeneration (ARMD) is the most common cause of blindness in the adult
population of the Western World. It affects the macula - the region of the retina most rich
in photoreceptors and responsible for central vision. The ethiology of ARMD remains poorly
understood. Population-based studies have demonstrated a complex ethiology, with
contributions from a combination of genetic and environmental factors.
Two major forms of ARMD are clinically distinguishable: the dry and wet form. The latter
represents the more aggressive clinical subgroup, and is characterized by the abnormal growth
of new blood vessels (neovascularization) under the macula, thus leading to the accumulation
of fluid under the retina, bleeding, progression to fibrosis, and finally loss of central
vision.
The pathogenesis of this neovascularization is not fully understood, although the VEGF
pathway is well known to be involved in angiogenesis and was implicated in the development of
the new vessels under the macula. The VEGFs are the most specific and potent stimulators of
the angiogenesis.
Molecules that bind and inactivate the VEGF have been developed for the treatment of ARMD and
they are applied in ARMD clinic through intra vitreal injections.The difference seen in
response to anti VEGF treatment for ARMD between the patients is suggestive for the presence
of factors influencing the effect of the drug. Some of these could be genetic variants within
genes involved in ARMD pathogenesis or VEGF pathway. Few associations with markers within
genes previously found to be related with the pathogenesis of ARMD have been found. It
remains unknown whether variants involved in the anti VEGF treatment response could influence
the therapeutic outcome.
The purpose of this trial is to evaluate the association between a panel of selected
polymorphic markers in the VEGF pathway and the response to therapy with anti VEGF antibody
for ARMD. The hypothesis is that the individual genotype influences the response to the anti
VEGF. This can lead to identification of genetic biomarkers allowing treatment
individualization and optimization of the visual outcomes.
Age-Related Macular Degeneration (ARMD) is the most common cause of blindness in the adult
population of the Western World. It affects the macula - the region of the retina most rich
in photoreceptors and responsible for central vision.
Despite this manifest importance, the ethiology of ARMD remains poorly understood.
Population-based studies have demonstrated a complex ethiology, with contributions from a
combination of genetic and environmental factors. Genome-wide association studies revealed
the presence of loci associated with susceptibility in a wide range of genes, including genes
involved in the complement system, cholesterol homeostasis, growth factor diffusion and
angiogenesis. Smoking has been identified as a major environmental factor.
Two major forms of ARMD are clinically distinguishable: the dry and wet form. The latter
represents the more aggressive clinical subgroup, and is characterized by the abnormal growth
of new blood vessels (neovascularization) under the macula, thus leading to the accumulation
of fluid under the retina, bleeding, progression to fibrosis, and finally loss of central
vision.
The pathogenesis of this neovascularization is not fully understood, although the VEGF
pathway is well known to be involved in angiogenesis and was implicated in the development of
the new vessels under the macula. The VEGFs are the most specific and potent stimulators of
the angiogenesis. VEGF-A is a 45kD glycoprotein binding to transmembrane tyrosine kinase
receptors, VEGFRs, which activates a cascade of downstream factors. VEGF-A has the strongest
pro-angiogenic effect in the retina by promoting proliferation, sprouting and tubing of the
endothelial cells. It can bind to at least two receptors -VEGFR1 and VEGFR2, although the
most of the proangiogenic activity appears to be mediated through VEGFR2. Expression of a
VEGFR2 isoform that lacks both the intracellular signaling domain and the transmembrane
domain, represents a soluble form of the receptor, inactivating VEGF extracellularly.
Similarly, molecules that bind and inactivate the VEGF have been developed for the treatment
of ARMD and they are applied in ARMD clinic through intra vitreal injections. These include
antibodies, a recombinant receptor fusion protein and a synthetic aptamer. The anti-VEGFA
antibodies - ranibizumab and bevacizumab, off-label, have been associated with limited
side-effects and significant therapeutic improvement, and became the standard in the
treatment of the wet form of ARMD. Indeed, for example in the first clinical trials for
ranibizumab, monthly injections of ranibizumab demonstrated an average gain in visual acuity
of 6.6 and 10.7 ETDRS letters after 24 months. However, currently most clinical centres apply
modified treatment protocols. Commonly used is an initial loading dose of three consecutive
monthly injections and subsequent follow-up and administration of additional injections
depending on the evolution of visual acuity, optical coherence tomography and fluorescein
angiography data . 25% of the ARMD patients show significant improvement of the visual
acuity, 70% maintain or show slightly increased visual acuity, and the remaining 5 percent of
the patients fail to respond to the treatment and continue to loose vision.
The difference seen in response to anti VEGF treatment for ARMD between the patients is
suggestive for the presence of factors influencing the effect of the drug. Some of these
could be genetic variants within genes involved in ARMD pathogenesis or VEGF pathway. Few
associations with markers within genes previously found to be related with the pathogenesis
of ARMD have been found. It remains unknown whether variants involved in the anti VEGF
treatment response could influence the therapeutic outcome.
A study demonstrated that the single nucleotide polymorphism (SNP) in VEGFR1 rs7993418 (TAC
codon) form is associated to resistance to the anti VEGF therapy in carcinoma patients. This
specific genotype leads to an increased expression of the VEGFR1 without changing the amino
acid content of the protein. The increased VEGFR1 protein is most likely due to higher
efficiency of messenger ribonucleic acid (mRNA) translation.
The purpose of this trial is to evaluate the association between a panel of selected
polymorphic markers in the VEGF pathway and the response to therapy with anti VEGF antibody
for ARMD. The hypothesis is that the individual genotype influences the response to the anti
VEGF. This can lead to identification of genetic biomarkers allowing treatment
individualization and optimization of the visual outcomes.
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