Brief Title
Identifying Genes and Mutations Underlying Retinitis Pigmentosa and Allied Diseases
Protocol ID
NCT02309866
Lead Sponsor
Hillel Yaffe Medical Center
Brief Summary
Retinitis Pigmentosa (RP) is the most common form of hereditary retinal degeneration,
with a worldwide prevalence of 1:3500. It is one of the most genetically heterogenous
conditions in humans, with over 100 causative genes and loci reported to date. However,
in approximately 40% of patients the underlying genetic causes are yet to be found.
The current study aims to identify causative RP genes and mutations in Israeli families
of various ethnic backgrounds. Identification of such genes will contribute significantly
to disease prevention (by identification of high risk families and appropriate genetic
counseling) and to the investigators understanding of retinal structure and function and
of the etiology of RP.
Detailed Description
Background: Retinitis Pigmentosa (RP) is a clinically and genetically heterogeneous
disease, which causes visual loss due to the premature death of retinal photoreceptors.
Over 100 genes and loci have been implicated in RP. However, the contribution of each of
these genes to the overall prevalence of RP is relatively small, and many of them are yet
to be found. These unidentified genes are likely to be very rare. The vast majority of
studies on the genetics of RP have been performed on the American and European
populations. Based on the investigators experience, the genetic makeup of the Israeli
population is unique, and many of the genetic alterations identified in Israeli patients
are novel.
Working hypothesis and aims: the investigators working hypothesis is that the Israeli
population is unique in terms of the identity and relative contribution of RP genes.
Therefore, the investigators aim is to perform a comprehensive genetic analysis of
affected Israeli individuals of various ethnic backgrounds, in order to identify novel RP
mutations and genes.
Methods: RP patients and family members will be continuously recruited to the study
through the Ophthalmology Department at Hillel Yaffe Medical Center, Hadera, Israel. The
relatively high proportion of founder mutations in the Israeli population allows us to
perform a quick and efficient mutation screening and identify the cause of disease in a
large number of newly recruited families. Patients who are negative for all relevant
mutations will be studied using whole exome sequencing. Bioinformatic analysis will be
used to identify possible pathogenic variants. Following verification, the investigators
will check their co-segregation with the disease in the entire family, and their
frequency in the relevant population.
Expected results: The immediate expected outcomes include an epidemiological overview of
RP distribution and etiology in the Israeli population, and identification of novel
causative genes and mechanisms. These genes are expected to play a crucial role in
retinal development and function, and hence their identification and characterization
will contribute significantly to the investigators understanding of retinal structure and
function and of the etiology of RP. The main expected long-term outcome is reduction in
the frequency of RP in Israel. This will be achieved by a combination of prevention (by
genetic screening and counseling among high-risk populations), and treatment (by
identification of patient groups with shared genetic diagnoses, who can be recruited to
clinical trials for evaluation of various treatment strategies).
Enrollment Count
100 participants
Eligibility Criteria
Inclusion Criteria:
- Patients with RP in which the genetic cause has not been identified yet and their
healthy family members
Exclusion Criteria:
- Patients with RP in which the genetic cause has already been identified
Filters
Retinitis Pigmentosa
UNKNOWN
CHILD
ADULT
OLDER_ADULT