Neurological Diseases Clinical Trial
Official title:
Finding Genes With NGS Techniques in Whom Mutations Cause Neurological Diseases
In Israel, because of special qualification in neurogenetics, during a 30 year career ,we
have found, characterized and treated at least 13 novel neurological diseases. The genetic
basis was elucidated with geneticist colleagues both in Israel and worldwide. The diseases
we have found encompass all the fields of pediatric neurology including intellectual
disability, epilepsy, muscle-nerve disorders, malformations of the brain, microcephaly,
macrocephaly, cerebellar ataxia, chorea. dystonia, cerebral palsy and many other symptoms
and signs.
We are especially interested in consanguineous families, in whom the parents are first or
second degree cousins. These families often bear autosomal - recessive diseases. If the
family is informative - with 2 or more affected children - then with current genetic
techniques there is a good chance of finding the causative gene to this specific disease.
This is not only a theoretical - academic accomplishment. In practice, after discovering the
gene, the family is given genetic counseling and in their further pregnancies the
geneticists will examine either by preimplantation genetic diagnosis (PGD) or amniocentesis
if the embryo is affected or not. In the early stages of the pregnancy if the embryo is
indeed affected by the disease caused by the gene we have found and the religious official
consents, genetic counseling can offer termination of pregnancy to the couple.
Needless to say, we know the immense burden of an affected child on the family, community
and society. The parents are guilt-ridden, the affected child draws extensive resources from
educational, health and rehabilitation authorities. We can contribute to the well-being of
the family and the clan (because many times the relatives are affected).
We can perform sophisticated genetic studies such as Whole Genome Sequencing and Whole Exome
Sequencing.After an informative family is recruited to the study, we will explain the aims
of the research. The parents and eligible patients will sign informed consent forms,
according to the local Helsinki Board. Blood samples will be taken in Israel, DNA extracted
in the Israeli lab and then shipped coded to the researchers in USA or Germany. If the
researchers will find a new gene the family will be notified and given appropriate genetic
counseling. We will continue to follow and treat the family onwards.
In Israel there are various sub-populations with a tendency to consanguinity. Among them are
the Arab-Muslim, Druze, Bedouin, Sephardi Jews and to a lesser extent Ashkenazi Jews.
Consanguinity (especially between 2 first cousins) exposes the couple to various genetic
diseases at a risk of 25% per each pregnancy. This phenomenon is based on Mendelian
autosomal-recessive inheritance. When the couple is from the same family or clan, or even
from the same ethnic origin , there is a probability that "dormant" abnormal genes will pass
through generations of intermarriage, thus rendering the couple as "carriers" and producing
a risk of 25% for the offspring to be affected.
Many of the autosomal-recessive diseases have neurological features such as : developmental
delay, intellectual disability, epilepsy and motor and/or sensory impairment. These diseases
carry a heavy burden on the family, community and the educational, health and welfare
authorities. The disabled children are often handicapped, go to special education programs,
are not independent in daily living tasks, are often sick and in need of hospitalization.
They will grow up needing special housing facilities. Their life span is usually shorter
than normal. These children are dependent on their parents, they subdue the parents to
misery, interparental conflicts and susceptibility to divorces. Most of the neurological
diseases are untreatable nowadays. Most of the medical effort focuses on their prevention.
For example, by finding the gene for a specific neurological condition, we could search for
that same gene in the couple's next pregnancy. If the fetus is found to be affected we could
offer genetic counseling and a possibility of pregnancy termination and so the family avoids
the birth of an affected sibling.
When an individual with a neurogenetic disease is enrolled to the study a careful history is
taken to characterize the neurological syndrome, to see if other family members are affected
by the same condition, and a pedigree is drawn. We compare the neurological signs and
symptoms to information data webs like " PUBMED" or "Online Mendelian Inheritance in Man",
and if we don't find a similar description we refer to the family as harboring a new disease
with a novel gene.
We work with neurogenetic colleagues abroad like Dr. Andy Singleton in National Institute of
Aging, NIH, U.S.A of Dr. Markus Schuelke from Charite Hospital, Berlin, Germany.
We take on ourselves to search for the families, explain to them what are the purposes of
the research and their consequences. If we suspect a new gene, we will ask the parents or
patients to sign informed consent forms according to our approved Helsinki board. We will
take a sample of 10 cc blood in order to extract DNA. The DNA will be extracted in the
genetic lab in Israel. A coded DNA will be sent to the researcher abroad. After 12 years the
sample will be returned coded to the lab in Israel.
The researchers abroad will use homozygosity mapping techniques as well as NEXT GENERATION
SEQUENCING like WHOLE EXOME SEQUENCING and WHOLE GENOME SEQUENCING.
If a new gene is found we will arrange for proper genetic counseling and explain the
implications of the genetic data on the individual and his family. We will provide the
family with symptomatic or palliative further therapy as needed.
;
Time Perspective: Prospective
| Status | Clinical Trial | Phase | |
|---|---|---|---|
| Completed |
NCT01371097 -
Progressive Resistance Strength Training (PRT) in Hospitalised Elderly Patients
|
N/A | |
| Completed |
NCT02790424 -
Adjustment Exploratory Protocols and Functional Evaluation of New Non Invasive Devices in Patient Volunteers
|
N/A | |
| Completed |
NCT02455284 -
In Vivo and ex Vivo Validation of MR Tractography of Brain White Matter Tracts - FIBRATLAS II-III
|
N/A | |
| Recruiting |
NCT04995848 -
Telepalliation - Digital Platform for Patients in Palliation and Their Relatives
|
N/A | |
| Completed |
NCT01783769 -
Evaluating the Impact That Personnel Traffic Through the Operating Room Has on Surgical Site Infections
|
N/A | |
| Completed |
NCT01463995 -
Prognosis in Neurological Intensive Care Unit Patients (proNICU Cohort)
|
||
| Recruiting |
NCT02018406 -
Establishment of Clinical Basis for Hematopoietic Growth Factors Therapy in Brain Injury
|
Phase 1/Phase 2 | |
| Terminated |
NCT00841984 -
In Vitro NMR Spectroscopy in Neurological Diseases
|
N/A | |
| Not yet recruiting |
NCT05515419 -
Allogeneic Cord Blood for Neurological Diseases in Adults
|
Early Phase 1 | |
| Completed |
NCT00560157 -
Nutritional and Metabolic Evaluation of a Tube Feeding Immune Enhancing Diet in ICU Patients
|
Phase 4 | |
| Completed |
NCT05486052 -
Rehabilitation With Biofeedback in Neurology
|
N/A | |
| Recruiting |
NCT04846764 -
Rapid Declarative Neocortical Declarative Learning in Aging and Memory Diseases (ANéRAVIMM)
|
N/A |