Population - Ashkenazi Jewish Genetic Diseases
A number of genetic
disorders occur more frequently in certain ethnic populations.In the
Ashkenazi Jewish population (those of Eastern European descent), it has
been estimated that one in four individuals is a carrier of one of
several genetic conditions.These diseases include Tay-Sachs Disease,
Canavan, Niemann-Pick, Gaucher, Familial Dysautonomia, Bloom Syndrome,
Fanconi anemia, Cystic Fibrosis and Mucolipidosis IV.Some of these
diseases may be severe and may result in the early death of a
child.Carrier screening is available for all of these diseases with a
simple blood test.
How are these diseases inherited?
In the nucleus of every cell in the body there are 46 chromosomes.Each
chromosome is a package that holds many genes.Our genes contain DNA, the
set of instructions that makes up who we are.All chromosomes (and the
genes that are on those chromosomes) come in pairs.We receive one member
of each pair of chromosomes from our mother and the other member of the
pair from our father.Sometimes there is a change in a gene (called a
mutation) that causes the gene to malfunction.
All of the above-mentioned conditions are inherited in an autosomal
recessive manner.This means that an affected person has a change in both
genes of the pair of genes, one change inherited from each
parent.Neither gene in the pair is working properly, which causes the
symptoms of the disease.
A carrier is someone who has a change in only one gene of the pair of
genes.Carriers are healthy individuals who are only at risk for passing
the gene change on to their children.Most often these diseases occur in
families with no prior history of the disease.
What are the diseases?
Tay-Sachs Disease is a condition where children develop normally until
about four to six months of age.It is at this time that the central
nervous system begins to degenerate.Individuals with Tay-Sachs Disease
lack an enzyme called hexosaminidase (Hex A).The child loses all motor
skills and becomes blind, deaf and unresponsive.Death usually occurs by
the age of four.The carrier rate in the Ashkenazi Jewish population is
approximately 1 in 25.More rare than the infantile type is Late Onset
Tay-Sachs Disease, where the progression of symptoms is slower and
milder.
Canavan Disease is very similar to Tay-Sachs Disease, with normal
development until age two to four months, followed by progressive loss
of previously attained skills.Most individuals with Canavan Disease die
by the age of five.An estimated 1 in 40 Ashkenazi Jews is a carrier for
this disease.
Niemann-Pick Disease – Type A is a disease in which a harmful amount of
a fatty substance accumulates in different parts of the body.Failure to
thrive and a progressive neurodegenerative course lead to death by three
years of age.The carrier rate in the Ashkenazi Jewish population is
approximately 1 in 90.
Gaucher Disease – Type 1 (pronounced go-shay) is a variable condition,
both in age of onset and in progression of symptoms.A painful, enlarged
and overactive spleen, with anemia and low white blood cell count are
usually the initial features of Gaucher Disease.Bone deterioration is a
major cause of discomfort and disability.Approximately 1 in 14 Ashkenazi
Jews is a carrier of this condition.Treatment is available.
Familial Dysautonomia (FD) is a disease that causes the autonomic and
sensory nervous systems to malfunction.This affects the regulation of
body temperature, blood pressure, stress response, normal swallowing and
digestion.An estimated 1 in 30 Ashkenazi Jews is a carrier of FD.
Bloom Syndrome is characterized by short stature, sun-sensitive facial
skin lesions, an increased susceptibility to infections and a higher
incidence of leukemia and certain cancers.The carrier rate is about 1 in
100 in the Ashkenazi Jewish population.
Fanconi anemia – Type C is a disease associated with short stature, bone
marrow failure and a predisposition to leukemia and other cancers.Some
children may have learning difficulties or mental
retardation.Approximately 1 in 89 Ashkenazi Jews is a carrier for this
condition.
Mucolipidosis IV (ML IV) is caused by the accumulation of certain
harmful substances throughout the body.Individuals with ML IV experience
a range of levels of motor and mental retardation, with developmental
delays often manifesting themselves as early as the first year of
life.Other symptoms can be related to the eyes, such as corneal
clouding, pseudostrabismus and retinal degeneration.
Cystic Fibrosis (CF) is a multi-system disorder that causes the body to
produce a thick mucus.The mucus accumulates primarily in the lungs and
the digestive tract, resulting in chronic lung infections and poor
growth.CF does not affect intelligence.The carrier rate for CF among all
Caucasian individuals is approximately 1 in 25.The CF carrier test has a
detection rate of 97% in the Ashkenazi Jewish population.
What if we both are carriers?
If two carriers of the same disorder have children, there is a 25%
chance of having an affected child, a 50% chance of having a child who
is a carrier like themselves, and a 25% chance of having a child who is
neither affected nor a carrier.If an individual is found to be a
carrier, genetic counseling is available at many clinics throughout the
country to discuss the implications of this finding.If partners are
found to be carriers of the same disorder(s), a genetic counselor can
provide information and support, which may be helpful in making
important family planning decisions.
The results of these tests are highly accurate.However, there is a
slight possibility that someone who tests negative for being a carrier
could still be a carrier.There may be rare mutations that DNA testing
may not pick up.
From:
http://www.jewishvirtuallibrary.org/jsource/Health/genetics.html
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