Beta-Thalassemia Clinical Trial
Official title:
Detection of β-thalassemia Carriers Among Close Relatives of β-thalassemia Children Attending Assiut University Children Hospital
Thalassemia is different in kids with microcytic hypochromic anemia than general population
because there is a confusion between symptoms of thalassemia and iron deficiency anemia in
kids and both of them differ in management and prognosis. otherwise the most commonest causes
of microcytic hypochromic anemia in kids are iron deficiency anemia and thalassemia and both
of them are more common in kids than in general population.
Thalassemia is different in Egypt than anywhere in the world because there is no accurate
estimation of incidence and prevalence of such dangerous disease in Egypt inspite of many
cases attending thalassemia center (hundreds) and this disease is autosomal recessive and its
incidence can be minimized by detection of carrier cases by gene study hopping that to be
done as a routine premarital investigation.
The term "thalassemia" is derived from the Greek words "Thalassa"(sea) and "Haema" (blood)
and refers to disorder associated with defective synthesis of α or β-globin subunits of
haemoglobin HbA
There are two main types of thalassemia:
α-thalassemia is one of the most common hemoglobin genetic abnormalities and is caused by the
reduced or absent production of the alpha globin chains. Alpha-thalassemia is prevalent in
tropical and subtropical world regions where malaria was and still is epidemic, but as a
consequence of the recent massive population migrations, alpha-thalassemia has become a
relatively common clinical problem in North America, North Europe, and Australia
β-thalassemia syndromes are a group of hereditary blood disorders characterized by reduced or
absent beta globin chain synthesis, resulting in reduced Hb in red blood cells (RBC),
decreased RBC production and anemia. Most thalassemias are inherited as recessive traits. The
phenotypes of homozygous or genetic heterozygous compound β-thalassemias include thalassemia
major and thalassemia intermedia. Individuals with thalassemia major usually come for medical
attention within the first two years of life and require regular RBC transfusions to survive.
Thalassemia intermedia include patients who present later and do not require regular
transfusion. Except in the rare dominant forms, heterozygous β-thalassemia results in the
clinically silent carrier state. HbE/ β-thalassemia and HbC/ β-thalassemia exhibit a great
range in terms of diversity of phenotypes and spectrum of severity. People who are carriers
of the disease received variant genes from one parent and normal gene from the other parent
Thalassemia is widespread throughout ,they are more prevalent in people living in South-East
Asia, South Asia, Middle East, and Mediterranean regions
Thalassemia is the most common form of inherited anemia worldwide. The World Health
Organization reports suggest that about 60,000 infants are born with a major thalassemia
every year. Although individuals originating from the tropical belt are most at risk, it is a
growing global health problem due to extensive population migrations
Population migration and intermarriage between different ethnic groups has introduced
thalassemia in almost every country of the world
In Egypt, β -thalassemia is the most common type with a carrier rate varying from 5.3 to 9%
and a gene frequency of 0.03. So, it was estimated that 1,000/1.5 million per year live
births will suffer from thalassemia disease in Egypt (total live births 1,936,205 in 2006)
β Thalassemia creates a social and financial burden for the patients' family and the Egyptian
government. The high frequency of beta-thalassemia carriers with increasing rate of newly
born cases is a pressing reason for the importance to develop prevention program for
beta-thalassemia in Egypt
The thalassaemia syndromes, particularly those requiring multiple blood transfusions, are a
serious burden on health services and a problem which may be increasing on a global scale .
Even milder syndromes, known as thalassaemia intermedia or non-transfusion dependent
thalassaemia, require careful follow up since complications are expected over time in the
natural course of the disease
The need for lifelong follow up and care and the occurrence of complications affecting major
organs such as liver, heart and endocrine glands, creates the need for organised expert
services and also the need for major resources in terms of essential drugs and donated blood
for transfusions. In terms of clinical outcomes, The investigator expect that patients will
survive with the best possible quality of life, if treated holistically in an expert centre
Detection of asymptomatic carriers by reliable laboratory methods is the cornerstone of
prevention of this serious health problem. high performance liquid chromatography (HPLC) has
become the preferred technique, as it can detect most of the clinically significant variants.
The simplicity of the automated system with internal sample preparation, superior resolution,
rapid assay time, and accurate quantification of hemoglobin fractions makes this an ideal
methodology for the routine clinical laboratory
Commonly occurring mutations of the HBB gene are detected by a number of polymerase chain
reaction (PCR)-based procedures. The most commonly used methods are reverse dot blot analysis
or primer-specific amplification with a set of probes or primers complementary to the most
common mutations in the population from which the affected individual originated
Other methods based on real-time PCR or microarray technology because of their
reproducibility, rapidity, and easy handling are potentially suitable for the routine
clinical laboratory
If targeted mutation analysis fails to detect the mutation, scanning or sequence analysis can
be used. Sensitivity of both mutation scanning and sequence analysis is 99%. In the meantime,
the presence of an extended deletion should be investigated by using multiplex
ligation-dependent probe amplification (MPLA)
Screening for genetic diseases aims to reduce the burden of these disorders on individuals by
identifying those at increased risk, thereby enabling individuals to receive information
about personal health, future health and/or potential health of offspring
At risk individuals must be provided with information regarding the mode of inheritance, the
genetic risk of having affected children and the natural history of the disease including the
available treatment and therapies under investigation
Several countries have set up comprehensive national prevention programs, which include
public awareness and education, carrier screening, and counseling, as well as information on
prenatal diagnosis and preimplantation diagnosis. These countries are Italy, Greece, Cyprus,
UK, France, Iran, Thailand, Australia, Singapore, Taiwan, Hong Kong, and Cuba
;
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