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Attention has been focussed on the
genetic metabolic diseases in which a defective gene causes an enzyme to be
either absent or ineffective in catalyzing a particular metabolic reaction
effectively. A potential approach to the treatment of genetic disorders in man
is gene therapy. This is a technique where the absent or faulty gene is
replaced by a working gene, so that the body can make the correct enzyme or
protein and consequently eliminate the root cause of the disease.
The first clinical gene therapy
was given in 1990 to a 4 years old with Adenosine Deaminase (ADA) deficiency.
This enzyme is crucial for the immune system to function. The disorder is
caused due to the deletion of the gene for Adenosine Deaminase. In some children,
ADA deficiency can be cured by bone marrow transplantation; in others, it can
be cured by enzyme replacement therapy in which functional ADA is given to the
patient by injection. The demerit in both of these approaches is that they are
not completely curative so gene therapy is the only alternative solution.
The first step towards gene therapy
is the growth of lymphocytes in a culture outside the body extracted from
the blood of patient. A functional ADA cDNA (Circular DNA) by using a
retroviral vector is then introduced into these lymphocytes which are
subsequently returned to the patient’s body. However, as these are not
immortal, the patient needs periodic infusion of such genetically engineered
lymphocytes but if the gene isolated from the bone marrow cells producing ADA
is introduced into cells at early embryonic stages then it could be a permanent
cure.
Before treatment for a genetic
disease can begin, an accurate diagnosis of the genetic defects needs to be made.
It is here that biotechnology is likely to have a great impact in near future.
Genetic Engineering research has produced a powerful tool for pinpointing
specific diseases rapidly and accurately. Short pieces of DNA (Deoxyribonucleic
Acid) called DNA probe can be designed to stick very specifically to certain
other pieces of DNA. The technique relies upon the fact that complementary
pieces of DNA stick together. DNA probes are more specific and have potential to
be more specific than conventional diagnostic methods and it should be possible
in near future to distinguish between defective genes and their normal
counterparts, an important development towards Genetic Enginnering.
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