Missing Body Defense Systems
The immune defense system is a body-wide network
of organs, tissues, cells, and protein substances
that work together to defend the body against attacks
by "foreign" invaders. These invaders,
called foreign antigens can be in the form of bacteria,
virus, fungi, parasites or even single proteins.
Once a foreign antigen is detected the immune system
attacks and destroys it. If the body is strong,
it can win the battle most of the time. When a major
component of the immune system is not functioning
correctly, medical intervention is necessary to
stay healthy and ward off infections.
The cells that make up the immune system develop
in the bone marrow in the form of the stem cells.
These develop into cells called B-lymphocytes, T-lymphocytes,
NK-lymphocytes and phagocytes. These primary
cell families and the proteins they produce make
up the most important components of the immune system.
These cells and proteins are all spread throughout
the body so they can react quickly to any problem.
The defining characteristic for SCID is always
a severe defect in T cell production and function,
with defects in B-lymphocytes as a primary or secondary
problem and, in some genetic types, in NK cell production
as well.
The B-Cells
When a foreign antigen invades the body T-helper
cells direct B-lymphocytes (or B-cells) to make
antibodies against it. These antibodies bind to
the foreign antigen, neutralize it and allow phagocytes
to digest and eliminate it completely. Problems
within B-cells cause antibody deficiencies that
may become evident as recurrent infections as early
as seven to nine months of age, at a time when maternal
antibodies that had passed through the placenta
during pregnancy have fallen to non-protective levels.
The T-Cells
There are three main forms of T-lymphocytes:
Helper (T-helper cells), Cytotoxic (cytotoxic T
cells) and Regulatory (T-reg or T-supressor) T cells.
T-helpers direct and assist all other immune
cells in attacking foreign antigens. T-cytotoxic
cells kill the unwanted antigens and T-reg cells
are the off-switch to an attack. They serve to limit
collateral damage. T-cells direct the rest of the
immune system to respond to foreign invaders; therefore,
problems in the T-lymphocyte system are generally
profound, causing severe combined immunodeficiency
syndromes (SCID) that declare themselves soon after
birth. Milder forms of T-lymphocyte dysfunction
(combined immunodeficiency - CID) may present later
in life, are generally less severe and are compatible
with longer survival.
SCID
|
| Some of The
Known Forms of SCID: |
Gene |
Lymphocyte
Phenotype |
| X-linked SCID (gamma
chain gene mutations) |
IL2RG |
T(-) B(+) NK(-) |
| |
|
|
Autosomal Recessive SCID
|
|
|
| Jak3 gene mutations |
JAK3 |
T(-) B(+) NK(-) |
| ADA gene mutations |
ADA |
T(-) B(-) NK(-) |
| IL-7R alpha-chain mutations |
IL7R alpha |
T(-) B(+) NK(+) |
| CD3 delta or epsilon mutations |
CD3 delta or epsilon |
T(-) B(+) NK(+) |
| RAG1/RAG2 mutations |
RAG1/RAG2 |
T(-) B(-) NK(+) |
| Artemis gene mutations |
ARTEMIS |
T(-) B(-) NK(+) |
| CD45 gene mutations |
CD45 |
T(-) B(+) NK(+) |
|
|
|
SCID or Severe Combine Immune Deficiency
is the most severe of the Primary Immune Deficiency
diseases. The defining characteristic of SCID
is the absence of T cells and, as a result, lack
of B cell function as well. Unless these defects
are corrected the child will die of opportunistic
infections before their first or second birthday.
As of this writing, there are ten known forms of
SCID. Often some of the combined immunodeficiencies
are mislabeled as SCID. Consequently, what some
call SCID are not listed in the table. Additionally,
there are a number of cases of SCID for which the
genetic cause is still undetermined. No matter what
the form of SCID though, the end result is that
critical immune defenses are missing and treatment
should be considered a pediatric emergency.
Inheritance
Autosomal recessive inheritance – Autosomal
recessive forms of SCID result when a child inherits
two defective copies of the same autosomal gene.
The parents in this case each carry one normal copy
of the gene and one abnormal copy. In the case of
an affected child, the child inherits both abnormal
copies. One form of SCID is ADA deficiency. This
condition results from the lack of an enzyme that
helps cells to get rid of toxic byproducts. Without
ADA, poisons build up and kill the lymphocytes.
It was in 1972 that the ADA deficiency form of SCID
was recognized, but ADA deficiency has an autosomal
recessive inheritance pattern that affects males
and females equally. It was known though that a
predominance of SCID patients were male, leading
researchers to suspect that an X-linked inheritance
also existed.
X-linked inheritance or X-SCID – A female
can be a silent carrier of a defective X- chromosome,
because her 2nd X chromosome compensates and consequently
she is unaffected. A male who inherits the defective
X chromosome, however, will be affected. X-linked
SCID affects only males and accounts for approximately
45% of all cases of SCID. It wasn't until 1993 that
Dr. Jennifer Puck and Dr. Warren Leonard simultaneously,
but independently, discovered the genetic defect
involved in X-linked SCID.
Treatment
Bone Marrow Transplantation - The first
two successful bone marrow transplants in the US
occurred in 1968. These 2 transplants were
both in primary immunodeficient patients, one with
SCID and the other with Wiskott-Aldrich Syndrome.
Both patients received marrow from related donors
who were HLA (Human Leucocyte Antigen) identical.
It was in 1973 that the first successful BMT between
unrelated patients was performed. This was
also on a SCID patient. Although unrelated,
the donor in this case was also 100% HLA matched
to the patient. The patient required multiple
infusions of marrow but ultimately engraftment was
achieved.
Bubbles - Between the years of 1968 and
1973 doctors were occasionally able to diagnosis
a case of SCID, however, if there was no HLA matched
sibling they were unable to correct the defect.
Unfortunately, most of these cases were not diagnosed
until the child was critically ill. In 1971
an unusual opportunity occurred. A mother
who had lost a child to SCID was pregnant with another
boy. Since the risk of another affected child
was a real possibility, plans were made on how to
keep this child healthy until his immune system
could be corrected. David was born on September
21, 1971 and was immediately placed into a specially
designed isolator crib where the air was specially
filtered and all items which went into the crib
were sterilized. It was quickly proven that
his immune system was indeed defective, but there
was hope that his older sister would be a match
for a bone marrow transplant. Unfortunately,
his sister was not a good match and at that time
there were no donor registries. The rest of
the family was tested, but no one was a match for
David. Consequently, as he grew, so
did his bubbles. The media during that time
chronicled his life and he became known to the world
as the "Bubble Boy".
It wasn't until the early 80's that a technique
was developed to use a bone marrow donor who was
less than a 100% match. This method eventually
made it possible to use a haploidentical or 1/2
matched donor for a successful BMT, which has been
and remains the most significant treatment development
for this condition over the past two decades.
Gene Therapy - While it's been proven over
several generations now that bone marrow transplants
can save the lives of SCID children, transplants
do not always work or they do not always completely
correct the defects. The next step in looking
for a more successful therapy is gene therapy.
The first experiments in gene therapy on humans
began in 1990. Two girls with ADA deficiency
SCID were treated, several times, over a 2 year
period, with T-cells carrying corrected DNA.
Basically, the researchers corrected the DNA in
a sample of the girls' T-cells and then returned
the T-cells to them. The success of these
early trials is debated. Periodic tests on
both girls show that their re-engineered cells are
surviving and producing the ADA enzyme, but both
girls continue to receive replacement enzyme therapy.
While this trial did not produce a completely successful
correction of the girls' immune systems, it did,
however, prove that if you put a correct gene into
enough cells in a patient you can correct the disease.
In April of 2000, an article was published in Science
Magazine which presented 2 cases of X-linked SCID
which had been treated by gene therapy. These
children had no prior treatment such as bone marrow
transplantation. These 2 patients, at the
time period of 10 and 11 months after therapy, were
exhibiting normal growth and development without
other treatment. Their cells appeared to be
working. These results demonstrated a selective
advantage existed for the corrected cells to engraft
and produce a corrected cell line. In all,
10 XSCID patients were treated in this trial.
However, those studying and watching gene therapy
received devastating news in an article published
in Science Magazine in October 2003. Two of
the boys treated had developed a form of T-cell
proliferation similar to leukemia. The insertion
of the corrected DNA into the defective cells had
occurred next to a specific leukemia inhibitor.
With news of this devastating event, most XSCID
gene therapy trials were placed on hold worldwide.
Currently, new ADA and XSCID trails have begun or
are in the process. Obviously, caution is
warranted. However, gene therapy still holds
the greatest hope for a true cure for this devastating
disease. |
