WORLD OF MICROBIOLOGY AND IMMUNOLOGY Severe combined immunodeficiency (SCID)509•
basis of serology is the recognition of an antigenby immune
mechanisms, with the subsequent production of an antibody.
In medical terminology, serology refers to a blood test
to detect the presence of antibodies against a microorganism.
The detection of antibodies can be qualitative (i.e., determin-
ing whether the antibodies are present) or quantitative (i.e.,
determining the quantity of an antibody produced). Some
microorganismscan stimulate the production of antibodies
that persist in a person’s blood for a long time. Thus, in a qual-
itative assay the detection of a particular antibody does not
mean that the person has a current infection. However, it does
mean that it is likely that at some time that person was infected
with the particular microbial pathogen. Serology assays can be
performed at various times and the level of antibody deter-
mined. If the antibody level rises, it usually is indicative of a
response to an infection. The body produces elevated amounts
of the antibody to help fight the challenging antigen.
Serology as a science began in 1901. Austrian American
immunologist Karl Landsteiner(1868–1943) identified groups
of red blood cells as A, B, and O. From that discovery came
the recognition that cells of all types, including blood cells,
cells of the body, and microorganisms carry proteins and other
molecules on their surface that are recognized by cells of the
immune system. There can be many different antigens on the
surface of a microorganism, with many different antibodies
being produced.
When the antigen and the antibody are in suspension
together, they react together. The reaction can be a visible one,
such as the formation of a precipitate made up of a complex of
the antigen and the antibody. Other serology techniques are
agglutination, complement-fixation and the detection of an
antigen by the use of antibodies that have been complexed
with a fluorescent compound.
Serological techniques are used in basic research, for
example, to decipher the response of immune systems and to
detect the presence of a specific target molecule. In the clini-
cal setting, serology is used to confirm infections and to type
the blood from a patient. Serology has also proven to be very
useful in the area of forensics, where blood typing can be vital
to establishing the guilt or innocence of a suspect, or the iden-
tity of a victim.See alsoAntibody and antigen; Antibody formation and kinet-
ics; Antibody-antigen, biochemical and molecular reactions;
Bacteria and bacterial infection; Immune system; Laboratory
techniques in immunologySESSILE BACTERIA•seeBIOFILM FORMATION AND
DYNAMIC BEHAVIORSEVERE COMBINED IMMUNODEFICIENCY
(SCID)Severe combined immunodeficiency (SCID)
Severe combined immunodeficiency(SCID) is a rare genetic
disease that is actually a group of inherited disorders charac-terized by a lack of immune response, usually occurring in
infants less than six months old. SCID is the result of a com-
bination of defects of both T-lymphocytesand B-lymphocytes.
Lymphocytes are white blood cells that are made in bone mar-
row, and many move to the thymus gland where they become
specialized immune T and B cells. In healthy individuals, T
cellsattack antigens while B cells make plasma cells that pro-
duce antibodies (immunoglobulins). However, this immune
response in SCID patients is absent making them very suscep-
tible to invading diseases, and thus children with untreated
SCID rarely live to the age of two years.
SCID is characterized by three main features. The
helper T-lymphocytes are functioning poorly or are absent, the
thymus gland may be small and functioning poorly or is
absent, and the stem cells in bone marrow, from which mature
T- and B-lymphocytes arise, are absent or defective in their
function. In all of these situations, little or no antibodies are
produced. If, for example, T-lymphocytes are never fully
developed, then the immune systemcan never function nor-
mally. Moreover, the results of these defects include the fol-
lowing: impairment of normal functioning T- and
B-lymphocytes, negative effects on the maturation process for
T-helper and T-suppressor cells, and elimination and damage
of the original source of the lymphocytes.
The immune disorders characterized in SCID arise
because of the inheritance of abnormal genes from one or both
parents. The most common form of SCID is linked to the X
chromosome inherited from the mother; this makes SCID more
common among males. The second most common defect is
caused by the inheritance of both parents’ abnormally inactive
genes governing the production of a particular enzyme that is
needed for the development of immunity, called adenosine
deaminase (ADA). Although many defective genes for other
forms of SCID have been identified in the last few years, sci-
entists do not fully understand all of the forms of the disease.
There are many specific clinical signs that are associ-
ated with SCID. After birth, an infant with SCID is initially
protected by the temporarily active maternal immune cells;
however, as the child ages, his or her immune system fails to
take over as the maternal cells become inactive. Pulmonary
problems such as pneumonia, non-productive coughs, inflam-
mationaround the bronchial tubes, and low alveolar oxygen
levels can affect the diseased infant repetitively. Chronic diar-
rhea is not uncommon, and can lead to severe weight loss,
malnutrition, and other gastrointestinal problem. Infants with
the disease have an unusual number of bacterial, fungal, viral,
or protozoal infections that are much more resistant to treat-
ment than in healthy children. Mouth thrushand yeastinfec-
tions, both fungal, appear in SCID patients and are very
resistant to treatment. Additionally, chronic bacterial and fun-
gal skin infectionsand several abnormalities of the blood cells
can persist.
Severe combined immunodeficiency is a disease that
can be successfully treated if it is identified early. The most
effective treatment has been hematopoietic stem cell trans-
plants that are best done with the bone marrow of a sister or
brother; however, the parent’s marrow is acceptable if the
infant is less than three months old. Early treatment can alsowomi_S 5/7/03 8:20 AM Page 509