PROSTAGLANDINS, and other biochemical messengers
determine histamine release and what histamine
binding will occur. Each histamine receptor regu-
lates a different response:
- H1 receptors are on cell membrane surfaces of
arteriole and capillary cells. H1 binding causes
the arterioles to dilate (open) and the capillar-
ies to increase the permeability of their walls.
The effect of these actions is to allow additional
fluid to seep from these blood vessels into the
interstitial spaces (spaces between cells). The
fluid floods the cells with INFECTION-fighting
molecules, notably antibodies and cytokines.
IMMUNOGLOBULIN E (IgE) binds with antigens
and allergens, triggering H1 release. H1 is pri-
marily responsible for type I hypersensitivity
reactions such as ALLERGIC RHINITISand ALLERGIC
ASTHMA. Common antihistamine medications
that block H1 receptor binding include diphen-
hydramine, chlorpheniramine, and hydrox-
yzine. - H2 receptors are in parietal cells of the
STOMACH. H2 binding acts to increase the flow of
gastric acid in the stomach. Excessive secretion
of histamine binding with H2 receptors is pri-
marily responsible for GASTROESOPHAGEAL REFLUX
DISORDER(GERD). Medications to limit histamine
secretion and H2 receptor binding include H2
ANTAGONIST(BLOCKER) MEDICATIONSsuch as cime-
tidine and ranitidine. - H3 receptors are neuroreceptors in the CENTRAL
NERVOUS SYSTEMwith high concentration in the
areas of the HYPOTHALAMUSthat regulate alert-
ness. H3 binding decreases NEURON(NERVEcell)
secretion of histamine, serotonin, acetylcholine,
EPINEPHRINE, and NOREPINEPHRINE. The effect is to
reduce alertness, which takes place as a natural
aspect of the circadian cycle (body’s rhythm of
sleep and wakefulness). These neurotransmit-
ters also affect the NAUSEAcenter. The antihista-
mine medications doxylamine and hydroxyzine
are highly effective H3 receptor blockers.
Doctors typically consider only H1 receptor
binding in the context of the immune response
and focus primarily on whether its actions to initi-
ate INFLAMMATIONare helpful or counterproductive.
See also ALLERGEN; ANTIBODY; ANTIGEN; LEUKOCYTE;
LEUKOTRIENES; MAST CELL; NEURORECEPTOR; NEURO-
TRANSMITTER; PROTON PUMP INHIBITOR(PPI) MEDICA-
TIONS.human leukocyte antigens (HLAs) Unique pro-
teins (antigens) present on every nucleated cell
(cell that has a nucleus) in the body. Also called
histocompatibility locus antigens, HLAs allow the
IMMUNE SYSTEMto identify cells as self (belonging to
the body). Genes on CHROMOSOME6, in a region
called the MAJOR HISTOCOMPATIBILITY COMPLEX(MHC),
regulate HLAs. Each person has unique HLAs. The
nomenclature (naming convention) for HLAs
identifies the ALLELEand GENElocus (position on
the chromosome), designating the former with a
letter and the latter with a number.
HLAs have various immune roles, including
identification of self and nonself cells. This func-
tion makes HLAs of crucial importance in ORGAN
TRANSPLANTATION. Incompatibility in HLAs can
result in GRAFT VS. HOST DISEASEand rejection of the
transplanted organ. IMMUNOSUPPRESSIVE THERAPYto
subdue the IMMUNE RESPONSEin people who have
organ transplants in part targets HLAs. Some
research suggests that HLAs also may play crucial
roles in the development of AUTOIMMUNE DISORDERS
such as SYSTEMIC LUPUS ERYTHEMATOSUS(SLE), MULTI-
PLE SCLEROSIS, and SJÖGREN’S SYNDROME.
Though there are nearly endless configurations
of HLAs, there are three broad groups of HLAs:
HLA-A, HLA-B, and HLA-DR. Each set of three is
called a haplotype. Every person has two specific
HLAs from each of the three groups, for a total of
two haplotypes (six HLAs). Each parent passes one
haplotype to each child. Tissue matching for organ
transplantation compares the donor’s six HLAs
with the recipient’s six HLAs. The more that
match, the more likely the organ transplant will
be successful. The fewer that match, the greater
the risk that the recipient’s immune system will
attack the donor organ.
The other key factor in HLA matching is
immune reactivity (ANTIBODYreaction). It is possi-
ble to develop antibodies to HLAs that, even with
a match, make it almost certain that the recipient
will reject the organ. The most common cause for
HLA antibodies is exposure to nonself HLA as a
result of BLOOD TRANSFUSION. HLA matching is not ahuman leukocyte antigens (HLAs) 267