W. Jean Dodds, DVM
posted in the files section of the K9Kitchen discussion group
with permission of the author
The Abstract
This article discusses the essential role of the immune system in
maintaining the body's overall general health and resistance to disease. The
focus will be on environmental factors or events which may cause or trigger
immune dysfunction leading to either immune deficiency or immune stimulation
(reactive or autoimmunity). Related to these events is the development of
cancer which is a disruption of cell growth control.
Overview of the Immune System
Immune competence is provided and maintained by two cellular systems which
involve lymphocytes. Lymphocytes are cells produced by the body's primary
(bone marrow and thymus) and secondary (lymph nodes and spleen) lymphatic
organs. They are descendants of the bone marrow's pool of stem cells, and
produce a circulating or humoral immune system derived from B-cells
(bursa-dependent or bone marrow derived), and a cellular or cell-mediated
immune system that derives from T-cells (thymus dependent).
B-Cell Immunity
B-cell immunity includes the circulating antibodies or immunoglobulins such
as IgG, IgM, IgA, IgD, and IgE. These antibodies provide an important
defense mechanism against disease in healthy individuals but can become
hyperactive or hypoactive in a variety of disease states. Hyperactive or
increased levels of immunoglobulins can occur in two ways: acutely, as a
reaction to disease or inflammatory insult ("acute phase" reaction); or
chronically, as in autoimmune or immune-mediated diseases, chronic
infections, and certain types of bone marrow and organ cancers. Hypoactive
or decreased levels of immunoglobulins can result from rare genetically
based immunodeficiency states such as agammaglobulinemia or
hypogammaglobulinemia, and from the immune suppression associated with
chronic viral, bacterial, or parasitic infection, cancers, aging,
malnutrition, drugs, toxins, pregnancy, lactation, and stress.
T-cell Immunity
T-cell, or cell-mediated immunity is the cellular mechanism whereby T-cells
act as coordinators and effectors of the immune system. Cell-mediated
immunity involves the lymph nodes, thymus, spleen, intestine (gut-associated
lymphoid tissue), tonsils, and a mucosal secretory immunity conveyed by IgA.
The major classes of T-cells are designated as helper, cytotoxic, and
suppressor cells. The helper cells "help" coordinate the immune response
whereas the cytotoxic cells comprise the effector network that participates
in removing virus-infected cells from the body. The third class of
suppressor T-cells is important in dampening the immune response when it
becomes overactive or out of regulatory control. Finally, cooperation
between the various T-cell classes and between T- and B-cells is an
important component of the normal humoral and cellular immune response.
Hyperactive cellular immune responses produce autoimmune and other
immune-mediated diseases while hypoactive cell-mediated immunity causes
immune suppression and incompetence. Classical examples of this latter
situation occur with retroviral infection such as human AIDS or the animal
equivalents (e.g. feline immunodeficiency virus, feline leukemia virus,
bovine leukemia virus, equine infectious anemia).
Introduction to Autoimmune Diseases
The term "autoimmunity" literally means immunity against self and is caused
by an immune-mediated reaction to self-antigens (i.e. failure of
self-tolerance). Susceptibility to autoimmune disease has a genetic basis in
humans and animals. Numerous viruses, bacteria, chemicals, toxins, and drugs
have been implicated as the triggering environmental agents in susceptible
individuals. This mechanism operates by a process of molecular mimicry
and/or non-specific inflammation. The resultant autoimmune diseases reflect
the sum of the genetic and environmental factors involved. Autoimmunity is
most often mediated by T-cells or their dysfunction. As stated in a recent
review, "perhaps the biggest challenge in the future will be the search for
the environmental events that trigger self-reactivity" (Sinha, Lopez and
McDevitt; Science, 248: 1380, 1990). Table 1 lists factors commonly
associated with autoimmune diseases.
The four main causative factors of autoimmune disease have been stated to
be: Genetic predisposition; Hormonal influences, especially of sex hormones;
Infections, especially of viruses; and Stress.
Immune-Suppressant Viruses
Immune-suppressant viruses of the retrovirus and parvovirus classes have
recently been implicated as causes of bone marrow failure, immune-mediated
blood diseases, hematologic malignancies (lymphoma and leukemia),
dysregulation of humoral and cell-mediated immunity, organ failure (liver,
kidney), and autoimmune endocrine disorders especially of the thyroid gland
(thyroiditis), adrenal gland (Addison's disease), and pancreas (diabetes).
Viral disease and recent vaccination with single or combination modified
live-virus vaccines, especially those containing distemper, adenovirus 1 or
2, and parvo virus are increasingly recognized contributors to
immune-mediated blood disease, bone marrow failure, and organ dysfunction.
Genetic predisposition to these disorders in humans has been linked to the
leucocyte antigen D-related gene locus of tile major histocompatibility
complex, and is likely to have parallel associations in domestic animals.
Drugs associated with aggravating immune and blood disorders include the
potentiated sulfonamides (trimethoprim-sulfa and ormetoprim-sulfa
antibiotics), the newer combination or monthly heartworm preventives, and
anticonvulsants, although any drug has the potential to cause side-effects
in susceptible individuals.
Immune Deficiency Diseases
Immune deficiency diseases sire a group of disorders in which normal host
defenses against disease are impaired. These include disruption of the
body's mechanical barriers to invasion (e.g. normal bacterial flora; the eye
and skin; respiratory tract cilia); defects in non-specific host defenses (e
.g. complement deficiency; functional white blood cell disorders), and
defects in specific host defenses (e.g. immunosuppression caused by
pathogenic bacteria, viruses and parasites; combined immune deficiency; IgA
deficiency; growth hormone deficiency).
Thyroid Disease and the Immune System
Thyroid dysfunction is the most frequently recognized endocrine disorder of
the dog. The most common form of canine thyroid disease is autoimmune
thyroiditis (equivalent to Hashimoto's disease of humans), which is a
familial autoimmune disease of inherited predisposition. As the thyroid
gland regulates metabolism of all body cellular functions, reduction of
thyroid function leading to hypothyroidism can produce a wide range of
clinical manifestations (Table 2). Because so many of the clinical signs of
thyroid dysfunction mimic symptoms resulting from other causes, it is
difficult to make an accurate diagnosis of thyroid-related illness without
appropriate veterinary laboratory tests combined with an experienced
professional interpretation of the test results. More specific details about
the accurate diagnosis of thyroid disease can be found in the literature
cited at the end of this article.
Genetic Screening for Thyroid Disease
Complete baseline thyroid panels and thyroid antibody tests can be used for
genetic screening of apparently healthy animals to evaluate their fitness
for breeding. Any dog having circulating antithyroid autoantibodies can
eventually develop clinical symptoms of thyroid disease or be susceptible to
other autoimmune diseases because their immune system is impaired.
Therefore, thyroid prescreening can he very important for selecting
potential breeding stock.
Thyroid testing for genetic screening purposes is unlikely to be meaningful before puberty. Screening is initiated, therefore, once healthy dogs and bitches have reached sexual maturity (between 10-14 months in males and during the first anestrous period for females following their maiden heat). Anestrus is a time when the female sexual cycle is quiescent thereby removing any influence of sex hormones on baseline thyroid function. This period generally begins 12 weeks from the onset of the previous heat and lasts 1 month or longer. The interpretation of results from baseline thyroid profiles in intact females is more reliable when they are tested in anestrus. Thus, testing for health screening is best performed at 12-16 weeks following the onset of the previous heat. Screening of intact females for other parameters like vWD, hip dysplasia, inherited eye disease, and wellness or reproductive checkups should also he scheduled in anestrus. Once the initial thyroid profiles are obtained, dogs and bitches should be rechecked on an annual basis to assess their thyroid and overall health. Annual results provide comparisons for early recognition of developing thyroid dysfunction. This permits treatment intervention, where indicated, to avoid the appearance or advancement of clinical signs associated with hypothyroidism. For optimal health, young dogs under 15-18 months of age should have thyroid baseline levels in the upper half of the adult normal ranges. This is because puppies and adolescent dogs require higher levels of thyroid hormones as they are still growing and maturing. Similarly, older animals beyond 8 or 9 years of age have slower metabolisms and so baseline thyroid levels of normal (euthyroid) dogs may be slightly below midrange. For optimum thyroid function of breeding stock, levels should be close to the midpoint of the laboratory normal ranges, because lower levels may be indicative of the tarry stages of thyroiditis among relatives of dog families previously documented to have thyroid disease. The difficulty in accurately diagnosing early thyroid disease is compounded by the fact that some patients with typical clinical signs of hypothyroidism have circulating thyroid levels within the normal range. A significant number of these patients will improve clinically when given thyroid medication. In such cases, blood levels of the hormones can be normal but tissue levels are inadequate to maintain health, and so, the patient shows clinical signs of hypothyroidism. This situation pertains in selenium deficiency (discussed below). While animals in this category should respond well to thyroid medication, only experienced clinicians are likely to recognize the need to place these dogs on a 6-8 week clinical trial of thyroid supplementation. This approach is safe and clinically appropriate, but it requires rechecking blood levels of thyroid hormones towards the end of the 6-8 week period to assure that the patient is receiving the correct dose of medication.
Other Factors Influencing Thyroid Metabolism
Because animals with autoimmune thyroid disease have generalized metabolic
imbalance and often have associated immunological dysfunction, it is
advisable to minimize their exposures to unnecessary drugs, toxins, and
chemicals, and to optimize their nutritional status with healthy balanced
diets. Wholesome nutrition is a key component of maintaining a healthy
immune system. In our experience, families of dogs susceptible to thyroid
and other autoimmune diseases show generalized improvement in health and
vigor when fed premium cereal-based diets preserved naturally with vitamins
E and C (without the addition of chemical antioxidant preservatives such as
BHA, BHT, or ethoxyquin). Fresh home-cooked vegetables with herbs, low fat
dairy products, and meats such as lamb, chicken, and turkey can he added as
supplements. Challenging the immune system of animals susceptible to these
disorders with polyvalent modified-live vaccines has been associated with
adverse effects in some cases (see below). Table 1 lists other agents that
should be avoided in susceptible or affected animals.
Nutritional influences can have a profound effect on thyroid metabolism. For
example, iodine deficiency in areas where cereal grain crops are grown on
iodine-deficient soil will impair thyroid metabolism because this mineral is
essential for formation of thyroid hormones. Recently an important link has
been shown between selenium deficiency and hypothyroidism. Again, cereal
grain crops grown on selenium-deficient soil will contain relatively low
levels of selenium. While commercial pet food manufacturers compensate for
variations in basal ingredients by adding vitamin and mineral supplements,
it is difficult to determine optimum levels for so many different breeds of
dogs having varying genetic backgrounds and metabolic needs. The
selenium-thyroid connection has significant clinical relevance, because
blood levels of total and free T4 rise with selenium deficiency. However,
this effect does not get transmitted to the tissues as evidenced by the fact
that blood levels of the regulatory thyroid stimulating hormone (TSH) are
also elevated or unchanged. Thus, selenium-deficient individuals showing
clinical signs of hypothyroidism could be overlooked on the basis that blood
levels of T4 hormones appeared normal. The selenium issue is further
complicated because chemical antioxidants can impair the bioavailability of
vitamin A, vitamin E and selenium and alter cellular metabolism by inducing
or lowering cytochrome p-450, glutathione peroxidase (a selenium-dependent
enzyme), and prostaglandin levels. As manufacturers of many premium pet
foods began adding the synthetic antioxidant, ethoxyquin, in the late
1980's, its effects along with those of other chemical preservatives (BHA.
BHT), are surely detrimental over the long term. The way to avoid this
problem is to use foods preserved with natural antioxidants such as vitamin
E and vitamin C.
Immunological Effects of Vaccines
Combining viral antigens, especially those of modified live virus (MLV) type
which multiply in the host, elicits a stronger antigenic challenge to the
animal. This is often viewed as desirable because a more potent immunogen
presumably mounts a more effective and sustained immune response. However,
it can also overwhelm the immunocompromised or even a healthy host that is
continually bombarded with other environmental stimuli and has a genetic
predisposition that promotes adverse response to viral challenge. This
scenario may have a significant effect on the recently weaned young puppy
that is placed in a new environment. Furthermore, while the frequency of
vaccinations is usually spaced 2-3 weeks span, some veterinarians have
advocated vaccination once a week in stressful situations. To me, this
practice makes no sense from a scientific or medical perspective. While
young puppies exposed this frequently to vaccine antigens may not
demonstrate overt adverse effects, their relatively immature immune systems
may he temporarily or more permanently harmed from such antigenic
challenges. Consequences in later life may be the increased susceptibility
to chronic debilitating diseases. Some veterinarians trace the increasing
current problems with allergic and immunological diseases to the
introduction of MLV vaccines some 20 years ago. While other environmental
factors no doubt have a contributing role, the introduction of these vaccine
antigens and their environmental shedding may provide the final insult that
exceeds the immunological tolerance threshold of some individuals in the pet
population.
Vaccine Dosage
Manufacturers of MLV combination vaccines recommend using the same dose for
animals of all ages and different sizes. It has never made any sense to
vaccinate toy and giant breed puppies (to choose two extremes) with the same
vaccine dosage. While these products provide sufficient excess of antigen
for the average sized animal, it is likely to be either too much for the toy
breeds or too little for the giant breeds. In addition, combining certain
specific viral antigens such as distemper with adenovirus 2 (hepatitis) has
been shown to influence the immune system by reducing lymphocyte numbers and
responsiveness.
Hormonal State During Vaccination
Relatively little attention has been paid to the hormonal status of the
patient at the time of vaccination. While veterinarians and vaccine
manufacturers are aware of the general rule not to vaccinate animals during
any period of illness, the same principle should apply to times of
physiological hormonal change. This is particularly important because of the
known role of hormonal change alone with infectious agents in triggering
autoimmune disease. Therefore, vaccinating animals at the beginning of,
during, or immediately after an estrous cycle is unwise, as would he
vaccinating animals during pregnancy or lactation. In this latter situation,
adverse effects can accrue not only to the dam but also because a newborn
litter is exposed to shed vaccine virus. One can even question the wisdom of
using MLV vaccines on adult animals in the same household because of
exposure of the mother and her litter to shed virus. Recent studies with MLV
heroes virus vaccines in cattle have shown them to induce necrotic changes
in the ovaries of heifers that were vaccinated during estrus. The vaccine
strain of this virus was also isolated from control heifers that apparently
became infected by sharing the same pasture with the vaccinates.
Furthermore, vaccine strains of these viral agents are known to be causes of
abortion and infertility following herd vaccination programs. If one
extrapolates these findings from cattle to the dog, the implications are
obvious.
Killed Versus Modified Live Vaccines
Most single and combination canine vaccines available today are of MLV
origin. This is based primarily on economic reasons and the belief that they
produce more sustained protection. A long-standing question remains,
however, concerning the comparative safety and efficacy of MLV versus killed
(inactivated) virus vaccines. A recent examination of the risks posed by MLV
vaccines concluded that they are intrinsically more hazardous than
inactivated products. The residual virulence and environmental contamination
resulting from the shedding of vaccine virus is a serious concern. More
importantly, the ability of new infective agents to develop and spread poses
a threat to both wild and domestic animal populations. The controversy in
weighing the risks and benefits of MLV versus killed vaccines is building.
Vaccine manufacturers seek to achieve minimal virulence (infectivity) while
retaining maximal immunogenicity (protection). This desired balance may he
relatively easy to achieve in clinically normal, healthy animals but may be
problematic for those with even minor immunologic deficit. The stress
associated with weaning, transportation, surgery, subclinical illness, and a
new home can also compromise immune function. Furthermore, the common viral
infections of dogs cause significant immunosuppression. Dogs harboring
latent viral infections may not be able to withstand the additional
immunological challenge induced by MLV vaccines. The increase in
vaccine-associated distemper and parvovirus diseases are but two examples of
this potential. So -- why are we causing disease by weakening the immune
system with frequent use of combination vaccine products? After all vaccines
are intended to protect against disease. It is well-recognized by experts in
the field that a properly constituted killed vaccine is always preferable to
one of MLV origin. Killed vaccines do not replicate in the vaccinated
animal, do not carry the risk of residual virulence and do not shed
attenuated viruses into the environment. On the other hand, MLV vaccines are
capable of stimulating a more sustained protective response. So what does
the future hold here? Veterinarians, scientists, breeders and owners need to
voice their concern and discontent with the present industrial vaccine
practices. We need to urge manufacturers to seek alternatives. Even if
killed vaccines are proven to be somewhat less efficacious (produce lower
levels or less sustained protection) than MLV products, they are more safe.
All killed vaccines on the market today have passed current efficacy and
safety standards in order to be licensed for use by the USDA. The issue is
to what extent being more effective elicits a benefit rather than a risk.
The future will evolve new approaches to vaccination including sub-unit
vaccines, recombinant vaccines using DNA technology, and killed products
with new adjuvants to boost and prolong protection. These are not simple
solutions to a problem, however, because early data from recombinant
vaccines against some human and mouse viruses have shown potentially
dangerous side-effects by damaging T-lymphocytes. Contributing factors were
shown to be the genetic background of the host, the time or dose of
infection, and the makeup of the vaccine. We are obviously still a long way
from producing a new generation of improved and safe vaccines. In the
meantime, we need to return to using killed products whenever they are
available and should consider giving them more often (twice yearly rather
than annually) for high-risk exposure situations. Vaccines, while necessary
and generally safe and efficacious, can be harmful or ineffective in
selected situations.
Cancer and Immunity
Proper regulation of cellular activity and metabolism is essential to normal
body function. Cell division is a process under tight regulatory control.
The essential difference between normal and tumor or cancerous cells is a
loss of growth control over the process of cell division. This can result
from various stimuli such as exposure to certain chemicals, viral infection,
and mutations, which cause cells to escape from the constraints that
normally regulate cell division. Proliferation of a cell or group of cells
in an uncontrolled fashion eventually gives rise to a growing tumor or
neoplasm. Of course, tumors can he both benign (a localized mass that does
not spread) or malignant (cancerous), in which the tumor grows and
metastasizes to many different sites via the blood or lymph.
Tumor cells also express a variety of proteins called "neoantigens" on their
surface, and many of these are different from antigens found on normal
cells. These new or altered proteins are recognized as foreign by the immune
system, and so trigger an immunological attack. There are a large number of
them known as tumor-specific or tissue-specific antigens, whereas others
recognize the blood group systems, histocompatibility complex, and viruses.
The situation in cancer is complex because not only can immunologically
compromised individuals become more susceptible to the effects of
cancer-producing viral agents and other chemical carcinogens, the cancer
itself can be profoundly immunosuppressive. The form of immunosuppression
usually varies with the tumor type. For example, lymphoid tumors (lymphomas
and leukemia) tend to suppress antibody formation, whereas tumors of T-cell
origin generally suppress cell-mediated immunity. In chemically induced
tumors, immunosuppression is usually due to factors released from the tumor
cells or associated tissues. The presence of actively growing tumor cells
presents a severe protein drain on an individual which may also impair the
immune response. Blocking factors present in the serum of affected animals
exist which can cause enhancement of tumor growth. Additionally,
immunosupression in tumor-bearing animals can be due to the development of
suppressor cells.
The body also contains a group of complimentary factors that provide a
protective effect against tumors and other immunologic or inflammatory
stresses. These are mixtures of proteins produced by T-cells and are
referred to as "cytokines." Cytokines include the interleukins, interferons,
tumor-necrosis factors, and lymphocyte-derived growth factors. Recent
studies have shown that normal levels of zinc are important to protect the
body against the damaging effects of the specific cytokine, tumor-necrosis
factor (TNF). Inadequate levels of zinc have been shown to promote the
effect of TNF in disrupting the normal endothelial barrier of blood vessels.
This could have a significant effect in promoting the metastasis of tumor
cells to different sites, thereby hastening the spread and growth of a
particular cancer.
Currently shout 15% of human tumors are known to have viral causes or
enhancement. Viruses also cause a number of tumors in animals and no doubt
the number of viruses involved will increase as techniques to isolate them
improve. The T-cell leukemias of humans and animals are examples of those
associated with retroviral infections. This same class of viruses has been
associated with the production of autoimmunity and immunodeficiency
diseases. The recent isolation of a retrovirus from a German Shepherd with
T-cell leukemia exemplifies the potential role of these agents in producing
leukemia and lymphomas in the dog.
The increased prevalence of leukemia and lymphomas in the Golden Retriever
and several other breeds is a case in point. Similarly, there has been an
increase in the prevalence of hemangiosarcomas (malignant tumors of the
vascular endothelium) primarily in the spleen, but also in the heart, liver
and skin. They occur most often in middle age or older dogs of medium to
large breeds. The German Shepherd dog is the breed at highest risk, but
other breeds including the Golden Retriever and Vizsla have shown a
significantly increased incidence especially in certain families. This
suggests that genetic and environmental factors play a role. It is tempting
to speculate that environmental factors that promote immune suppression or
dysregulation contribute to failure of immune surveillance mechanisms. These
protect the body against the infectious and environmental agents which
induce carcinogenesis and neoplastic change.
Nutritional Factors and the Immune System
As alluded to above, an adequate nutritional state is important in managing
a variety of inherited and other metabolic diseases as well as for a healthy
immune system. Examples where nutritional management is important in
inherited disorders includes: adding ingredients to the diet to make it more
alkaline for Miniature Schnauzers with calcium oxalate bladder or kidney
stones; use of the vitamin A derivative. etretinate in Cocker Spaniels and
other breeds with idiopathic seborrhea of the skin; management with drugs
and diet of diseases such as diabetes mellitus and the copper-storage
disease prevalent in breeds like the Bedlington Terrier, West Highland White
Terrier, and Doberman Pinscher; and treatment of vitamin B-12 deficiency in
Giant Schnauzers. Other nutritional influences include the vitamin
K-dependent coagulation defect elicited in Devon Rex cats following
vaccination; hip dysplasia in puppies fed excessive calories;
osteochondritis dissecans in dogs fed high levels of calcium; and
hypercholesterolemia in inbred sled dogs fed high fat diets.
Nutritional factors that play an important role in immune function include
zinc, selenium and vitamin E, vitamin B-6 (pyridoxine),and linoleic acid.
Deficiencies of these compounds impairs both circulating (humoral) as well
as cell-mediated immunity. The requirement for essential nutrients increases
during periods of rapid growth or reproduction and also may increase in
geriatric individuals, because immune function and the bioavailability of
these nutrients generally wanes with aging. As with any nutrient, however,
excessive supplementation can lead to significant clinical problems, many of
which are similar to the respective deficiency states of these ingredients.
Supplementation with vitamins and minerals should only be given with the
advice of a professional nutritionist and should not be viewed as a
substitute for feeding premium quality fresh and/or commercial dog foods.
BIBLIOGRAPHY
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