Abstract
Background
Toxoplasmosis is caused by the Toxoplasma gondii parasite. The parasite is intracellular and can result in severe complications leading to death in immuno-deficient patients in particular. Diabetes is an important factor that increases susceptibility and risk of various infections in the host.
Objectives
The present study focused on the serologic detection of Toxoplasma gondii infection in diabetic patients.
Materials and Methods
Through a case-control study, overall 184 serum samples including 91 from diabetic cases and 93 from healthy non-diabetic controls were investigated. Cases and controls were matched for age and gender. Serum samples were tested for sugar by an enzymatic method, and IgG antibodies were tested against Toxoplasma gondii by ELISA method.
Results
The prevalence of IgG antibodies against Toxoplasma gondii in diabetic patients and healthy controls were 60.43% and 38% respectively. Risk of toxoplasmosis infection in diabetic patients with was two folds higher than healthy controls (RR = 2.21, 95% CI; 1.6 – 3.7, P = 0.001).
Conclusions
Diabetes may be caused by Toxoplasma gondii. Presence of T. gondii in the pancreas at the same time could directly undermines the pancreas cells. When β cells are destroyed, insulin secretion would then be affected. Probably the destruction of T. gondii affects nervous system and damages pancreatic cells leading to increased risk of diabetes.
Keywords: Diabetes, Infection, Serum, Toxoplasma gondii
1. Background
Toxoplasmosis is a disease caused by the protozoan parasite Toxoplasma gondii. Up to one third of the world's human population is estimated to be carrying a Toxoplasma infection and the life cycle of this parasite plays a huge role in its easy transmission (1). Only a minority develop serious clinical disease, such as congenital or cerebral toxoplasmosis is associated with an immature and a deficient immunity. So the parasite can be considered as the major cause of central nervous system infections in patients with congenital toxoplasmosis and AIDS (2, 3). The important role played by CD8 T cells in control of Toxoplasma gondii infection (4). Immune protection against many intracellular pathogens including viruses, bacteria and protozoa is provided by robust CD8 T-cell responses. Naïve CD8 T cells are found in lymphoid tissues where, after infection, they encounter an antigen-presenting cell (APC) (5). The APC presents pathogen-derived antigens and provides the appropriate signals to T cells to cause their activation. This activation leads to the proliferation, differentiation, and acquisition of effectors functions of the antigen-specific CD8 T cell. Activated antigen-specific CD8 T-cell effectors functions include secretion of cytokines IFNγ and TNFα and cytotoxicity, which promote further development of adaptive immunity and control pathogens (6-8).
Effects of Toxoplasma gondii on central nervous system has been defined by multiple foci of enlarging necrosis and microglial nodules (9).The immune-histo-chemical studies have investigated the distribution of lesions in verity of animal tissues that are experimentally inoculated with T. gondii (10, 11). During acute phase of toxoplasmosis, tissue necrosis may be found in various organs including lung, liver, spleen, heart and pancreas (12). In the chronic infection, necrosis always often found in brain and eye. Immuno-histo-chemical techniques have already been used to investigate the distribution of lesions and protozoa in young piglets that were experimentally inoculated with T. gondii. According to WHO; diabetes is a chronic disease that occurs when the pancreas does not produce enough insulin, or when the body cannot effectively use the insulin it produces Hyperglycaemia, or raised blood sugar, is a common effect of uncontrolled diabetes and over time leads to serious damage to many of the body's systems, especially the nerves and blood vessels (13).
Diabetes increases the host’s sensitivity and risk of susceptibility to various infections (14). Based on statistics, the number of people diagnosed with diabetes was in excess of 2.5 million within the age range of 25 to 64 in 2007 (15). It is predicted that 366 million would suffer from diabetes around the world in 2030 (16). The present study shows correlation diabetes and toxoplasmosis. Currently, the levels of IgG and IgM antibodies in serum can easily be measured using available techniques (17). Serologic methods are techniques used to measure the level of infection to Toxoplasmasis in humans and animals. Amongst these methods, the most common techniques are ELISA and IFA or indirect immuno-florescence (18).
2. Objectives
The present study aimed to investigate the effects of Toxoplamasis on uncontrolled diabetes and on the level of outbreak of infection in patients, depending on age, with differing immune systems and dietary habits. Hence, the level of IgG antibody against Toxoplasma gondii in the serum of diabetic patients is measured.
3. Materials and Methods
Through a case-control study, overall 184 serum samples including 91 from diabetic patients and the remaining 93 from healthy non-diabetic controls were investigated. Cases and controls were matched for age and gender. Once sampling was performed, the level of glucose (FBS) was read employing an enzymatic method. In this method, 10 landa serum and 1ml of designated solution was mixed and left for 10 minutes at 37 °C Benmary to be incubated. Then the results were read using Spectrophotometer at wavelength 545nm. Serums were then kept at -20 °C for ELISA testing. Finally, the level of IgG antibody against Toxoplasma gondii was measured using the ELISA method and an IgG Toxoplasma Gondii kit provided by the Pishtaz Teb Zaman Co. with 100% sensitivity and 99% specificity. The proposal of the present study was approved by the Baghiyatallah University Ethical Committee.
4. Results
The abundance distribution for 184 studied samples is demonstrated in Table 1. A positive IgG Toxoplasmosis was observed in 60.43% and 38.7% of diabetic cases and health controls respectively (Table 1). Overall, 54.54% and 45.46% of the diabetic categories were females and males respectively.
Table 1. Abundance Distribution of Toxoplasmosis Cases .
| Category | No | + Toxoplasmosis, No. (%) |
|---|---|---|
| Diabetic Cases | 91 | 55 (60.43) |
| Healthy Controls | 93 | 36 (38.7) |
| Total | 184 | 91 (49.6) |
It is found that 24 patients of the diabetic category had glucose levels of 200 – 300 mg/dl which is perceived to be more abundant than the other 2 glucose levels, i.e. 140 – 200 and 300 – 400 mg/dl (Table 2).
Table 2. Glucose Level (FBS) and Toxoplasmosis Infection .
| Glucose levels (Mg/dl) | + Toxoplasmosis, No. (%) |
|---|---|
| 140-200 | 18 (32.7) |
| 200-300 | 24 (43.6) |
| 300-400 | 13 (23.6) |
| Total | 55 (100) |
Risk of toxoplasmosis infection in diabetic patients with was 2 folds higher than healthy controls (RR = 2.21, 95 CI; 1.6 – 3.7, P = 0.001) (Table 3).
Table 3. Proportional Distribution of Toxoplasmosis between Diabetic and Non-Diabetic People .
| Toxoplasmosis | Diabetic Cases, No. | Non-diabetic Controls, No. |
|---|---|---|
| Positive | 55 | 38 |
| Negative | 36 | 55 |
| Total | 91 | 93 |
| Risk estimation | (RR = 2.21, 95 CI; 1.6 – 3.7, P = 0.001) | |
5. Discussions
This investigation was carried out with a density of more than 1.20 (units). Overall, 60.43% of diabetic patients and only 38.7% of non-diabetic controls were positive for the Toxoplasmosis gondii antibody. Therefore, these findings suggest that Toxoplasmosis patients are more susceptible to be diabetics than those without. Destruction of the pancreas occurs in three phases of Toxoplasma gondii:
1. Hyperactive phase (hyper-period) in which β-cell destruction of nerve cells and less interference in the insect in a hyperactive state of the pancreas, insulin secretion is sometimes excessive, often resulting in low blood sugar, or a too low blood sugar, this stage is often during adolescence.
2. Disordered phase (compensatory phase), in which neurons and pancreatic β-cells have a considerable amount of damage, under normal circumstances, secretion of insulin will be inadequate, the body will start the compensatory function. Thus, this phase of insulin secretion over time, when few in the disordered state.
3. Decline phase (recession), in which nerve cells and β-cells destruction of more compensatory function reached its limits (19).
A recent experimental study has described that pancreatitis due to Toxoplasmosis in cats. Toxoplasma Gondii & Amphimerus Pseudofelineus are microbial agents associated with the disease (20). A stimulative effect of insulin on Toxoplasma gondii replication in cells (in vitro) has recently been reported. The number of tachyzoites increased rapidly, with insulin concentrations of between 10–2 and 10–1 μg/ml (21). Several studies have reported diabetes insipitus in particular (22-24), and other diseases such as Alzheimer (25) in patient with congenital toxoplasmosis. The tissue necrosis in pancreas during acute toxoplasmosis has also been reported (26).
The present study is limited by confounding factors associated with diabetes mellitus. We have been trying to reduce confounders by epidemiological approaches such as individual matching and by setting inclusion and exclusion criteria according to latest definitions of diabetes by the World Health Organization. Thus, Toxoplasmosis has also been implicated as a possible contributing factor in chronic pancreatitis also the inadequacy of insulin secretion, sustained blood and increased urine sugar. By further destruction of Toxoplasma gondii series of complications such as blindness, diabetic foot, coronary heart disease, and hypertension are expected.
Acknowledgments
The authors express their deep gratitude to Mr. Behrooz Hajian Tehrani (the president of Pishtaz Teb Co.), Dr. Butorabi and Mr. Mustafa Sarbandi for their technical supports throughout the present research.
Footnotes
Implication for health policy/practice/research/medical education:
Destruction of the pancreas may be occurs in toxoplasmosis infection. Thus Toxoplasmosis has also been implicated as a possible contributing factor in chronic pancreatitis also the inadequacy of insulin secretion, sustained blood and increased urine sugar.
Authors’ Contribution:
None declared.
Financial Disclosure:
There is no financial disclosure.
Funding/Support:
There is no funding or support.
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