Level of Organochlorine Pesticide in Prediabetic and Newly Diagnosed Diabetes Mellitus Patients with Varying Degree of Glucose Intolerance and Insulin Resistance among North Indian Population

Article information

Diabetes Metab J. 2021;45(4):558-568
Publication date (electronic) : 2021 January 15
doi : https://doi.org/10.4093/dmj.2020.0093
1Department of Environmental Studies, University of Delhi (North Campus), Delhi, India
2Department of Endocrinology, University College of Medical Sciences, University of Delhi, Delhi, India
3Environmental Biochemistry and Molecular Biology Laboratory, Department of Biochemistry, University College of Medical Sciences, University of Delhi, Delhi, India
Corresponding author: Basu Dev Banerjee https://orcid.org/0000-0002-8348-3989 Environmental Biochemistry and Molecular Biology Laboratory, Department of Biochemistry, University College of Medical Sciences, University of Delhi, Dilshad Garden, Delhi 110095, India E mail: banerjeebd@hotmail.com
Received 2020 April 13; Accepted 2020 October 18.

Abstract

Background

Organochlorine pesticides (OCPs) exposure may induce an endocrine disruption which may lead to the risk of developing diabetes through alteration and disturbance of glucose metabolism, insulin resistance, and destruction of β-cells. The present study determines the recent trend of OCPs residue in blood samples and their association with the known risk factors responsible for developing the risk of diabetes among the North Indian population.

Methods

Blood sample of 300 patients (100 each of normal glucose tolerance [NGT], prediabetes and newly detected diabetes mellitus [DM]) between the age group of 30 to 70 years were collected. OCPs residue in whole blood samples was analyzed by using gas chromatography equipped with a 63Ni selective electron capture detector.

Results

Significantly higher levels of β-hexachlorocyclohexane (HCH), dieldrin, and p,p’-dichloro-diphenyl-dichloroethylene (DDE) were found in the prediabetes and newly detected DM groups as compared to NGT group. Insulin resistance showed to be significantly positive correlation with β-HCH and dieldrin. Also, fasting and postprandial glucose levels were significantly positively correlated with levels of β-HCH, dieldrin, and p,p’-DDE. Further, when OCPs level was adjusted for age and body mass index (BMI), it was found that β-HCH, dieldrin, and p,p’-DDE levels in blood increases the risk of diabetes by 2.70, 2.83, and 2.55 times respectively. Moreover, when we adjust OCPs level based on BMI categories (BMI <23, ≥23, and ≤25, and >25 kg/m2); β-HCH and p,p’-DDE showed a significant risk of developing newly detected DM with BMI >25 and ≥23 and ≤25 kg/m2.

Conclusion

The OCPs level present in the environment may be responsible for biological, metabolic, and endocrine disruptions within the human body which may increase the risk of developing newly detected DM. Hence, OCPs exposure can play a crucial role in the etiology of diabetes.

INTRODUCTION

Persistent organic pollutants (POPs) are characterized by their unique properties such as persistence lipophilicity, toxic effects, bioaccumulation, and long-drawn-out transport in the environment. POPs include organochlorine pesticides (OCPs) group such as aldrin, dieldrin, α-endosulfan, β-endosulfan, hexachlorocyclohexane (HCH) and its isomers, p,p’-dichlorodiphenyl-dichloroethylene (DDE), p,p’-dichloro-diphenyl-trichloroethane (DDT), and p,p’-dichloro-diphenyl-dichloroethane (DDD). According to a survey based on the usage of pesticides, 40% of pesticides used belongs to the organochlorines class [1,2]. In Asia, India is one of the largest producers of general pesticides and ranks 12th worldwide [3].

In India, approximately 70% of the population lives in rural areas. The rural population is more prone to environmental contamination due to contaminated drinking water, food, and air. Human exposure to OCPs occurs mainly through air, soil, water, flora, fauna, and food chain [4]. The agglomeration of environmental pollutants in human being suggested that it has a significant contribution to the occurrence of the diseases [5].

Diabetes mellitus (DM) is a metabolic disorder caused by insulin resistance, hypertension, hyperglycemia, and limit insulin secretion. Environmental toxicants affect the cofactors responsible for the risk of developing newly detected DM. Environmental toxicants, including organic pollutants, OCPs, heavy metals, and pharmaceutical chemical components increase insulin resistance and also interfere with total cholesterol (TC), triglycerides (TG), and glucose metabolism [6]. OCPs are supposed to be a major factor in increasing type 2 diabetes mellitus (T2DM) [5] and among these only 6% can be interpreted by genetic and heritable factors which include overweight, genetic, and sex [7,8]. Agricultural chemicals are causal factor for environmental contamination [9]. OCPs exposure through occupational or accidental practices were also reported for modified glucose metabolism, increased risk of T2DM, and insulin resistance [10,11]. The recent OCPs level in blood samples of newly diagnosed DM and prediabetes represents the current exposure to human beings. As OCPs have a long half-life with assimilation, bioaccumulation, and biomagnification properties, it causes some deleterious effects which may further promote the risk of developing newly detected DM. The present study showed recent OCPs exposure and also correlates the OCPs level with biological parameters. This study also showed the level of OCPs in blood are associated with the risk factors responsible for the conversion of prediabetes to newly detected DM with respect to lipid metabolism, insulin resistance, and glucose intolerance among the North Indian population with reference to the etiology of diabetes.

METHODS

Study population

It was a case-control study conducted on 100 normal glucose tolerance (NGT) control, 100 prediabetes, and 100 newly detected DM cases in the age group of 30 to 70 years. Age and sex were matched for all study groups. The study was carried out at Environmental Biochemistry and Molecular Biology Laboratory, Department of Biochemistry in collaboration with the Centre for Diabetes, Endocrinology, and Metabolism (DEM), University College of Medical Sciences (UCMS), University of Delhi, and Guru Teg Bahadur (GTB) Hospital, Dilshad Garden, Delhi, India. The study was carried out between February 2016 to February 2019 and the criteria for recruitment of patients were as follows. (1) No history of hypertension, known hypothyroidism, chronic diarrhea, malabsorption, hypothyroidism, Cushing syndrome, and DM. (2) Patients recently diagnosed with prediabetes and diabetes were included in the study. No patient was on medication at the time of the recruitment. (3) All patients (cases and control) were from the same geographic location.

Controls were also selected from the same location, who was visiting GTB Hospital with patients. After fulfilling the inclusion and exclusion criteria subjects were called for a standard oral glucose intolerance test (OGTT) for diagnosis of recently diagnosed prediabetes and newly detected DM groups. No patient was previously exposed or working with any kind of pesticide-related practice. Clinical assessment and anthropometry measurements were performed during OGTT. Education was divided into five grading systems (illiterate, 0–4, 5–10, 11–12, and graduate or above). Also, food habit was divided into vegetarian and non-vegetarian. Fat consumption was recorded based on the monthly intake of ghee and other dairy products. Prior written consent was also taken from the patients who were willing to participate in the study. The study was approved by the institutional ethics committee on human research (IEC-HR) (UCMS/IEC-HR/2015/24/FACULTY/1), UCMS, and GTB Hospital, University of Delhi, Delhi. Written consent form was obtained from all the subjects prior to start the study.

Sample collection and estimation

Blood samples were collected in the sample collection room of DEM center, UCMS, and GTB Hospital (University of Delhi), Dilshad Garden, Delhi. Blood (3 mL) was withdrawn from the patient after a minimum of 8 hours of overnight fasting (F) for estimation of OGTT, lipid profile, insulin, glycosylated hemoglobin (HbA1c), and OCPs. Plasma glucose levels were estimated on the same day by using glucose oxidase and peroxidase (Randox, Crumlin, UK) [3]. Clinical parameters such as glycosylated hemoglobin (HbA1c), plasma glucose level (F and postprandial [PP]), TC, TG, high-density lipoprotein cholesterol (HDL-C), and low-density lipoprotein cholesterol (LDL-C), and insulin were also analyzed. Insulin levels were estimated by radioimmune assay (Beckman coulter IM3210; Beckman coulter, Brea, CA, USA). Insulin resistance was calculated using the homeostasis model assessment of insulin resistance (HOMA-IR) and homeostasis model assessment of β-cell function (HOMA-β). The levels of TC was measured by the cholesterol oxidase-peroxidase (CHOD-POD) method [12], TG estimation was based on Werener and Gabriesulsen (1981) method using the Randox UK kit (enzymatic method). Estimation of HDL-C was done by Autopure HDL-C Accurex biomedicals kits (Accurex, Mumbai, India), and serum LDL-C and very-low-density lipoprotein cholesterol (VLDL-C) were calculated using formula LDL-C=TC–HDL-C–(TG/5) and VLDL-C=TG/5. Furthermore, demographic details like age, body mass index (BMI), and waist were also measured at the time of OGTT. Standardized methods were used for anthropometric measurements, including height, weight, and waist circumference [13]. Height and body weight were measured in very light weighed clothes and without shoes. The BMI was calculated using the formula, weight (kg)/height2 (m2) [14].

Pesticide residue analysis

The analysis of OCPs residue carried out in blood samples was as follows: isomers of HCH (α, β, and γ), aldrin, dieldrin, o,p’- DDE, p,p’-DDE, and p,p’-DDD. The extraction of OCPs was carried out using (2:1) hexane and acetone of high performance liquid chromatography grade as solvent [15]. Using mixed standard, five samples of blood in triplicate were spiked with 5 and 25 ng/mL, respectively. Analysis of the extract was done with gas chromatography (Perkin Elmer, Waltham, MA, USA) equipped with a 63Ni selective electron capture detector [15]. The column named DB-5 (non-polar, low bleed and has a high temperature) having a length of 60 m and an internal diameter (ID) of 0.25 mm was used. The detection limit of the method was 4 pg/mL for each OCP. The limit of detection of the detector was 0.05 pg perchloroethylene when nitrogen was used as a carrier gas. The average recovery of the samples spiked exceeded 95%. In pesticide analysis, a quality check was always ran two times in a day to maintain its accuracy and reproducibility. The levels of pesticide were expressed as parts per billion (ppb).

Statistical analysis

Data presentation and statistical analysis were completed using Microsoft Excel version 2010 (Microsoft, Redmond, WA, USA) and SPSS software version 17.0 (SPSS Inc., Chicago, IL, USA). P<0.05 was taken to be significant. Unpaired t-test was applied for sociodemographic and clinical data in cases and control for analysis of quantitative and chi-square/Fisher test for qualitative data, respectively. An independent t-test was used to calculate difference between two groups and one-way analysis of variance (ANOVA) within three groups with normally distributed data. Mann-Whitney test (for non-Gaussian models) was applied to find significance among three groups for pesticide analysis. Correlations of OCPs with different parameters were analyzed by Spearman’s coefficient correlation. To identify significant predictors for OCPs, a multinomial logistic regression model was applied with HbA1c levels as the dependent variable, and the OCPs levels in the blood as the independent variable. Blood OCPs level were adjusted to remove the effect of confounding factors.

RESULTS

A total of 300 adult patients were enrolled in the study, 100 controls (NGT), 100 prediabetes, and 100 newly detected DM. The sociodemographic characteristics like sex, educational status, occupation, food habit, fat intake, and source of drinking water of study groups are summarized in Table 1.

Sociodemographic characteristics of control, prediabetes, and newly detected diabetes mellitus subjects

The literacy level and working status were lower (P=0.04 and P=0.001, respectively) in the newly detected DM group as compared to the other two groups. Non-vegetarian, high-fat consumption, and under groundwater consumption were significantly high in the newly detected DM group in comparison to prediabetes and controls (P=0.018, P=0.001, and P=0.05, respectively). Most of the study subjects were residing in urban slums according to the survey and questionnaire. The baseline data of general characteristics like age, BMI, waist, HbA1c, plasma glucose levels (F and PP), insulin and insulin resistance, TC, TG, HDL-C, and LDL-C were summarized in Table 2.

Comparison of clinical and anthropometric parameters of control, prediabetes, and newly detected DM subjects

When the NGT group was compared with the prediabetes group (Group I vs. Group II), BMI, glucose F, and PP was found significantly higher (P=0.025, P=0.05, and P<0.001) in the prediabetes group. Waist (P<0.001), BMI (P<0.001), HbA1c (P<0.001), glucose F and PP (P<0.001), insulin level (P<0.001), HOMA-IR (P<0.001), TG (P=0.044), and LDL-C (P=0.025) were found highly significant in the newly detected DM group as compared to NGT (Group 1 vs. Group 3). However, when the newly detected DM group was compared with the prediabetes group (Group 2 vs. Group 3) waist circumference (P= 0.03), BMI (P<0.001), HbA1c (P< 0.001), glucose F (P<0.001), and PP (P<0.001), insulin level (P<0.001), HOMA-IR (P<0.001), and HOMA-β (P<0.001) were found significantly higher in the newly detected DM group (Table 2).

Blood samples were analyzed for OCPs residue namely isomer of HCH, aldrin, dieldrin, p,p’-DDD, o,p’-DDE, and p,p’- DDE. The mean±standard deviation levels of individual pesticides among the study group were shown in Fig. 1 (Supplementary Table 1). Significantly high levels of β-HCH (P=0.033, P<0.001), aldrin (P=0.033, P<0.001), dieldrin (P≤0.001), and p,p’-DDE (P≤0.001) were found in the prediabetes and newly detected DM group as compared to the control group. Also, a higher levels of β-HCH (P=0.014), aldrin (P=0.020), and dieldrin (P<0.015) were found in the newly detected DM group as compared to the prediabetes group.

Fig. 1.

Organochlorine pesticides (OCPs) level in blood samples of control, prediabetic, and newly detected diabetes mellitus (DM) group. The values of OCPs are expressed in mean; error bar denotes±standard deviation; all differences were significant at P<0.05 levels. ppb, parts per billion; HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichlorodiphenyl-dichloroethane. a These denote significant with regards to controls, b These denote significant with regards to prediabetic, c These denote significant with regards newly detected DM.

In Table 3, BMI was found to be positively correlated with α-HCH (P=0.001, r=0.24), β-HCH (P=0.01, r=0.21), and aldrin (P=0.001, r=0.23). HbA1c correlated significantly with aldrin (P=0.05, r=0.15), dieldrin (P≤0.001, r=0.27) and p,p’- DDE (P=0.006, r=0.20). Also F and PP glucose were correlated positively with levels of β-HCH (P=0.01 and P≤0.001; r=0.19 and r=0.29), aldrin (P=0.05 and P=0.007; r=0.14 and r=0.20) and dieldrin (P<0.001; r=0.26 and r=0.31). However, β-HCH (P=0.002, r=0.23), dieldrin (P=0.003, r=0.22) showed significant correlation with HOMA-IR. Insulin levels showed significant correlation with β-HCH (P≤0.001, r=0.26) and dieldrin (P=0.008, r= 0.19). Moreover, p,p’-DDE was significantly positively correlated only with PP glucose levels (P<0.001, r=0.26). Although, HDL-C levels were negatively correlated with β-HCH (P=0.03, r=–0.16), dieldrin (P=0.04, r=–0.15). This showed that β-HCH, dieldrin and p,p’-DDE were significantly correlated with BMI, HbA1c, F and PP, insulin, and HOMA-IR.

Correlation of blood organochlorine pesticides level with biochemical parameters in the study group

When we analyze the correlation of OCPs with itself and one another, we have found that β-HCH was significantly correlated with γ-HCH, aldrin, and p,p’-DDE (Supplementary Table 2). Also, aldrin and dieldrin showed a strong correlation with each other. While, p,p’-DDE showed a significant correlation with β-HCH, aldrin, dieldrin, and o,p’-DDE.

In context to this, we analyzed the association of fat intake, food habit, fat intake and sources of drinking water with OCPs (Supplementary Figs. 1-3), we have found that non-vegetarians have a strong association with β-HCH, dieldrin, o,p’-DDE, and p,p’-DDE. However, a strong association of OCPs with high-fat intake subjects were found in the study group. So we can say that fat might be responsible for the storage and accumulation of OCPs in the human body among North Indians. Further, a significant strong association of OCPs with groundwater samples were also found in the study.

When we analyzed risk with multiple logistic regression model, we found that in the unadjusted model (Model 1) blood levels of β-HCH (odds ratio [OR], 2.63; 95% confidence interval [CI], 1.35 to 5.12), dieldrin (OR, 2.83; 95% CI, 1.46 to 5.49), and p,p’-DDE (OR, 2.49; 95% CI, 1.28 to 4.85) were found to increase the risk of insulin resistance and glucose in tolerance by 2.63, 2.83, and 2.49 times respectively (Table 4). Also, when OCPs data was adjusted for age and BMI (Model 2) again β-HCH (OR, 2.70; 95% CI, 1.38 to 5.29), dieldrin (OR, 2.83; 95% CI, 1.46 to 5.52), and p,p’-DDE (OR, 2.55; 95% CI, 1.29 to 5.02) blood levels were found to increase the risk of insulin resistance and glucose intolerance by 2.70, 2.83, and 2.55 times respectively. Moreover, after adjusting OCPs for TG and TC (Model 3), β-HCH (OR, 2.88; 95% CI, 1.45 to 5.71), dieldrin (OR, 2.71; 95% CI, 1.39 to 5.31), and p,p’-DDE (OR, 2.63; 95% CI, 1.33 to 5.19) blood levels were found to increase the risk factors for newly detected DM by 2.88, 2.71, and 2.63 times respectively. Likewise, when adjusted for demographic parameters like food habit, fat, and drinking water (Model 4), β-HCH (OR, 2.40; 95% CI, 1.18 to 4.87), dieldrin (OR, 2.18; 95% CI, 1.10 to 4.33), and p,p’-DDE (OR, 1.76; 95% CI, 0.89 to 3.51) blood levels were found to increase the risk factor of newly detected DM by 2.40, 2.18, and 1.76 times, respectively (Table 4).

Multiple logistic regression models for the concentration of OCPs and risk of diabetes

When we adjusted the OCPs data for BMI categories, we have found that risk is strongly associated with subjects having higher BMI, i.e., BMI ≥23 and ≤25 and >25 kg/m2 (Table 5). When OCPs data was adjusted for BMI ≥23 and ≤25 kg/m2, β-HCH (OR, 1.80; P=0.012), dieldrin (OR, 1.95; P=0.046), and p,p’-DDE (OR, 1.29; P=0.050) blood levels were found to increase the risk of developing newly detected DM by 1.80, 1.95, and 1.29 times, respectively. Also, when we adjusted for BMI >25 kg/m2, we have found the risk of developing newly detected DM by 10.05, 7, and 10.66 times, respectively. This further confirms that β-HCH, dieldrin and p,p’-DDE increase the risk of developing newly detected DM.

Multiple logistic regression models for the concentration of OCPs and risk of diabetes based on the BMI categories

DISCUSSION

The present study showed the recent trend of OCPs in human blood sample and also identified its associated risk of developing newly detected DM (which is the primary stage of diabetes) with altered glucose intolerance, lipid dysfunction, and insulin resistance in the North Indian population. This study also showed that OCPs level in blood was strongly correlated with insulin resistance with varying degrees of glucose intolerance, even after adjustment for confounding factors like; BMI (≥23 and ≤25 and >25 kg/m2), TC, age, and serum TG. This study also observed the level of pesticide responsible for developing prediabetes and its further expansion to newly detected DM. Human beings are exposed to OCPs through air and water contaminated with industrial waste as well as through agricultural goods and consumer products [16]. However, continuous use of OCPs without proper safety measures also causes accumulation of OCPs residue in the human body [17]. Various epidemiological studies also showed the positive association of OCPs with T2DM [18,19].

To investigate, we have analyzed 300 blood samples divided into three groups as cases (prediabetes and newly detected DM) and control (NGT). In the present study, we have found significantly high levels of β-HCH in prediabetes and newly detected DM group when compared to controls. This is in line with earlier studies reported high OCPs level in T2DM as compared to the control group [20-23]. A higher level of β-HCH represents a current exposure that is either through polluted air, food, drinking water. Although, a public health program has completely banned the usage of these pesticides in India since April 1997 HCH is still in use in developing countries like India and China, and it is likely to affect health chronically. As HCH is the most stubborn OCP and get cleared from the body very slowly as compared to other isomers, it is easily detected in human blood.

In the present study, we have also found that the level of dieldrin in prediabetes and newly detected DM groups were higher in comparison to the control group and showed a significant association with HbA1c, glucose tolerance and insulin resistance. The findings of this study were in support of a previously reported study by Post et al. [24], 2010 that increased level of HbA1c in the blood was significantly correlated with the high level of dieldrin in the human body [24,25]. Various rigorous agricultural activities cause leakage and seepage of OCPs (aldrin, HCH, DDT, and its metabolites, etc.) into water bodies and soil which may enter into the human body and may damage the normal functioning of the body [26]. Further, the continuous increase of environmental pollutants in the human body may lead to the disruption of the normal functioning of the body and may result in the occurrence of various kind of diseases [5]. The type of pesticide, duration and route of exposure, and the individual health status (e.g., age, BMI, fat, drinking water, nutritional deficiencies, and healthy/damaged skin) are determining factors for the level of pesticides in the body.

In the study, levels of p,p’-DDE in the blood of prediabetes and newly detected DM group was also higher as compared to the control group (Fig. 1). This observation has been supported by an earlier report by Son et al. [27]. The occurrence of metabolites of DDT in serum showed the presence of DDT in the environment. Although, DDT was banned by various countries but still it is in use for various vector control programs. The half-life of p,p’-DDT and its metabolites have been assumed to be 6 to 7 years [28]. DDT has a long half-life with bioaccumulation and magnification properties and also persistent so it can still be detected in the environment [29]. OCPs and their other metabolites were assumed to impart a higher risk of increasing T2DM and other associated problems [30]. So, monitoring blood OCPs level from time to time is necessary to maintain human health and to minimize the problems associated with it.

As indicated by this study, higher levels of OCPs in blood disturb the glucose plasma levels, insulin resistance and disrupt β-cells which increases the risk of developing diabetes. We have found a strong positive correlation of β-HCH, dieldrin, and p,p’-DDE with glucose F and PP, insulin, and HOMA-IR in the blood which showed that these may be somehow associated with each other (Table 3). In demographic data, we have found that non-vegetarians, fat intake, and groundwater were positively and significantly associated with the increased level of OCPs in human blood. As obesity is a major risk factor for T2DM and excess fat consumption is directly related to obesity development. DDT tends to get stored in body fat and it was also showed by correlation and regression in this study. Fat and age have a strong protective effect on storing OCP in the human body. Various studies confirmed that p,p’-DDE was the most expected residue among all the pesticides found in high-fat products. In comparison to the southern part of India, North India has a high consumption of ghee and dairy products [31,32]. In the present study, we have also found that food habits and fat have a significant association with blood OCPs level (Supplementary Figs. 1 and 2). This observation has been supported by and Tuomi et al. [33] in 2005 and Sladek et al. [34] in 2007. Higher OCPs level in the blood of prediabetes and diabetes group and its strong correlation with F, PP, lipid, insulin, and HOMA-IR again confirms that continuous exposure of OCPs via environmental exposure (i.e., food, fat intake, drinking water, and air) may tend to increase the OCPs load in the human body which may increase the risk of developing diabetes by disturbing various biological functions within the body. So, the government needs to implement some very strong regulations on the illegal use of DDT and HCH.

Further, the result of multivariate logistic regression analysis in this study confirmed that β-HCH, dieldrin, and p,p’-DDE levels in the prediabetes and newly detected DM group were of dominant influence on human health especially with people of higher age, BMI (>25 kg/m2), fat, and lipid. Changes in lipid level and glucose metabolism were strongly interrelated with the OCPs exposure [35-37]. Disruption during the main phase of development can lead to susceptible changes in tissue, expression of a gene or other genetic composition that may lead to long-term or permanent dysfunction. This may result in increased vulnerability to chronic diseases such as obesity, metabolic syndrome, diabetes, cardiovascular diseases, and varying types of cancer [38]. This study also concludes that OCPs may play a major role in the disruption of the biological functioning of the body which in turn associated with the development of T2DM risk in the North Indian population. This study gives a recent trend of OCP in human blood and its outcomes on biochemical parameters which are one of the important aspects for maintaining public health. This study also has a few limitations. First, because of the small sample size, stratified analysis was not possible and maybe some associations were chance findings. Second, confirmation of the cause-result relationship with this study is not possible.

In conclusion, the study concludes that high OCPs level in the blood may lead to glucose intolerance and insulin resistance which may cause the risk of developing T2DM. Also, high OCPs level in the body of patients with higher BMI indicate that patients with higher BMI have higher risk of developing T2DM after a certain period. This study also showed the level of OCPs in blood are associated with the risk factors responsible for the conversion of prediabetes to newly detected DM such as lipid metabolism, insulin resistance, and glucose intolerance among North Indian population. OCPs level present in the environment may be considered as one of the major factors for metabolic and endocrine disruptions and might play a crucial role in the etiology of diabetes. Future studies should encourage the estimation of OCPs through the route of exposure such as ingestion, inhalation and dermal contact and its correlation in blood levels, lipid, HbA1c, and glucose homeostasis to better understand the mechanism behind these endocrine changes.

Supplementary Materials

Supplementary materials related to this article can be found online at https://doi.org/10.4093/dmj.2020.0093.

Supplementary Table 1.

OCPs levels in blood samples of control, pre-diabetic, and newly detected DM group

dmj-2020-0093-suppl1.pdf
Supplementary Table 2.

Correlation between organochlorine pesticides in the study subjects

dmj-2020-0093-suppl2.pdf
Supplementary Fig. 1.

Association of food habit with blood organochlorine pesticides (OCPs) level in study subjects. The value of OCPs are expressed in mean; error bar denotes ±standard deviation; P denotes significance of t-test; All differences were significant at P<0.05 levels. HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichloro-diphenyl-dichloroethane. aP≤0.05.

dmj-2020-0093-suppl3.pdf
Supplementary Fig. 2.

Association of fat with blood organochlorine pesticides (OCPs) level in study subjects. The value of OCPs are expressed in mean; error bar denotes ±standard deviation. HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichloro-diphenyl-dichloroethane.

dmj-2020-0093-suppl4.pdf
Supplementary Fig. 3.

Association of sources of drinking water with respect to blood organochlorine pesticides (OCPs) level in study subjects. The values of OCPs are expressed in mean. All differences were significant at P<0.05 levels. HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichloro-diphenyl-dichloroethane. aThese denotes significant with regards to tap water, bThese denotes significant with regards to ground water, cThese denotes significant with regards to filter water.

dmj-2020-0093-suppl5.pdf

Notes

CONFLICTS OF INTEREST

No potential conflict of interest relevant to this article was reported.

AUTHOR CONTRIBUTIONS

Conception or design: A.J.U., B.D.B., S.V.M.

Acquisition, analysis, or interpretation of data: S.T.,B.K.M., T.S., N.T., B.D.B., S.V.M.

Drafting the work or revising: S.T., B.K.M., T.S., N.T., B.D.B.,S.V.M

Final approval of the manuscript: S.T., A.J.U., B.D.B., S.V.M.

FUNDING

The University of Delhi provided the purse research grant, 2016 under funding of Department of Science and Technology (DST) to one of the senior authors (Abdul Jamil Urfi).

Acknowledgements

One of the authors, Shipra Tyagi was recipient of the Inspire Senior Research Fellowship (SRF) (IF160105).

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Article information Continued

Fig. 1.

Organochlorine pesticides (OCPs) level in blood samples of control, prediabetic, and newly detected diabetes mellitus (DM) group. The values of OCPs are expressed in mean; error bar denotes±standard deviation; all differences were significant at P<0.05 levels. ppb, parts per billion; HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichlorodiphenyl-dichloroethane. a These denote significant with regards to controls, b These denote significant with regards to prediabetic, c These denote significant with regards newly detected DM.

Table 1.

Sociodemographic characteristics of control, prediabetes, and newly detected diabetes mellitus subjects

Parameter Control (Group 1) (n=100) Prediabetes (Group 2) (n=100) Newly detected DM (Group 3) (n=100) P value
Sex 0.621
 Male 47 56 43
 Female 53 44 57
Educational type 0.040a
 Illiterate 41 31 59
 0–5 5 8 11
 5–10 25 26 6
 10–12 29 22 17
 Graduate or above 0 13 7
Occupation 0.001a
 Working 63 57 36
 Non-working 37 43 64
Food habit 0.018a
 Vegetarian 47 49 30
 Non-vegetarian 53 51 70
Fat, /mo 0.001a
 0–200 g 28 33 56
 200–500 g 3 5 8
 600–1,500 g 25 31 17
 1,500 g and above 44 31 19
Source of drinking water 0.041a
 Tap water 74 64 59
 Ground water 7 9 14
 Filter water 19 27 27

DM, diabetes mellitus.

a

P≤0.05 is significant.

Table 2.

Comparison of clinical and anthropometric parameters of control, prediabetes, and newly detected DM subjects

Parameter Control (Group 1) (n=100) Prediabetes (Group 2) (n=100) Newly detected DM (Group 3) (n=100) P value
Age, yr 43.90±6.79 44.50±6.47 43.78±7.67 1 vs. 2=0.639
1 vs. 3=0.927
2 vs. 3=0.575
BMI, kg/m2 28.23±6.02 31.05±5.72 34.1±0.72 1 vs. 2=0.025a
1 vs. 3 <0.001a
2 vs. 3 <0.001a
Waist, cm 92.85±16.38 95.78±15.51 101.70±12.42 1 vs. 2=0.281
1 vs. 3=0.001a
2 vs. 3=0.030a
Systolic blood pressure, mm Hg 127.42±9.63 127.92±8.59 129.51±10.13 1 vs. 2=0.675
1 vs. 3=0.088
2 vs. 3=0.425
Diastolic blood pressure, mm Hg 77.09±11 78.58±10.58 78.92±11 1 vs. 2=0.589
1 vs. 3=0.678
2 vs. 3=0.485
HbA1c, % 5.24±0.31 5.51±0.52 7.14±1.75 1 vs. 2=0.171
1 vs. 3 <0.001a
2 vs. 3 <0.001a
Glucose fasting, mg/dL 86.52±6.59 97.68±11.38 138.30±53.53 1 vs. 2=0.05a
1 vs. 3 <0.001a
2 vs. 3 <0.001a
Glucose PP, mg/dL 107.90±17.79 154.58±22.39 285.25±93.85 1 vs. 2 <0.001a
1 vs. 3 <0.001a
2 vs. 3 <0.001a
Insulin, mIU/L 11.44±5.77 14.52±11.47 30.38±10.60 1 vs. 2=0.081
1 vs. 3 <0.001a
2 vs. 3 <0.001a
HOMA-IR 2.45±1.27 3.52±2.85 11.06±7.59 1 vs. 2=0.220
1 vs. 3 <0.001a
2 vs. 3 <0.001a
TC, mg/dL 183.31 ±67.19 192.67±47.63 194.48±44.36 1 vs. 2=0.344
1 vs. 3=0.259
2 vs. 3=0.854
TG, mg/dL 141.02±66.09 152.33±69.53 166.96±74.49 1 vs. 2=0.378
1 vs. 3=0.044a
2 vs. 3=0.255
HDL-C, mg/dL 44.85±10.52 43.92±13.16 42.53±9.06 1 vs. 2=0.644
1 vs. 3=0.252
2 vs. 3=0.494
LDL-C, mg/dL 112.03±48.05 114.04±49.38 127.98±69.75 1 vs. 2=0.337
1 vs. 3=0.025a
2 vs. 3=0.196

Values are presented as mean±standard deviation.

DM, diabetes mellitus; BMI, body mass index; HbA1c, glycosylated hemoglobin; PP, postprandial; HOMA-IR, homeostasis model assessment of insulin resistance; TC, total cholesterol; TG, total triglycerides; HDL-C, high-density lipoprotein cholesterol; LDL-C, low-density lipoprotein cholesterol.

a

P≤0.05 was significant.

Table 3.

Correlation of blood organochlorine pesticides level with biochemical parameters in the study group

Parameter Correlation BMI Waist Hb1Ac Fasting PP TC TG HDL-C Insulin HOMA-IR
α-HCH P value 0.001 0.39 0.48 0.84 0.79 0.73 0.77 0.30 0.97 0.90
r 0.24a –0.06 0.05 0.01 0.02 0.02 0.02 –0.07 –0.003 –0.009
β-HCH P value 0.005 0.66 0.22 0.01 0.00 0.83 0.50 0.03 0.00 0.002
r 0.21a 0.03 0.09 0.19b 0.29a –0.02 –0.05 –0.16b 0.26a 0.23a
γ-HCH P value 0.12 0.49 0.76 0.64 0.93 0.78 0.43 0.22 0.49 0.54
r 0.11 –0.05 –0.02 0.03 0.006b 0.021 –0.05 –0.09 0.05b 0.05b
Aldrin P value 0.001 0.16 0.05 0.05 0.007 0.73 0.45 0.89 0.05 0.08
r 0.23a 0.10 0.15b 0.14 0.20a –0.02 0.06 –0.01 0.14 0.13
Dieldrin P value 0.88 0.82 0.00 0.00 0.00 0.89 0.85 0.04 0.008 0.003
r 0.01 0.02 0.27a 0.26a 0.31a –0.01 –0.01 –0.15b 0.19a 0.22a
o,p’-DDE P value 0.31 0.84 0.56 0.85 0.63 0.55 0.30 0.33 0.04 0.34
r –0.08 0.01 0.04 0.01 0.04 –0.04 0.07 –0.07 0.15b 0.07
p,p’-DDE P value 0.96 0.47 0.006 0.22 0.00 0.77 0.48 0.56 0.11 0.44
r 0.004 0.05 0.20a 0.09 0.26a 0.02 0.05 0.04 0.12 0.06
p,p’-DDD P value 0.43 0.96 0.44 0.84 0.49 0.46 0.37 0.37 0.73 0.93
r 0.06 0.004 –0.06 0.01 0.05 –0.05 –0.07 –0.07 –0.03 –0.007

BMI, body mass index; HbA1c, glycosylated hemoglobin; PP, postprandial; TC, total cholesterol; TG, total triglycerides; HDL-C, high-density lipoprotein cholesterol; HOMA-IR, homeostasis model assessment of insulin resistance; HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichloro-diphenyl-dichloroethane.

a

P≤0.01,

b

P≤0.05.

Table 4.

Multiple logistic regression models for the concentration of OCPs and risk of diabetes

Parameter Model 1
Model 2
Model 3
Model 4
OR (95% CI) P value OR (95% CI) P value OR (95% CI) P value OR (95% CI) P value
α-HCH 1.19 (0.64–2.19) 0.579 1.17 (0.63–2.19) 0.685 1.12 (0.60–2.08) 0.719 1.31 (0.67–2.52) 0.427
β-HCH 2.63 (1.35–5.12) 0.004a 2.70 (1.38–5.29) 0.004a 2.88 (1.45–5.71) 0.002a 2.40 (1.18–4.87) 0.015b
γ-HCH 1.14 (0.62–2.12) 0.674 1.22 (0.64–2.32) 0.545 1.08 (0.58–2.02) 0.806 0.92 (0.48–1.75) 0.398
Aldrin 1.45 (0.76–2.76) 0.263 1.60 (0.81–3.17) 0.176 1.49 (0.77–2.86) 0.232 0.97 (0.50–1.88) 0.934
Dieldrin 2.83 (1.46–5.49) 0.002a 2.83 (1.46–5.52) 0.002a 2.71 (1.39–5.31) 0.004a 2.18 (1.10–4.33) 0.025b
o,p’-DDE 1.23 (0.67–2.27) 0.506 1.23 (0.66–2.27) 0.520 1.31 (0.70–2.43) 0.398 1.16 (0.61–2.23) 0.643
p,p’-DDE 2.49 (1.28–4.85) 0.007a 2.55 (1.29–5.02) 0.007a 2.63 (1.33–5.19) 0.005a 1.76 (0.89–3.51) 0.050b
p,p’DDD 0.77 (0.42–1.42) 0.398 0.81 (0.43–1.51) 0.506 0.81 (0.43–1.49) 0.494 1.14 (0.59–2.19) 0.698

Model 1: crude ratio; Model 2: adjusted for age and body mass index; Model 3: adjusted for triglycerides and cholesterol; Model 4: adjusted for demographic data.

OR, odds ratio; CI, confidence interval; HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichloro-diphenyl-dichloroethane.

a

P≤0.01,

b

P≤0.05.

Table 5.

Multiple logistic regression models for the concentration of OCPs and risk of diabetes based on the BMI categories

Parameter BMI <23 kg/m2
BMI ≥23 and ≤25 kg/m2
BMI >25 kg/m2
OR (95% CI) P value OR (95% CI) P value OR (95% CI) P value
α-HCH 0.60 (0.09–3.98) 0.597 1.78 (0.87–3.64) 0.109 0.36 (0.06–2.15) 0.262
β-HCH 1.80 (0.85–3.80) 0.012a 4.00 (0.50–24.98) 0.191 10.05 (1.36–43.05) 0.024a
γ-HCH 1.50 (0.23–9.79) 0.672 0.97 (0.48–1.97) 0.947 0.52 (0.067–4.0) 0.529
Aldrin 1.50 (0.37–12.8) 0.347 0.80 (0.38–1.66) 0.550 0.40 (0.03–5.25) 0.485
Dieldrin 1.40 (0.19–2.43) 0.738 1.95 (0.95–3.98) 0.046a 7.00 (0.97–30.57) 0.050a
o,p’-DDE 0.90 (0.13–6.08) 0.914 1.50 (0.74–6.05) 0.262 0.375 (0.61–4.30) 0.290
p,p’-DDE 1.33 (0.14–7.37) 0.800 1.29 (0.59–8.82) 0.050a 10.66 (1.38–36.03) 0.013a
p,p’-DDD 2.40 (0.29–10.78) 0.416 1.21 (0.59–3.45) 0.601 1.78 (0.28–11.1) 0.538

Model crude ratio.

BMI, body mass index; OR, odds ratio; CI, confidence interval; HCH, hexachlorocyclohexane; DDE, dichloro-diphenyl-dichloroethylene; DDD, dichloro-diphenyl-dichloroethane.

a

P≤0.05.