- 1Laboratório de Farmacologia Molecular, Instituto de Ciências Biológicas, Universidade Federal do Pará, Belém, Brazil
- 2Department of Analytical Chemistry and Food Technology, Faculty of Environmental Sciences and Biochemistry, University of Castilla-La Mancha, Toledo, Spain
- 3Laboratório de Investigações em Neurodegeneração e Infecção (Hospital Universitário João de Barros Barreto), Universidade Federal do Pará, Belém, Brazil
- 4Laboratório de Neuroquímica Molecular e Celular, Instituto de Ciências Biológicas, Universidade Federal do Pará, Belém, Brazil
- 5Departamento de Bioquímica e Imunologia, Universidade Federal de Minas Gerais, Belo Horizonte, Brazil
- 6Neuroscience Research Group, CEUMA University, São Luís, Brazil
- 7Laboratório de Genética Humana e Médica, Instituto de Ciências Biológicas, Universidade Federal do Pará, Belém, Brazil
- 8Instituto Federal de Educação, Itaituba, Brazil
- 9Laboratório da Biologia da Cicatrização, Ontogenia e Nutrição de Tecidos, Departamento de Morfologia e Instituto de Biomedicina, Escola de Medicina, Universidade Federal do Ceará, Fortaleza, Brazil
Human exposure to mercury is a serious problem of public health in Amazon. As in other vulnerable populations throughout the world, Amazonian riverine populations are chronically exposed to this metal and some symptoms of mercury intoxication were already detected in these populations. However, studies on the genetic susceptibility to mercury toxicity in the Amazon are scarce, and they tested a limited number of individuals. In this context, apolipoprotein E gene (APOE) is a key element with a well-established association among their alleles and the neurodegenerative consequences of mercury intoxication. However, no studies have addressed APOE genotyping in Amazonian exposed populations. Additionally, epidemiological studies with APOE genotyping in Amazon have been restricted to indigenous populations. Therefore, this work analyzed for the first time the genotypic and allelic profiles of APOE in Amazonian riverine populations chronically exposed to mercury. Eight hundred and twenty three individuals were enrolled in our study donating blood (794) and/or hair (757). APOE genotyping was analyzed by real-time PCR. Total mercury and mercury species were quantified by ICP-MS and GC-pyro-AFS, respectively. Genomic ancestry markers were evaluated by multiplex-PCR reaction, separated by capillary electrophoresis on the ABI 3130 Genetic Analyzer instrument and analyzed on GeneMapper ID v3.2. The 𝜀3 and 𝜀3/𝜀3 were the most frequent allele and genotype, respectively, followed by 𝜀4 allele and 𝜀3/𝜀4 genotype. Only 𝜀2/𝜀2 genotype was not found, suggesting that the absence of this genotype is a generalized phenomenon in Amazon. Also, our data supported an association between the presence of APOE4 and the Amerindian origin in these populations. Fifty-nine individuals were identified at maximum risk with levels of mercury above 10 μg/g and the presence of APOE4. Interestingly, among individuals with high mercury content, APOE4-carriers had high mercury levels than APOE2-carriers, pointing to a different heavy metal accumulation according to the APOE allele. These data suggest that APOE4, in addition to a possible pharmacodynamic effect, may influence pharmacokinetically the mercury exposure causing its higher accumulation and leading to worse deleterious consequences. Our results may aid in the development of prevention strategies and health policy decision-making regarding these at-risk vulnerable populations.
Introduction
Human exposure to mercury is presently a major public health concern worldwide (Sheehan et al., 2014; Andreoli and Sprovieri, 2017). Since 2013, a growing number of countries are agreeing to join efforts aiming to protect human health and the environment against the deleterious effects of this heavy metal. The result of the conceptualization of this collaborative platform was the Minamata Convention on Mercury1, endorsed by the World Health Organization2 (WHO) and ratified by Brazil on August, 2017.
Brazil is a continent-sized country that faces huge challenges in the consolidation of an universal healthcare system (Coutinho and Silva Junior, 2015; Muzaka, 2017). The northern region of Brazil is almost entirely occupied by the Amazon rainforest, where human populations have been suffering from mercury exposure since the 1980s, when the “the gold rush” occurred (Berzas Nevado et al., 2010). According to the WHO, tropical populations near gold mining locations show the highest weekly mercury intake among all vulnerable populations in the world, reaching almost four times the FAO/WHO reference level of 2.2 μg/g (Sheehan et al., 2014). In addition to gold mining activities, other anthropogenic alterations of the Amazonian environment such as hydroelectric power dams may be contributing to release the mercury containing in soils, facilitating the methylation of the metal, and making it available for human exposure (Marques et al., 2011; Hacon et al., 2014; Fearnside, 2015; Arrifano et al., 2018b).
The main human populations affected by mercury exposure in Amazon are remote communities with two different profiles, also known as indigenous and riverine people. The indigenous populations are native organized into tribes who are direct descendants of the original populations that lived in Amazon before the European colonization. Brazilian laws recognize and protect these populations, presently living at protected lands (reservoirs). The riverine populations are rural communities located at riverbanks, with high genetic introgression due to colonization and immigration and with no special protection by Brazilian laws. Both populations share some characteristics, such as economy of subsistence, fish as the main protein of the diet and no sanitary conditions or piped water (Piperata, 2007). Also, both of them live in remote areas with difficult access to health centers (da Silva Souza et al., 2018).
Worryingly, several studies have demonstrated high mercury content in hair of some riverine populations in Amazon (Berzas Nevado et al., 2010; Marques et al., 2013; Hacon et al., 2014; Hoshino et al., 2015; Arrifano et al., 2018b). These communities are exposed mainly to methylmercury (MeHg) through consumption of contaminated fish (Berzas Nevado et al., 2010; Rodriguez Martin-Doimeadios et al., 2014; Arrifano et al., 2018b), as other vulnerable populations throughout the world (Drescher et al., 2014; Strain et al., 2015; Langeland et al., 2017; Salazar-Camacho et al., 2017). MeHg is the most toxic specie of mercury with diverse effects, such as neurotoxicity and genotoxicity among others (Crespo-Lopez et al., 2011, 2016; Farina et al., 2011). Still, the neurotoxic effects of MeHg are recognized as the most deleterious consequences in humans (Farina et al., 2011; Arrifano et al., 2018a). MeHg intoxication can produce several neurological effects, such as motor and visual impairment, mood change and memory loss (Grandjean et al., 1999; Dolbec et al., 2000; Rodrigues et al., 2007; Fillion et al., 2011a,b; Khoury et al., 2015; Costa et al., 2017; Da Silva-Junior et al., 2017). The neurodegeneration caused by this metal was already associated with the development of neurodegenerative diseases such as Alzheimer’s and Parkinson’s (Farina et al., 2013; Chin-Chan et al., 2015). Despite this scenario and the importance of developing adequate prevention strategies, studies on the genetic susceptibility to mercury toxicity in the Amazon are scarce, and they tested a limited number of individuals (Klautau-Guimarães et al., 2005; Jacob-Ferreira et al., 2010, 2011; Barcelos et al., 2013, 2015; de Oliveira et al., 2014; Rocha et al., 2016), probably because the difficulties to reach these communities and the demanding conditions to carry out these studies.
Although some markers of genetic susceptibility to mercury toxicity have been proposed in recent years (reviewed by Andreoli and Sprovieri, 2017), apolipoprotein E gene (APOE for the gene; and ApoE for the protein) is a key element in this scenario, with a well-established association among their alleles and the neurodegenerative consequences (Godfrey et al., 2003; Wojcik et al., 2006; Ng et al., 2013, 2015; Woods et al., 2014; Snoj Tratnik et al., 2017). ApoE is a glycoprotein involved in several brain functions, including lipid metabolism, axonal growth, synaptic formation and neuronal repair (Xu et al., 2014; Arrifano et al., 2018a). APOE is a polymorphic gene with three common alleles, 𝜀2, 𝜀3 and 𝜀4, which differ in the arginine and cysteine contents at positions 112 and 158 of the protein (Mahley et al., 2009; Arrifano et al., 2018a). ApoE3 shows a cysteine and an arginine at positions 112 and 158, respectively, whereas ApoE2 has two cysteines and ApoE4 has two arginines at both positions (Mahley et al., 2009). The presence of APOE4 is the only genetic risk factor confirmed in the development of late-onset Alzheimer Disease (Bertram, 2009; Xu et al., 2014) and it is presently the gene with more studies demonstrating an association with the susceptibility to mercury-induced neurotoxicity in adults (Andreoli and Sprovieri, 2017; Arrifano et al., 2018a).
Therefore, this work analyzed, for the first time in Amazon, the apolipoprotein E genotyping in riverine populations chronically exposed to mercury. The possible associations with ancestry and exposure were also studied.
Materials and Methods
Participants
Amazonian riverine populations chronically exposed to mercury via consumption of contaminated fish were included in the present work (Figure 1). Participants were from two locations (Tapajós River basin and Tucuruí Lake) that were demonstrably exposed to mercury in the past and in the present (Berzas Nevado et al., 2010; Rodriguez Martin-Doimeadios et al., 2014; Khoury et al., 2015; Arrifano et al., 2018b) and included adults (≥18 years) living in the area for at least 2 years.
FIGURE 1. Map of Brazil (obtained from the Instituto Brasileiro de Geografia e Estatística, Brazil) showing the States and their capitals (black stars). Yellow circles indicate the locations (–4.287121, –55.984106, and –3.800897, –49.811848) of riverine populations participating of this study. Photographs illustrates some conditions of the riverine populations: difficult access (above), river as a key element (below left) and precarious facilities (below right).
The present study followed the guidelines established by both the Declaration of Helsinki and the Conselho Nacional de Ética em Pesquisa com Seres Humanos (CONEP, Brazil) and it was approved with the CAAE no. 43927115.4.0000.0018. All participants gave written consent to participate after understanding the purpose of this work.
Anthropometric Data and Self-Reported Conditions
Gender, age, fish-intake and the existence of drug dependency (including tobacco and alcohol), pre-existent chronic diseases and chronic pharmaceutical treatments were registered for each participant. Also, weight and height were measured.
Sample Collection
Approximately, 0.1 g of hair from the occipital region (1–2 cm from the scalp) with clean stainless scissors and 2 mL of blood were drawn and stored (in paper envelopes at room temperature and frozen in EDTA vacutainer tubes, respectively).
DNA Extraction
Genomic DNA was isolated from whole blood with the Purelink Genomic DNA Mini Kit (ThermoFisher, Brazil), according to manufactures’ instructions. Quantitation of DNA was performed using the Qubit dsDNA BR Assay Kit on a Qubit 3.0 fluorimeter (ThermoFisher, Brazil).
Apolipoprotein E Genotyping
APOE genotype of each participant was detected by real time-PCR with TaqMan® assays using the StepOnePlus® equipment (ThermoFisher, Brazil). Two APOE single-nucleotide polymorphisms (SNPs), rs429358 and rs7412, corresponding to the positions 112 and 158 of the protein, respectively, were analyzed. For each SNP the reactions were performed in duplicate on 96-well microtiter plates with final volume of 10 μl, containing 5 μl of 2× TaqMan Universal PCR Master Mix (ThermoFisher, Brazil), 25 nmol/l of each probe (FAM or VIC-labeled), and 0.5 μl of DNA (30–100 ng). The run conditions were 40 cycles of denaturation at 92°C for 15 s and hybridization and extension at 60°C for 1 m. Each SNP’s probes had two sequences labeled with a different dye VIC/FAM to the polymorphisms C/T, respectively. This technique permits the identification of the six possible genotypes: 𝜀2/𝜀2; 𝜀2/𝜀3; 𝜀2/𝜀4; 𝜀3/𝜀3; 𝜀3/𝜀4; and 𝜀4/𝜀4, according the combination of fluorescence detected for each position. So, 𝜀2 had only the detection of FAM fluorescence; 𝜀3 had FAM for rs429358 and VIC for rs7412 fluorescence detection and; 𝜀4 had only VIC detection for both SNPs.
Ancestry
Genomic ancestry analysis was performed based on the method described elsewhere (Ramos et al., 2016), using 61 autosomal ancestry informative markers (AIMs). Two multiplex PCR reactions of 20 and 22 markers were performed and amplicons were analyzed by electrophoresis using the ABI Prism 3130 sequencer and GeneMapper ID v.3.2 software. The individual proportions of European, African, and Amerindian genetic ancestries were estimated using STRUCTURE v.2.3.3 software, assuming three parental populations (European, African, and Amerindian).
Quantification of Total Mercury and Methylmercury in Human Hair
Extraction of Hg species was performed in a closed-vessel microwave oven using 100 mg of hair sample and 10 mL of 6 N nitric acid as extractant. Microwave vessels were sealed and irradiated for 5 min at 80°C after a 5 min ramping time. A clear solution was obtained after microwave irradiation. Extraction blanks were also prepared in the same manner in each batch.
Total mercury content in hair samples were determined by inductively coupled plasma mass spectrometry (ICP-MS, Thermo Fisher Corporation) and mercury species were determined by GC-pyro-AFS system according to Arrifano et al. (2018b). For total mercury analysis, extracts were directly analyzed after the adequate dilution. For mercury species determination, 2 mL of the acidic extracts were subjected to derivatization with sodium tetraethylborate and mercury species were extracted in hexane. For derivatization, the pH of the extracts was adjusted to 3.9 using ammonia (30%) and 5 mL of 0.1 M acetic acid-sodium acetate buffer. Then, 2 mL of hexane and 500 μL of (3%, w/v) were added and the mixture was manually shaken for 5 min. The sample was centrifugated for 5 min at 600 g. The organic layer was transferred to a chromatographic glass vial and stored at -18°C until analysis. The certified reference material human hair ERM-DB001 (Sigma-Aldrich, Brazil) was used for quality control of mercury analysis.
Statistical Analysis
Gaussian distribution of data was verified with D’Agostino-Pearson normality test. Accordingly, data were then analyzed with Mann–Whitney test to compare groups. Correlations between variables were tested by Spearman test. Distributions and frequencies were evaluated with Chi-square or Fisher’s exact tests. Hardy–Weinberg equilibrium (HWE) was tested to verify whether APOE genetic variation remained at equilibrium. For all analysis, p < 0.05 was considered statistically significant.
Results
Anthropometric data of the participants of the present study are showed in Table 1. Except for the distribution of gender, no significant difference was detected for all anthropometric parameters between participants from the two regions.
Figure 2, Table 2, and Supplementary Table S1 includes the genotypic and allelic frequencies of apolipoprotein E found in the participants. Only the 𝜀2/𝜀2 genotype of APOE gene was not found. No difference was detected between participants from Tapajós and Tucuruí. For the following analyses with APOE4-carriers or non-carriers, the individuals with the 𝜀2/𝜀4 genotype (14 participants) were not included since both alleles may show opposite effects on mercury intoxication.
FIGURE 2. Allelic distributions of apolipoprotein E gene in global (mainly developed countries), South American, Amazonian indigenous, and Amazonian riverine populations. Data are from Singh et al. (2006) and this work.
TABLE 2. Genotypic and allelic distributions and frequencies (f) of apolipoprotein E in riverine populations of the Amazon.
Ancestry markers revealed a significant high contribution of European origin, followed by Amerindian and by African origins (Table 3) (Kruskal–Wallis test, p < 0.0001). No difference in ancestry distribution was detected between participants from Tapajós and Tucuruí.
Considering that no difference was found between Tapajós and Tucuruí in both distributions of ancestry and apolipoprotein E genotypes and alleles, we studied the possible association of the presence of ApoE4 and ancestry for the total population. APOE4-carriers (𝜀4/𝜀4 and 𝜀3/𝜀4) showed a significant higher proportion of Amerindian origin when compared to that of non-carriers (Table 4).
TABLE 4. Ancestry profile of the Amazonian riverine individuals according to be apolipoprotein 𝜀4 allele (APOE4) carrier or not.
To confirm the present exposure of the populations, we quantified the mercury content in hair of participants. Seven hundred and fifty-seven participants agreed to donate a hair sample for mercury quantification. Total mercury level in hair was 4.84 μg/g (2.30–9.66) as median and interquartile ranges, being 87.8% (83.7–90.3) MeHg. Mercury levels were correlated with the frequency of fish intake (number of meals per week) (Spearman test, p < 0.05). There was no correlation of age with total mercury concentrations (Spearman test, p > 0.05). However, men showed significantly higher mercury levels than women, consuming also higher amounts of fish (Mann–Whitney test, p < 0.001). Moreover, the median level of mercury was significantly higher in Tucuruí (8.12, 3.65–14.99 μg/g) than in Tapajós (3.62, 1.77–6.47 μg/g) (Mann–Whitney test, p < 0.001), therefore, the following analyses with mercury levels were carried out for three universes of sampling (the total of participants, those from Tapajós and those from Tucuruí) to reveal any difference between locations.
No significant difference was found in allelic frequencies of APOE between individuals with high and low mercury levels (Table 5A). These results were observed even when rigorous exclusion criteria were additionally applied (which are not always present in studies of human exposure), guaranteeing the elimination of most confounding factors and the potential for mercury levels to be significantly influenced by altered hepatic and/or renal function (Table 5B).
TABLE 5. Allelic frequencies of apolipoprotein E gene in participants with total mercury levels above (High Hg) and below (Low Hg) the limit of 10 μg/g.
Interestingly, when APOE2-carriers (𝜀2/𝜀3) were compared to APOE4-carriers, mercury levels of the latter ones were significantly higher in individuals with high mercury content (Figure 3). It is important to note that both groups included similar proportions of men and women and consumed similar amounts and frequencies of fish meals (Table 6). These results already point to a different mercury bioaccumulation affected by APOE alleles in high mercury participants. This difference was not detected in individuals with mercury levels below the limit (Figure 3).
FIGURE 3. Total mercury levels in hair of APOE2-carriers and APOE4-carriers in Amazonian riverine population. Individuals with 𝜀2/𝜀4 genotypes were not included in the present analysis. (A) Participants with mercury levels below 10 μg/g (n = 47 and 172 for APOE2- and APOE4-carriers, respectively); (B) Participants with mercury levels ≥10 μg/g (n = 12 and 59 for APOE2- and APOE4-carriers, respectively). Data are presented as median and interquartile ranges. ∗p < 0.05. Mann–Whitney test.
TABLE 6. Anthropometric profile and fish consumption (frequency and amount) in APOE2- and APOE4-carriers with high levels of mercury (≥10 μg/g).
Discussion
This work showed for the first time the genotypic and allelic distribution of apolipoprotein E in Amazonian riverine populations and its association with ancestry. Additionally, our data revealed that individuals exposed to high mercury levels showed a more Amerindian ancestral background. Interestingly, a higher accumulation of mercury was detected in APOE4-carriers when compared to APOE2-carriers.
Amazon is the largest tropical forest in the world, most of the area belonging to Brazil. Currently, Brazilian Amazon is occupied by more than 17 million people (IBGE, 2016), being one of the huge challenges in healthcare that faces this developing country with an emerging economy (Muzaka, 2017). Amazonian populations show the lowest human development index (Atlas of Human Development in Brazil, 2013) with a significant part of the population living far away from the main cities and organized in small riverine communities or widespread family based houses. Presently, Amazonian riverine populations has a particular life style with the river as a central element (Figure 1): water for cooking is obtained from the river or hand-dug wells, fish is the main protein of the diet (usually included in many meals per week) and trash is sometimes dumped into the river (Piperata, 2007). A different number of women and men participated in our study (Table 1), which is usually found in epidemiological studies with Amazonian population (Krewer et al., 2011; Valentini et al., 2016). The hypothesis raised to explain this difference is that, in these communities, women may be more careful with health than men may (Gomes et al., 2007). Interestingly, in Tucuruí participation of men was as high as that of women (Table 1), probably because men commanded the boats with all the family to the collection point (personal observation). Notably, of the initial 823 participants that attended to the collection point, only 29 individuals abstained to donate blood (or the collection was not possible), contributing for the representability of the sample.
To our knowledge, this is the larger epidemiological study of mercury-related genetic factors carried out in Amazonian riverine population (Klautau-Guimarães et al., 2005; Jacob-Ferreira et al., 2010, 2011; Barcelos et al., 2013, 2015; de Oliveira et al., 2014; Rocha et al., 2016). Additionally, studies genotyping APOE gene are really scarce in Amazonian populations and they are limited to small indigenous tribes, such as Yanomami or Tsiname (Crews et al., 1993; Marin et al., 1997; Jaramillo-Correa et al., 2001; Trumble et al., 2017).
Our results demonstrated that 𝜀3 and 𝜀3/𝜀3 were the most frequent allele and genotype, respectively (Table 2), followed by 𝜀4 allele and 𝜀3/𝜀4 genotype. Other interesting result is despite of the large number of participants, the 𝜀2/𝜀2 genotype was not detected (Table 2). Previous studies with smaller samples of participants from Amazonian indigenous tribes (Crews et al., 1993; Marin et al., 1997; Jaramillo-Correa et al., 2001; Trumble et al., 2017) did not find this genotype either (Figure 2). Based on our data with a large number of participants, the absence of the 𝜀2/𝜀2 genotype would not be restricted to the indigenous profile in Amazon, suggesting that it could be a general phenomenon in Amazonian populations.
When compared to other populations around the world (Figure 2), we observed a profile of allelic and genotypic frequencies in Amazonian riverine populations, similar to that found in other populations of South-America, characterized by a higher frequency of 𝜀4 allele and a lower frequency of 𝜀2 allele (Singh et al., 2006). In fact, approximately 33% of the participants of the present study carried at least one copy of the 𝜀4 allele (Table 2).
The 𝜀4 allele is considered the ancestral one in the genus Homo, which would have been progressively lost due to the high risk involving the development of neurodegeneration and cardiovascular diseases (Singh et al., 2006; Eisenberg et al., 2010; Trumble et al., 2017). Hypothesis were already raised to explain its higher prevalence in developing countries or traditional societies, such as an apparent increased resistance to pathogens and/or a rebalancing in cholesterol levels in conditions of increased metabolic rate (which would partially compensate the increased risk of neurodegeneration) (Corbo and Scacchi, 1999; Mahley and Rall, 1999; Singh et al., 2006; Mahley et al., 2009; Eisenberg et al., 2010; Trumble et al., 2017). The possible association with Amerindian origin make us to analyze the ancestral background of the participants of the study.
Historically, the colonization by the Europeans lead to a high genetic exchange of the Amazonian population (Cavalcante et al., 2015). Brazilian population shows a trihybrid ancestry with three major contributors (Amerindian, European, and African) (Parra et al., 2003; Lins et al., 2010). In most of the Brazilian regions, the European origin provides the highest contribution (Lins et al., 2010). Amazonian riverine population also shows this profile with 42.4% of European ancestry (Table 3). In this population, Amerindian contribution was significantly higher than African. Interestingly, APOE4-carriers showed a significant higher Amerindian contribution than that of APOE4 non-carriers (Table 4), suggesting a possible association between the two factors. Considering that in the Amazon, the Amerindian profile may be associate to primitive societies, our results would be in agreement with the idea that the 𝜀4 allele remains significantly prevalent in economies of foraging and/or with food restrictions (Corbo and Scacchi, 1999) and/or when metabolic rate is elevated due to the high energetic expenditure on cooling/thermogenesis (for example Eisenberg et al., 2010). In this case, APOE4-carriers would show an adaptive advantage because the higher cholesterol absorption and body burden when compared to those of 𝜀3/𝜀3 individuals (Corbo and Scacchi, 1999).
Both populations included in the present work preserve some of the traditional characteristics linked to indigenous ancestry and local sources, such as subsistence economy (they grow vegetables and fruits to eat in the yards of their homes), fishing (fish is the main source of these proteins), and hunting (Piperata, 2007). Nowadays, fish is still the central element of the diet, usually with seven or more meals a week (Passos et al., 2008; Piperata et al., 2011; Dufour et al., 2016). Unfortunately, these food habits in Amazon can contribute to human exposure to mercury when the fish is contaminated (Passos et al., 2008; Berzas Nevado et al., 2010; Arrifano et al., 2018b). Our data revealed a significant correlation between fish intake and mercury levels, pointing to fish consumption as the origin of mercury exposure. Mercury is present in Amazon from both natural (soil) and anthropogenic sources (artisanal gold mining and dams, among others) (Wasserman et al., 2003; Berzas Nevado et al., 2010; Arrifano et al., 2018b). Once in the river, mercury undergoes biotransformation to MeHg, being incorporated in the food chain, and contaminating the fish. Therefore, it is relatively usual find mercury-intoxicated populations in Amazon (Grandjean et al., 1999; Dolbec et al., 2000; Rodrigues et al., 2007; Fillion et al., 2011b; Khoury et al., 2015).
In our study, we performed the mercury determination in hair of 757 participants (only 66 individuals abstained to donate or the collection of the sample was not possible). No correlation between mercury levels and age was found supporting the fact that age may not be an influencing factor for mercury exposure in adults. Accordingly, previous works already demonstrated no association between both factors in adults (Hoshino et al., 2015; Arrifano et al., 2018b), although it can be observed in children (Barbosa et al., 1998; Pinheiro et al., 2007; Marques et al., 2016). Moreover, it is also relatively frequent to find higher mercury levels in men than those in women, usually attributed to a higher consumption of fish (Dolbec et al., 2000; Fillion et al., 2006; Passos et al., 2007; Ashe, 2012), as we detected in our study.
Mercury levels usually found in hair varies between 0 and 2 μg/g (WHO, 2008) in non-exposed populations. In our study, median value of exposure was more than twice those levels, confirming the exposure of the population. Moreover, a substantial part of the participants (26%) showed a mercury content in hair above the limit of 10 μg/g previously recommended (Grandjean et al., 1997; Harada et al., 1999; NRC, 2000). Mercury found in hair was mainly in organic form, as MeHg. This high proportion of the organic species and the significant correlation with fish intake are in agreement with the oral exposure via contaminated fish that is found in these regions (Berzas Nevado et al., 2010; Rodriguez Martin-Doimeadios et al., 2014; Arrifano et al., 2018b). Exposure detected in Tucuruí was higher than that presently observed in Tapajós region, confirming our preliminary data with this population (Arrifano et al., 2018b).
Therefore, in this scenario of mercury exposure, the possible advantage of carrying APOE4 would turn it on a disadvantage, with the presence of this allele implying an increased susceptibility to neurotoxicity (Godfrey et al., 2003; Wojcik et al., 2006; Ng et al., 2013, 2015; Woods et al., 2014; Snoj Tratnik et al., 2017). In our study, we found 247 individuals considered susceptible to mercury neurotoxicity, 215 with the 𝜀3/𝜀4 genotype and 32 with the 𝜀4/𝜀4 genotype. Association between the presence of APOE4 and the worsening of mercury intoxication (including symptoms such as poorer motor performance, memory, and learning) have been well-established in human studies (see Arrifano et al., 2018a for a review). However, the events underlying this strong correlation are not totally understood. Taking into account that both factors, APOE4 and exposure to mercury, share some similar molecular mechanisms, it was already proposed that ApoE4 would cause mainly toxicodynamic changes that could act in a synergistic way with the effects of mercury, increasing the injury and cell death (Arrifano et al., 2018a).
For the first time in Amazon, 59 individuals were identified with maximum risk showing mercury content in hair above 10 μg/g and the presence of ApoE4. Worryingly, the highest mercury content in hair found in the present work, 75.80 μg/g, was from an 𝜀4/𝜀4 individual. No difference was detected in allelic distribution of APOE between all participants with low and high levels of mercury (Table 5). Nevertheless, when the APOE4-carriers were compared to the APOE2-carriers we observed an interesting fact (Figure 3). When mercury exposure is below 10 μg/g, no difference in mercury levels is detected between APOE4 and APOE2-carriers; however, for individuals with high levels, mercury burden was significantly higher in APOE4 (Figure 3). Moreover, no association with an increased consumption in frequency or amount of fish meals in APOE4-carriers was detected (Table 6), eliminating the possibility that this bioaccumulation may be due to a higher intake of contaminated fish. Two conclusions can be reached based on our data: first, APOE4 and APOE2 are associated with different effects in mercury accumulation and second, the apparent pharmacokinetic influence would be of major importance with exposure above 10 μg/g.
To our knowledge, this is the first study with human populations demonstrating an association between the presence of APOE4 and an increased accumulation of mercury. These data seems to be in agreement with the hypothesis proposed by Pendergrass and Haley (1995) suggesting that ApoE4 would show a decreased ability to bind the metal when compared to ApoE2 isoform. The organs with constitutively high content in ApoE, such as CNS, would be especially affected by this reduced ability of ApoE4 of chelating mercury. This phenomenon may facilitate the presence of the free form of the metal, allowing it to remain available and to accumulate in CNS. This would explain the increased susceptibility of APOE4-carriers to neurotoxicity. Although additional studies in animal models are needed to definitively establish the causal relationship, our data have already demonstrated the prerequisite for the existence of this cause-effect in humans: the presence of an association between both factors. Therefore, in addition to the possible pharmacodynamic effect, the pharmacokinetic influence of ApoE would become a key element for the worse deleterious consequences of mercury exposure.
Conclusion
This work shows for the first time the genotypic and allelic profiles of APOE in Amazonian riverine populations, suggesting that the absence of 𝜀2/𝜀2 is a generalized phenomenon in Amazonian riverine populations and perhaps in the overall Amazon region. Our data support an association between APOE4 and the Amerindian genetic background in these populations. Fifty-nine individuals were identified at maximum risk with levels of mercury above 10 μg/g and the presence of APOE4. This study also supports that ApoE4, in addition to a possible pharmacodynamic effect, may influence pharmacokinetically the mercury exposure causing a higher mercury bioaccumulation, which may lead to later neurodegenerative diseases with aging. All this knowledge is essential to improve prevention strategies and health policy decision-making regarding these at-risk vulnerable populations.
Author Contributions
GA, MA-O, JS-M, BM, JA-L, JdN, RO, and MC-L discussed and conceptualized the work. GA, MA-O, JS-M, BM, LS-P, and MC-L participated in the expeditions of sample collection. RM-D, MJ-M, and SF-T quantified mercury levels. GA analyzed ApoE genotypes and alleles. MA, SS, and ÂR-d-S evaluated ancestry markers. GA, SS, and MC-L analyzed data. GA and MC-L wrote the initial draft of the manuscript and worked on subsequent revisions. GA, RM-D, MJ-M, MdO, JS-M, BM, JA-L, JdN, MA, SS, ÂR-d-S, LS-P, RO, and MC-L worked on revising the manuscript.
Funding
This work was supported by Conselho Nacional de Ciência e Tecnologia em Pesquisa (CNPq, Brazil; Grant Nos. 467143/2014-5, 447568/2014-0, and 307564/2017-7), Pró-Reitoria de Pesquisa da Universidade Federal do Pará (PROPESP-UFPA, Brazil), Ministerio de Economía y Competitividad (MINECO, Spain; Grant Nos. CTQ-2013-48411-P and CTQ2016-78793-P), and Coordenação de Aperfeiçoamento de Pessoal de Nivel Superior (CAPES, Brazil). GA, JdN, ÂR-d-S, SS, and MC-L thank CNPq for their research fellowships. Also, MA-O thanks CAPES for his Ph.D. fellowship. SF-T thanks JCCM for his Ph.D. fellowship (Grant No. SBPLY/16/180501/000356).
Conflict of Interest Statement
The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.
Acknowledgments
We are truly grateful to the health staff, community leaders and all participants of the communities for their warm, welcome, and essential support of this study. Also, the team of Radio Tucuruí and Secretaría de Saúde do Municipio de Tucuruí are sincerely acknowledged for their valuable help.
Supplementary Material
The Supplementary Material for this article can be found online at: https://www.frontiersin.org/articles/10.3389/fgene.2018.00285/full#supplementary-material
Footnotes
References
Andreoli, V., and Sprovieri, F. (2017). Genetic aspects of susceptibility to mercury toxicity: an overview. Int. J. Environ. Res. Public Health 14:93. doi: 10.3390/ijerph14010093
Arrifano, G. P. F., de Oliveira, M. A., Souza-Monteiro, J. R., Paraense, R. O., Ribeiro-Dos-Santos, A., Vieira, J., et al. (2018a). Role for apolipoprotein E in neurodegeneration and mercury intoxication. Front. Biosci. 10, 229–241.
Arrifano, G. P. F., Martin-Doimeadios, R. C. R., Jimenez-Moreno, M., Ramirez-Mateos, V., da Silva, N. F. S., Souza-Monteiro, J. R., et al. (2018b). Large-scale projects in the amazon and human exposure to mercury: the case-study of the Tucurui dam. Ecotoxicol. Environ. Saf. 147, 299–305. doi: 10.1016/j.ecoenv.2017.08.048
Ashe, K. (2012). Elevated mercury concentrations in humans of Madre de Dios. Peru. PLoS One 7:e33305. doi: 10.1371/journal.pone.0033305
Barbosa, A. C., Silva, S. R., and Dorea, J. G. (1998). Concentration of mercury in hair of indigenous mothers and infants from the Amazon basin. Arch. Environ. Contam. Toxicol. 34, 100–105. doi: 10.1007/s002449900291
Barcelos, G. R., Grotto, D., de Marco, K. C., Valentini, J., Lengert, A., de Oliveira, A. A., et al. (2013). Polymorphisms in glutathione-related genes modify mercury concentrations and antioxidant status in subjects environmentally exposed to methylmercury. Sci. Total Environ. 46, 319–325. doi: 10.1016/j.scitotenv.2013.06.029
Barcelos, G. R., Souza, M. F., Oliveira, A. A., Lengert, A., Oliveira, M. T., Camargo, R. B., et al. (2015). Effects of genetic polymorphisms on antioxidant status and concentrations of the metals in the blood of riverside amazonian communities co-exposed to Hg and Pb. Environ. Res. 138, 224–232. doi: 10.1016/j.envres.2015.02.017
Bertram, L. (2009). Alzheimer’s disease genetics current status and future perspectives. Int. Rev. Neurobiol. 84, 167–184. doi: 10.1016/S0074-7742(09)00409-7
Berzas Nevado, J. J., Rodriguez Martin-Doimeadios, R. C., Guzman Bernardo, F. J., Jimenez Moreno, M., Herculano, A. M., do Nascimento, J. L., et al. (2010). Mercury in the Tapajos River basin. Environ. Int. 36, 593–608. doi: 10.1016/j.envint.2010.03.011
Cavalcante, L. N., Stefano, J. T., Machado, M. V., Mazo, D. F., Rabelo, F., Sandes, K. A., et al. (2015). Genetic ancestry analysis in non-alcoholic fatty liver disease patients from Brazil and Portugal. World J. Hepatol. 7, 1433–1438. doi: 10.4254/wjh.v7.i10.1433
Chin-Chan, M., Navarro-Yepes, J., and Quintanilla-Vega, B. (2015). Environmental pollutants as risk factors for neurodegenerative disorders: alzheimer and parkinson diseases. Front. Cell. Neurosci. 9:124. doi: 10.3389/fncel.2015.00124
Corbo, R. M., and Scacchi, R. (1999). Apolipoprotein E (APOE) allele distribution in the world. Is APOE∗4 a ’thrifty’ allele? Ann. Hum. Genet. 63(Pt 4), 301–310.
Costa, J. M. F. J., Lima, A., Rodrigues, D. J., Khoury, E. D. T., Souza, G. D. S., Silveira, L. C. L., et al. (2017). Emotional and motor symptoms in riverside dwellers exposed to mercury in the Amazon. Rev. Bras. Epidemiol. 20, 212–224. doi: 10.1590/1980-5497201700020003
Coutinho, W. F., and Silva Junior, W. S. (2015). Diabetes care in Brazil. Ann. Glob. Health 81, 735–741. doi: 10.1016/j.aogh.2015.12.010
Crespo-Lopez, M. E., Costa-Malaquias, A., Oliveira, E. H., Miranda, M. S., Arrifano, G. P., Souza-Monteiro, J. R., et al. (2016). Is low non-lethal concentration of methylmercury really safe? PLoS One 11:e0162822. doi: 10.1371/journal.pone.0162822
Crespo-Lopez, M. E., Macedo, G. L., Arrifano, G. P., Pinheiro Mda, C., do Nascimento, J. L., and Herculano, A. M. (2011). Genotoxicity of mercury: contributing for the analysis of amazonian populations. Environ. Int. 37, 136–141. doi: 10.1016/j.envint.2010.08.009
Crews, D. E., Kamboh, M. I., Mancilha-Carvalho, J. J., and Kottke, B. (1993). Population genetics of apolipoprotein A-4. Hum. Biol. 65, 211–224.
da Silva, Souza, A., de Almeida Goncalves, Sachett, J., Alcantara, J. A., Freire, M., et al. (2018). Snakebites as cause of deaths in the Western Brazilian Amazon: why and who dies? Toxicon 145, 15–24. doi: 10.1016/j.toxicon.2018.02.041
Da Silva-Junior, F. M. R., Oleinski, R. M., Azevedo, A. E. S., Monroe, K., Dos Santos, M., Da Silveira, T. B., et al. (2017). Vulnerability associated with ”symptoms similar to those of mercury poisoning” in communities from Xingu River, Amazon basin. Environ. Geochem. Health 40, 1145–1154. doi: 10.1007/s10653-017-9993-7
de Oliveira, A. A., de Souza, M. F., Lengert, A., de Oliveira, M. T., Camargo, R. B., Braga, G. U., et al. (2014). Genetic polymorphisms in glutathione (GSH-) related genes affect the plasmatic Hg/whole blood Hg partitioning and the distribution between inorganic and methylmercury levels in plasma collected from a fish-eating population. Biomed. Res. Int. 2014:940952. doi: 10.1155/2014/940952
Dolbec, J., Mergler, D., Sousa Passos, C. J., Sousa, de Morais, S., and Lebel, J. (2000). Methylmercury exposure affects motor performance of a riverine population of the Tapajos river. Int. Arch. Occup. Environ. Health 73, 195–203. doi: 10.1007/s004200050027
Drescher, O., Dewailly, E., Diorio, C., Ouellet, N., Sidi, E. A., Abdous, B., et al. (2014). Methylmercury exposure. J. Expo. Sci. Environ. Epidemiol. 24, 608–614. doi: 10.1038/jes.2013.96
Dufour, D. L., Piperata, B. A., Murrieta, R. S., Wilson, W. M., and Williams, D. D. (2016). Amazonian foods and implications for human biology. Ann. Hum. Biol. 43, 330–348. doi: 10.1080/03014460.2016.1196245
Eisenberg, D. T., Kuzawa, C. W., and Hayes, M. G. (2010). Worldwide allele frequencies of the human apolipoprotein E gene: climate, local adaptations, and evolutionary history. Am. J. Phys. Anthropol. 143, 100–111. doi: 10.1002/ajpa.21298
Farina, M., Avila, D. S., da Rocha, J. B., and Aschner, M. (2013). Metals, oxidative stress and neurodegeneration: a focus on iron, manganese and mercury. Neurochem. Int. 62, 575–594. doi: 10.1016/j.neuint.2012.12.006
Farina, M., Rocha, J. B., and Aschner, M. (2011). Mechanisms of methylmercury-induced neurotoxicity: evidence from experimental studies. Life Sci. 89, 555–563. doi: 10.1016/j.lfs.2011.05.019
Fearnside, P. M. (2015). Amazon dams and waterways: Brazil’s Tapajos Basin plans. Ambio 44, 426–439. doi: 10.1007/s13280-015-0642-z
Fillion, M., Lemire, M., Philibert, A., Frenette, B., Weiler, H. A., Deguire, J. R., et al. (2011a). Visual acuity in fish consumers of the Brazilian Amazon: risks and benefits from local diet. Public Health Nutr. 14, 2236–2244. doi: 10.1017/S1368980011001765
Fillion, M., Mergler, D., Sousa Passos, C. J., Larribe, F., Lemire, M., and Guimaraes, J. R. (2006). A preliminary study of mercury exposure and blood pressure in the Brazilian Amazon. Environ. Health 5:29. doi: 10.1186/1476-069X-5-29
Fillion, M., Philibert, A., Mertens, F., Lemire, M., Passos, C. J., Frenette, B., et al. (2011b). Neurotoxic sequelae of mercury exposure: an intervention and follow-up study in the Brazilian Amazon. Ecohealth 8, 210–222. doi: 10.1007/s10393-011-0710-1
Godfrey, M. E., Wojcik, D. P., and Krone, C. A. (2003). Apolipoprotein E genotyping as a potential biomarker for mercury neurotoxicity. J. Alzheimers Dis. 5, 189–195. doi: 10.3233/JAD-2003-5303
Gomes, R., Nascimento, E. F., and Araujo, F. C. (2007). [Why do men use health services less than women? Explanations by men with low versus higher education] Cad. Saude Publica 23, 565–574. doi: 10.1590/S0102-311X2007000300015
Grandjean, P., Weihe, P., White, R. F., Debes, F., Araki, S., Yokoyama, K., et al. (1997). Cognitive deficit in 7-year-old children with prenatal exposure to methylmercury. Neurotoxicol. Teratol. 19, 417–428. doi: 10.1016/S0892-0362(97)00097-4
Grandjean, P., White, R. F., Nielsen, A., Cleary, D., and de Oliveira Santos, E. C. (1999). Methylmercury neurotoxicity in Amazonian children downstream from gold mining. Environ. Health Perspect. 107, 587–591. doi: 10.1289/ehp.99107587
Hacon, S. S., Dorea, J. G., Fonseca Mde, F., Oliveira, B. A., Mourao, D. S., Ruiz, C. M., et al. (2014). The influence of changes in lifestyle and mercury exposure in riverine populations of the Madeira River (Amazon Basin) near a hydroelectric project. Int. J. Environ. Res. Public Health 11, 2437–2455. doi: 10.3390/ijerph110302437
Harada, M., Nakachi, S., Cheu, T., Hamada, H., Ono, Y., Tsuda, T., et al. (1999). Monitoring of mercury pollution in Tanzania: relation between head hair mercury and health. Sci. Total Environ. 227, 249–256. doi: 10.1016/S0048-9697(99)00031-5
Hoshino, A., Pacheco-Ferreira, H., Sanches, S. G., Carvallo, R., Cardoso, N., Perez, M., et al. (2015). Mercury exposure in a riverside Amazon population. Int. Arch. Otorhinolaryngol. 19, 135–140. doi: 10.1055/s-0034-1544115
IBGE (2016). Available at: http://www.ibge.gov.br/home/estatistica/populacao/estimativa2016/default.shtm
Jacob-Ferreira, A. L., Lacchini, R., Gerlach, R. F., Passos, C. J., Barbosa, F. Jr., and Tanus-Santos, J. E. (2011). A common matrix metalloproteinase (MMP)-2 polymorphism affects plasma MMP-2 levels in subjects environmentally exposed to mercury. Sci. Total Environ. 409, 4242–4246. doi: 10.1016/j.scitotenv.2011.07.013
Jacob-Ferreira, A. L., Passos, C. J., Gerlach, R. F., Barbosa, F. Jr., and Tanus-Santos, J. E. (2010). A functional matrix metalloproteinase (MMP)-9 polymorphism modifies plasma MMP-9 levels in subjects environmentally exposed to mercury. Sci. Total Environ. 408, 4085–4092. doi: 10.1016/j.scitotenv.2010.05.036
Jaramillo-Correa, J. P., Keyeux, G., Ruiz-Garcia, M., Rodas, C., and Bernal, J. (2001). Population genetic analysis of the genes APOE. Hum. Hered. 52, 14–33. doi: 10.1159/000053351
Khoury, E. D., Souza Gda, S., da Costa, C. A., de Araujo, A. A., de Oliveira, C. S., Silveira, L. C., et al. (2015). Somatosensory psychophysical losses in inhabitants of riverside communities of the Tapajos River Basin. PLoS One 10:e0144625. doi: 10.1371/journal.pone.0144625
Klautau-Guimarães, M. D. N., D’Ascenção, R., Caldart, F. A., Grisolia, C. K., Souza, J. R. D., Barbosa, A. C., et al. (2005). Analysis of genetic susceptibility to mercury contamination evaluated through molecular biomarkers in at-risk Amazon amerindian populations. Genet. Mol. Biol. 28, 827–832. doi: 10.1590/S1415-47572005000500027
Krewer, C. C., Ribeiro, E. E., Ribeiro, E. A., Moresco, R. N., da Rocha, M. I., Montagner, G. F., et al. (2011). Habitual intake of guarana and metabolic morbidities: an epidemiological study of an elderly Amazonian population. Phytother. Res. 25, 1367–1374. doi: 10.1002/ptr.3437
Langeland, A. L., Hardin, R. D., and Neitzel, R. L. (2017). Mercury levels in human hair and farmed fish near Artisanal and small-scale gold mining communities in the Madre de Dios River Basin, Peru. Int. J. Environ. Res. Public Health 14:E302. doi: 10.3390/ijerph14030302
Lins, T. C., Vieira, R. G., Abreu, B. S., Grattapaglia, D., and Pereira, R. W. (2010). Genetic composition of Brazilian population samples based on a set of twenty-eight ancestry informative SNPs. Am. J. Hum. Biol. 22, 187–192. doi: 10.1002/ajhb.20976
Mahley, R. W., and Rall, S. C. Jr. (1999). Is epsilon4 the ancestral human apoE allele? Neurobiol. Aging 20, 429–430. doi: 10.1016/S0197-4580(99)00081-0
Mahley, R. W., Weisgraber, K. H., and Huang, Y. (2009). Apolipoprotein E: structure determines function, from atherosclerosis to Alzheimer’s disease to AIDS. J. Lipid Res. 50(Suppl.), S183–S188. doi: 10.1194/jlr.R800069-JLR200
Marin, G. B., Tavella, M. H., Guerreiro, J. F., Santos, S. E. B., and Zago, M. A. (1997). Absence of the E2 allele of apolipoprotein in Amerindians. Braz. J. Genet. 20, 741–743. doi: 10.1590/S0100-84551997000400029
Marques, R. C., Abreu, L., Bernardi, J. V., and Dorea, J. G. (2016). Traditional living in the Amazon: extended breastfeeding, fish consumption, mercury exposure and neurodevelopment. Ann. Hum. Biol. 43, 360–370. doi: 10.1080/03014460.2016.1189962
Marques, R. C., Bernardi, J. V., Dorea, J. G., Brandao, K. G., Bueno, L., Leao, R. S., et al. (2013). Fish consumption during pregnancy, mercury transfer, and birth weight along the Madeira River Basin in Amazonia. Int. J. Environ. Res. Public Health 10, 2150–2163. doi: 10.3390/ijerph10062150
Marques, R. C., Dorea, J. G., McManus, C., Leao, R. S., Brandao, K. G., Vieira, I. H., et al. (2011). Hydroelectric reservoir inundation (Rio Madeira Basin, Amazon) and changes in traditional lifestyle: impact on growth and neurodevelopment of pre-school children. Public Health Nutr. 14, 661–669. doi: 10.1017/S136898001000248X
Muzaka, V. (2017). Lessons from Brazil: on the difficulties of building a universal health care system. J. Glob. Health 7:010303. doi: 10.7189/jogh.07.010303
Ng, S., Lin, C. C., Hwang, Y. H., Hsieh, W. S., Liao, H. F., and Chen, P. C. (2013). Mercury, APOE, and children’s neurodevelopment. Neurotoxicology 37, 85–92. doi: 10.1016/j.neuro.2013.03.012
Ng, S., Lin, C. C., Jeng, S. F., Hwang, Y. H., Hsieh, W. S., and Chen, P. C. (2015). Mercury, APOE, and child behavior. Chemosphere 120, 123–130. doi: 10.1016/j.chemosphere.2014.06.003
Parra, F. C., Amado, R. C., Lambertucci, J. R., Rocha, J., Antunes, C. M., and Pena, S. D. (2003). Color and genomic ancestry in Brazilians. Proc. Natl. Acad. Sci. U.S.A. 100, 177–182. doi: 10.1073/pnas.0126614100
Passos, C. J., Da Silva, D. S., Lemire, M., Fillion, M., Guimaraes, J. R., Lucotte, M., et al. (2008). Daily mercury intake in fish-eating populations in the Brazilian Amazon. J. Expo. Sci. Environ. Epidemiol. 18, 76–87. doi: 10.1038/sj.jes.7500599
Passos, C. J., Mergler, D., Fillion, M., Lemire, M., Mertens, F., Guimaraes, J. R., et al. (2007). Epidemiologic confirmation that fruit consumption influences mercury exposure in riparian communities in the Brazilian Amazon. Environ. Res. 105, 183–193. doi: 10.1016/j.envres.2007.01.012
Pendergrass, J. C., and Haley, B. E. (1995). “Mercury-EDTA complex specifically blocks brain beta-tubulin-gtp interactions: similarity to observations in Alzheimer’s disease. status quo and perspective of Amalgam and other dental materials,” in Proceedings of the International Symposium, ed. G. N. Schrauzer (Stuttgart: Georg Thieme Verlag), 98–105.
Pinheiro, M. C., Crespo-Lopez, M. E., Vieira, J. L., Oikawa, T., Guimaraes, G. A., Araujo, C. C., et al. (2007). Mercury pollution and childhood in Amazon riverside villages. Environ. Int. 33, 56–61. doi: 10.1016/j.envint.2006.06.024
Piperata, B. A. (2007). Nutritional status of Ribeirinhos in Brazil and the nutrition transition. Am. J. Phys. Anthropol. 133, 868–878. doi: 10.1002/ajpa.20579
Piperata, B. A., Spence, J. E., Da-Gloria, P., and Hubbe, M. (2011). The nutrition transition in Amazonia: rapid economic change and its impact on growth and development in ribeirinhos. Am. J. Phys. Anthropol. 146, 1–13. doi: 10.1002/ajpa.21459
Ramos, B. R., Mendes, N. D., Tanikawa, A. A., Amador, M. A., dos Santos, N. P., dos Santos, S. E., et al. (2016). Ancestry informative markers and selected single nucleotide polymorphisms in immunoregulatory genes on preterm labor and preterm premature rupture of membranes: a case control study. BMC Pregnancy Childbirth 16:30. doi: 10.1186/s12884-016-0823-1
Rocha, A. V., Rita Cardoso, B., Zavarize, B., Almondes, K., Bordon, I., Hare, D. J., et al. (2016). GPX1 Pro198Leu polymorphism and GSTM1 deletion do not affect selenium and mercury status in mildly exposed Amazonian women in an urban population. Sci. Total Environ. 571, 801–808. doi: 10.1016/j.scitotenv.2016.07.054
Rodrigues, A. R., Souza, C. R., Braga, A. M., Rodrigues, P. S., Silveira, A. T., Damin, E. T., et al. (2007). Mercury toxicity in the Amazon: contrast sensitivity and color discrimination of subjects exposed to mercury. Braz. J. Med. Biol. Res. 40, 415–424. doi: 10.1590/S0100-879X2007000300018
Rodriguez Martin-Doimeadios, R. C., Berzas Nevado, J. J., Guzman Bernardo, F. J., Jimenez Moreno, M., Arrifano, G. P., Herculano, A. M., et al. (2014). Comparative study of mercury speciation in commercial fishes of the Brazilian Amazon. Environ. Sci. Pollut. Res. Int. 21, 7466–7479. doi: 10.1007/s11356-014-2680-7
Salazar-Camacho, C., Salas-Moreno, M., Marrugo-Madrid, S., Marrugo-Negrete, J., and Diez, S. (2017). Dietary human exposure to mercury in two artisanal small-scale gold mining communities of northwestern Colombia. Environ. Int. 107, 47–54. doi: 10.1016/j.envint.2017.06.011
Sheehan, M. C., Burke, T. A., Navas-Acien, A., Breysse, P. N., McGready, J., and Fox, M. A. (2014). Global methylmercury exposure from seafood consumption and risk of developmental neurotoxicity: a systematic review. Bull. World Health Organ. 92, 254F–269F. doi: 10.2471/BLT.12.116152
Singh, P. P., Singh, M., and Mastana, S. S. (2006). APOE distribution in world populations with new data from India and the UK. Ann. Hum. Biol. 33, 279–308. doi: 10.1080/03014460600594513
Snoj Tratnik, J., Falnoga, I., Trdin, A., Mazej, D., Fajon, V., Miklavcic, A., et al. (2017). Prenatal mercury exposure, neurodevelopment and apolipoprotein E genetic polymorphism. Environ. Res. 152, 375–385. doi: 10.1016/j.envres.2016.08.035
Strain, J. J., Yeates, A. J., van Wijngaarden, E., Thurston, S. W., Mulhern, M. S., McSorley, E. M., et al. (2015). Prenatal exposure to methyl mercury from fish consumption and polyunsaturated fatty acids: associations with child development at 20 mo of age in an observational study in the Republic of Seychelles. Am. J. Clin. Nutr. 101, 530–537. doi: 10.3945/ajcn.114.100503
Trumble, B. C., Stieglitz, J., Blackwell, A. D., Allayee, H., Beheim, B., Finch, C. E., et al. (2017). Apolipoprotein E4 is associated with improved cognitive function in Amazonian forager-horticulturalists with a high parasite burden. FASEB J. 31, 1508–1515. doi: 10.1096/fj.201601084R
Valentini, J., Passos, C. J. S., Garcia, S. C., Davidson, R., Lucotte, M., Mertens, F., et al. (2016). Blood antioxidant nutrients in riparian villagers of the Brazilian Amazon: its associations with wet/dry seasons and modulation by sociodemographic determinants. Cad. Saúde Colet. 24, 21–31. doi: 10.1590/1414-462X201500040159
Wasserman, J. C., Hacon, S., and Wasserman, M. A. (2003). Biogeochemistry of mercury in the Amazonian environment. Ambio 32, 336–342. doi: 10.1579/0044-7447-32.5.336
Wojcik, D. P., Godfrey, M. E., Christie, D., and Haley, B. E. (2006). Mercury toxicity presenting as chronic fatigue, memory impairment and depression: diagnosis, treatment, susceptibility, and outcomes in a New Zealand general practice setting (1994-2006). Neuro Endocrinol. Lett. 27, 415–423.
Woods, J. S., Heyer, N. J., Russo, J. E., Martin, M. D., and Farin, F. M. (2014). Genetic polymorphisms affecting susceptibility to mercury neurotoxicity in children: summary findings from the casa pia children’s amalgam clinical trial. Neurotoxicology 44, 288–302. doi: 10.1016/j.neuro.2014.07.010
Keywords: ApoE, Tapajós, Tucuruí, human, methylmercury, ancestry, allele, genotype
Citation: Arrifano GPF, Martín-Doimeadios RCR, Jiménez-Moreno M, Fernández-Trujillo S, Augusto-Oliveira M, Souza-Monteiro JR, Macchi BM, Alvarez-Leite JI, do Nascimento JLM, Amador MT, Santos S, Ribeiro-dos-Santos Â, Silva-Pereira LC, Oriá RB and Crespo-Lopez ME (2018) Genetic Susceptibility to Neurodegeneration in Amazon: Apolipoprotein E Genotyping in Vulnerable Populations Exposed to Mercury. Front. Genet. 9:285. doi: 10.3389/fgene.2018.00285
Received: 29 March 2018; Accepted: 10 July 2018;
Published: 27 July 2018.
Edited by:
Joanna A. Ruszkiewicz, Albert Einstein College of Medicine, United StatesReviewed by:
Bensu Karahalil, Gazi University, TurkeyCristiane Lenz Dalla Corte, Federal University of Pampa, Brazil
Copyright © 2018 Arrifano, Martín-Doimeadios, Jiménez-Moreno, Fernández-Trujillo, Augusto-Oliveira, Souza-Monteiro, Macchi, Alvarez-Leite, do Nascimento, Amador, Santos, Ribeiro-dos-Santos, Silva-Pereira, Oriá and Crespo-Lopez. This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
*Correspondence: Maria E. Crespo-Lopez, maria.elena.crespo.lopez@gmail.com; ecrespo@ufpa.br