Molecular epidemiologic evidence for diabetogenic effects of dioxin exposure in U.S. Air Force veterans of the Vietnam war.BACKGROUND: One of the outcomes positively associated with dioxin exposure in humans is type 2 diabetes type 2 diabetes n. See diabetes mellitus. . OBJECTIVES: This study was conducted in order to find the molecular biological evidence for the diabetogenic action of dioxin in adipose adipose /ad·i·pose/ (ad´i-pos) 1. fatty. 2. the fat present in the cells of adipose tissue. ad·i·pose adj. Of, relating to, or composed of animal fat; fatty. samples from Vietnam veterans. METHODS: We obtained 313 adipose tissue adipose tissue (ăd`əpōs'): see connective tissue. adipose tissue or fatty tissue Connective tissue consisting mainly of fat cells, specialized to synthesize and contain large globules of fat, within a samples both from Vietnam veterans who were exposed to dioxin (Operation Ranch Hand Operation Ranch Hand was a U.S. Military operation during part of the Vietnam War, lasting from 1962 until 1971. It involved spraying an estimated 19 million US gallons of defoliants over rural areas of South Vietnam in an attempt to deprive the Viet Cong of ) and from comparison veterans who served in Southeast Asia with no record of dioxin exposure. We conducted quantitative reverse-transcribed polymerase chain reaction polymerase chain reaction (pŏl`ĭmərās') (PCR), laboratory process in which a particular DNA segment from a mixture of DNA chains is rapidly replicated, producing a large, readily analyzed sample of a piece of DNA; the process is studies on selected marker mRNAs from these samples. RESULTS: We found the most sensitive and reliable molecular indicator of dioxin-induced diabetes to be the ratio of mRNA of glucose transporter 4 (GLUT4) and nuclear transcription factor kappa B (NF[kappa]B), a marker of inflammation. This ratio showed significant correlations to serum dioxin residues and to fasting glucose fasting glucose Fasting blood sugar, fasting plasma glucose Endocrinology Glucose obtained from a Pt who has had nothing–except water by mouth for 8+ hrs; FG is used in evaluating Pts for possible DM Ref range 65-115 mg/dL non-diabetic; 110-140 mg/dL, among those in the Ranch Hand group and, surprisingly, even in the comparison group, who have low levels of dioxin comparable to the general public. Such a correlation in the comparison group was particularly significant among those with known risk factors such as obesity and family history of diabetes. CONCLUSIONS: These results show that the GLUT4:NF[kappa]B ratio is a reliable marker for the diabetogenic action of dioxin, particularly at very low exposure levels that are not much higher than those found in the general public, implying a need to address current exposure levels. KEY WORDS: adipose tissue, Agent Orange, biological markers, diabetes, fasting glucose, glucose transporter type 4, inflammation, molecular epidemiology molecular epidemiology Molecular medicine An evolving field that combines the tools of standard epidemiology–case studies, questionnaires and monitoring of exposure to external factors with the tools of molecular biology–eg, restriction endonucleases, , NF[kappa]B, tetrachlorodibenzodioxin. Environ Health Perspect 114:1677-1683 (2006). doi:10.1289/ehp.9262 available via http://dx.doi.org/[Online 3 August 2006] ********** Many veterans of the Vietnam War Vietnam War, conflict in Southeast Asia, primarily fought in South Vietnam between government forces aided by the United States and guerrilla forces aided by North Vietnam. were exposed to 2,3,7,8-tetrachlorodibenzo-p-dioxin (TCDD or dioxin), which was present as a contaminant contaminant /con·tam·i·nant/ (kon-tam´in-int) something that causes contamination. contaminant something that causes contamination. in the herbicide formulation Agent Orange [Booker 2001; Institute of Medicine (IOM IOM See: Index and Option Market ) 2000, 2003]. Indeed, significant residues of dioxin have been found in their serum, even after many years, attesting to the fact of their initial exposure and to the long half-life of dioxin, which is estimated to be 7.6 years (95% confidence interval confidence interval, n a statistical device used to determine the range within which an acceptable datum would fall. Confidence intervals are usually expressed in percentages, typically 95% or 99%. , 7.0-8.2 years) (Michalek and Tripathi 1999). Those dioxin residue levels are relatively high among veterans of Operation Ranch Hand (ORH ORH Worcester (Airport) ORH Operation Restore Hope ORH Worcester, MA, USA - Worcester /James D O'Brien Field (Airport Code) ) (Michalek and Tripathi 1999), the operation responsible for the handling and the actual aerial spraying of Agent Orange and other dioxin-contaminated herbicides in Vietnam from 1962 to 1971. Because of the health implications, many epidemiologic studies have been conducted to identify the possible harmful effects of dioxin on exposed veterans (Frumkin 2003; IOM 2000). Among the recent findings, one of the most consistently identified diseases statistically associated with dioxin exposure is type 2 diabetes mellitus Type 2 diabetes mellitus One of the two major types of diabetes mellitus, characterized by late age of onset (30 years or older), insulin resistance, high levels of blood sugar, and little or no need for supple-mental insulin. (Henriksen et al.1997; Michalek et al. 1999). This conclusion is also supported by the results of similar epidemiologic studies such as those of the population exposed to high levels of dioxin in Seveso, Italy (Bertazzi et al. 1998; Pesatori et al. 2003), industrial workers (Vena et al. 1998), and Korean Vietnam veterans who were also exposed to Agent Orange (Kim et al. 2003). Despite the epidemiologic evidence for the positive correlation, it has been difficult to explain the mechanistic basis of action of dioxin in causing type 2 diabetes in humans. Because the actual levels of dioxin residues among U.S. veterans are not as high as those of the Seveso population (Bertazzi et al. 1998) or the industrially exposed cohort (Vena et al. 1998) and because small amounts of dioxin and dioxin-type chemicals are also found among general populations in industrialized in·dus·tri·al·ize v. in·dus·tri·al·ized, in·dus·tri·al·iz·ing, in·dus·tri·al·iz·es v.tr. 1. To develop industry in (a country or society, for example). 2. nations, some scientists question the cause-effect relationship between dioxin residues in humans and an increased incidence of diabetes (Remillard and Bunce n. 1. a sudden unexpected piece of good fortune. Noun 1. bunce - a sudden happening that brings good fortune (as a sudden opportunity to make money); "the demand for testing has created a boom for those unregulated laboratories where boxes of 2002). To address this important environmental health question, we conducted a molecular epidemiologic study on the state of expression of selected biomarkers in adipose tissue samples from participants in the Air Force Health Study. The Air Force Health Study was designed to determine whether veterans of ORH experienced adverse health effects and whether those health effects, if they exist, can be attributed to exposure to herbicides or their dioxin contaminant (Wolfe et al. 1990). The ORH veterans were exposed to herbicides during flight operations, herbicide preparation, and maintenance of the aircraft and herbicide spray equipment. The examination content of the Air Force Health Study emphasized detection of medical end points suspected of being associated with exposure to dioxin, so extensive data on health status and health behaviors were collected on ORH veterans and a matched comparison group of background-exposed veterans. Adipose tissue was selected for study because of its significant role in the etiology of type 2 diabetes (Scheen 2003). Type 1 diabetes type 1 diabetes n. See diabetes mellitus. , considered genetic with onset at an early age, was not included as an end point in the Air Force Health Study protocol and so was not considered in this study. We hypothesized two possible pathways for TCDD-induced glucose intolerance. In one pathway involving oncogenes oncogenes 1. genes carried by tumor viruses that are directly and solely responsible for the neoplastic transformation of host cells. Many oncogenes function after integration into the DNA of the host cell and some up-regulate normal downstream host cell genes to cause neoplasia. , Src [GenBank accession no. M16243 (GenBank 2006)], would activate MYC (GenBank accession no. V00568; Jahner and Hunter 1991), which is a direct controller of CCAAT/enhancer binding protein-[alpha] (C/EBP[alpha]; GenBank accession no. NM_004364; Freytag and Geddes 1992). Src is known to be essential for TCDD-induced wasting in mice (Dunlap et al. 2002), and C/EBP[alpha] is a master switch for adipocytes that causes the up-regulation of lipid accumulation processes (MacDougald and Lane 1995). In the other pathway, which involves inflammation, there would be increased production of the cytokine Cytokine Any of a group of soluble proteins that are released by a cell to send messages which are delivered to the same cell (autocrine), an adjacent cell (paracrine), or a distant cell (endocrine). tumor necrosis tumor necrosis Death of tumor tissue, a common event in aggressive CAs in which the tumor rapidly outgrows its blood supply, resulting in tumor cell death. Cf Apoptosis. factor-[alpha] (TNF-[alpha]; GenBank accession no. NM_000594), one of the major mediators of dioxin-induced cell inflammatory reactions (Alsharif et al. 1994; Kern et al. 2002; Matsumura 2003; Taylor et al. 1992). TNF-[alpha] is produced by adipocytes also in response to obesity, causing increased expression of the transcription factor NF[kappa]B, and leading eventually to down-regulation of the insulin receptor insulin receptor A heterodimeric membrane receptor composed of α and β chains, which has tyrosine kinase activity after binding insulin; IR deficiency is a rare cause of DM and may be due to a gene rearrangement, causing a deletion in the and the major insulin-responsive glucose transporter GLUT4 (Halle et al. 1998). To test the contributions of each pathway we measured mRNA expression of the genes c-Src, C/EBP[alpha], NF[kappa]B, and GLUT4 in adipose tissue. In addition we measured GAPDH GAPDH Glyceraldehyde-3-Phosphate Dehydrogenase (also seen as G3PDH) , a housekeeping gene (Gorzelniak et al. 2001), for use as a normalization In relational database management, a process that breaks down data into record groups for efficient processing. There are six stages. By the third stage (third normal form), data are identified only by the key field in their record. standard to correct for differences in cDNA synthesis efficiency. Materials and Methods The details of basic study design and subject selection have been published previously (Wolfe et al. 1990). The Air Force Health Study compares the health, mortality experience, and reproductive outcomes of ORH veterans with a comparison group of other Air Force veterans who served in Southeast Asia during the same period (1962-1971) the ORH unit was active but who were not involved with spraying herbicides. Comparison veterans were matched to ORH veterans on date of birth, race (black, nonblack non·black or non-Black or non-black n. A person who is not Black. non·black  adj. ), and military occupation (officer pilot, officer
navigator, nonflying officer, enlisted flyer, enlisted ground crew).
Periodic physical examinations and in-person interviews were conducted
in 1982, 1985, 1987, 1992, 1997, and 2002-2003. The methods used in
these studies were approved by the institutional review boards at the
participating medical treatment facilities. Participation was voluntary,
and informed consent was given by subjects at the examination sites.
Dioxin in serum collected from the veterans in 1987 and 1992 was measured by the Centers for Disease Control and Prevention Centers for Disease Control and Prevention (CDC), agency of the U.S. Public Health Service since 1973, with headquarters in Atlanta; it was established in 1946 as the Communicable Disease Center. using high-resolution gas chromatography/high resolution mass spectrometry mass spectrometry or mass spectroscopy Analytic technique by which chemical substances are identified by sorting gaseous ions by mass using electric and magnetic fields. (Patterson et al. 1987). The between-assay coefficient of variation Coefficient of Variation A measure of investment risk that defines risk as the standard deviation per unit of expected return. at three different concentrations of dioxin ranged from 9.4% to 15.5%. For those veterans whose serum dioxin level was below the limit of detection, we assigned a level equal to the detection limit divided by the square root of 2 (Hornung and Reed 1990). Dioxin results were expressed in parts per trillion on a serum lipid serum lipid Any major lipid in the circulation–total cholesterol, HDL, LDL, TGs. See Cholesterol, Triglyceride. weight basis. Fasting glucose (milligrams per deciliter deciliter /dec·i·li·ter/ (dL) (des´i-le?ter) one tenth (10minus;1) of a liter; 100 milliliters. Deciliter (dL) 100 cubic centimeters (cc). Mentioned in: Hypercholesterolemia ) was determined with Paramax equipment (model 720 ZX; Baxter Scientific Instruments, Deerfield, IL). Body mass index (BMI BMI body mass index. BMI abbr. body mass index Body mass index (BMI) A measurement that has replaced weight as the preferred determinant of obesity. ) was defined as weight divided by the square of height, and percent body fat (PBF PBF Perry Bible Fellowship (online comic; also seen as TPBF) PBF Pretty Boy Floyd (Floyd Mayweather, boxer) PBF Play-By-Forum (game) PBF Power Burst Facility PBF Percent Body Fat ) was defined as (1.264 x BMI) - 13.305 (Knapik et al. 1983). Before the commencement of the 1997 physical examination, 650 veterans were randomly selected according to a four-way factorial factorial For any whole number, the product of all the counting numbers up to and including itself. It is indicated with an exclamation point: 4! (read “four factorial”) is 1 × 2 × 3 × 4 = 24. defined by service group (ORH, comparison), diabetic status (diabetic, nondiabetic), age (young, born during or after 1942; old, born before 1942), and body fat (lean, PBF [less than or equal to] 25; obese, PBF > 25) from those who had been compliant in the 1992 examination (n = 2,233) after excluding those who had a missing dioxin measurement (n = 78) or diabetes prior to service in Southeast Asia (n = 5), died (n = 55), or refused to participate (n = 6). The desired sample size (n = 650) represented 31.12% of the eligible veterans (n = 2,089), and a sample including approximately 31.12% was randomly selected from each of the 16 cells. Final numbers are shown in Table 1. Type 2 diabetes mellitus cases were diagnosed during the post-Vietnam period from the end of the veteran's last tour of duty to 31 December 2000. Veterans who had a verified history of diabetes by medical diagnosis or exhibited a 2-hr postprandial postprandial /post·pran·di·al/ (-pran´de-al) occurring after a meal. post·pran·di·al adj. Following a meal, especially dinner. glucose laboratory value of [greater than or equal to] 200 mg/dL were classified as diabetic. Veterans not meeting these criteria were defined as nondiabetic. At the 1997 examination, the selected veterans were invited to submit to an extraction of 2-15 g of lateral abdominal subcutaneous adipose tissue by liposuction Liposuction Definition Liposuction, also known as lipoplasty or suction-assisted lipectomy, is cosmetic surgery performed to remove unwanted deposits of fat from under the skin. . Of these, 107 were excluded because of medications they were taking, 106 were determined to be too lean, 66 refused, 3 were medically deferred, 1 could not be scheduled, and 54 were not asked, leaving 313 to complete the procedure. The specimens were flash frozen in liquid nitrogen at the clinic and shipped to the laboratory in dry ice, thawed on ice, washed in sterile phosphate buffer solution Noun 1. phosphate buffer solution - a solution containing a phosphate buffer PBS buffer solution - a solution containing a buffer to remove blood, refrozen, and stored at -80[degrees]C until sample analysis. We extracted RNA RNA: see nucleic acid. RNA in full ribonucleic acid One of the two main types of nucleic acid (the other being DNA), which functions in cellular protein synthesis in all living cells and replaces DNA as the carrier of genetic from approximately 500 mg tissue from each sample using TRIzol LS (Invitrogen, Carlsbad, CA), followed by a digest with RNase-free DNase I (Roche Applied Science, Indianapolis, IN) and a repeat extraction. The yield of RNA was determined spectrophotometrically. Specimens from two individuals were used up in preliminary studies. We synthesized cDNA from 1 [micro]g total RNA using the Omniscript RT Kit (Qiagen, Valencia, CA), modifying the kit instructions by doubling the Oligo-dT primer and 10X buffer amounts and adjusting the water amount to yield 40 [micro]l total volume. Using conventional Taq DNA polymerase DNA polymerase /DNA po·lym·er·ase/ (pah-lim´er-as) any of various enzymes catalyzing the template-directed incorporation of deoxyribonucleotides into a DNA chain, particularly one using a DNA template. (Qiagen), 99 cDNA samples were amplified in duplicate to reduce variation due to saturation effects. Amplified fragments were separated on a 1% agarose agarose more highly purified form of agar with similar uses to agar and widely used in the separation of nucleic acid fragments. gel alongside a DNA ladder of 100-bp increments, which was included to confirm fragment molecular weights. Band density was quantified digitally using the ChemiImager 4400, version 5.5 (Alpha Innotech, San Leandro, CA). Primers used for GAPDH, c-Src, and NF[kappa]B were previously described (Ercolani et al. 1988; Kubota et al. 2001; Meyer et al. 1991), whereas we designed primers for C/EBP[alpha] [5'-TTCCGGTGCCTCCTGAAAGC-3' (sense) and 5'-ACAGCCAGATCTCTAGGTCT-3' (antisense antisense, DNA or RNA manipulated in a laboratory so that its components (nucleotides) form a complementary copy of normal, or "sense," messenger RNA (mRNA; see nucleic acid). )] and GLUT4 [5'-CAACTGGACGAGCAACTTCA-3' (sense) and 5'-CCAGCTTCCCAATTCTACCA-3' (antisense)]. Amplification conditions were as follows: 2 min initial denaturation denaturation, term used to describe the loss of native, higher-order structure of protein molecules in solution. Most globular proteins exhibit complicated three-dimensional folding described as secondary, tertiary, and quarternary structures. at 94[degrees]C, cycling steps of 1 min denaturation at 94[degrees]C, 1 min annealing annealing (ənēl`ĭng), process in which glass, metals, and other materials are treated to render them less brittle and more workable. , and 1 min elongation at 72[degrees]C, ending with 10 min final elongation at 72[degrees]C. Annealing temperatures and cycle numbers were 60[degrees]C and 25 for GAPDH and C/EBP[alpha]; 55[degrees]C and 25 for c-Src; 60[degrees]C and 30 for GLUT4; and 62[degrees]C and 32 for NF[kappa]B. One sample was designated as the internal standard for polymerase chain reaction (PCR PCR polymerase chain reaction. PCR abbr. polymerase chain reaction Polymerase chain reaction (PCR) ) and repeated in each run and on each gel in order to compare between runs. The remaining 212 cDNA samples were analyzed without duplication by real-time PCR on the LightCycler (Roche Applied Science) using the QuantiTect SYBR Green PCR kit (Qiagen) (Vogel et al. 2005) for GAPDH, c-Src, and GLUT4, and LightCycler FastStart DNA DNA: see nucleic acid. DNA or deoxyribonucleic acid One of two types of nucleic acid (the other is RNA); a complex organic compound found in all living cells and many viruses. It is the chemical substance of genes. Master SYBR Green I (Roche Applied Science) for C/EBP[alpha] and NF[kappa]B. We designed a new GAPDH primer pair using PRIMER 3 (Rozen and Skaletsky 2000): 5'-GAGTCAACGGATTTGGTCGT-3' (sense) and 5'-TTGATTTTGGAGGGATCTCG-3' (antisense). PCR conditions followed kit instructions, with annealing temperatures and extension times of 54[degrees]C and 12 sec for GAPDH, 53[degrees]C and 28 sec for c-Src, 55[degrees]C and 20 sec for GLUT4, 60[degrees]C and 28 sec for C/EBP[alpha], and 62[degrees]C and 17 sec for NF[kappa]B. We increased the magnesium chloride magnesium chloride Warning - High-alert drug! Chloromag, Mag 64, Mag Delay, Slo-Mag Pharmacologic class: Mineral Therapeutic class: concentration for the LightCycler kit to 4 mM, and the PCR product size was checked on a 1% agarose gel. We calculated relative sample concentrations from crossing point data using the transform [2.sup.-x]. To make LightCycler-determined values from different runs comparable to each other and to conventional values, we reran re·ran v. Past tense and past participle of rerun. subsets of samples from each run in a common run. We performed general linear model statistical analysis using SAS (1) (SAS Institute Inc., Cary, NC, www.sas.com) A software company that specializes in data warehousing and decision support software based on the SAS System. Founded in 1976, SAS is one of the world's largest privately held software companies. See SAS System. software, version 9.1 for Windows (SAS Institute, Cary, NC). We considered and dismissed main effects models of PCR values in terms of dioxin with adjustment for age, body fat, diabetic status, and exposure group because none of these yielded significant results. Subsequently, interaction models involving the product of dioxin with age, body fat, and group were considered; many of these indicated significant interactions, motivating stratification. PCR values were transformed for analysis using various log and power transforms as needed as needed prn. See prn order. to remove skewness Skewness A statistical term used to describe a situation's asymmetry in relation to a normal distribution. Notes: A positive skew describes a distribution favoring the right tail, whereas a negative skew describes a distribution favoring the left tail. . For purpose of analysis, body fat categories of lean and obese were based on 1997 measurements. All statistical testing was two-sided, with a significance level of p = 0.05. Results Raw mRNA values for expression of the four genes studied, before GAPDH normalization, had interquartile ranges of 2.2-fold for C/EBP[alpha], 3.3-fold for NF[kappa]B, 3.4-fold for GLUT4, and 3.6-fold for c-Src. By comparison, the interquartile range for GAPDH was > 6-fold. GAPDH-normalized gene expression values for c-Src, NF[kappa]B, and C/EBP[alpha], after transformation, were significantly negatively correlated with transformed GAPDH values p < 0.001). One of the most statistically significant correlations of mRNA expressions or their ratios to change in PBF was the ratio of GLUT4 to NF[kappa]B (GLUT4:NF[kappa]B ratio) among combined nondiabetic subjects at p < 0.001 (Figure 1A). The ratio of GLUT4 to C/EBP[alpha] (p = 0.002, data not shown) and the ratio of Src to NF[kappa]B (p = 0.031, data not shown) also showed significant correlations to PBF in the same population. In all cases the value of the ratio tended to drop with increasing PBF among nondiabetic subjects, as shown in Figure 1A compared with the corresponding diabetic subjects, which showed no relationship (e.g., Figure 2B). The differences in these ratios between the nondiabetic and diabetic populations were significant in all three cases. To increase the sensitivity of detection of this physiologic change, we adopted the GLUT4:NF[kappa]B ratio as the main marker. Further analyses of nondiabetic subgroups using the same GLUT4:NF[kappa]B ratio showed that, among nondiabetic individuals in the comparison group without family history of diabetes, there was actually no negative or positive correlation to body weight change (Figure 1C). In contrast, among the corresponding subgroup (nondiabetic with no family history of diabetes) in the ORH group (Figure 1D), we found a significant negative correlation (p = 0.003). Even among nondiabetic comparison subjects, those with a family history of diabetes showed a negative slope (Figure 1E; p = 0.03), which was also statistically different (p = 0.05) from the slope in Figure 1C. To study the effect of dioxin on the expression of each marker, we subdivided each group into quartiles according to measured levels of serum dioxin residues and compared gene expression ratios among nondiabetic individuals of these subgroups. GLUT4:GAPDH and NF[kappa]B:GAPDH ratios showed significant differences among quartiles (Figure 2A, B). A similar result was obtained when GLUT4 was compared to C/EBPa instead of GAPDH (data not shown). However, the ratio that gave us the clearest trend with dioxin was again GLUT4:NF[kappa]B (Figure 2C). The most conspicuous difference between the two service groups was the direction of slopes. Veterans of the first quartile Quartile A statistical term describing a division of observations into four defined intervals based upon the values of the data and how they compare to the entire set of observations. Notes: Each quartile contains 25% of the total observations. of the comparison group had a significantly higher GLUT4:NF[kappa]B ratio than those of the second and third dioxin quartiles, exhibiting a negative relationship to dioxin residues; in contrast, Agent Orange-exposed ORH subjects clearly showed a positive trend. Among comparison subjects, only the highest dioxin residue quartile contradicted the downward trend. In view of this finding, we further analyzed the relationships between the GLUT4:NF[kappa]B ratio and dioxin exposure in the full cohort of veterans (Figure 3A vs. Figure 3B). In general, dioxin was associated with an increase in the GLUT4:NF[kappa]B ratio in the ORH group, whereas there was no trend in the comparison group. Further analyses of several subgroups within each service group revealed that the GLUT4:NF[kappa]B ratio tended to decline when serum dioxin increased among nondiabetic individuals in the comparison group who are obese and have a family history of diabetes (Figure 3C). Other subgroups that showed significantly different GLUT4:NF[kappa]B responses to increasing serum dioxin were the combined (comparison + ORH) subgroup consisting of obese subjects with a family history of diabetes (Figure 3D) compared with the combined subgroup of lean subjects with a family history of diabetes (Figure 3E). To test the validity of using the GLUT4:NF[kappa]B ratio as a molecular parameter to assess diabetogenic conditions, we analyzed its relationship to the high levels of serum glucose after fasting (fasting glucose). As seen in Figure 4A, the fasting glucose levels stayed within a narrow range of values among all (comparison + ORH) nondiabetic study subjects over the wide range of GLUT4:NF[kappa]B ratios, as expected. In contrast, among all diabetic subjects (Figure 4B), those with lower GLUT4:NF[kappa]B ratios exhibited higher fasting glucose levels. We further checked the relationship between PBF and fasting glucose levels in all nondiabetic subjects (Figure 4C) compared with all diabetic subjects (Figure 4D). We found a significant relationship in nondiabetic subjects (r = 0.27, p < 0.001) but not in diabetic subjects (r = -0.05, p = 0.73). Next, we studied the relationship between the levels of fasting glucose and serum dioxin to further test our premise that dioxin acts as a diabetogenic agent. When both nondiabetic and diabetic subjects were combined within each service group, we found a positive correlation between fasting glucose and serum dioxin levels in the comparison group (Figure 4E; p = 0.02). In contrast, these two parameters were not correlated in the corresponding ORH subgroup (Figure 4F). Discussion Initially we conducted a preliminary survey of the expressions of the proposed markers in all samples to see which markers or their combinations would give a reliable indication of physiologic conditions leading to diabetes. To aid in this process, we formulated a working hypothesis that the diabetogenic action of TCDD could be phenotypically similar to that of obesity. Therefore, we studied the relationship between mRNA expression of those selected markers and PBF gain over the last 5 years among veterans. Of all of the molecular markers and their combinations examined, the most readily recognizable gene expression effects were those of the GLUT4:NF[kappa]B ratio in response to the presence of dioxin, as assessed in the serum of the veterans. This observation agrees well with the generally accepted view that in the case of obesity-induced type 2 diabetes TNF-[alpha] plays the central role through its action to activate NF[kappa]B, which down-regulates GLUT4 (Ruan et al. 2002). Theoretically, if the TNF-[alpha]-NF[kappa]B pathway is activated, a rise in NF[kappa]B expression will lead to a drop in GLUT4 expression; thus, the ratio is expected to be more responsive than either individual gene normalized by a housekeeping gene. The trends for GLUT4:C/EBP[alpha] and Src:NF[kappa]B may represent merely weaker responses of ratios that contain the GLUT4 or NF[kappa]B component of the GLUT4:NF[kappa]B ratio. This GLUT4:NF[kappa]B ratio marker approach was most effective in detecting the effect of dioxin at low-to-medium levels of exposure, corresponding to the lower three quartiles in the comparison group (Figure 1). This range of dioxin levels corresponds to 1-5.3 ppt ppt abbr. 1. parts per thousand 2. parts per trillion . In fact the highest dioxin level for the entire comparison group is 16.3 ppt. The level of dioxin in serum lipids among U.S. workers that Sweeney et al. (1997-1998) found in their comparison group was 0-20 ppt, indicating that the range we found in the comparison group in the present study was not much different from that of the general public in the United States. In this regard, it is important to point out that we found significant signs of dioxin-correlated diabetogenic tendency among comparison group subjects with low levels of dioxin, particularly in those with genetic (family history of diabetes) and physiologic (obesity) risk factors (Figure 3C). Furthermore, dioxin, even at this low concentration range, definitely has an effect on the levels of fasting glucose (Figure 4E). The GLUT4:NF[kappa]B response to dioxin exposure levels found in the lower three quartiles of the comparison group also agrees well with the data obtained from cell models (Ruan et al. 2002) and animal models (Dunlap et al. 2002; Liu and Matsumura 1995). The observation that the GLUT4:NF[kappa]B ratio declined with weight gain, independent of exposure history (Figure 1A) and with higher serum dioxin residues among comparison individuals (Figure 2C), particularly obese individuals with family history of diabetes (Figure 3C), suggests that dioxin works synergistically syn·er·gis·tic adj. 1. Of or relating to synergy: a synergistic effect. 2. Producing or capable of producing synergy: synergistic drugs. 3. with known diabetes risk factors to alter glucose metabolism glucose metabolism, n the process by which simple sugars found in many foods are processed and used to produce energy in the form of ATP. Once consumed, glucose is absorbed by the intestines and into the blood. in a way that resembles the inflammation mechanism of weight gain. The GLUT4:NF[kappa]B ratio appears to be a useful biomarker for the detection of the diabetogenic action of these factors. The inflammation mechanism also seems to operate at low background levels of dioxin, as seen in the three lowest serum dioxin quartiles (i.e., those with [less than or equal to] 5.3 ppt) of the larger group of background-exposed veterans (Figure 2C). Such an observation alone would not constitute a proof for the identical action mechanism of dioxin to diabetogenic action of obesity, but it allows us to formulate a hypothesis along this line of logic to help our future studies. We found the GLUT4:NF[kappa]B ratio to be a reliable parameter in assessing the state of diabetes. Diabetic subjects with lowered GLUT4:NF[kappa]B were less able to regulate blood glucose blood glucose Diabetology The principal sugar produced by the body from food–especially carbohydrates, but also from proteins and fats; glucose is the body's major source of energy, is transported to cells via the circulation and used by cells in the presence , whereas nondiabetic subjects maintained fasting glucose levels within a narrow range of values, independent of GLUT4:NF[kappa]B (Figure 4A, B). However, our finding regarding this effect of GLUT4:NF[kappa]B was somewhat surprising in view of the lack of correlation of GLUT4:NF[kappa]B with weight gain among diabetic subjects (Figure 1B); this finding suggests that once the study subjects develop diabetes, the GLUT4:NF[kappa]B ratio does not work well as a biomarker for obesity. However, the GLUT4:NF[kappa]B ratio does work as a biomarker for elevated fasting glucose (Figure 4B). The important message derived from Figure 4B is that the workable range or the usefulness of the GLUT4:NF[kappa]B ratio as a biomarker depends largely on the factor against which it is being regressed. Thus, one should not assume automatically that the state of disease makes it impossible to use this biomarker on all diabetes-related cellular changes. Among nondiabetic veterans without a family history of diabetes (i.e., healthy subpopulation sub·pop·u·la·tion n. A part or subdivision of a population, especially one originating from some other population: microbial subpopulations. Noun 1. ) in the comparison group, we found no detectable effect of obesity on the GLUT4:NF[kappa]B ratio (Figure 1C), indicating the existence of normal homeostatic homeostatic pertaining to homeostasis. control. In contrast, the corresponding subgroup from the ORH group clearly showed the effect of obesity (Figure 1D) as though they already had the genetic risk factor, as in the case of the subgroup with a family history of diabetes in the comparison group (Figure 1E). This set of data also supports our interpretation that dioxin acts as one of the risk factors for diabetes. As we expected, fasting glucose levels were reliable parameters in judging the diabetogenic effects of obesity among nondiabetic subjects (Figure 4C) at the early stage of developing diabetes but not at the later stage, as seen in diabetic subjects (Figure 4D). In addition, the observation that fasting glucose is higher among subjects in the comparison group who had higher serum dioxin levels complements the observation of Henriksen et al. (1997), who found increased fasting glucose with higher levels of dioxin in a larger cohort of Agent Orange-exposed veterans. The decrease in the expression of GLUT4 in adipose tissue has been shown to be associated with non-insulin-dependent diabetes. Minokoshi et al. (2003) found that tissue-specific ablation of GLUT4 and insulin receptor in adipose tissue or muscle in mice led to insulin resistance Insulin Resistance Definition Insulin resistance is not a disease as such but rather a state or condition in which a person's body tissues have a lowered level of response to insulin, a hormone secreted by the pancreas that helps to regulate the level and diabetes in the mice lacking adipose GLUT4 expression but not in those missing GLUT4 only in muscles. In humans, Garvey et al. (1991) found that an 80% decrease in GLUT4 protein per cell in the adipocytes of diabetic subjects compared with lean nondiabetic controls was associated with a 56% decrease in maximally insulin-stimulated glucose uptake. The level of GLUT4 mRNA was correlated with the amount of GLUT4 protein (r = 0.77) in their controls but not in their diabetic subjects. There are also precedents indicating that the change in NF[kappa]B is correlated to diabetes. NF[kappa]B is a nuclear transcription factor that is known to be activated by inflammatory signaling of several agents, including TNF-[alpha], and to transmit their messages into the nucleus. Although we did not include TNF-[alpha] in the present study, its involvement in the toxic action of dioxin is well known (Alsharif et al. 1994; Taylor et al. 1992). TNF-[alpha] is one of the major mediators of dioxin-induced cell inflammatory reactions (Matsumura 2003). Furthermore, the role of TNF-[alpha] in the development of insulin resistance and type 2 diabetes, particularly in the case of obesity-induced diabetes, is now becoming well recognized (Das 1999). Indeed, obesity induces increased expression of TNF-[alpha] and NF[kappa]B, leading to down-regulation of insulin receptor and decreasing expression of GLUT4 (Halle et al. 1998). Our observation in the present study that the GLUT4:NF[kappa]B ratio dramatically decreases among nondiabetic veterans who experienced a relatively recent increase in body fat attests to the correctness of this diagnosis. We did not include measurements of other compounds with dioxin-like activity because these were not available in this population until well after the period of this study. Sweeney et al. (1997-1998) found that use of toxic equivalents (TEQ TEQ Toxicity Equivalent TEQ Time Domain Equalizer TEQ Teacher Education Quarterly TEQ Terra Est Quaestuosa (web-based game, Spanish: Lland is Profitable) TEQ The Evil Quakkers (gaming clan) ; the body burden of TCDD-equivalent activity from all compounds) led to a narrowing of the differences between acute- and background-exposed populations. Furthermore, the phenoxy herbicides in the Agent Orange formulation are known peroxisome Peroxisome An intracellular organelle found in all eukaryotes except the archezoa (original lifeforms). In electron micrographs, peroxisomes appear round with a diameter of 0.1–1. proliferators and thus may have antidiabetic action (Remillard and Bunce 2002). With such confounding factors acting to obscure the effects of TCDD, the results we did find are all the more noteworthy. One major question that remains unanswered is why the overall relationship between the GLUT4:NF[kappa]B ratio and serum dioxin levels show the "V" shape (Figure 2C), indicating a reversal of dioxin's effect at levels higher than the background range. This is puzzling because, in all other cases, either the GLUT4:NF[kappa]B ratio or dioxin levels showed straightforward relationships to other parameters analyzed. One possibility is that veterans with dioxin residue levels > 5.3 ppt are experiencing the effects of cachexia cachexia /ca·chex·ia/ (kah-kek´se-ah) a profound and marked state of constitutional disorder; general ill health and malnutrition. , a typical effect of dioxin exposure. It involves massive loss of adipose tissues in most animals studied, including humans (Matsumura 2003). In this regard, it is interesting to note the similarities in the direction of slopes between Figure 3A and Figure 3D, and between Figure 3B and Figure 3E, indicating that as a whole, comparison subjects are similar to combined (comparison + ORH) nondiabetic obese subjects with a family history of diabetes with respect to their GLUT4:NF[kappa]B response to dioxin. In the same manner, ORH subjects are similar to combined (comparison + ORH) nondiabetic lean subjects with family history of diabetes, despite the fact that there is no difference in the frequency of obesity between comparison and ORH subjects. Such an observation favors the view that wasting syndrome is already taking place among those exposed to high levels of dioxin and that ORH subjects as a whole are responding to dioxin as though they were lean. Another possibility is that in human adipose tissues, unlike the case of mice, chronic exposure to high concentrations of dioxin could trigger a strong negative feedback reaction through activation of major "negative regulators" to counteract excessive inflammatory insults. The observation that three of the parameters we studied, NF[kappa]B, C/EBP[alpha], and GLUT4 expression, show this phenomenon of "reversal" at high dioxin concentrations > 5.3 ppt supports this interpretation. Nevertheless, much more work is needed to prove or disprove these hypotheses. It is also important to point out that, despite the above "reversal" phenomenon in the relationship between GLUT4:NF[kappa]B ratio and dioxin, all nondiabetic individuals with significant dioxin residues, including those with residue levels > 5.3 ppt, still show the clear sign of the obesity-related risk of diabetes, judging by the results of experiments shown in Figure 4C. Conclusions In conclusion, by using this molecular epidemiologic approach we found definitive evidence indicating that a diabetogenic shift occurred in the biochemistry of adipose tissues from Vietnam veterans who were exposed to dioxin-containing Agent Orange herbicide preparations. Such a diabetogenic effect of dioxin was observed even among comparison group veterans, particularly those with diabetes risk factors such as obesity and/or a family history of diabetes, despite the fact that their levels of exposure are not really different from those of the general public in the United States. The major implication of the present study is, therefore, that the potential health hazard of dioxin and active dioxintype chemicals, even at the current level of public exposure, must be taken seriously. Further research is needed to fully elucidate the precise mechanism through which dioxin promotes type 2 diabetes in humans. REFERENCES Alsharif NZ, Hassoun E, Bagchi M, Lawson T, Stohs SJ. 1994. The effects of anti-TNF-alpha antibody and dexamethasone dexamethasone /dex·a·meth·a·sone/ (dek?sah-meth´ah-son) a synthetic glucocorticoid used primarily as an antiinflammatory in various conditions, including collagen diseases and allergic states; it is the basis of a screening test in the on TCDD-induced oxidative stress in mice. Pharmacology 48:127-136. Bertazzi PA, Bernucci I, Brambilla G, Consonni D, Pesatori AC. 1998. The Seveso studies on early and long-term effects of dioxin exposure: a review. Environ Health Perspect 106(suppl 2):625-633. Booker SM. 2001. Dioxin in Vietnam: fighting a legacy war. Environ Health Perspect 109:A116-A117. Das UN. 1999. GLUT-4, tumor necrosis factor tumor necrosis factor n. Abbr. TNF A protein that is produced in the presence of an endotoxin, especially by monocytes and macrophages, is able to attack and destroy tumor cells, and exacerbates chronic inflammatory diseases. , essential fatty acids Essential fatty acids Sources of fat in the diet, including omega-3 and omega-6 fatty acids. Mentioned in: Nutritional Supplements and daf-genes and their role in insulin resistance and non-insulin dependent diabetes mellitus. Prostglandins Leukot Essent Fatty Acids 60:13-20. Dunlap DY, Ikeda I, Nagashima H, Vogel CF, Matsumura F. 2002. Effects of src-deficiency on the expression of in vitro toxicity of TCDD in a strain of c-src knockout mice procured through six generations of backcrossings to C57BL/6 mice. Toxicology 172:125-141. Ercolani L, Florence B, Denaro M, Alexander M. 1988. Isolation and complete sequence of a functional glyceraldehyde-3-phosphate dehydrogenase dehydrogenase /de·hy·dro·gen·ase/ (de-hi´dro-jen-as?) an enzyme that catalyzes the transfer of hydrogen or electrons from a donor, oxidizing it, to an acceptor, reducing it. de·hy·dro·gen·ase n. gene. J Biol Chem 263:15335-15341. Freytag SO, Geddes TJ. 1992. Reciprocal regulation of adipogenesis by Myc and C/EBP alpha. Science 256:379-382. Frumkin H. 2003. Agent Orange and cancer: an overview for clinicians. CA Cancer J Clin 53:245-255. Garvey WT, Maianu L, Huecksteadt TP, Birnbaum MJ, Molina JM, Ciaraldi TP. 1991. Pretranslational suppression of a glucose transporter protein causes insulin resistance in adipocytes from patients with non-insulin-dependent diabetes mellitus non-in·su·lin-de·pend·ent diabetes mellitus n. Abbr. NIDDM See diabetes mellitus. non-insulin-dependent diabetes mellitus Type 2 diabetes mellitus, see there and obesity. J Clin Invest 87:1072-1081. GenBank. 2006. GenBank Overview. Available: http://www.ncbi.nlm.nih.gov/Genbank/index.html [accessed 18 September 2006]. Gorzelniak K, Janke J, Engeli S, Sharma AM. 2001. Validation of endogenous controls for gene expression studies in human adipocytes and preadipocytes. Horm Metab Res 33:625-627. Halle M, Berg A, Northoff H, Keul J. 1998. Importance of TNF-alpha and leptin Leptin A protein hormone that affects feeding behavior and hunger in humans. At present it is thought that obesity in humans may result in part from insensitivity to leptin. in obesity and insulin resistance: a hypothesis on the impact of physical exercise. Exerc Immunol Rev 4:77-94. Henriksen GL, Ketchum NS, Michalek JE, Swaby JA. 1997. Serum dioxin and diabetes mellitus in veterans of Operation Ranch Hand. Epidemiology 8:252-258. Hornung RW, Reed DR. 1990. Estimation of average concentration in the presence of nondetectable values. App Occup Environ Hyg 5:46-51. Institute of Medicine. 2000. Veterans and Agent Orange: Update 2000. Washington, DC:National Academy Press. Institute of Medicine. 2003, Veterans and Agent Orange: Update 2002. Washington, DC:National Academy Press. Jahner D, Hunter T. 1991. The stimulation of quiescent rat fibroblasts Fibroblasts A type of cell found in connective tissue; produces collagen. Mentioned in: Skin Grafting by v-src and v-fps oncogenic oncogenic /on·co·gen·ic/ (-jen´ik) giving rise to tumors or causing tumor formation; said especially of tumor-inducing viruses. on·co·gen·ic or on·cog·e·nous adj. protein-tyrosine kinases leads to the induction of a subset of immediate early genes. Oncogene oncogene Gene that can cause cancer. It is a sequence of DNA that has been altered or mutated from its original form, the proto-oncogene (see mutation). Proto-oncogenes promote the specialization and division of normal cells. 6:1259-1268. Kern PA, Dicker-Brown A, Said ST, Kennedy R, Fonseca VA. 2002. The stimulation of tumor necrosis factor and inhibition of glucose transport and lipoprotein lipase in adipose cells by 2,3,7,8-tetrachlorodibenzo-p-dioxin. Metabolism 51:65-68. Kim JS, Lim HS, Cho SI, Cheong HK, Lim MK. 2003. Impact of Agent Orange exposure among Korean Vietnam veterans. Ind Health 41:149-157. Knapik JJ, Burse burse n. 1. A purse. 2. Ecclesiastical A flat cloth case for carrying the corporal that is used in celebrating the Eucharist. [Late Latin bursa; see bursa.] RL, Vogel JA. 1983. Height, weight, percent body fat, and indices of adiposity adiposity /ad·i·pos·i·ty/ (ad?i-pos´i-te) obesity. cerebral adiposity fatness due to cerebral disease, especially of the hypothalamus. adiposity obesity. for young men and women entering the US Army. Aviat Space Environ Med 54:223-231. Kubota Y, Tanaka T, Kitanaka A, Ohnishi H, Okutani Y, Waki M, et al. 2001. Src transduces erythropoietin-induced differentiation signals through phosphatidylinositol 3-kinase. EMBO J 20:5666-5677. Liu PC, Matsumura F. 1995. Differential effects of 2,3,7,8-tetrachlorodibenzo-p-dioxin on the "adipose-type" and "braintype" glucose transporters in mice. Mol Pharmacol 47:65-73. MacDougald OA, Lane MD. 1995. Transcriptional regulation of gene expression Gene modulation redirects here. For information on therapeutic regulation of gene expression, see therapeutic gene modulation.
. during adipocyte adipocyte /ad·i·po·cyte/ (-sit?) fat cell. ad·i·po·cyte n. See fat cell. adipocyte differentiation. Annu Rev Biochem 64:345-373. Matsumura F. 2003. On the significance of the role of cellular stress response reactions in the toxic actions of dioxin. Biochem Pharmacol 66:527-540. Meyer R, Hatada EN, Hohmann HP, Haiker M, Bartsch C, Rothlisberger U, et al. 1991. Cloning of the DNA-binding subunit of human nuclear factor kappa B: the level of its mRNA is strongly regulated by phorbol phorbol /phor·bol/ (for´bol) a polycyclic alcohol occurring in croton oil; it is the parent compound of the phorbol esters. phorbol ester ester or tumor necrosis factor alpha. Proc Natl Acad Sci USA 88:966-970. Michalek JE, Akhtar FZ, Kiel JL. 1999. Serum dioxin, insulin, fasting glucose, and sex hormone binding globulin Sex hormone-binding globulin (SHBG) is a glycoprotein that binds to sex hormones, specifically testosterone and estradiol. Other steroid hormones such as progesterone, cortisol, and other corticosteroids are bound by transcortin. in veterans of Operation Ranch Hand. J Clin Endocrinol Metab 84:1540-1543. Michalek JE, Tripathi RC. 1999. Pharmacokinetics of TCDD in veterans of Operation Ranch Hand: 15-year follow-up. J Toxicol Environ Health A57:369-378. Minokoshi Y, Kahn CR, Kahn BB. 2003. Tissue-specific ablation of the GLUT4 glucose transporter or the insulin receptor challenges assumptions about insulin action and glucose homeostasis homeostasis Any self-regulating process by which a biological or mechanical system maintains stability while adjusting to changing conditions. Systems in dynamic equilibrium reach a balance in which internal change continuously compensates for external change in a feedback . J Biol Chem 278:33609-33612. Patterson DG Jr, Hampton L, Lapeza CR Jr, Belser WT, Green V, Alexander L, et al. 1987. High-resolution gas chromatographic/high-resolution mass spectrometric analysis of human serum on a whole-weight and lipid basis for 2,3,7,8-tetrachlorodibenzo-p-dioxin. Anal Chem 59:2000-2005. Pesatori AC, Consonni D, Bachetti S, Zochetti C, Bonzini M, Baccarelli A, et al. 2003. Short-and long-term morbidity and mortality Morbidity and Mortality can refer to:
Remillard RB, Bunce NJ. 2002. Linking dioxins to diabetes: epidemiology and biologic plausibility. Environ Health Perspect 110:853-858. Rozen S, Skaletsky HJ. 2000. PRIMER 3 on the WWW WWW or W3: see World Wide Web. (World Wide Web) The common host name for a Web server. The "www-dot" prefix on Web addresses is widely used to provide a recognizable way of identifying a Web site. for general users and for biologist programmers. In: Bioinformatics Methods and Protocols: Methods in Molecular Biology (Krawetz S, Misener S, eds). Totowa, NJ:Humana Press, 365-386. Ruan H, Hacohen N, Golub TR, Van Parijs L, Lodish HF. 2002. Tumor necrosis factor-alpha Tumor necrosis factor (TNF, cachexin or cachectin and formally known as tumor necrosis factor-alpha) is a cytokine involved in systemic inflammation and is a member of a group of cytokines that all stimulate the acute phase reaction. suppresses adipocyte-specific genes and activates expression of preadipocyte genes in 3T3-L1 adipocytes: nuclear factor-kappaB activation by TNF-alpha is obligatory. Diabetes 51:1319-1336. Scheen AJ. 2003. Pathophysiology pathophysiology /patho·phys·i·ol·o·gy/ (-fiz?e-ol´ah-je) the physiology of disordered function. path·o·phys·i·ol·o·gy n. 1. of type 2 diabetes. Acta Clin Belg 58:335-341. Sweeney MH, Calvert GM, Egeland GA, Fingerhut MA, Halperin WE, Piacitelli LA. 1997-1998. Review and update of the results of the NIOSH NIOSH National Institute for Occupational Safety & Health, see there NIOSH Recommendations for Safety & Health Standards Agent NIOSH REL*/OSHA PEL† Health effects medical study of workers exposed to chemicals contaminated with 2,3,7,8-tetrachlorodibenzodioxin. Teratog Carcinog Mutagen mutagen: see mutation. mutagen Any agent capable of altering a cell's genetic makeup by changing the structure of the hereditary material, DNA. Many forms of electromagnetic radiation (e.g. 17(4-5):241-247. Taylor MJ, Lucier GW, Mahler JF, Thompson M, Lockhart AC, Clark GC. 1992. Inhibition of acute TCDD toxicity by treatment with anti-tumor necrosis factor antibody or dexamethasone. Toxicol Appl Pharmacol 117:126-132. Vena J, Boffetta P, Becher H, Benn T, Bueno-de-Mesquita HB, Coggon D, et al. 1998. Exposure to dioxin and nonneoplastic mortality in the expanded IARC international cohort study of phenoxy herbicide and chlorophenol production workers and sprayers. Environ Health Perspect 106(suppl 2):645-653. Vogel CF, Sciullo E, Wong P, Kuzmicky P, Kado N, Matsumura F. 2005. Induction of proinflammatory cytokines Cytokines Chemicals made by the cells that act on other cells to stimulate or inhibit their function. Cytokines that stimulate growth are called "growth factors. and C-reactive protein in human macrophage macrophage /mac·ro·phage/ (mak´ro-faj) any of the large, mononuclear, highly phagocytic cells derived from monocytes that occur in the walls of blood vessels (adventitial cells) and in loose connective tissue (histiocytes, phagocytic cell line U937 exposed to air pollution particulates. Environ Health Perspect 113:1536-1541. Wolfe WH, Michalek JE, Miner JC, Rahe A, Silva J, Thomas WF, et al. 1990. Health status of Air Force veterans occupationally exposed to herbicides in Vietnam. I. Physical Health. JAMA JAMA abbr. Journal of the American Medical Association 264:1824-1831. Phillip Thomas Fujiyoshi, (1) Joel Edmund Michalek, (2) and Fumio Matsumura (1) (1) Department of Environmental Toxicology, University of California-Davis, Davis, California, USA; (2) The University of Texas Health Science Center at San Antonio UTHSCSA is the largest comprehensive health sciences university in South Texas. Located in the South Texas Medical Center, it serves San Antonio and all of the 50,000 square mile (130,000 km²) area of central and south Texas. , San Antonio, Texas “San Antonio” redirects here. For other uses, see San Antonio (disambiguation). San Antonio is the second most populous city in Texas, the third most populous metropolitan area in Texas, and is the seventh most populous city in the United States. As of the 2006 U.S. , USA Address correspondence to F. Matsumura, Department of Environmental Toxicology, University of California The University of California has a combined student body of more than 191,000 students, over 1,340,000 living alumni, and a combined systemwide and campus endowment of just over $7.3 billion (8th largest in the United States). , One Shields Ave., Davis, CA 95616 USA. Telephone: (530) 752-4251. Fax: (530) 752-3394. E-mail: fmatsumura@ucdavis.edu This study was funded by U.S. Air Force contract #4400020591, subproject #01-0813-32-8280-906-721900, with support from the U.C. Davis Center for Environmental Health Sciences for use of the Molecular Biology Core facility under center grants P30-ES05707 and R01-ES05233 from the National Institute of Environmental Health Sciences The National Institute of Environmental Health Sciences (NIEHS) is one of 27 Institutes and Centers of the National Institutes of Health (NIH),which is a component of the Department of Health and Human Services (DHHS). The Director of the NIEHS is Dr. David A. Schwartz. . The authors declare they have no competing financial interests. Received 12 April 2006; accepted 3 August 2006.
Table 1. Sample sizes and demographics.
Group/diabetic Age Lean Obese Total
status category (n) (n) (n)
Comparison
Nondiabetic Young 58 18 76
Old 56 24 80
Diabetic Young 3 7 10
Old 9 9 18
ORH
Nondiabetic Young 46 13 59
Old 40 11 51
Diabetic Young 4 4 8
Old 6 5 11
Total 313
|
|
||||||||||||||||||
Printer friendly
Cite/link
Email
Feedback
Reader Opinion