HOMA Insulin Resistance Index Research Articles

Insulin resistance and secretion change after 3 years follow-up and the risk for developing diabetes in non-diabetic adults

Purpose : To determine 3-years natural change of insulin resistance and secretion in non-diabetic Chinese adults and corresponding risk for developing diabetes. Methods : Population-based cohort study was performed in Chinese adults (35-74 years) from 2009 to 2015. Fasting plasma glucose and serum insulin was determined in 1882 subjects (701 men) at baseline and re-tested in 1087 (377 men). Insulin resistance was estimated with HOMA insulin resistance index (HOMA-IR) and insulin secretion with HOMA insulin secretion index (HOMA-IS). The change of HOMA-IR and HOMA-IS was calculated as: the value at follow-up minus that at baseline

Informativity of the method of correlation adaptometry for assessing the severity of the corrective effect of combined use therapeutic physical factors on the example of metabolic syndrome

BACKGROUND: Evaluation of the effectiveness of the use of therapeutic physical factors using the method of correlation adaptometry is based on the effect of increasing the number of severity of correlation dependencies between the parameters characterizing the functional state of the body under the action of a stressor.
 AIM: Evaluation of the effectiveness of the combined use of transcranial magnetotherapy and a pulsed low-frequency electrostatic field in patients with metabolic syndrome using the method of correlation adaptometry.
 MATERIALS AND METHODS: The study involved 100 patients with a diagnosis of metabolic syndrome established in accordance with clinical guidelines. All patients were divided into four groups of 25 by simple fixed randomization. Patients in the control group received a placebo effect (imitation of physiotherapeutic effects with the device turned off) for 10 days of observation, in comparison group 1 ― exposure to a low-frequency electrostatic field, in comparison group 2 ― transcranial magnetotherapy with a traveling magnetic field, in the main group ― exposure to a pulsed electrostatic field in combination with transcranial magnetotherapy. The objectification of the effects of physiotherapy (evaluation of functional, biochemical and hormonal parameters) was based on a two-stage examination (before and after a course of treatment).
 RESULTS: Correlation adaptometry was based on the results of correlation analysis using a correlation matrix of variables characterizing the condition of patients after course correction. For each of the four groups of patients, 28 correlation coefficients were determined. For each group, 378 correlation coefficients were calculated, presented as the weight of the correlation graph. Additionally, the indicator of the average adaptive correlation was calculated. It is shown that the use of therapeutic physical factors is accompanied by a decrease in the weight of the correlation graph, which indicates the severity of the clinical effect due to the sanogenetic action of physiofactors. The most pronounced decrease was noted in the group of combined physiotherapy. Correlation analysis between the parameters of the average adaptive correlation and the integral coefficient of therapy efficiency showed that there is a strong, negative significant relationship between the HOMA insulin resistance index and the Quetelet index, chosen as the most informative variables.
 CONCLUSION: It is concluded that the method of correlation adaptometry is highly informative in assessing the effectiveness of using a pulsed low-frequency electrostatic field, transcranial magnetotherapy and their combined effects in patients with metabolic syndrome. A decrease in the indicator of the average adaptive correlation indicates an increase in the functional reserves of the system, the patterns of which are changes in certain estimated parameters that are not related to each other.

Value of C-peptide-based insulin resistance index for evaluating correlation between insulin resistance and serum uric acid level in individuals undergoing health examination

To investigate the value of C-peptide-based insulin resistance index in evaluating the correlation between insulin resistance and serum uric acid (Ua) level in subjects undergoing health examination. The data of 46 017 subjects undergoing health examination were retrospectively collected from the Second Medical Center of PLA General Hospital from January, 2017 to December, 2021. The subjects were divided into Ua≤420 μmol/L group and Ua>420 μmol/L group for comparison of HOMA insulin resistance index (HOMA2-IR) and HOMA insulin resistance-C peptide (HOMA2 IR-CP). The correlations of HOMA2-IR and HOMA2 IR-CP with Ua level were analyzed using Pearson correlation analysis and linear regression analysis. Hierarchical interaction analysis was conducted to assess the differences in the association between insulin resistance index and Ua level in different subgroups. The ROC curve was used to evaluate the predictive ability of insulin resistance index for an increased Ua level. The levels of HOMA2-IR and HOMA2 IR-CP were significantly lower in Ua≤420 μmol/L group than in Ua>420 μmol/L group. Univariate Pearson correlation analysis showed a weak correlation of HOMA2-IR with Ua (r=0.262, P<0.001) and moderate correlation of HOMA2 IR-CP with Ua (r=0.409, P<0.001). Multivariate linear regression analysis, after adjustment for confounding factors, demonstrated that HOMA2-IR (R2=0.445, P<0.001) and HOMA2 IR-CP (R2=0.461, P<0.001) were both factors affecting Ua level. Hierarchical interaction analysis showed that the association of insulin resistance index with Ua level varied significantly with gender, age, and glucose metabolism (P<0.001). ROC curve showed that the areas under the curve predicted an increased Ua level by HOMA2-IR and HOMA2 IR-CP were 0.662 and 0.722, respectively. HOMA2 IR-CP is a more accurate indicator for assessing the correlation between insulin resistance and Ua level.

Effects of PM2.5 and high-fat diet interaction on blood glucose metabolism in adolescent male Wistar rats: A serum metabolomics analysis based on ultra-high performance liquid chromatography/mass spectrometry

Fine particulate matter (PM2.5) and high-fat diet (HFD) are known to contribute to blood glucose metabolic disorders. However, limited research has investigated the combined impact of PM2.5 and HFD on blood glucose metabolism. This study aimed to explore the joint effects of PM2.5 and HFD on blood glucose metabolism in rats using serum metabolomics and to identify involved metabolites and metabolic pathways. The 32 male Wistar rats were exposed to filtered air (FA) or PM2.5 (real-world inhaled, concentrated PM2.5, 8 times the ambient level, ranging from 131.42 to 773.44 μg/m3) and fed normal diet (ND) or HFD for 8 weeks. The rats were divided into four groups (n = 8/group): ND-FA, ND-PM2.5, HFD-FA and HFD-PM2.5 groups. Blood samples were collected to determine fasting glucose (FBG), plasma insulin and glucose tolerance test and HOMA Insulin Resistance (HOMA-IR) index was calculated. Finally, the serum metabolism of rats was analyzed by ultra-high performance liquid chromatography/mass spectrometry (UHPLC-MS). Then we constructed the partial least squares discriminant analysis (PLS-DA) model to screen the differential metabolites, and performed pathway analysis to screen the main metabolic pathways. Results showed that combined effect of PM2.5 and HFD caused changes in glucose tolerance, increased FBG levels and HOMA-IR in rats and there were interactions between PM2.5 and HFD in FBG and insulin. By metabonomic analysis, the serum differential metabolites pregnenolone and progesterone, which involved in steroid hormone biosynthesis, were two different metabolites in the ND groups. In the HFD groups, the serum differential metabolites were L-tyrosine and phosphorylcholine, which involved in glycerophospholipid metabolism, and phenylalanine, tyrosine, and tryptophan biosynthesis. When PM2.5 and HFD coexist, they may lead to more severe and complex effects on glucose metabolism by affecting lipid metabolism and amino acid metabolism. Therefore, reducing PM2.5 exposure and controlling dietary structure are important measures for preventing and reducing glucose metabolism disorders.

Independent association of hypovitaminosis d with non-alcoholic fatty liver disease in people with chronic spinal cord injury: a cross-sectional study.

Non-alcoholic fatty liver disease (NAFLD) and hypovitaminosis D are highly prevalent in people with spinal cord injury (SCI) and could exert an unfavorable influence on cardiovascular profile and rehabilitation outcomes. We aimed to assess the independent association between low 25-hydroxy vitamin D (25(OH)D) levels and NAFLD in people with chronic (> 1year) SCI. One hundred seventy-three consecutive patients with chronic SCI (132 men and 41 women) admitted to a rehabilitation program underwent clinical/biochemical evaluations and liver ultrasonography. NAFLD was found in 105 patients (60.7% of the study population). They were significantly older and exhibited a poorer leisure time physical activity (LTPA) and functional independence in activities of daily living, a greater number of comorbidities and a higher prevalence of metabolic syndrome (MetS) and its correlates, including lower HDL and higher values of body mass index (BMI), systolic blood pressure, HOMA-index of insulin resistance and triglycerides. 25(OH)D levels were significantly lower in NAFLD (median: 10.6ng/ml, range: 2.0-31.0) than in non-NAFLD group (22.5ng/ml, 4.2-51.6). When all these variables were included in a multiple logistic regression analysis, a significant independent association with NAFLD only persisted for lower 25(OH)D levels, a greater number of comorbidities and a poorer LTPA. The ROC analysis revealed that 25(OH)D levels < 18.25ng/ml discriminated patients with NAFLD with a sensitivity of 89.0% and a specificity of 73.0% (AUC: 85.7%; 95%CI: 79.6-91.7%). NAFLD was exhibited by 83.9% of patients with 25(OH)D levels < 18.25ng/ml and by 18% of those with 25(OH)D levels ≥ 18.25ng/ml (p < 0.0001). In people with chronic SCI, 25(OH)D levels < 18.25ng/ml may represent a marker of NAFLD independent of MetS-related features. Further studies are warranted to define the cause-effect relationships of this association.

Differential remodeling of subcutaneous white and interscapular brown adipose tissue by long-term exercise training in aged obese female mice

Obesity exacerbates aging-induced adipose tissue dysfunction. This study aimed to investigate the effects of long-term exercise on inguinal white adipose tissue (iWAT) and interscapular brown adipose tissue (iBAT) of aged obese mice. Two-month-old female mice received a high-fat diet for 4 months. Then, six-month-old diet-induced obese animals were allocated to sedentarism (DIO) or to a long-term treadmill training (DIOEX) up to 18 months of age. In exercised mice, iWAT depot revealed more adaptability, with an increase in the expression of fatty acid oxidation genes (Cpt1a, Acox1), and an amelioration of the inflammatory status, with a favorable modulation of pro/antiinflammatory genes and lower macrophage infiltration. Additionally, iWAT of trained animals showed an increment in the expression of mitochondrial biogenesis (Pgc1a, Tfam, Nrf1), thermogenesis (Ucp1), and beige adipocytes genes (Cd137, Tbx1). In contrast, iBAT of aged obese mice was less responsive to exercise. Indeed, although an increase in functional brown adipocytes genes and proteins (Pgc1a, Prdm16 and UCP1) was observed, few changes were found on inflammation-related and fatty acid metabolism genes. The remodeling of iWAT and iBAT depots occurred along with an improvement in the HOMA index for insulin resistance and in glucose tolerance. In conclusion, long-term exercise effectively prevented the loss of iWAT and iBAT thermogenic properties during aging and obesity. In iWAT, the long-term exercise program also reduced the inflammatory status and stimulated a fat-oxidative gene profile. These exercise-induced adipose tissue adaptations could contribute to the beneficial effects on glucose homeostasis in aged obese mice.

Effect of different pigmented cooked common beans on glucose and lipid metabolism in obese rats and 3T3 L1 cells

The effect of Azufrasin (yellow coat seed) and Flor de Junio (FJ) Dalia (pink-cream coat seed) cooked bean varieties was evaluated in high fat and fructose diet-fed rats to identify their health beneficial effects on obesity-related metabolic alterations. FJ Dalia and Azufrasin daily supplementation (10%) for six months decreased body weight (5–7%), serum triglycerides (28.5–36.4%), HOMA insulin resistance index (59.6–62.3%), and serum TNF-α (40.5–45.0%); moreover, FJ Dalia increased serum adiponectin (77.5%). Polyphenol-, phytosterol-, and saponin-rich extracts from Azufrasin and FJ Dalia were evaluated in 3T3 L1 cells. Both varieties up-regulated, Cpt1a and Acadm (fatty acid β-oxidation), and Glut4, Irs1, and Pi3k (insulin signaling cascade) and down-regulated Pparg and Cebpa (adipogenesis) and Fasn and Acaca (lipogenesis). These activities were associated with their high content of soyasaponins A3, Af, and Be for adipogenesis and lipid metabolism, as well as eriodictyol, ellagic acid, hesperidin and (+)-catechin and (−)-epicatechin and their derivatives, and β-campesterol hexoside for insulin signaling cascade. FJ Dalia and Azufrasin cooked beans could be consumed to ameliorate obesity and its metabolic complications.

Physical Activity and Insulin Sensitivity Independently Attenuate the Effect of FTO rs9939609 on Obesity.

The association between FTO rs9939609 and obesity is modified by physical activity (PA) and/or insulin sensitivity (IS). We aimed to assess whether these modifications are independent, to assess whether PA and/or IS modify the association between rs9939609 and cardiometabolic traits, and to elucidate underlying mechanisms. Genetic association analyses comprised up to 19,585 individuals. PA was self-reported, and IS was defined based on inverted HOMA insulin resistance index. Functional analyses were performed in muscle biopsies from 140 men and in cultured muscle cells. The BMI-increasing effect of the FTO rs9939609 A allele was attenuated by 47% with high PA (β [SE], -0.32 [0.10] kg/m2, P = 0.0013) and by 51% with high IS (-0.31 [0.09] kg/m2, P = 0.00028). Interestingly, these interactions were essentially independent (PA, -0.20 [0.09] kg/m2, P = 0.023; IS, -0.28 [0.09] kg/m2, P = 0.0011). The rs9939609 A allele was also associated with higher all-cause mortality and certain cardiometabolic outcomes (hazard ratio, 1.07-1.20, P > 0.04), and these effects tended to be weakened by greater PA and IS. Moreover, the rs9939609 A allele was associated with higher expression of FTO in skeletal muscle tissue (0.03 [0.01], P = 0.011), and in skeletal muscle cells, we identified a physical interaction between the FTO promoter and an enhancer region encompassing rs9939609. Greater PA and IS independently reduced the effect of rs9939609 on obesity. These effects might be mediated through altered expression of FTO in skeletal muscle. Our results indicated that PA and/or other means of increasing insulin sensitivity could counteract FTO-related genetic predisposition to obesity.

Korelacija FLI indeksa masne jetre sa indeksima insulinske rezistencije kod pacijenata sa metaboličkim sindromom

Introduction: Metabolic syndrome includes insulin resistance, visceral obesity, hypertension and dyslipidemia, which together lead to an increased risk of atherosclerosis, cardiovascular diseases, and diabetes mellitus. Insulin resistance is considered a pathophysiological mechanism underlying metabolic syndrome, characterized by inadequate glucose metabolism, hyperinsulinemia and lipid imbalance. Non-alcoholic fatty liver disease is a chronic disease characterized by microvesicular steatosis and isn't a consequence of the use of drugs, alcohol, or inherited diseases and is a hepatic manifestation of metabolic syndrome. Aim: Since insulin resistance is pathophysiologically related to metabolic liver diseases, the aim of this study was to investigate the correlation of the FLI index with insulin resistance indices HOMA and QUICKI, but also a comparison of the insulin resistance index HOMA, Quicki and Tyg and the FLI index of fatty liver in the complete sample and in the groups of overweight and obese patients with characteristics of the metabolic syndrome. Material and methods: The study included 70 patients who met the criteria for the diagnosis of metabolic syndrome and who were selected by reviewing the medical documentation. Patients were divided into two groups. Group A were overweight patients (BMI 25 - 29.9 kg/m2). Group B were obese patients (BMI &gt; 30 kg/m2). Insulin resistance index values were compared between groups and then correlated by statistical analysis with FLI index within groups and in a complete sample. Results: Statistical analysis found a correlation between the FLI index and the insulin resistance index HOMA (p = 0.03) in a complete sample. A statistically significant difference in the values of the FLI index between the examined groups was proved (p = 0.001). Conclusion: The positive correlation between the FLI index with the HOMA index speaks in favor of the interrelationship between insulin resistance and fatty liver in patients with metabolic syndrome. In this case, insulin resistance can be a predictor for the development of non-alcoholic fatty liver disease, steatosis, steatohepatitis, hepatocellular carcinoma and cardiovascular diseases.

LBMON175 Nadir Growth Hormone Concentrations In Patients With Acromegaly Relate To Disease Activity, Glucose Metabolism, BMI And Sex

Abstract Background In healthy subjects, nadir growth hormone (GH) concentrations following an oral glucose load are related to BMI, gender and estrogen use. To date, very few data exist on factors influencing nadir GH in patients with acromegaly. Methods Glucose suppression tests (2h-75g) were performed in 166 patients with acromegaly not receiving any acromegaly-specific medical therapy: 132 OGTTs were performed at the initial disease diagnosis and 126 after at least one pituitary surgery. Glucose, insulin and C-peptide were measured every 30 minutes and the metabolic response was evaluated by minimal model analysis. Uni- and multivariate regression analysis was performed to test the relationship between nadir GH concentrations, patient characteristics and parameters of disease activity, lipid and glucose metabolism. Results In patients with active acromegaly (46% males), nadir glucose concentrations positively correlated to fasting IGF-1 (expressed as fold-ULN; p&amp;lt;0. 001), fasting insulin and C-peptide (both p=0. 004), HOMA-insulin resistance index (p=0. 016), and prehepatic beta-cell function (p=0. 002), but not to BMI and gender. In multivariate analysis, fasting C-peptide and IGF-1 were both independent predictors of nadir GH levels in patients with newly diagnosed acromegaly (p&amp;lt;0. 001). When testing for sex-specific predictors of nadir GH, we found a negative relationship between nadir GH and age in male patients, but not in females. After surgery, IGF-1 decreased from 805.5 (3.2 xULN, IQR 437.8) to 277.5 ng/ml (1.1 xULN, IQR 234. 0) and nadir GH after glucose suppression decreased from 8.8 (IQR 16.2) to 0.5 ng/ml (IQR 1.9). The decrease in biomarkers of disease activity following surgery leads to changes in predictors of nadir GH: postoperatively nadir GH relates to IGF-1 (p&amp;lt;0. 001), prehepatic beta-cell function (p=0. 02), weight (p=0. 031) and BMI (p=0. 044), with beta-cell-function being the only independent predictor in multivariate analysis (p=0. 003). When postoperative OGTTs performed in men and women were separately analyzed, nadir GH remained in a positive relationship to GH and IGF-1 in both sexes, but the relationship with beta-cell-function and other parameters of glucose metabolism remained significant only in male patients. In addition, postoperative nadir GH in male patients positively relates to LDL-cholesterol and triglycerides, and negatively to gonadal axis activity. Conclusion Here we describe that nadir GH concentrations in patients with acromegaly are mainly determined by parameters of disease activity and beta-cell function, but not by BMI and sex. A positive relationship between nadir GH and weight/BMI is only observed following improvement of disease activity after surgery, but appears mainly influenced by morphologic gender differences, as it disappears when male and female cohorts are analyzed separately. Presentation: Monday, June 13, 2022 12:30 p.m. - 2:30 p.m.

The reproductive endocrine feature and conception outcome of women with unknown etiological menstrual cycle (36–45 days) with long follicular phase

Objective To explore the reproductive endocrine feature and conception outcome of women with unknown etiological long menstrual cycle (LMC) (36–45 days) with long follicular phase. Methods In the cohort study, we included 80 women with unknown etiological long menstrual cycle of biphasic basal body temperature (BBT) lasting for 36–45 days and 87 controls with normal cycle of biphasic BBT into LMC group and NMC group, respectively. Serum hormone levels, fasting glucose, and insulin of participants were tested, and ovulation was observed by ultrasound. The conception outcome was followed up within 12 menstrual cycles. Results In the LMC group, the rate of abnormality of HOMA-insulin resistance index (40.0% vs. 20.7%, p < .01), luteal phase defect (30.9% vs. 13.8%, p < .05) and abnormality of FSH/LH ratio (15.6% vs. 5.7%, p < .05) were all significantly higher, but the serum estradiol level on the day before ovulation (261.10 pg/mL vs. 320.26 pg/mL, p < .01) was lower. The rate of poor ovulation quality (31.3% vs.15.4%, p < .05) in the LMC group was significantly higher than the NMC group. In the LMC group, the natural conception rate within 12 menstrual cycles was lower (41.9% vs. 66.2%, p < .01), whereas the spontaneous abortion rate in early pregnancy (29.0% vs. 9.8%, p < .05) and the conversion rate (21.6% vs. 5.2%, p < .01) to anovulation within 12 cycles were significantly higher. Conclusions Women with unknown etiological menstrual cycle (36–45 days) with long follicular phase have greater endocrine abnormality and higher risk of spontaneous abortion, infertility, and conversion to anovulation. Moderate early intervention may be advisable for these women, especially those who wish to get pregnant.

Correlation between the accumulation of skin glycosylation end products and the development of type 2 diabetic peripheral neuropathy

BackgroundThe accumulation of advanced glycation end products (AGEs) occurring in skin tissues can be measured by AGE Reader. Here, we assessed the correlation between AGEs values and the development of type 2 diabetic peripheral neuropathy (DPN).MethodsThe basic clinical information of 560 patients with T2DM was collected through an electronic system. AGEs and diabetic complication risk score was measured by AGE Reader, a non-invasive optical signal detector. All of the participants were classified into 4 groups based on Dyck criteria: grade 0 (non-DPN group), grade 1 (early stage group), grade 2 (middle stage group) and grade 3 (advanced group). Pearson correlation analysis and Spearman correlation analysis were used to evaluate the correlation between AGEs and other indexes. The sensitivity and specificity of glycosylated products were evaluated by ROC curve.ResultsWith the increase of DPN severity, the accumulative AGEs showed an increasing trend. Significant differences (P = 0.000) of AGEs were found among grades 0, 1, 2, and 3 of DPN, and significant differences (P = 0.000) of AGEs were found between grades 1 and 3. There were significant differences in DPN risk score between grades 0, 1, 2, and 3, between grades 1, 2, and 3, and between grades 2 and 3 (P < 0.01 or P < 0.05). AGEs were positively correlated with age, blood uric acid, disease course, systolic blood pressure, the risk scores of the four major complications of diabetes, renal function indicators (serum creatinine, Cystatin C, homocysteine, the ratio of urinary albumin and creatinine, urinary microalbumin, α-microglobulin, urinary transferrin, urinary immunoglobulin), inflammatory indicators (white blood cell count, neutrophil count, neutrophil-to-lymphocyte ratio, C-reactive protein), and TCSS score. However, it was negatively correlated with BMI,fasting insulin, insulin 1–3 h postprandial, lymphocyte count, HOMA insulin resistance index and estimated glomerular filtration rate. The area under the AGEs cumulant and neuropathy risk score curve was 0.769 and 0.743, respectively. The confidence intervals were (71.2–82.6%) and (68.8–79.9%), respectively. The maximum Youden’s index of AGEs cumulant was 0.440, and the corresponding AGEs cumulant value was 77.65. The corresponding sensitivity and specificity were 0.731 and 0.709, respectively. Furthermore, the maximum Youden’s index of neuropathy risk score was 0.385, and the corresponding neuropathy risk score was 66.25. The corresponding sensitivity and the specificity were 0.676 and 0.709, respectively.ConclusionThe cumulative amount of skin AGEs can be used as the diagnostic index and the prediction and evaluation index of DPN severity. Moreover, the diabetic peripheral neuropathy risk score can predict the risk of DPN in patients with T2DM.

IDF21-0114 Comparative Study of the Clinical Profile of FCPD and T2DM patients and Assess the Link of inflammatory markers and IR

Background: In progression of type 2 diabetes mellitus, inflammation plays an extremely vital and critical role along with insulin resistance (IR) and in long term results in further worsening of complications specially in fibrocalculous pancreatic diabetic patients (FCPD). FCPD is an uncommon form of diabetes that occurs as a result of chronic calcific pancreatitis, in the absence of alcohol abuse. Diabetes in FCPD is often brittle and difficult to control and most patients require multiple doses of insulin for control of glycemia. Aim: To assess the link between bio-inflammatory markers and IR in fibrocalculous pancreatic diabetic patients. Method: It is a cross sectional observational study. hsCRP was considered for assessing bio-inflammatory factor and HOMA index for IR among 70 FCPD subjects and 100 type 2 diabetes (T2DM). FCPD was diagnosed by evidence of ductal dilation measured by ultrasonography or by presence of pancreatic calculi on abdominal X-ray and absence of alcoholism, or other known causes of chronic pancreatitis in existing T2DM subjects. Results: 59.6±4.8 years was the mean age of the FCPD group whereas 37.4±5.1 years were for T2DM groups. FCPD patients had an earlier age at onset of diabetes (36.3 ± 15.1 years vs. 46.0±10.0 years; P = 0.031). BMI (20.7±2.1 vs 25.6±3.2 kg/m2), serum total cholesterol (147±34 vs 174±41 mg/dl), triglyceride (142±43 vs 217±94 mg/dl), and LDL cholesterol levels (91±24 vs 109±36 mg/dl) were significantly lower among FCPD patients than the T2DM patients (P<0.001). 22 subjects in FCPD group and 39 subjects in T2DM group were also diagnosed with retinopathy after initial fundoscopy. Glycated hemoglobin levels (HbA1C) were significantly higher in patients with FCPD as compare to T2DM group (9.4±2.2 vs 8.5±1.2 %, p<0.001). HOMA index among the FCPD group was 4.21 ± 1.1where as it was 5.37 ± 1.8 in T2DM group with significant P value (<0.05). A statistically significant difference (p < 0.001) was observed between the FCPD and T2DM in hsCRP (3.7±1.1 vs 1.6± 0.8). Discussion: Insulin resistance as measured by HOMA IR and inflammatory markers measured by hsCRP were found to be higher in pancreatic patients to that of type 2 DM. Despite the fact that the prevalence of FCPD being low, considering its impact of the condition on the quality of life (QOL) of the patients periodic screening is required specially for T2DM patients who complains of weight loss, back pain, abdominal pain, steatorrhoea or jaundice. Longer survival of FCPD patients also mandates periodic screening for possible risk of pancreatic adenocarcinoma.

Senescent macrophages in the human adipose tissue as a source of inflammaging

Obesity is a major risk factor for type 2 diabetes and a trigger of chronic and systemic inflammation. Recent evidence suggests that an increased burden of senescent cells (SCs) in the adipose tissue of obese/diabetic animal models might underlie such pro-inflammatory phenotype. However, the role of macrophages as candidate SCs, their phenotype, the distribution of SCs among fat depots, and clinical relevance are debated. The senescence marker β-galactosidase and the macrophage marker CD68 were scored in visceral (vWAT) and subcutaneous (scWAT) adipose tissue from obese patients (n=17) undergoing bariatric surgery and control patients (n=4) subjected to cholecystectomy. A correlation was made between the number of SCs and BMI, serum insulin, and the insulin resistance (IR) index HOMA. The monocyte cell line (THP-1) was cultured in vitro in high glucose milieu (60 mM D-glucose) and subsequently co-cultured with human adipocytes (hMADS) to investigate the reciprocal inflammatory activation. In obese patients, a significantly higher number of SCs was observed in vWAT compared to scWAT; about 70% of these cells expressed the macrophage marker CD68; and the number of SCs in vWAT, but not in scWAT, positively correlated with BMI, HOMA-IR, and insulin. THP-1 cultured in vitro in high glucose milieu acquired a senescent-like phenotype (HgSMs), characterized by a polarization toward a mixed M1/M2-like secretory phenotype. Co-culturing HgSMs with hMADS elicited pro-inflammatory cytokine expression in both cell types, and defective insulin signaling in hMADS. In morbid obesity, expansion of visceral adipose depots involves an increased burden of macrophages with senescent-like phenotype that may promote a pro-inflammatory profile and impair insulin signaling in adipocytes, supporting a framework where senescent macrophages fuel obesity-induced systemic inflammation and possibly contribute to the development of IR.

Антропометрична характеристика підлітків з ознаками метаболічного синдрому

An analysis of recent global research on the prevalence of obesity and its consequences, including metabolic syndrome, among adolescents is a matter of considerable concern. The same unfavorable tendencies are observed in Ukraine among modern youth. Therefore, an effective strategy for the detection and follow-up of adolescents is urgently needed for the timely treatment of obesity and the prevention of threatening complications. Purpose — to analyze and generalize anthropometrical indicators in adolescents with signs of metabolic syndrome to improve the management of this category of patients. Materials and methods. 200 obese adolescents (aged 16 years: 100 boys and 100 girls) were examined in the clinic of the Institute of Children and Adolescents Health Care of the National Academy of Medical Sciences of Ukraine. The control group consisted of 30 healthy children of the same age category. The criteria for the diagnosis of metabolic syndrome (MS) in children, proposed by the International Diabetes Federation [IDF, 2007], were used, which allowed to divide patients into two groups: 1 — with signs of MS (50.0%) and 2 — without signs of MS (50.0%), each of which included 100 patients. Patients underwent an anthropometric examination with the calculation of the following indicators: body mass index (BMI), the waist;to;growth ratio (WC/height) and waist circumference to hip circumference ratio (WC/HC). Blood lipid profile as a marker of atherogenesis, carbohydrate metabolism (fasting serum glucose, the level of immunoreactive insulin with the calculation of insulin resistance index HOMA) were also studied in detail. Results. The anthropometric analysis showed that in adolescents with MS the main indicators (BMI, WC/height, WC/HC), the degree of abdominal obesity were statistically significantly higher (p&lt;0.05). When comparing the results by gender, probable differences were found between boys and girls: indicators of body weight, waist circumference, WC/HC, which were statistically significantly higher in boys (p&lt;0.05). Characterization of lipid metabolism in the patients showed signs of atherogenic dyslipidemia (increased cholesterol levels, low and very low density lipoproteins, atherogenic factor, triglycerides, β-lipoproteins levels and tendencies to lower the levels of high density lipoproteins) with a significant predominance among those surveyed with MS (p&lt;0.05). Conclusions. Promising careful anthropometric monitoring of obese adolescents will identify and predict trends in the disease, the risk of complications, which will increase the effectiveness of preventive measures for metabolic syndrome. The research was carried out in accordance with the principles of the Helsinki Declaration. The study protocol was approved by the Local Ethics Committee of all participating institution. The informed consent of the patient was obtained for conducting the studies. No conflict of interest was declared by the authors. Key words: adolescents, metabolic syndrome, anthropometry, diagnostics, dyslipidemia.

Пролежні м’яких тканин у хворих на цукровий діабет 2-го типу: клінічні стратегії, показники інсулінорезистентності та аспекти комплексного лікування

Вступ. Причинами виникнення пролежневих трофічних виразок є ішемія та нейротрофічні зміни тканин, викликані їх тривалою хронічною компресією, постійним патологічним зволоженням та зсувом тканин, що детермінує виникнення локальної ішемії. Мета роботи: дослідити клінічні варіанти та гнійні ускладнення пролежнів у хворих на цукровий діабет (ЦД) 2-го типу з позицій наявності інсулінорезистентності (ІР) у контексті оптимізації комплексного лікування. Матеріали і методи. Загальну вибірку ретро- та проспективного аналізу становили результати комплексного лікування 112 пацієнтів. Наявність ЦД 2-го типу пiдтверджено в 37 пацієнтів, 27 пацієнтів iз пролежнями без ускладнень (І–ІІІ стадії) та ЦД становили І групу порівняння, iз пролежнями IV стадії — ІІ групу порівняння, інші 75 осiб — групу контролю. Результати. У хворих на ЦД 2-го типу (І група порівняння) спостерігалося вірогідно значуще зменшення НОМА-індексу функції β-клітин та збільшення НОМА-індексу ІР (8,31 ± 0,02, р &lt; 0,01). У хворих на ЦД 2-го типу з наявністю ускладнених пролежнів (ІІ група порівняння) зареєстровано більш значне підвищення показників циркулюючого інсуліну (p2 &lt; 0,01), НОМА-індексу ІР (p2 &lt; 0,05) та значне зменшення НОМА-індексу функції β-клітин (р &lt; 0,05). При проведенні кореляційного аналізу показникiв НОМА-ІР та концентрації елементів у крові кореляційний зв’язок був встановлений тільки у хворих на ЦД 2-го типу (І та ІІ групи порівняння): між показником НОМА-ІР та вмістом Mg2+ в еритроцитах виявлено негативний сильний кореляційний зв’язок (r = –0,72; Р &lt; 0,01), між НОМА-ІР та концентрацією Zn2+ у сироватці крові — негативний зв’язок середньої сили (r = –0,66; p &lt; 0,01) та між НОМА-ІР й рівнем Cr3+ у сироватці крові — негативний кореляційний (r = –0,69; p &lt; 0,01). Висновки. Перевагою запропонованої класифікації пролежнів м’яких тканин та послідовності комплексного лікування є врахування особливостей патогенезу, морфогенезу та клінічного перебігу пролежнів з ускладненнями, які мають вплив на перебіг загоєння та потребують адекватних стратегій лікування гнійних ран — TIME і DOMINATE, що, на нашу думку, детермінує можливість впровадження в клінічну практику відділень паліативної допомоги, інших стаціонарних та амбулаторних закладів охорони здоров’я.

Clinical and pathogenetic significance of comorbid osteoporosis in diabetes mellitus in women with menopause

Background. Osteoporosis is a serious problem due to the high morbidity, mortality and significant costs for medical care. Moreover, in women in the menopausal period, bone fragility due to osteoporosis is more pronounced, and osteoporotic vertebral fractures are three times more common than in men. Type 2 diabetes mellitus (DM) is closely associated with osteoporosis, and some hormonal and peptide markers of bone metabolism simultaneously determine bone mineralization and the state of carbohydrate metabolism. The purpose was to assess the course of diabetes in women during menopause and to study the clinical and pathogenetic relationship with the presence of osteoporosis in them. Materials and methods. Two hundred and sixty-one women with menopause were examined. They were divided into two groups: 17 % with DM (main one) and 83 % without DM (comparison group). In 51 % of cases, osteoporosis was diagnosed (osteopenia and osteoporosis ratio was 4 : 1). The study of carbohydrate metabolism included the determination of insulin resistance HOMA index and the severity of metabolic syndrome, blood levels of insulin, glucose, glycosylated hemoglobin and C-peptide, and markers of bone metabolism were serum parameters of parathyroid hormone, calcitonin, osteocalcin, osteopontin, alkaline phosphatase activity, chemical elements (Ca, P, Mg, Co, Cr, Cu, Mn, Pb, Se, Sr, Zn). Results. DM was diagnosed in 34 % of women with osteoporosis, which directly correlates with their age, frequency and severity of other signs of metabolic syndrome (hyperinsulinemia, hyperlipidemia, hyperuricemia, arterial hypertension, obesity), the absence of cases of normal lipidemia and type IIA lipid metabolism disorders, but with the prevalence of type IIB, a higher rate of alkaline phosphatase activity in the blood and lower values of osteopontin and selenium. Besides, DM severity is closely related to the parameters of mineral bone density and phosphatemia level, and the development of diabetic retinopathy, nephropathy and peripheral macro-/microangiopathy, respectively, depends on the content of selenium, zinc and osteopontin, and the rate of calcemia has prognostic significance. Conclusions. The pathogenetic significance of comorbid osteoporosis, parameters of bone mineral density and markers of bone metabolism in the blood serum of women with menopause in the development of DM, the severity of its course and complications has been proven, and the indicators of osteopontin, calcium, selenium and zinc have prognostic significance.

Risk factors of the development of vascular and neuropathic complications in patients with type 2 diabetes mellitus and autoimmune thyroiditis

Issues of the formation and progression of late complications of diabetes mellitus remain interesting and foreground today, especially in cases of type 2 diabetes mellitus (dm) combined with other endocrine diseases. The pathogenetic relation between the mechanisms leading to blood vessels and nerves damage against the background of diabetes mellitus, and, for example, mechanisms of autoimmune thyroid abnormality (ait), is far from being unambiguous, but the very fact of its existence cannot be denied.Purpose: to determine the predominant type of comorbidity (trans-syndromal, trans-nosological or chronological) and the level of comorbidity according to the disease rating scale (cirs) in patients with type 2 diabetes and ait, to study the structure of later complications of diabetes mellitus in this group of patients and to assess the contribution of certain factors to increased risk of complications.Methods. 428 patients were examined in a specialized endocrinology department, and two groups were formed: an observation group — 213 people with diagnosed type 2 diabetes and ait, and a comparison group — 215 people with a diagnosis of type 2 diabetes. These groups were comparable in age, the duration of diabetes, body mass index, correction of the disease. The analysis included clinical and laboratory parameters, the results of hormones level studies (tsh, free t4, insulin, c-peptide) and antibodies (at-tpo), thyroid ultrasonography, calculation of the insulin resistance index (homa) and the comorbidity index (cirs — cumulative illness rating scale) followed by a correlation-regression analysis of statistical data. The state of the peripheral nervous system was evaluated with the use of electromyography in patients of both groups, and the severity of diabetic neuropathy was evaluated with the use of the neuropathy disability score and vas (visual analogue scale) scales. The state of the vascular system was studied according to the data of ultrasound examination of the vessels of the lower extremities, echocardiography, and ophthalmoscopy.Results. The obtained data made it possible to determine the factors infl uencing the risk of type 2 diabetes complications developement, and to establish that neuropathic complications begin and progress faster in patients with comorbid endocrine pathology, however, there is no such dependence for vascular complications. According to the linear regression equation of the dependence of total complications on the duration of the disease, it was revealed that the development of vascular complications in patients with combined endocrinopathy occurs even more slowly than in patients with diabetes. The contribution of diabetes compensation and identifi ed risk factors to the progression of diabetic complications was less important for patients with endocrinopathies. As for evaluating the contribution of individual parameters, the most signifi cant were the duration of diabetes mellitus, albuminuria, atherosclerosis of the vessels of the lower extremities.Conclusion. In addition to the known risk factors for the development and progression of vascular complications, in patients with overlapping endocrinopathy, the preservation of residual insulin secretion and renal function (chronic kidney disease, proteinuria) were important. the prevalence of “total” Complications in the group of patients with combined endocrine pathology was lower, however, neuropathic complications in the same group were observed more often,т which indicates the primary eff ect of thyroid dysfunction on the structure of the nervous tissue.

New opportunities for the correction of non-alcoholic fatty liver disease in men with type 2 diabetes mellitus and hypogonadism

Background: The common pathogenetic relations of type 2 diabetes mellitus (T2DM), testosterone (T) deficiency and non-alcoholic fatty liver disease (NAFLD) have indicated a new direction in the study of their mutual influence. It was found that NAFLD is more pronounced in men with T2DM and hypogonadism than in eugonadal patients and associated with hyperinsulinemia, insulin resistance, impaired lipid metabolism and adipose tissue dysfunction. However, the effects of testosterone replacement therapy (TRT) on the severity of NAFLD in men with hypogonadism have not been studied.Aims: To study the effect of TRT on the severity of NAFLD in men with T2DM and hypogonadism.MATERIALS AND METHODS: Anthropometric data, biochemical parameters (alanine aminotransferase (ALT), aspartate aminotransferase (AST), gamma-glutamyltranspeptidase (GGTP), glucose, immunoreactive insulin, HOMA index, glycosylated hemoglobin, lipidogram), ELISA analysis (total T, LH, sex hormone binding globulin, resistin, adiponectin, leptin), as well as magnetic resonance imaging with determination of the liver fat fraction were examined.Results: The study included 60 men with T2DM and hypogonadism (mean age 54 [49; 57] years), who were randomized into 2 groups: 1 (n=30) - patients who received 1% transdermal T gel (50 mg/day) in addition to standard hypoglycemictherapy; 2 (n=30) - patients who received standard hypoglycemic therapy. The follow-up period was 6 months. T therapy was associated with a decrease in liver enzyme levels: AST by 31%, ALT by 21%, and GGTP by 15.9% (p&lt;0.05) and the hepatic fat fraction by 1.7 times, which reflect the regress of liver inflammation, and, consequently, a decrease in the severity of NAFLD. Moreover, TRT has improved the function of adipose tissue - reduced the concentration of leptin by 1.4 times and resistin by 1.5 times, which was accompanied by an increase in adiponectin level by 1.3 times (p&lt;0.01). The use of TRT was associated with decrease in the severity of visceral obesity, hyperinsulinemia by 1.5 times, an insulin resistance index HOMA by 2.2 times, fasting glycaemia and HbA1c levels, despite constant hypoglycemic therapy. Statistically significant decrease in the levels of total cholesterol and triglycerides was observed in men receiving TRT. Thus, a decrease in adipose tissue dysfunction and insulin resistance in men receiving TRT can be considered as a pathogenetic mechanism responsible for improving liver function and reducing the severity of NAFLD.Conclusions: TRT in men with T2DM and hypogonadism is accompanied by regress of inflammatory activity in liver and intensity of hepatocytes steatosis, reflected by decrease in liver enzymes levels and liver fat fraction.

Evidence for Training-Induced Changes in miRNA Levels in the Skeletal Muscle of Patients With Type 2 Diabetes Mellitus.

Physical training can improve glycemic control in patients with type 2 diabetes mellitus (T2DM). However, the underlying mechanisms are not entirely clear. An interesting piece of the puzzle could be the regulation of micro-RNAs (miRNAs). They are important modulators of protein expression. Some miRNAs were found to be both linked to poor glycemic control/insulin resistance (with evidence from in vivo and/or in vitro studies) and dysregulated in the skeletal muscle of T2DM patients. This pilot study examines whether a 3-month endurance training program [three times a week, 70–80% peak heart rate (HRpeak)] can down-regulate their levels in T2DM men (n = 7). One skeletal muscle biopsy sample was obtained from each patient at T1 (6 weeks pre-intervention), one at T2 (1 week pre-intervention) and one at T3 (3–4 days post-intervention). miRNA-27a-3p, −29a-3p, −29b-3p, −29c-3p, −106b-5p, −135a-5p, −143-3p, −144-3p, −194-5p, and − 206 levels were determined by RT-qPCR. Friedman ANOVA and post-hoc tests showed that miRNA-29b-3p, −29c-3p and -135a-5p levels were significantly reduced post-training (T3 vs. T2 and/or T1). Glycated hemoglobin (HbA1c) and HOMA insulin resistance index did not change significantly. However, HbA1c was reduced in 6 of 7 patients post-training. Furthermore, Spearman’s rank correlation analyses with all values from all time points showed significant negative associations between miRNA-29c-3p, −106b-5p, −144-3p and −194-5p levels and cardiorespiratory fitness (VO2peak). The study results imply that regular exercise and improving one’s physical fitness is helpful for the regulation of skeletal muscle miRNAs in T2DM patients. Whether or not changes in the miRNA profile can affect the clinical situation of T2DM patients warrants further research.