Your search keyword '"Joglekar, Mugdha V."' showing total 48 results

1. Short-chain fatty acids and insulin sensitivity: a systematic review and meta-analysis.

Author

Pham, Nhan H T, Joglekar, Mugdha V, Wong, Wilson K M, Nassif, Najah T, Simpson, Ann M, and Hardikar, Anandwardhan A

Subjects

FASTING, ONLINE information services, META-analysis, MEDICAL information storage & retrieval systems, CONFIDENCE intervals, SYSTEMATIC reviews, BLOOD sugar, INSULIN sensitivity, INSULIN, TREATMENT effectiveness, DESCRIPTIVE statistics, RESEARCH funding, MEDLINE, SHORT-chain fatty acids

Abstract

Context There is substantial evidence that reduced short-chain fatty acids (SCFAs) in the gut are associated with obesity and type 2 diabetes, although findings from clinical interventions that can increase SCFAs are inconsistent. Objective This systematic review and meta-analysis aimed to assess the effect of SCFA interventions on fasting glucose, fasting insulin, and homeostatic model assessment of insulin resistance (HOMA-IR). Data Sources Relevant articles published up to July 28, 2022, were extracted from PubMed and Embase using the MeSH (Medical Subject Headings) terms of the defined keywords [(short-chain fatty acids) AND (obesity OR diabetes OR insulin sensitivity)] and their synonyms. Data analyses were performed independently by two researchers who used the Cochrane meta-analysis checklist and the PRISMA guidelines. Data Extraction Clinical studies and trials that measured SCFAs and reported glucose homeostasis parameters were included in the analysis. Standardized mean differences (SMDs) with 95%CIs were calculated using a random-effects model in the data extraction tool Review Manager version 5.4 (RevMan 5.4). The risk-of-bias assessment was performed following the Cochrane checklist for randomized and crossover studies. Data Analysis In total, 6040 nonduplicate studies were identified, 23 of which met the defined criteria, reported fasting insulin, fasting glucose, or HOMA-IR values, and reported change in SCFA concentrations post intervention. Meta-analyses of these studies indicated that fasting insulin concentrations were significantly reduced (overall effect: SMD = −0.15; 95%CI = −0.29 to −0.01, P = 0.04) in treatment groups, relative to placebo groups, at the end of the intervention. Studies with a confirmed increase in SCFAs at the end of intervention also had a significant effect on lowering fasting insulin (P = 0.008). Elevated levels of SCFAs, compared with baseline levels, were associated with beneficial effects on HOMA-IR (P < 0.00001). There was no significant change in fasting glucose concentrations. Conclusion Increased postintervention levels of SCFAs are associated with lower fasting insulin concentrations, offering a beneficial effect on insulin sensitivity. Systematic Review Registration PROSPERO registration number CRD42021257248. [ABSTRACT FROM AUTHOR]

Published

2024

2. MicroRNAs Signature Panel Identifies Heavy Drinkers with Alcohol-Associated Cirrhosis from Heavy Drinkers without Liver Injury.

Author

Shihana, Fathima, Joglekar, Mugdha V., Schwantes-An, Tae-Hwi, Hardikar, Anandwardhan A., and Seth, Devanshi

Subjects

ALCOHOLISM, MICRORNA, ALCOHOL, LIVER injuries, GENOME-wide association studies, GENETIC variation

Abstract

Simple Summary: Alcohol-associated liver disease (ALD) is a preventable disease if identified early, but current biomarkers lack specificity to identify who amongst drinkers will progress to advanced disease, i.e., cirrhosis. MicroRNAs are small molecules that play a regulatory role in several diseases, are affected by alcohol and may be important players in alcohol use disorders, such as ALD. So far, microRNAs associated with ALD are based on comparisons with non-drinking healthy controls. Our new approach was to compare global miRNA profiles in heavy drinking patients without liver injury versus heavy drinkers with cirrhosis to identify miRNAs specific to liver disease. Our novel discoveries include (i) the identification of a set of microRNAs that differentiated drinkers with cirrhosis from those without liver injury; (ii) an inverse relationship of microRNAs expression with disease severity, suggesting their potential use in monitoring disease progression; (iii) the identification of microRNA target pathways involved in cell death, inflammation, fibrosis and fat metabolism; (iv) and the association of some microRNAs with known genetic risks involved in triglyceride metabolism, underscoring the growing role of lipids (fats) in ALD. This study advances knowledge in the field by identifying new microRNAs as potential diagnostic and/or therapeutic targets. Background: Alcohol-associated liver disease (ALD) is the most common disorder of prolonged drinking. Mechanisms underlying cirrhosis in such patients remain unclear. MicroRNAs play regulatory role in several diseases, are affected by alcohol and may be important players in alcohol use disorders, such as cirrhosis. Methods: We investigated serum samples from heavy chronic alcohol users (80 g/day (male) and 50 g/day (female) for ≥10 years) that were available from our previously reported GenomALC study. A subset of GenomALC drinkers with liver cirrhosis (cases, n = 24) and those without significant liver disease (drinking controls, n = 23) were included. Global microRNA profiling was performed using high-throughput real-time quantitative PCR to identify the microRNA signatures associated with cirrhosis. Ingenuity Pathway Analysis (IPA) software was utilized to identify target mRNAs of significantly altered microRNAs, and molecular pathways were analysed. Identified microRNAs were analysed for correlation with traditional liver disease biomarkers and risk gene variants previously reported from GenomALC genome-wide association study. Results: The expression of 21 microRNAs was significantly downregulated in cases compared to drinking controls (p < 0.05, ∆∆Ct > 1.5-fold). Seven microRNAs (miR-16, miR-19a, miR-27a, miR-29b, miR-101, miR-130a, and miR-191) had a highly significant correlation (p < 0.001) with INR, bilirubin and MELD score. Three microRNAs (miR-27a, miR-130a and miR-191) significantly predicted cases with AUC-ROC 0.8, 0.78 and 0.85, respectively (p < 0.020); however, INR performed best (0.97, p < 0.001). A different set of six microRNAs (miR-19a, miR-26a, miR-101, miR-151-3p, miR-221, and miR-301) showed positive correlation (ranging from 0.32 to 0.51, p < 0.05) with rs10433937:HSD17B13 gene variant, associated with the risk of cirrhosis. IPA analysis revealed mRNA targets of the significantly altered microRNAs associated with cell death/necrosis, fibrosis and increased steatosis, particularly triglyceride metabolism. Conclusions: MicroRNA signatures in drinkers distinguished those with liver cirrhosis from drinkers without liver disease. We identified mRNA targets in liver functions that were enriched for disease pathogenesis pathways. [ABSTRACT FROM AUTHOR]

Published

2023

3. Optimised plasma sample preparation and LC‐MS analysis to support large‐scale proteomic analysis of clinical trial specimens: Application to the Fenofibrate Intervention and Event Lowering in Diabetes (FIELD) trial.

Author

O'Rourke, Matthew B., Januszewski, Andrzej S., Sullivan, David R., Lengyel, Imre, Stewart, Alan J., Arya, Swati, Ma, Ronald C., Galande, Sanjeev, Hardikar, Anandwardhan A., Joglekar, Mugdha V., Keech, Anthony C., Jenkins, Alicia J., and Molloy, Mark P.

Published

2023

4. The link between glycemic control measures and eye microvascular complications in a clinical cohort of type 2 diabetes with microRNA-223-3p signature.

Author

Da’as, Sahar I., Ahmed, Ikhlak, Hasan, Waseem H., Abdelrahman, Doua A., Aliyev, Elbay, Nisar, Sabah, Bhat, Ajaz Ahmad, Joglekar, Mugdha V., Hardikar, Anandwardhan A., Fakhro, Khalid A., and Akil, Ammira S. Al-Shabeeb

Abstract

Background: Type 2 diabetes (T2D) is a critical healthcare challenge and priority in Qatar which is listed amongst the top 10 countries in the world, with its prevalence presently at 17% double the global average. MicroRNAs (miRNAs) are implicated in the pathogenesis of (T2D) and long-term microvascular complications including diabetic retinopathy (DR). Methods: In this study, a T2D cohort that accurately matches the characteristics of the general population was employed to find microRNA (miRNA) signatures that are correlated with glycemic and β cell function measurements. Targeted miRNA profiling was performed in (471) T2D individuals with or without DR and (491) (non-diabetic) healthy controls from the Qatar Biobank. Discovery analysis identified 20 differentially expressed miRNAs in T2D compared to controls, of which miR-223-3p was significantly upregulated (fold change:5.16, p = 3.6e−02) and positively correlated with glucose and hemoglobin A1c (HbA1c) levels (p-value = 9.88e−04 and 1.64e−05, respectively), but did not show any significant associations with insulin or C-peptide. Accordingly, we performed functional validation using a miR-223-3p mimic (overexpression) under control and hyperglycemia-induced conditions in a zebrafish model. Results: Over-expression of miR-223-3p alone was associated with significantly higher glucose (42.7 mg/dL, n = 75 vs 38.7 mg/dL, n = 75, p = 0.02) and degenerated retinal vasculature, and altered retinal morphology involving changes in the ganglion cell layer and inner and outer nuclear layers. Assessment of retinal angiogenesis revealed significant upregulation in the expression of vascular endothelial growth factor and its receptors, including kinase insert domain receptor. Further, the pancreatic markers, pancreatic and duodenal homeobox 1, and the insulin gene expressions were upregulated in the miR-223-3p group. Conclusion: Our zebrafish model validates a novel correlation between miR-223-3p and DR development. Targeting miR-223-3p in T2D patients may serve as a promising therapeutic strategy to control DR in at-risk individuals. [ABSTRACT FROM AUTHOR]

Published

2023

5. Early emergence of sexual dimorphism in offspring leukocyte telomere length was associated with maternal and children's glucose metabolism—a longitudinal study.

Author

Wong, Kwun Kiu, Cheng, Feifei, Lim, Cadmon K. P., Tam, Claudia H. T., Tutino, Greg, Yuen, Lai Yuk, Wang, Chi Chiu, Hou, Yong, Chan, Michael H. M., Ho, Chung Shun, Joglekar, Mugdha V., Hardikar, Anandwardhan A., Jenkins, Alicia J., Metzger, Boyd E., Lowe Jr., William L., Tam, Wing Hung, and Ma, Ronald C. W.

Subjects

SEXUAL dimorphism, GLUCOSE metabolism, TELOMERES, LEUCOCYTES, LONGITUDINAL method

Abstract

Background: Leukocyte telomere length (LTL) is suggested to be a biomarker of biological age and reported to be associated with metabolic diseases such as type 2 diabetes. Glucose metabolic traits including glucose and insulin levels have been reported to be associated with LTL in adulthood. However, there is relatively little research focusing on children's LTL and the association with prenatal exposures. This study investigates the relationship between maternal and offspring glucose metabolism with offspring LTL in early life. Methods: This study included 882 mother-child pairs from the HAPO Hong Kong Field Centre, with children evaluated at age 7.0 ± 0.4 (mean ± SD) years. Glucose metabolic traits including maternal post-load glucose during pregnancy, children's glucose and insulin levels, and their derived indices at follow-up were measured or calculated. Offspring LTL was assessed using real-time polymerase chain reaction. Results: Sex- and age-adjusted children's LTL was found to be associated with children's HOMA-IR (β=−0.046 ± 0.016, p=0.005). Interestingly, both children's and maternal post-load glucose levels were positively associated with children's LTL. However, negative associations were observed between children's LTL and children's OGTT insulin levels. In addition, the LTL in females was more strongly associated with pancreatic beta-cell function whilst LTL in males was more strongly associated with OGTT glucose levels. Conclusions: Our findings suggest a close association between maternal and offspring glucose metabolic traits with early life LTL, with the offspring sex as an important modifier of the disparate relationships in insulin production and response. [ABSTRACT FROM AUTHOR]

Published

2022

6. Circulating microRNAs from early childhood and adolescence are associated with pre-diabetes at 18 years of age in women from the PMNS cohort.

Author

Joglekar, Mugdha V., Kunte, Pooja S., Wong, Wilson K.M., Bhat, Dattatray. S., Satoor, Sarang N., Patil, Rohan R., Karandikar, Mahesh S., Fall, Caroline H. D., Yajnik, Chittaranjan S., and Hardikar, Anandwardhan A.

Subjects

PREDIABETIC state, MICRORNA, GLUCOSE intolerance, TYPE 2 diabetes, MATERNAL nutrition

Abstract

With type 2 diabetes presenting at younger ages, there is a growing need to identify biomarkers of future glucose intolerance. A high (20%) prevalence of glucose intolerance at 18 years was seen in women from the Pune Maternal Nutrition Study (PMNS) birth cohort. We investigated the potential of circulating microRNAs in risk stratification for future pre-diabetes in these women. Here, we provide preliminary longitudinal analyses of circulating microRNAs in normal glucose tolerant (NGT@18y, N = 10) and glucose intolerant (N = 8) women (ADA criteria) at 6, 12 and 17 years of their age using discovery analysis (OpenArray™ platform). Machine-learning workflows involving Lasso with bootstrapping/leave-one-out cross-validation identified microRNAs associated with glucose intolerance at 18 years of age. Several microRNAs, including miR-212-3p, miR-30e-3p and miR-638, stratified glucose-intolerant women from NGT at childhood. Our results suggest that circulating microRNAs, longitudinally assessed over 17 years of life, are dynamic biomarkers associated with and predictive of pre-diabetes at 18 years of age. Validation of these findings in males and remaining participants from the PMNS birth cohort will provide a unique opportunity to study novel epigenetic mechanisms in the life-course progression of glucose intolerance and enhance current clinical risk prediction of pre-diabetes and progression to type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2022

7. Short-chain fatty acid concentrations in the incidence and risk-stratification of colorectal cancer: a systematic review and meta-analysis.

Author

Alvandi, Ehsan, Wong, Wilson K. M., Joglekar, Mugdha V., Spring, Kevin J., and Hardikar, Anandwardhan A.

Abstract

Background: The beneficial role of gut microbiota and bacterial metabolites, including short-chain fatty acids (SCFAs), is well recognized, although the available literature around their role in colorectal cancer (CRC) has been inconsistent.Methods: We performed a systematic review and meta-analysis to examine the associations of fecal SCFA concentrations to the incidence and risk of CRC. Data extraction through Medline, Embase, and Web of Science was carried out from database conception to June 29, 2022. Predefined inclusion/exclusion criteria led to the selection of 17 case-control and six cross-sectional studies for quality assessment and analyses. Studies were categorized for CRC risk or incidence, and RevMan 5.4 was used to perform the meta-analyses. Standardized mean differences (SMD) with 95% confidence intervals (CI) were calculated using a random-effects model. Studies lacking quantitation were included in qualitative analyses.Results: Combined analysis of acetic, propionic, and butyric acid revealed significantly lower concentrations of these SCFAs in individuals with a high-risk of CRC (SMD = 2.02, 95% CI 0.31 to 3.74, P = 0.02). Additionally, CRC incidence was higher in individuals with lower levels of SCFAs (SMD = 0.45, 95% CI 0.19 to 0.72, P = 0.0009), compared to healthy individuals. Qualitative analyses identified 70.4% of studies reporting significantly lower concentrations of fecal acetic, propionic, butyric acid, or total SCFAs in those at higher risk of CRC, while 66.7% reported significantly lower concentrations of fecal acetic and butyric acid in CRC patients compared to healthy controls.Conclusions: Overall, lower fecal concentrations of the three major SCFAs are associated with higher risk of CRC and incidence of CRC. [ABSTRACT FROM AUTHOR]

Published

2022

8. Vitamin D Levels During Pregnancy Are Associated With Offspring Telomere Length: A Longitudinal Mother-Child Study.

Author

Kwun Kiu Wong, Feifei Cheng, Di Mao, Lim, Cadmon K. P., Tam, Claudia H. T., Chi Chiu Wang, Lai Yuk Yuen, Chan, Michael H. M., Chung Shun Ho, Joglekar, Mugdha V., Hardikar, Anandwardhan A., Jenkins, Alicia J., Metzger, Boyd E., Lowe Jnr., William L., Wing Hung Tam, and Ma, Ronald C. W.

Subjects

BIOMARKERS, METABOLIC disorders, VITAMIN D

Abstract

Context: Leukocyte telomere length (LTL) is a biomarker of biological aging and is associated with metabolic diseases such as type 2 diabetes. Insufficient maternal vitamin D was associated with increased risk for many diseases and adverse later life outcomes. Objective: This study investigates the relationship between vitamin D levels and offspring LTL at early life. Methods: This observational, longitudinal, hospital-based cohort study included eligible mother-child pairs from the HAPO Hong Kong Field Centre, with 853 offspring at age 6.96 ± 0.44 (mean ± SD) years. LTL was measured using real-time polymerase chain reaction while serum vitamin D metabolites 25(OH)D2, 25(OH)D3, and 3-epi-25(OH)D3 were measured in maternal blood (at gestation 24-32 weeks) and cord blood by liquid chromatography–mass spectrometry. Results: LTL at follow-up was significantly shorter in boys compared with girls (P < 0.001) at age 7. Childhood LTL was negatively associated with childhood BMI (β ± SE = -0.016 ± 0.007)(P = 0.02) and HOMA-IR (β ± SE = −0.065 ± 0.021)(P = 0.002). Multiple linear regression was used to evaluate the relationship between 25(OH)D and LTL, with covariate adjustments. Childhood LTL was positively correlated with total maternal 25(OH)D (0.048 ± 0.017) (P = 0.004) and maternal 3-epi-25(OH)D3 (0.05 ± 0.017) (P = 0.003), even after adjustment for covariates. A similar association was also noted for cord 3-epi-25(OH)D3 (0.037 ± 0.018) (P = 0.035) after adjustment for offspring sex and age. Conclusion: Our findings suggest 25(OH)D3 and 3-epi-25(OH)D3 in utero may impact on childhood LTLs, highlighting a potential link between maternal vitamin D and biological aging. [ABSTRACT FROM AUTHOR]

Published

2022

9. The microRNA-29 family: role in metabolism and metabolic disease.

Author

Dalgaard, Louise T., Sørensen, Anja E., Hardikar, Anandwardhan A., and Joglekar, Mugdha V.

Subjects

METABOLIC disorders, ANTISENSE nucleic acids, TYPE 2 diabetes, GESTATIONAL diabetes, DIABETIC nephropathies, METABOLISM, INSULIN

Abstract

The microRNA-29 family members miR-29a-3p, miR-29b-3p, and miR-29c-3p are ubiquitously expressed and consistently increased in various tissues and cell types in conditions of metabolic disease, obesity, insulin resistance, and type 2 diabetes. In pancreatic β cells, miR-29a is required for normal exocytosis, but increased levels are associated with impaired β-cell function. Similarly, in liver, miR-29 species are higher in models of insulin resistance and type 2 diabetes, and either knock-out or depletion using a microRNA inhibitor improves hepatic insulin resistance. In skeletal muscle, miR-29 family upregulation is associated with insulin resistance and altered substrate oxidation, and similarly, in adipocytes, overexpression of miR-29a leads to insulin resistance. Blocking miR-29a using nucleic acid antisense therapeutics show promising results in preclinical animal models of obesity and type 2 diabetes, although the widespread expression pattern of miR-29 family members complicates the exploration of single target tissues. However, in fibrotic diseases, such as in late complications of diabetes and metabolic disease (diabetic kidney disease, nonalcoholic steatohepatitis), miR-29 species expression is suppressed by TGF-β allowing increased extracellular matrix collagen to form. In the clinical setting, circulating levels of miR-29a and miR-29b are consistently increased in type 2 diabetes and in gestational diabetes and are also possible prognostic markers for deterioration of glucose tolerance. In conclusion, miR-29 family miRNAs play an essential role in various organs relevant to intermediary metabolism and its upregulation contributes to impaired glucose metabolism, whereas it suppresses fibrosis development. Thus, a correct balance of levels of miR-29 family miRNA seems important for cellular and organ homeostasis in metabolism. [ABSTRACT FROM AUTHOR]

Published

2022

10. Analysis of Half a Billion Datapoints Across Ten Machine-Learning Algorithms Identifies Key Elements Associated With Insulin Transcription in Human Pancreatic Islet Cells.

Author

Wong, Wilson K. M., Thorat, Vinod, Joglekar, Mugdha V., Dong, Charlotte X., Lee, Hugo, Chew, Yi Vee, Bhave, Adwait, Hawthorne, Wayne J., Engin, Feyza, Pant, Aniruddha, Dalgaard, Louise T., Bapat, Sharda, and Hardikar, Anandwardhan A.

Subjects

ISLANDS of Langerhans, MACHINE learning, INSULIN, TYPE 1 diabetes, TYPE 2 diabetes

Abstract

Machine learning (ML)-workflows enable unprejudiced/robust evaluation of complex datasets. Here, we analyzed over 490,000,000 data points to compare 10 different ML-workflows in a large (N=11,652) training dataset of human pancreatic single-cell (sc-)transcriptomes to identify genes associated with the presence or absence of insulin transcript(s). Prediction accuracy/sensitivity of each ML-workflow was tested in a separate validation dataset (N=2,913). Ensemble ML-workflows, in particular Random Forest ML-algorithm delivered high predictive power (AUC=0.83) and sensitivity (0.98), compared to other algorithms. The transcripts identified through these analyses also demonstrated significant correlation with insulin in bulk RNA-seq data from human islets. The top-10 features, (including IAPP, ADCYAP1, LDHA and SST) common to the three Ensemble ML-workflows were significantly dysregulated in scRNA-seq datasets from Ire-1αβ-/- mice that demonstrate dedifferentiation of pancreatic β-cells in a model of type 1 diabetes (T1D) and in pancreatic single cells from individuals with type 2 Diabetes (T2D). Our findings provide direct comparison of ML-workflows in big data analyses, identify key elements associated with insulin transcription and provide workflows for future analyses. [ABSTRACT FROM AUTHOR]

Published

2022

11. Shortened Leukocyte Telomere Length Is Associated With Glycemic Progression in Type 2 Diabetes: A Prospective and Mendelian Randomization Analysis.

Author

Cheng, Feifei, Luk, Andrea O., Shi, Mai, Huang, Chuiguo, Jiang, Guozhi, Yang, Aimin, Wu, Hongjiang, Lim, Cadmon K.P., Tam, Claudia H.T., Fan, Baoqi, Lau, Eric S.H., Ng, Alex C.W., Wong, Kwun Kiu, Carroll, Luke, Lee, Heung Man, Kong, Alice P., Keech, Anthony C., Chow, Elaine, Joglekar, Mugdha V., and Tsui, Stephen K.W.

Subjects

TYPE 2 diabetes, TELOMERES, LEUCOCYTES, CHINESE people

Abstract

Objective: Several studies support associations between relative leukocyte telomere length (rLTL), a biomarker of biological aging and type 2 diabetes. This study investigates the relationship between rLTL and the risk of glycemic progression in patients with type 2 diabetes.Research Design and Methods: In this cohort study, consecutive Chinese patients with type 2 diabetes (N = 5,506) from the Hong Kong Diabetes Register with stored baseline DNA and available follow-up data were studied. rLTL was measured using quantitative PCR. Glycemic progression was defined as the new need for exogenous insulin.Results: The mean (SD) age of the 5,349 subjects was 57.0 (13.3) years, and mean (SD) follow-up was 8.8 (5.4) years. Baseline rLTL was significantly shorter in the 1,803 subjects who progressed to insulin requirement compared with the remaining subjects (4.43 ± 1.16 vs. 4.69 ± 1.20). Shorter rLTL was associated with a higher risk of glycemic progression (hazard ratio [95% CI] for each unit decrease [to ∼0.2 kilobases]: 1.10 [1.06-1.14]), which remained significant after adjusting for confounders. Baseline rLTL was independently associated with glycemic exposure during follow-up (β = -0.05 [-0.06 to -0.04]). Each 1-kilobase decrease in absolute LTL was on average associated with a 1.69-fold higher risk of diabetes progression (95% CI 1.35-2.11). Two-sample Mendelian randomization analysis showed per 1-unit genetically decreased rLTL was associated with a 1.38-fold higher risk of diabetes progression (95% CI 1.12-1.70).Conclusions: Shorter rLTL was significantly associated with an increased risk of glycemic progression in individuals with type 2 diabetes, independent of established risk factors. Telomere length may be a useful biomarker for glycemic progression in people with type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2022

12. Decrease in Plasma miR-27a and miR-221 After Concussion in Australian Football Players.

Author

Shultz, Sandy R, Taylor, Caroline J, Aggio-Bruce, Riemke, O'Brien, William T, Sun, Mujun, Cioanca, Adrian V, Neocleous, George, Symons, Georgia F, Brady, Rhys D, Hardikar, Anandwardhan A, Joglekar, Mugdha V, Costello, Daniel M, O'Brien, Terence J, Natoli, Riccardo, and McDonald, Stuart J

Subjects

AUSTRALIAN football players, AUSTRALIAN football, BRAIN concussion, MICRORNA, BRAIN injuries

Abstract

Introduction: Sports-related concussion (SRC) is a common form of brain injury that lacks reliable methods to guide clinical decisions. MicroRNAs (miRNAs) can influence biological processes involved in SRC, and measurement of miRNAs in biological fluids may provide objective diagnostic and return to play/recovery biomarkers. Therefore, this prospective study investigated the temporal profile of circulating miRNA levels in concussed male and female athletes. Methods: Pre-season baseline blood samples were collected from amateur Australian rules football players (82 males, 45 females). Of these, 20 males and 8 females sustained an SRC during the subsequent season and underwent blood sampling at 2-, 6- and 13-days post-injury. A miRNA discovery Open Array was conducted on plasma to assess the expression of 754 known/validated miRNAs. miRNA target identified were further investigated with quantitative real-time PCR (qRT-PCR) in a validation study. Data pertaining to SRC symptoms, demographics, sporting history, education history and concussion history were also collected. Results: Discovery analysis identified 18 candidate miRNA. The consequent validation study found that plasma miR-221-3p levels were decreased at 6d and 13d, and that miR-27a-3p levels were decreased at 6d, when compared to baseline. Moreover, miR-27a and miR-221-3p levels were inversely correlated with SRC symptom severity. Conclusion: Circulating levels of miR-27a-3p and miR-221-3p were decreased in the sub-acute stages after SRC, and were inversely correlated with SRC symptom severity. Although further studies are required, these analyses have identified miRNA biomarker candidates of SRC severity and recovery that may one day assist in its clinical management. [ABSTRACT FROM AUTHOR]

Published

2022

13. Relative leucocyte telomere length is associated with incident end-stage kidney disease and rapid decline of kidney function in type 2 diabetes: analysis from the Hong Kong Diabetes Register.

Author

Cheng, Feifei, Luk, Andrea O., Wu, Hongjiang, Tam, Claudia H. T., Lim, Cadmon K. P., Fan, Baoqi, Jiang, Guozhi, Carroll, Luke, Yang, Aimin, Lau, Eric S. H., Ng, Alex C. W., Lee, Heung Man, Chow, Elaine, Kong, Alice P. S., Keech, Anthony C., Joglekar, Mugdha V., So, Wing Yee, Hardikar, Anandwardhan A., Chan, Juliana C. N., and Jenkins, Alicia J.

Abstract

Aims/hypothesis: Few large-scale prospective studies have investigated associations between relative leucocyte telomere length (rLTL) and kidney dysfunction in individuals with type 2 diabetes. We examined relationships between rLTL and incident end-stage kidney disease (ESKD) and the slope of eGFR decline in Chinese individuals with type 2 diabetes. Methods: We studied 4085 Chinese individuals with type 2 diabetes observed between 1995 and 2007 in the Hong Kong Diabetes Register with stored baseline DNA and available follow-up data. rLTL was measured using quantitative PCR. ESKD was diagnosed based on the ICD-9 code and eGFR. Results: In this cohort (mean ± SD age 54.3 ± 12.6 years) followed up for 14.1 ± 5.3 years, 564 individuals developed incident ESKD and had shorter rLTL at baseline (4.2 ± 1.2 vs 4.7 ± 1.2, p < 0.001) than the non-progressors (n = 3521). On Cox regression analysis, each ∆∆Ct decrease in rLTL was associated with an increased risk of incident ESKD (HR 1.21 [95% CI 1.13, 1.30], p < 0.001); the association remained significant after adjusting for baseline age, sex, HbA1c, lipids, renal function and other risk factors (HR 1.11 [95% CI 1.03, 1.19], p = 0.007). Shorter rLTL at baseline was associated with rapid decline in eGFR (>4% per year) during follow-up (unadjusted OR 1.22 [95% CI 1.15, 1.30], p < 0.001; adjusted OR 1.09 [95% CI 1.01, 1.17], p = 0.024). Conclusions/interpretation: rLTL is independently associated with incident ESKD and rapid eGFR loss in individuals with type 2 diabetes. Telomere length may be a useful biomarker for the progression of kidney function and ESKD in type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2022

14. Decrease in Plasma miR-27a and miR-221 After Concussion in Australian Football Players.

Author

Shultz, Sandy R., Taylor, Caroline J., Aggio-Bruce, Riemke, O'Brien, William T., Mujun Sun, Cioanca, Adrian V., Neocleous, George, Symons, Georgia F., Brady, Rhys D., Hardikar, Anandwardhan A., Joglekar, Mugdha V., Costello, Daniel M., O'Brien, Terence J., Natoli, Riccardo, and McDonald, Stuart J.

Subjects

AUSTRALIAN football players, AUSTRALIAN football, BRAIN concussion, MICRORNA, HISTORY of sports

Abstract

Introduction: Sports-related concussion (SRC) is a common form of brain injury that lacks reliable methods to guide clinical decisions. MicroRNAs (miRNAs) can influence biological processes involved in SRC, and measurement of miRNAs in biological fluids may provide objective diagnostic and return to play/recovery biomarkers. Therefore, this prospective study investigated the temporal profile of circulating miRNA levels in concussed male and female athletes. Methods: Pre-season baseline blood samples were collected from amateur Australian rules football players (82 males, 45 females). Of these, 20 males and 8 females sustained an SRC during the subsequent season and underwent blood sampling at 2-, 6- and 13-days postinjury. A miRNA discovery Open Array was conducted on plasma to assess the expression of 754 known/validated miRNAs. miRNA target identified were further investigated with quantitative real-time PCR (qRT-PCR) in a validation study. Data pertaining to SRC symptoms, demographics, sporting history, education history and concussion history were also collected. Results: Discovery analysis identified 18 candidate miRNA. The consequent validation study found that plasma miR-221-3p levels were decreased at 6d and 13d, and that miR-27a-3p levels were decreased at 6d, when compared to baseline. Moreover, miR-27a and miR-221-3p levels were inversely correlated with SRC symptom severity. Conclusion: Circulating levels of miR-27a-3p and miR-221-3p were decreased in the sub-acute stages after SRC, and were inversely correlated with SRC symptom severity. Although further studies are required, these analyses have identified miRNA biomarker candidates of SRC severity and recovery that may one day assist in its clinical management. [ABSTRACT FROM AUTHOR]

Published

2022

15. A bird's eye view of the dynamics of pancreatic β‐cell heterogeneity.

Author

Joglekar, Mugdha V., Dong, Charlotte X., Wong, Wilson K. M., Dalgaard, Louise Torp, and Hardikar, Anandwardhan A.

Subjects

INSULIN, HETEROGENEITY, UNFOLDED protein response, PANCREATIC beta cells

Abstract

To better appreciate the dynamic nature of -cells, we performed pseudotime analyses using publicly available human islet single-cell sequencing databases14 and filtered these to select for -cells(N = 3,679). Observations of limited proliferative potential in (human) -cells, shorter transcript turnover times and ER stress leading to cellular damage do not support a fixed state model of leader/follower cells or the insulin transcript heterogeneity observed within -cells. CONCLUDING REMARKS Current technologies reporting -cell heterogeneity enable molecular profiling of human islets at single-cell resolution, however, we are largely limited to follow functional/transcriptomic information from the same cell over extended periods (days-weeks). Recently, in an impressive Patch-seq study,4 human islet cell exocytosis and transcriptomes were examined at single-cell resolution demonstrating functional heterogeneity in -cell exocytosis as measured by changes in membrane capacitance. [Extracted from the article]

Published

2021

16. Continuous subcutaneous insulin infusion alters microRNA expression and glycaemic variability in children with type 1 diabetes.

Author

Scott, Emma S., Januszewski, Andrzej S., Carroll, Luke M., Fulcher, Gregory R., Joglekar, Mugdha V., Hardikar, Anandwardhan A., Jones, Timothy W., Davis, Elizabeth A., and Jenkins, Alicia J.

Subjects

INSULIN, MICRORNA, TYPE 1 diabetes, GLYCEMIC index, C-peptide

Abstract

To determine whether continuous subcutaneous insulin infusion (CSII) vs. multiple daily injections (MDI) therapy from near-diagnosis of type 1 diabetes is associated with reduced glycaemic variability (GV) and altered microRNA (miRNAs) expression. Adolescents (74% male) within 3-months of diabetes diagnosis (n = 27) were randomized to CSII (n = 12) or MDI. HbA1c, 1-5-Anhydroglucitol (1,5-AG), high sensitivity C-peptide and a custom TaqMan qPCR panel of 52 miRNAs were measured at baseline and follow-up (median (LQ-UQ); 535 (519–563) days). There were no significant differences between groups in baseline or follow-up HbA1c or C-peptide, nor baseline miRNAs. Mean ± SD 1,5-AG improved with CSII vs. MDI (3.1 ± 4.1 vs. − 2.2 ± − 7.0 mg/ml respectively, P = 0.029). On follow-up 11 miRNAs associated with diabetes vascular complications had altered expression in CSII-users. Early CSII vs. MDI use is associated with lower GV and less adverse vascular-related miRNAs. Relationships with future complications are of interest. [ABSTRACT FROM AUTHOR]

Published

2021

17. Postpartum circulating microRNA enhances prediction of future type 2 diabetes in women with previous gestational diabetes.

Author

Joglekar, Mugdha V., Wong, Wilson K. M., Ema, Fahmida K., Georgiou, Harry M., Shub, Alexis, Hardikar, Anandwardhan A., and Lappas, Martha

Abstract

Aims/hypothesis: Type 2 diabetes mellitus is a major cause of morbidity and death worldwide. Women with gestational diabetes mellitus (GDM) have greater than a sevenfold higher risk of developing type 2 diabetes in later life. Accurate methods for postpartum type 2 diabetes risk stratification are lacking. Circulating microRNAs (miRNAs) are well recognised as biomarkers/mediators of metabolic disease. We aimed to determine whether postpartum circulating miRNAs can predict the development of type 2 diabetes in women with previous GDM. Methods: In an observational study, plasma samples were collected at 12 weeks postpartum from 103 women following GDM pregnancy. Utilising a discovery approach, we measured 754 miRNAs in plasma from type 2 diabetes non-progressors (n = 11) and type 2 diabetes progressors (n = 10) using TaqMan-based real-time PCR on an OpenArray platform. Machine learning algorithms involving penalised logistic regression followed by bootstrapping were implemented. Results: Fifteen miRNAs were selected based on their importance in discriminating type 2 diabetes progressors from non-progressors in our discovery cohort. The levels of miRNA miR-369-3p remained significantly different (p < 0.05) between progressors and non-progressors in the validation sample set (n = 82; 71 non-progressors, 11 progressors) after adjusting for age and correcting for multiple comparisons. In a clinical model of prediction of type 2 diabetes that included six traditional risk factors (age, BMI, pregnancy fasting glucose, postpartum fasting glucose, cholesterol and triacylglycerols), the addition of the circulating miR-369-3p measured at 12 weeks postpartum improved the prediction of future type 2 diabetes from traditional AUC 0.83 (95% CI 0.68, 0.97) to an AUC 0.92 (95% CI 0.84, 1.00). Conclusions: This is the first demonstration of miRNA-based type 2 diabetes prediction in women with previous GDM. Improved prediction will facilitate early lifestyle/drug intervention for type 2 diabetes prevention. [ABSTRACT FROM AUTHOR]

Published

2021

18. Insulin micro-secretion in Type 1 diabetes and related microRNA profiles.

Author

Januszewski, Andrzej S., Cho, Yoon Hi, Joglekar, Mugdha V., Farr, Ryan J., Scott, Emma S., Wong, Wilson K. M., Carroll, Luke M., Loh, Yik W., Benitez-Aguirre, Paul Z., Keech, Anthony C., O'Neal, David N., Craig, Maria E., Hardikar, Anandwardhan A., Donaghue, Kim C., and Jenkins, Alicia J.

Subjects

TYPE 1 diabetes, MICRORNA, INSULIN, PANCREATIC beta cells, ENZYME-linked immunosorbent assay

Abstract

The aim of this cross-sectional study was to compare plasma C-peptide presence and levels in people without diabetes (CON) and with Type 1 diabetes and relate C-peptide status to clinical factors. In a subset we evaluated 50 microRNAs (miRs) previously implicated in beta-cell death and associations with clinical status and C-peptide levels. Diabetes age of onset was stratified as adult (≥ 18 y.o) or childhood (< 18 y.o.), and diabetes duration was stratified as ≤ 10 years, 10–20 years and > 20 years. Plasma C-peptide was measured by ultrasensitive ELISA. Plasma miRs were quantified using TaqMan probe-primer mix on an OpenArray platform. C-peptide was detectable in 55.3% of (n = 349) people with diabetes, including 64.1% of adults and 34.0% of youth with diabetes, p < 0.0001 and in all (n = 253) participants without diabetes (CON). C-peptide levels, when detectable, were lower in the individuals with diabetes than in the CON group [median lower quartile (LQ)–upper quartile (UQ)] 5.0 (2.6–28.7) versus 650.9 (401.2–732.4) pmol/L respectively, p < 0.0001 and lower in childhood versus adult-onset diabetes [median (LQ–UQ) 4.2 (2.6–12.2) pmol/L vs. 8.0 (2.3–80.5) pmol/L, p = 0.02, respectively]. In the childhood-onset group more people with longer diabetes duration (> 20 years) had detectable C-peptide (60%) than in those with shorter diabetes duration (39%, p for trend < 0.05). Nine miRs significantly correlated with detectable C-peptide levels in people with diabetes and 16 miRs correlated with C-peptide levels in CON. Our cross-sectional study results are supportive of (a) greater beta-cell function loss in younger onset Type 1 diabetes; (b) persistent insulin secretion in adult-onset diabetes and possibly regenerative secretion in childhood-onset long diabetes duration; and (c) relationships of C-peptide levels with circulating miRs. Confirmatory clinical studies and related basic science studies are merited. [ABSTRACT FROM AUTHOR]

Published

2021

19. Urinary microRNAs as non-invasive biomarkers for toxic acute kidney injury in humans.

Author

Shihana, Fathima, Wong, Wilson K. M., Joglekar, Mugdha V., Mohamed, Fahim, Gawarammana, Indika B., Isbister, Geoffrey K., Hardikar, Anandwardhan A., Seth, Devanshi, and Buckley, Nicholas A.

Subjects

MICRORNA, BIOMARKERS, ACUTE kidney failure, OXALIC acid, GLYPHOSATE

Abstract

MicroRNAs in biofluids are potential biomarkers for detecting kidney and other organ injuries. We profiled microRNAs in urine samples from patients with Russell's viper envenoming or acute self-poisoning following paraquat, glyphosate, or oxalic acid [with and without acute kidney injury (AKI)] and on healthy controls. Discovery analysis profiled for 754 microRNAs using TaqMan OpenArray qPCR with three patients per group (12 samples in each toxic agent). From these, 53 microRNAs were selected and validated in a larger cohort of patients (Russell's viper envenoming = 53, paraquat = 51, glyphosate = 51, oxalic acid = 40) and 27 healthy controls. Urinary microRNAs had significantly higher expression in patients poisoned/envenomed by different nephrotoxic agents in both discovery and validation cohorts. Seven microRNAs discriminated severe AKI patients from no AKI for all four nephrotoxic agents. Four microRNAs (miR-30a-3p, miR-30a-5p, miR-92a, and miR-204) had > 17 fold change (p < 0.0001) and receiver operator characteristics area-under-curve (ROC-AUC) > 0.72. Pathway analysis of target mRNAs of these differentially expressed microRNAs showed association with the regulation of different nephrotoxic signaling pathways. In conclusion, human urinary microRNAs could identify toxic AKI early after acute injury. These urinary microRNAs have potential clinical application as early non-invasive diagnostic AKI biomarkers. [ABSTRACT FROM AUTHOR]

Published

2021

20. A MicroRNA Signature in Acute Coronary Syndrome Patients and Modulation by Colchicine.

Author

Barraclough, Jennifer Y., Joglekar, Mugdha V., Januszewski, Andrzej S., Martínez, Gonzalo, Celermajer, David S., Keech, Anthony C., Hardikar, Anandwardhan A., and Patel, Sanjay

Subjects

ACUTE coronary syndrome, COLCHICINE, PATIENTS' rights, MICRORNA, TREATMENT effectiveness, PRASUGREL

Abstract

Background: Circulating microRNAs (miRNAs) may play a pathogenic role in acute coronary syndromes (ACS). It is not yet known if miRNAs dysregulated in ACS are modulated by colchicine. We profiled miRNAs in plasma samples simultaneously collected from the aorta, coronary sinus, and right atrium in patients with ACS.Methods: A total of 396 of 754 miRNAs were detected by TaqMan real-time polymerase chain reaction from EDTA-plasma in a discovery cohort of 15 patients (n = 3 controls, n = 6 ACS standard therapy, n = 6 ACS standard therapy plus colchicine). Fifty-one significantly different miRNAs were then measured in a verification cohort of 92 patients (n = 13 controls, n = 40 ACS standard therapy, n = 39 ACS standard therapy plus colchicine). Samples were simultaneously obtained from the coronary sinus, aortic root, and right atrium.Results: Circulating levels of 30 of 51 measured miRNAs were higher in ACS standard therapy patients compared to controls. In patients with ACS, levels of 12 miRNAs (miR-17, -106b-3p, -191, -106a, -146a, -130a, -223, -484, -889, -425-3p, -629, -142-5p) were lower with colchicine treatment. Levels of 7 of these 12 miRNA were higher in ACS standard therapy patients compared to controls and returned to levels seen in control individuals after colchicine treatment. Three miRNAs suppressed by colchicine (miR-146a, miR-17, miR-130a) were identified as regulators of inflammatory pathways. MicroRNAs were comparable across sampling sites with select differences in the transcoronary gradient of 4 miRNA.Conclusion: The levels of specific miRNAs elevated in ACS returned to levels similar to control individuals following colchicine. These miRNAs may mediate ACS (via inflammatory pathways) or increase post-ACS risk, and could be potentially used as biomarkers of treatment efficacy. [ABSTRACT FROM AUTHOR]

Published

2020

21. Shortened Relative Leukocyte Telomere Length Is Associated With Prevalent and Incident Cardiovascular Complications in Type 2 Diabetes: Analysis From the Hong Kong Diabetes Register.

Author

Cheng, Feifei, Luk, Andrea O., Tam, Claudia H.T., Fan, Baoqi, Wu, Hongjiang, Yang, Aimin, Lau, Eric S.H., Ng, Alex C.W., Lim, Cadmon K.P., Lee, Heung Man, Chow, Elaine, Kong, Alice P., Keech, Anthony C., Joglekar, Mugdha V., So, Wing Yee, Jenkins, Alicia J., Chan, Juliana C.N., Hardikar, Anandwardhan A., and Ma, Ronald C.W.

Subjects

TYPE 2 diabetes, TELOMERES, SYSTOLIC blood pressure, GLYCOSYLATED hemoglobin, CHINESE people, FAMILIAL hypercholesterolemia

Abstract

Objective: Several studies support potential links between relative leukocyte telomere length (rLTL), a biomarker of biological aging, and type 2 diabetes. This study investigates relationships between rLTL and incident cardiovascular disease (CVD) in patients with type 2 diabetes.Research Design and Methods: Consecutive Chinese patients with type 2 diabetes (N = 5,349) from the Hong Kong Diabetes Register for whom DNA obtained at baseline was stored and follow-up data were available were studied. rLTL was measured by using quantitative PCR. CVD was diagnosed on the basis of ICD-9 code.Results: Mean follow-up was 13.4 years (SD 5.5 years). rLTL was correlated inversely with age, diabetes duration, blood pressure, HbA1c, and urine albumin-to-creatinine ratio (ACR), and positively with estimated glomerular filtration rate (eGFR) (all P < 0.001). Subjects with CVD at baseline had a shorter rLTL (4.3 ± 1.2 ΔΔCt) than did subjects without CVD (4.6 ± 1.2 ΔΔCt) (P < 0.001). Of the 4,541 CVD-free subjects at baseline, the 1,140 who developed CVD during follow-up had a shorter rLTL (4.3 ± 1.2 ΔΔCt) than those who remained CVD-free after adjusting for age, sex, smoking, and albuminuria status (4.7 ± 1.2 ΔΔCt) (P < 0.001). In Cox regression models, shorter rLTL was associated with higher risk of incident CVD (for each unit decrease, hazard ratio 1.252 [95% CI 1.195-1.311], P < 0.001), which remained significant after adjusting for age, sex, BMI, systolic blood pressure, LDL cholesterol, HbA1c, eGFR, and ACR (hazard ratio 1.141 [95% CI 1.084-1.200], P < 0.001).Conclusions: rLTL is significantly shorter in patients with type 2 diabetes and CVD, is associated with cardiometabolic risk factors, and is independently associated with incident CVD. Telomere length may be a useful biomarker for CVD risk in patients with type 2 diabetes. [ABSTRACT FROM AUTHOR]

Published

2020

22. Circulating human microRNA biomarkers of oxalic acid-induced acute kidney injury.

Author

Shihana, Fathima, Joglekar, Mugdha V., Raubenheimer, Jacques, Hardikar, Anandwardhan A., Buckley, Nicholas A., and Seth, Devanshi

Subjects

ACUTE kidney failure, OXALIC acid, MICRORNA, CALCIUM oxalate, BIOMARKERS, NEPHROTOXICOLOGY

Abstract

Oxalic acid-induced nephrotoxicity and acute kidney injury result from formation of calcium oxalate crystals. Oxalic acid-induced acute kidney injury is a significant problem in many parts of the world. Circulating biomarkers that can accurately and reproducibly detect acute kidney injury are highly desirable. We used a high sensitivity discovery platform to identify signature microRNAs to distinguish healthy individuals never exposed to oxalic acid (n = 4) from those who were exposed to oxalic acid but had no injury (NOAKI; n = 4), moderate injury (AKIN2; n = 4) or severe injury (AKIN3; n = 4). Longitudinal analyses identified 4–8 h post-ingestion as the best time to detect AKIN2/3. We validated a signature of 53 microRNAs identified in the discovery, in a second cohort of individuals exposed to oxalic acid (NOAKI = 11, AKIN2 = 8 and AKIN3 = 18) and healthy controls (n = 19). Thirteen microRNAs were significantly downregulated in acute kidney injury patients compared to NOAKI within 8-h post-ingestion. Five microRNAs (miR-20a, miR-92a, miR-93, miR-195, miR-451) had a highly significant correlation with normalized urinary albumin, serum creatinine at 24 h and creatinine clearance. Logistic regression of these microRNAs had AUC-ROC of 0.85 predicting AKIN2/3 and discriminated patients from healthy controls (AUC-ROC = 0.93). mRNA targets of these microRNAs identified oxidative stress pathways of nephrotoxicity in proximal tubule and glomeruli nephrotoxicity. In conclusion, the downregulation of multiple circulating microRNAs in patients correlated with the severity of oxalic acid-induced acute kidney injury. A set of microRNAs (miR-20a, miR-92a, miR-93, miR-195, miR-451) could be promising biomarkers for early detection of oxalic acid-induced acute kidney injury. [ABSTRACT FROM AUTHOR]

Published

2020

23. Directed differentiation into insulin-producing cells using microRNA manipulation.

Author

Williams, Michael D., Joglekar, Mugdha V., Hardikar, Anandwardhan A., and Wong, Wilson K. M.

Abstract

Our commentary is focused on three studies that used microRNA overexpression methods for directed differentiation of stem cells into insulin-producing cells. Islet transplantation is the only cell-based therapy used to treat type 1 diabetes mellitus. However, due to the scarcity of cadaveric donors and limited availability of good quality and quantity of islets for transplant, alternate sources of insulin-producing cells are being studied and used by researchers. This commentary provides an overview of distinct studies focused on manipulating microRNA expression to optimize differentiation of embryonic stem cells or induced pluripotent stem cells into insulin-producing cells. These studies have used different approaches to overexpress microRNAs that are highly abundant in human islets (such as miR-375 and miR-7) in their differentiation protocol to achieve better differentiation into functional islet beta (β)-cells. [ABSTRACT FROM AUTHOR]

Published

2020

24. Postpartum Circulating Cell-Free Insulin DNA Levels Are Higher in Women with Previous Gestational Diabetes Mellitus Who Develop Type 2 Diabetes in Later Life.

Author

Lappas, Martha, Georgiou, Harry M., Willcox, Jane C., Permezel, Michael, Shub, Alexis, Maynard, Cody-Lee, Joglekar, Mugdha V., and Hardikar, Anandwardhan A.

Subjects

CELL-free DNA, GESTATIONAL diabetes, TYPE 2 diabetes, DNA, INSULIN

Abstract

Background. Women with previous gestational diabetes mellitus (GDM) have evidence of postpartum β-cell dysfunction, which increases their risk of developing type 2 diabetes (T2DM) later in life. Elevated levels of circulating cell-free preproinsulin (INS) DNA correlate with dying β-cells in both mice and humans. The aim of this study was to determine if cell-free circulating INS DNA levels are higher in women with previous GDM who develop T2DM. Methods. We used droplet digital (dd) PCR to measure the levels of cell-free circulating methylated and unmethylated INS DNA in plasma from 97 women with normal glucose tolerance (NGT), 12 weeks following an index GDM pregnancy. Women were assessed for up to 10 years for the development of T2DM. Results. In the follow-up period, 22% of women developed T2DM. Compared with NGT women, total cell-free INS DNA levels were significantly higher in women who developed T2DM (P=0.02). There was no difference in cell-free circulating unmethylated and methylated INS DNA levels between NGT women and women who developed T2DM (P=0.09 and P=0.07, respectively). Conclusions. In women with a previous index GDM pregnancy, postpartum levels of cell-free circulating INS DNA are significantly higher in those women who later developed T2DM. [ABSTRACT FROM AUTHOR]

Published

2019

25. Non-Coding RNA in Pancreas and β-Cell Development.

Author

Wong, Wilson K. M., Sørensen, Anja E., Joglekar, Mugdha V., Hardikar, Anand A., and Dalgaard, Louise T.

Subjects

NON-coding RNA, PANCREAS, FETAL development, MICRORNA, CELL differentiation

Abstract

In this review, we provide an overview of the current knowledge on the role of different classes of non-coding RNAs for islet and β-cell development, maturation and function. MicroRNAs (miRNAs), a prominent class of small RNAs, have been investigated for more than two decades and patterns of the roles of different miRNAs in pancreatic fetal development, islet and β-cell maturation and function are now emerging. Specific miRNAs are dynamically regulated throughout the period of pancreas development, during islet and β-cell differentiation as well as in the perinatal period, where a burst of β-cell replication takes place. The role of long non-coding RNAs (lncRNA) in islet and β-cells is less investigated than for miRNAs, but knowledge is increasing rapidly. The advent of ultra-deep RNA sequencing has enabled the identification of highly islet- or β-cell-selective lncRNA transcripts expressed at low levels. Their roles in islet cells are currently only characterized for a few of these lncRNAs, and these are often associated with β-cell super-enhancers and regulate neighboring gene activity. Moreover, ncRNAs present in imprinted regions are involved in pancreas development and β-cell function. Altogether, these observations support significant and important actions of ncRNAs in β-cell development and function. [ABSTRACT FROM AUTHOR]

Published

2018

26. Expression of miR-206 in human islets and its role in glucokinase regulation.

Author

Joglekar, Mugdha V., Wong, Wilson K. M., Maynard, Cody-Lee, Umrani, Malati R., Martin, David, Loudovaris, Thomas, Thomas, Helen E., Dalgaard, Louise T., and Hardikar, Anandwardhan A.

Abstract

Inappropriate insulin secretion from β-cells is considered as an early sign of impaired glucose tolerance and type 2 diabetes (T2D). Glucokinase (GCK) is an important enzyme that regulates glucose metabolism and ensures that the normal circulating glucose concentrations are maintained. GCK expression is induced by glucose and regulated via transcription factors and regulatory proteins. Recently, microRNA-206 (miR-206) was reported to regulate GCK and alter glucose tolerance in normal and high-fat diet-fed mice. Although the study findings have implications for human diabetes, studies in human islets are lacking. Here, we analyze human islets from individuals without or with T2D, using TaqMan-based real-time qPCR at the tissue (isolated islet) level as well as at single cell resolution, to assess the relationship between miR-206 and GCK expression in normal and T2D human islets. Our data suggest that, unlike mouse islets, human islets do not exhibit any correlation between miR-206 and GCK transcripts. These data implicate the need for further studies aimed toward exploring its potential role(s) in human islets. [ABSTRACT FROM AUTHOR]

Published

2018

27. Generation of Human Islet Progenitor Cells via Epithelial-to-Mesenchymal Transition.

Author

Wong, Wilson, Hardikar, Anandwardhan A., and Joglekar, Mugdha V.

Published

2016

28. Connexins and microRNAs: Interlinked players in regulating islet function?

Author

Umrani, Malati R., Joglekar, Mugdha V., Somerville Glover, Ella, Wong, Wilson, and Hardikar, Anandwardhan A.

Published

2017

29. Characterizing Cellular Identity at One Cell Resolution.

Author

Ranjan, Amaresh K., Joglekar, Mugdha V., and Hardikar, Anandwardhan A.

Published

2015

30. Circulating microRNAs in Diabetes Progression: Discovery, Validation, and Research Translation.

Author

Farr, Ryan J., Joglekar, Mugdha V., and Hardikar, Anandwardhan A.

Published

2015

31. Manipulation and Assessment of Gut Microbiome for Metabolic Studies.

Author

Satoor, Sarang N., Patil, Deepak P., Kristensen, Holly D., Joglekar, Mugdha V., Shouche, Yogesh, and Hardikar, Anandwardhan A.

Published

2014

32. Pdx1 (GFP/w) Mice for Isolation, Characterization, and Differentiation of Pancreatic Progenitor Cells.

Author

Williams, Michael D., Wong, Wilson, Rixon, Amanda, Satoor, Sarang N., Hardikar, Anandwardhan A., and Joglekar, Mugdha V.

Published

2014

33. Lineage-Committed Pancreatic Progenitors and Stem Cells.

Author

Wong, Wilson, Joglekar, Mugdha V., Satoor, Sarang N., Sahu, Subhshri, Parekh, Vishal S., and Hardikar, Anandwardhan A.

Published

2014

34. Human Pancreatic Progenitors: Implications for Clinical Transplantation in Diabetes.

Author

Joglekar, Mugdha V. and Hardikar, Anandwardhan A.

Published

2013

35. Isolation, Expansion, and Characterization of Human Islet-Derived Progenitor Cells.

Author

Joglekar, Mugdha V. and Hardikar, Anandwardhan A.

Published

2012

36. Simultaneous imaging of microRNA or mRNA territories with protein territory in mammalian cells at single cell resolution.

Author

Ranjan, Amaresh Kumar, Joglekar, Mugdha V., Atre, Ashwini N., Patole, Milind, Bhonde, Ramesh R., and Hardikar, Anandwardhan A.

Published

2012

37. A Protocol for Measurement of Noncoding RNA in Human Serum.

Author

Taylor, Caroline J., Satoor, Sarang N., Ranjan, Amaresh K., Pereira Cotta, Maria V., and Joglekar, Mugdha V.

Subjects

MICRORNA, GENE expression, MESSENGER RNA, BIOMARKERS, SERUM, POLYMERASE chain reaction

Abstract

MicroRNAs (miRNAs) are small noncoding RNAs that act as regulators of gene expression by targeting mature messenger RNAs. Following the initial report of the presence of miRNAs in serum and plasma a number of studies have successfully demonstrated the use of these miRNAs as biomarkers of disease. Currently, there are many methods of isolating total RNA from liquid samples. Here, we describe a simple, cost effective method for extraction of RNA from human serum as well as subsequent real time PCR analysis of miRNA levels. [ABSTRACT FROM AUTHOR]

Published

2012

38. Human bone marrow-derived mesenchymal cells differentiate and mature into endocrine pancreatic lineage in vivo.

Author

Phadnis, Smruti M., Joglekar, Mugdha V., Dalvi, Maithili P., Muthyala, Sudhakar, Nair, Prabha D., Ghaskadbi, Surendra M., Bhonde, Ramesh R., and Hardikar, Anandwardhan A.

Subjects

BONE marrow, MESENCHYMAL stem cells, TREATMENT of diabetes, ISLANDS of Langerhans transplantation, PARACRINE mechanisms, CELL differentiation

Abstract

Background aims. The scarcity of human islets for transplantation remains a major limitation of cell replacement therapy for diabetes. Bone marrow-derived progenitor cells are of interest because they can be isolated, expanded and offered for such therapy under autologous/allogeneic settings. Methods. We characterized and compared human bone marrow-derived mesenchymal cells (hBMC) obtained from (second trimester), young (1--24 years) and adult (34--81 years) donors. We propose a novel protocol that involves assessment of paracrine factors from regenerating pancreas in differentiation and maturation of hBMC into endocrine pancreatic lineage in vivo. Results. We observed that donor age was inversely related to growth potential of hBMC. Following in vitro expansion and exposure to specific growth factors involved in pancreatic development, hBMC migrated and formed islet-like cell aggregates (ICA). ICA show increased abundance of pancreatic transcription factors (Ngn3, Brn4, Nkx6.1, Pax6 and Isl1). Although efficient differentiation was not achieved in vitro, we observed significant maturation and secretion of human c-peptide (insulin) upon transplantation into pancreactomized and Streptozotocin (STZ)-induced diabetic mice. Transplanted ICA responded to glucose and maintained normoglycemia in diabetic mice. Conclusions. Our data demonstrate that hBMC have tremendous in vitro expansion potential and can be differentiated into multiple lineages, including the endocrine pancreatic lineage. Paracrine factors secreted from regenerating pancreas help in efficient differentiation and maturation of hBMC, possibly via recruiting chromatin modulators, to generate glucose-responsive insulin-secreting cells. [ABSTRACT FROM AUTHOR]

Published

2011

39. Circulating microRNA Biomarkers of Diabetic Retinopathy.

Author

Joglekar, Mugdha V., Januszewski, Andrzej S., Jenkins, Alicia J., and Hardikar, Anandwardhan A.

Subjects

MICRORNA, BIOMARKERS, DIABETIC retinopathy, RANDOMIZED controlled trials, BLIND experiment, PLACEBOS

Abstract

The article discusses a study by Zampetaki et al. which is said to be an important advance in the field of microRNA (miRNA) biomarkers with implications in the areas of disease pathogenesis, prognostication, monitoring and therapeutics. It assessed 300 samples from 2 diabetic retinopathy (DR)-related randomized, double-blind, parallel-design and placebo-controlled clinical trials and identified miR27b and miR-320a as being significantly and independently associated with high DR risk.

Published

2016

40. Human pancreatic islet progenitor cells demonstrate phenotypic plasticity in vitro.

Author

DALVI, MAITHILI P., UMRANI, MALATI R., JOGLEKAR, MUGDHA V., and HARDIKAR, ANANDWARDHAN A.

Abstract

Phenotypic plasticity is a phenomenon that describes the occurrence of 2 or more distinct phenotypes under diverse conditions. This article discusses the work carried out over the past few years in understanding the potential of human pancreatic islet-derived progenitors for cell replacement therapy in diabetes. The phenotypic plasticity exhibited by pancreatic progenitors during reversible epithelial-to-mesenchymal transition (EMT) and possible role of microRNAs in regulation of this process is also presented herein. [ABSTRACT FROM AUTHOR]

Published

2009

41. Mesenchymal stem cells: immunobiology and role in immunomodulation and tissue regeneration.

Author

Kode, Jyoti A., Mukherjee, Shayanti, Joglekar, Mugdha V., and Hardikar, Anandwardhan A.

Subjects

CORD blood, EMBRYOLOGY, THERAPEUTICS, STEM cells, HYPOGLYCEMIC agents

Abstract

Mesenchymal stem cells (MSC) are multipotent cells that differentiate into osteoblasts, myocytes, chondrocytes and adipocytes as well as insulin-producing cells. The mechanism underlying their in vivo differentiation is not clear and is thought to be caused by spontaneous cell fusion or factors present in the microenvironment. However, their ease of isolation, high 'ex-vivo' expansion potential and ability to differentiate into multiple lineages make them attractive tools for potential use in cell therapy. MSC have been isolated from several tissues, including bone/bone marrow, fat, Wharton's jelly, umbilical cord blood, placenta and pancreas. The 'immunosuppressive' property of human MSC makes them an important candidate for cellular therapy in allogeneic settings. Use of allogeneic MSC for repair of large defects may be an alternative to autologous and allogeneic tissue-grafting procedures. An allogeneic approach would enable MSC to be isolated from any donor, expanded and cryopreserved, providing a readily available source of progenitors for cell replacement therapy. Their immunomodulatory properties have raised the possibility of establishing allogeneic MSC banks for tissue regeneration. These facts are strongly reflected in the current exponential growth in stem cell research in the pharmaceutical and biotechnology communities. Current knowledge regarding the immunobiology and clinical application of MSC needs to be strengthened further to establish MSC as a safe and effective therapeutic tool in regenerative medicine. This paper discusses human MSC with particular reference to the expression of their surface markers, their role as immunomodulators and their multilineage differentiation potential and possible use in tissue regeneration and repair. [ABSTRACT FROM AUTHOR]

Published

2009

42. Epithelial-to-mesenchymal transition in pancreatic islet β cells.

Author

Joglekar, Mugdha V. and Hardikar, Anandwardhan A.

Published

2010

43. MicroRNAs as Prognostic Markers in Acute Coronary Syndrome Patients—A Systematic Review.

Author

Barraclough, Jennifer Y., Joan, Michelyn, Joglekar, Mugdha V., Hardikar, Anandwardhan A., and Patel, Sanjay

Subjects

ACUTE coronary syndrome, META-analysis, CARDIOVASCULAR diseases risk factors, FALSE discovery rate, CELL differentiation, MICRORNA

Abstract

Background: The potential utility of microRNAs (miRNAs) in the diagnosis, prognosis, and treatment of multiple disease states has been an area of great interest since their discovery. In patients with cardiovascular disease, there is a large pool of literature amassed from the last decade assessing their diagnostic and prognostic potential. This systematic review sought to determine whether existing literature supports the use of miRNAs as prognostic markers after an Acute Coronary Syndrome (ACS) presentation. Methods: A systematic review of published articles from 2005–2019 using MEDLINE and EMBASE databases was undertaken independently by two reviewers. Studies addressing prognosis in an ACS population yielded 32 studies and 2 systematic reviews. Results/conclusion: 23 prospective studies reported significant differences in miRNA levels and 16 compared the predictive power of miRNAs. The most common miRNAs assessed included miR-133a, -208b, -21, -1, -34a, -150, and -423, shown to be involved in cell differentiation, apoptosis, and angiogenesis. Barriers to the use of miRNAs as prognostic markers include bias in miRNA selection, small sample size, variable normalization of data, and adjustment for confounders. Therefore, findings from this systematic review do not support the use of miRNAs for prognostication post-ACS beyond traditional cardiovascular risk factors, existing risk scores, and stratifications tools. [ABSTRACT FROM AUTHOR]

Published

2019

44. Phlda3 regulates beta cell survival during stress.

Author

Bensellam, Mohammed, Chan, Jeng Yie, Lee, Kailun, Joglekar, Mugdha V., Hardikar, Anandwardhan A., Loudovaris, Thomas, Thomas, Helen E., Jonas, Jean-Christophe, and Laybutt, D. Ross

Subjects

PANCREATIC beta cells, CYTOKINES, ENDOPLASMIC reticulum, OXIDATIVE stress, THAPSIGARGIN

Abstract

The loss of functional beta cell mass characterises all forms of diabetes. Beta cells are highly susceptible to stress, including cytokine, endoplasmic reticulum (ER) and oxidative stress. This study examined the role of pleckstrin homology-like, domain family A, member 3 (Phlda3) in beta cell survival under stress conditions and the regulatory basis. We found that the mRNA levels of Phlda3 were markedly upregulated in vivo in the islets of diabetic humans and mice. In vitro, exposure of MIN6 cells or islets to cytokines, palmitate, thapsigargin or ribose upregulated Phlda3 mRNA and protein levels, concurrent with the induction of ER stress (Ddit3 and Trb3) and antioxidant (Hmox1) genes. Furthermore, H2O2 treatment markedly increased PHLDA3 immunostaining in human islets. Phlda3 expression was differentially regulated by adaptive (Xbp1) and apoptotic (Ddit3) unfolded protein response (UPR) mediators. siRNA-mediated knockdown of Xbp1 inhibited the induction of Phlda3 by cytokines and palmitate, whereas knockdown of Ddit3 upregulated Phlda3. Moreover, knockdown of Phlda3 potentiated cytokine-induced apoptosis in association with upregulation of inflammatory genes (iNos, IL1β and IκBα) and NFκB phosphorylation and downregulation of antioxidant (Gpx1 and Srxn1) and adaptive UPR (Xbp1, Hspa5 and Fkbp11) genes. Knockdown of Phlda3 also potentiated apoptosis under oxidative stress conditions induced by ribose treatment. These findings suggest that Phlda3 is crucial for beta cell survival under stress conditions. Phlda3 regulates the cytokine, oxidative and ER stress responses in beta cells via the repression of inflammatory gene expression and the maintenance of antioxidant and adaptive UPR gene expression. Phlda3 may promote beta cell survival in diabetes. [ABSTRACT FROM AUTHOR]

Published

2019

45. Placenta Stem/Stromal Cell–Derived Extracellular Vesicles for Potential Use in Lung Repair.

Author

Kim, Sally Yunsun, Joglekar, Mugdha V., Hardikar, Anandwardhan A., Phan, Thanh Huyen, Khanal, Dipesh, Tharkar, Priyanka, Limantoro, Christina, Johnson, Jancy, Kalionis, Bill, and Chrzanowski, Wojciech

Published

2019

46. Levels of circulating insulin cell-free DNA in women with polycystic ovary syndrome – a longitudinal cohort study.

Author

Udesen, Pernille Bækgaard, Sørensen, Anja Elaine, Joglekar, Mugdha V., Hardikar, Anandwardhan A., Wissing, Marie Louise Muff, Englund, Anne-Lis Mikkelsen, and Dalgaard, Louise Torp

Subjects

POLYCYSTIC ovary syndrome, ANOVULATION, DIABETES in women, TYPE 1 diabetes, LONGITUDINAL method, DNA, TYPE 2 diabetes

Abstract

Background: Women with Polycystic Ovary Syndrome (PCOS) present a heterogeneous reproductive and metabolic profile with an increased lifetime risk of Type 2 Diabetes (T2D). Early biomarkers of these metabolic disturbances in PCOS women have not been identified. The abundance of circulating insulin gene promotor cell-free DNA (INS cfDNA) was shown to be valuable as a predictive biomarker of β-cell death in individuals with Type 1 diabetes (T1D) as well as with gestational diabetes. Since β-cell death is common to the development of T1D as well as in T2D, we aimed to investigate if insulin-coding DNA is more abundant in circulation of PCOS women (vs Controls) and if their levels change after 6 yr. follow-up as a potential measure to predict future T2D. Methods: A cohort of 40 women diagnosed with PCOS according to Rotterdam 2003 criteria and eight healthy controls were examined at baseline and 6 years follow-up. Clinical measurements for evaluation of glucose homeostasis as well as blood/serum samples were obtained at each visit. Methylated and unmethylated INS cfDNA were quantified using droplet digital PCR. Differences between groups were assessed using Kruskall-Wallis test and Wilcoxon Signed rank test. Results: At baseline, there was no detectable difference in copy number (copies/μL) of methylated (p = 0.74) or unmethylated INS cfDNA (p = 0.34) between PCOS and Control groups. At follow up, neither methylated (p = 0.50) nor unmethylated INScfDNA levels (p = 0.48) differed significantly between these groups. Likewise, when pooling the groups, there was no difference between baseline and follow up, in terms of copies of methylated or unmethylated INS cfDNA (p = 0.38 and p = 0.52, respectively). There were no significant correlations between counts of unmethylated or methylated cfDNA and the clinical measurements of β-cell function and pre-diabetes. Conclusion: The circulating level of unmethylated and methylated INScfDNA is similar between PCOS and Controls and cannot be used to predict islet β-cell loss and progression to Type 2 diabetes in a 6-year follow-up. Trial registration: The Danish Data Protection Agency (REG-31-2016. Approval: 01-12-2015) and by the Danish Scientific Ethical committee of Region Zealand (Journal no. SJ-525. Approval: 13-06-2016), Clinicaltrials.gov, (NCT03142633, registered 1. March, 2017, Retrospectively registered). [ABSTRACT FROM AUTHOR]

Published

2019

47. Islet-like cell clusters occur naturally in human gall bladder and are retained in diabetic conditions.

Author

Sahu, Subhshri, Joglekar, Mugdha V., Dumbre, Ramesh, Phadnis, Smruti M., Tosh, David, and Hardikar, Anandwardhan A.

Subjects

CASE studies, GALLBLADDER diseases, DIAGNOSTIC ultrasonic imaging, GALLBLADDER surgery, GALLSTONES, CHOLECYSTECTOMY

Abstract

The article presents a case study of a 53-year-old woman with persistent stomachache due to gallstone pain. Following an ultrasonography examination, the patient then electively decided to undergo for cholecystectomy, a surgical removal of the gall bladder. The patient was said to be diabetic for 12 years and has took combinations of drugs and/or insulin injection as advised by her physician. Discussion on the laboratory results of the patient's gall bladder is also offered.

Published

2009

48. Circulating microRNAs: understanding the limits for quantitative measurement by real-time PCR.

Author

Hardikar, Anandwardhan A, Farr, Ryan J, and Joglekar, Mugdha V

Published

2014