Your search keyword '"Shirish Damle"' showing total 9 results

1. Bioenergetic variation is related to autism symptomatology

Author

Agustin Legido, Li Yin, Shirish Damle, Leanna Delhey, Stephen G. Kahler, Shannon Rose, Michael J. Goldenthal, Rebecca Wynne, John Slattery, Richard E. Frye, Ekim Nur Kilinc, and Marie Tippett

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Neurology, Bioenergetics, Autism Spectrum Disorder, Citrate (si)-Synthase, Complex IV, Biochemistry, behavioral disciplines and activities, Developmental psychology, Electron Transport Complex IV, Social Skills, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, Cognition, mental disorders, Complex I, medicine, Citrate synthase, Humans, Child, Adaptive behavior, Electron Transport Complex I, biology, medicine.disease, 030104 developmental biology, Variation (linguistics), Autism spectrum disorder, Social function, Child, Preschool, Electron transport chain, biology.protein, Autism, Female, Original Article, Neurology (clinical), Symptom Assessment, Psychology, Energy Metabolism, Mitochondrial dysfunction, 030217 neurology & neurosurgery, Clinical psychology

Abstract

Autism spectrum disorder (ASD) has been associated with mitochondrial dysfunction but few studies have examined the relationship between mitochondrial function and ASD symptoms. We measured Complex I and IV and citrate synthase activities in 76 children with ASD who were not receiving vitamin supplementation or medication. We also measured language using the Preschool Language Scales or Clinical Evaluation of Language Fundamentals, adaptive behavior using the Vineland Adaptive Behavioral Scale, social function using the Social Responsiveness Scale and behavior using Aberrant Behavior Checklist, Childhood Behavior Checklist and the Ohio Autism Clinical Impression Scale. Children with ASD demonstrated significantly greater variation in mitochondrial activity compared to controls with more than expected ASD children having enzyme activity outside of the normal range for Citrate Synthase (24%), Complex I (39%) and Complex IV (11%). Poorer adaptive skills were associated with Complex IV activity lower or higher than average and lower Complex I activity. Poorer social function and behavior was associated with relatively higher Citrate Synthase activity. Similar to previous studies we find both mitochondrial underactivity and overactivity in ASD. This study confirms an expanded variation in mitochondrial activity in ASD and demonstrates, for the first time, that such variations are related to ASD symptoms.

Published

2017

2. The Effect of Mitochondrial Supplements on Mitochondrial Activity in Children with Autism Spectrum Disorder

Author

Marie Tippett, John Slattery, Agustin Legido, Sirish C. Bennuri, Michael J. Goldenthal, Ekim Nur Kilinc, Shirish Damle, Stephen G. Kahler, Richard E. Frye, Li Yin, Shannon Rose, and Leanna Delhey

Subjects

0301 basic medicine, Antioxidant, Mitochondrial disease, medicine.medical_treatment, Buccal swab, lcsh:Medicine, autism spectrum disorder, Complex IV, Pharmacology, folate, fatty acids, antioxidants, B12, Complex I, electron transport chain, mitochondrial disease, mitochondrial dysfunction, Article, 03 medical and health sciences, 0302 clinical medicine, medicine, Citrate synthase, chemistry.chemical_classification, biology, business.industry, lcsh:R, Folate supplementation, Fatty acid, General Medicine, medicine.disease, 030104 developmental biology, chemistry, Biochemistry, Autism spectrum disorder, Expert opinion, biology.protein, business, 030217 neurology & neurosurgery

Abstract

Treatment for mitochondrial dysfunction is typically guided by expert opinion with a paucity of empirical evidence of the effect of treatment on mitochondrial activity. We examined citrate synthase and Complex I and IV activities using a validated buccal swab method in 127 children with autism spectrum disorder with and without mitochondrial disease, a portion of which were on common mitochondrial supplements. Mixed-model linear regression determined whether specific supplements altered the absolute mitochondrial activity as well as the relationship between the activities of mitochondrial components. Complex I activity was increased by fatty acid and folate supplementation, but folate only effected those with mitochondrial disease. Citrate synthase activity was increased by antioxidant supplementation but only for the mitochondrial disease subgroup. The relationship between Complex I and IV was modulated by folate while the relationship between Complex I and Citrate Synthase was modulated by both folate and B12. This study provides empirical support for common mitochondrial treatments and demonstrates that the relationship between activities of mitochondrial components might be a marker to follow in addition to absolute activities. Measurements of mitochondrial activity that can be practically repeated over time may be very useful to monitor the biochemical effects of treatments.

Published

2017

3. An miRNA Expression Signature for the Human Colonic Stem Cell Niche Distinguishes Malignant from Normal Epithelia

Author

Gregory E. Gonye, Skye A. Schmidt, Sepehr Sedigh Haghighat, Tao Zhang, Isidore Rigoutsos, Pamela J. Green, Monica Accerbi, Jeremy Z. Fields, Juan P. Palazzo, Shirish Damle, Lynn M. Opdenaker, Deni S. Galileo, Shirin R. Modarai, Bruce M. Boman, and Vignesh Viswanathan

Subjects

0301 basic medicine, Cancer Research, Pathology, medicine.medical_specialty, Colorectal cancer, Biology, Malignant transformation, 03 medical and health sciences, Intestinal mucosa, Cancer stem cell, Cell Line, Tumor, microRNA, medicine, Humans, Intestinal Mucosa, Stem Cell Niche, Cell Proliferation, LGR5, Cell cycle, medicine.disease, MicroRNAs, 030104 developmental biology, Oncology, Cancer research, Neoplastic Stem Cells, Stem cell, Colorectal Neoplasms

Abstract

Malignant transformation of tissue stem cells (SC) may be the root of most cancer. Accordingly, we identified miRNA expression patterns in the normal human colonic SC niche to understand how cancer stem cells (CSC) may arise. In profiling miRNA expression in SC-enriched crypt subsections isolated from fresh, normal surgical specimens, we identified 16 miRNAs that were differentially expressed in the crypt bottom, creating an SC signature for normal colonic epithelia (NCE). A parallel analysis of colorectal cancer tissues showed differential expression of 83 miRNAs relative to NCE. Within the 16 miRNA signature for the normal SC niche, we found that miR-206, miR-007-3, and miR-23b individually could distinguish colorectal cancer from NCE. Notably, miR-23b, which was increased in colorectal cancer, was predicted to target the SC-expressed G protein-coupled receptor LGR5. Cell biology investigations showed that miR-23b regulated CSC phenotypes globally at the level of proliferation, cell cycle, self-renewal, epithelial–mesenchymal transition, invasion, and resistance to the colorectal cancer chemotherapeutic agent 5-fluorouracil. In mechanistic experiments, we found that miR-23b decreased LGR5 expression and increased ALDH+ CSCs. CSC analyses confirmed that levels of LGR5 and miR-23b are inversely correlated in ALDH+ CSCs and that distinct subpopulations of LGR5+ and ALDH+ CSCs exist. Overall, our results define a critical function for miR-23b, which, by targeting LGR5, contributes to overpopulation of ALDH+ CSCs and colorectal cancer. Cancer Res; 77(14); 3778–90. ©2017 AACR.

Published

2016

4. Nuclear-mitochondrial cross-talk in global myocardial ischemia. A time-course analysis

Author

Shirish Damle, José Marín-García, Gordon W. Moe, and Bodh I. Jugdutt

Subjects

Mitochondrial DNA, Clinical Biochemistry, Myocardial Ischemia, Ischemia, Oxidative phosphorylation, Biology, Mitochondrion, DNA, Mitochondrial, Mitochondria, Heart, Mitochondrial Proteins, Organ Culture Techniques, Oxygen Consumption, Gene expression, medicine, Animals, Humans, cardiovascular diseases, Molecular Biology, Heart metabolism, Oligonucleotide Array Sequence Analysis, Cardioprotection, Nuclear Proteins, Cell Biology, General Medicine, medicine.disease, Coronary Vessels, Molecular biology, Rats, Cell biology, Disease Models, Animal, Gene Expression Regulation, Reperfusion, Ischemic preconditioning, Energy Metabolism

Abstract

Myocardial ischemia results in early and progressive damage to mitochondrial structure and function, but the molecular events leading to these changes have not been clearly established. We hypothesized that mitochondrial dysfunction and a coordinated expression of nuclear and mitochondrial genes occur in a time-dependent manner by relating the time courses of changes in parameters of mitochondrial bioenergetics after ischemia-reperfusion. Using a Langendorff rat heart model, mitochondrial bioenergetics and protein levels were assessed at different times of ischemia and ischemia/reperfusion. Mitochondrial and nuclear gene expression (super array analysis) and mitochondrial DNA levels were evaluated after late ischemia. Ischemia induced progressive and marked decreases in complex I, III, and V activities. Reperfusion (15, 30, and 60 min) after 45 min of ischemia had little further effect on enzyme activities or respiration. Super array analysis after 45 min ischemia revealed increased levels of the proteins with more pronounced increases in the corresponding mRNAs. Expression of mitochondrial and nuclear genes involved in oxidative phosphorylation increased after 45 min of ischemia but not after reperfusion. Myocardial ischemia induces mitochondrial dysfunction and differential but coordinated expression of nuclear and mitochondrial genes in a time-dependent manner. Our observations are pertinent to the search for molecular stimuli that generate mitochondrial defects and alter mitochondrial and nuclear transcriptional responses that may impact ischemic preconditioning and cardioprotection.

Published

2012

5. Regional Distribution of Mitochondrial Dysfunction and Apoptotic Remodeling in Pacing-Induced Heart Failure

Author

YeQing Pi, Shirish Damle, José Marín-García, Gordon W. Moe, and Michael J. Goldenthal

Subjects

Mitochondrial DNA, medicine.medical_specialty, Respiratory chain, Apoptosis, Mitochondrion, Mitochondria, Heart, Dogs, Internal medicine, medicine, Animals, Transcription factor, Heart Failure, Ventricular Remodeling, ATP synthase, biology, business.industry, Cardiac Pacing, Artificial, Cell biology, Disease Models, Animal, Oxidative Stress, Cytosol, biology.protein, Cardiology, Apoptosis-inducing factor, Cardiology and Cardiovascular Medicine, business, Signal Transduction

Abstract

Background Specific myocardial mitochondrial enzymatic dysfunction and apoptotic remodeling occur in pacing-induced heart failure. We sought to define their regional distribution and molecular basis in the failing heart. Methods and Results Enzyme dysfunction was assessed in mitochondrial subpopulations and immunoblot analysis was performed using homogenate proteins from the left atria (LA) and left ventricle (LV) of paced and control mongrel dogs. A greater range of enzymatic defects (complex I, III, and V) was found in mitochondria subpopulations from the LV as compared with the LA (where only complex V was defective). Analysis of paced LV proteins demonstrated a downregulated expression of both mitochondrial genes (eg, cytochrome b ) and nuclear genes (eg, ATP synthase β subunit, mitochondrial creatine kinase). Protease-activated products of both mitochondrial (eg, apoptosis inducing factor) and cytosolic (eg, caspase-3) apoptogenic proteins were increased in both the LA and LV. Nuclear-localized apoptotic markers (eg, p53, p21) were also significantly increased in the LV of paced dogs. Conclusion Abnormal activity of several mitochondrial enzymes and increased apoptogenic pathway appear to be mediated, at least in part, by an orchestrated shift in expression (both nuclear and mitochondrial DNA) of respiratory chain subunits (eg, cyt b , ATP-β), mitochondrial bioenergetic enzymes (eg, mitochondrial creatine kinase), global transcription factor (eg, PGC-1), and apoptotic proteins (eg, p53, p21) with distinct differences in their regional distribution and in the subpopulations of mitochondria affected.

Published

2009

6. Analyzing Alkaline Proteins in Human Colon Crypt Proteome

Author

Xin-Ming, Li, Bhavinkumar B, Patel, Elena L, Blagoi, Maketa D, Patterson, Steven H, Seeholzer, Steven H, Seehozer, Tao, Zhang, Shirish, Damle, Zhenqiang, Gao, Bruce, Boman, and Anthony T, Yeung

Subjects

Cell Extracts, Gene isoform, Gel electrophoresis, Proteome, Colon, Isoelectric focusing, Crypt, Proteins, General Chemistry, Hydrogen-Ion Concentration, Biology, Biochemistry, Molecular biology, Histone, Ribosomal protein, biology.protein, Humans, Electrophoresis, Gel, Two-Dimensional, Immobilized pH gradient, Isoelectric Focusing, Colorectal Neoplasms

Abstract

Normal human colon crypt protein extract was resolved by two-dimensional gel electrophoresis using pH 6-11 immobilized pH gradient strips in the first dimension. The optimized isoelectric focusing protocol includes cup-loading sample application at the anode and 1.2% hydroxyethyl disulfide (DeStreak), 15% 2-propanol and 5% glycerol in the rehydration buffer. Spots were well resolved across the entire pH range up to 11. A total of 311 protein spots were identified by mass spectrometry and peptide mass mapping. After combining isoforms, 231 nonredundant proteins were grouped into 16 categories according to their subcellular locations, and 17 categories according to their physiological functions. Histone proteins, ribosomal proteins and mitochondrial proteins were among the well-resolved highest p/ proteins. Application of this protocol to the analysis of normal and neoplastic colon crypts will contribute to the proteomic study of colorectal tumorigenesis since a significant portion of the human proteins is in basic pH range.

Published

2004

7. Adaptive changes in the expression of nuclear and mitochondrial encoded subunits of cytochrome c oxidase and the catalytic activity during hypoxia

Author

Shirish Damle, Narayan G. Avadhani, Camasamudram Vijayasarathy, Subbuswamy K. Prabu, and Cynthia M. Otto

Subjects

chemistry.chemical_classification, Oxidase test, Mitochondrial DNA, biology, Protein subunit, Hypoxia (medical), Biochemistry, Molecular biology, chemistry.chemical_compound, Enzyme, chemistry, medicine, biology.protein, Cytochrome c oxidase, Glycolysis, medicine.symptom, Heme

Abstract

The effects of physiologically relevant hypoxia on the catalytic activity of cytochrome c oxidase (CytOX), mitochondrial gene expression, and both nuclear and mitochondrial encoded CytOX mRNA levels were investigated in murine monocyte macrophages, mouse C2C12 skeletal myocytes and rat adrenal pheochromocytoma PC12 cells. Our results suggest a coordinated down regulation of mitochondrial genome-coded CytOX I and II and nuclear genome-coded CytOX IV and Vb mRNAs during hypoxia. Hypoxia also caused a severe decrease in mitochondrial transcription rates, and associated decrease in mitochondrial transcription factor A. The enzyme from hypoxia exposed cells exhibited altered subunit content as revealed by blue native gel electrophoresis. There was a generalized decline in mitochondrial function that led to a decrease in total cellular heme and ATP pools. We also observed a decrease in mitochondrial heme aa3 content and decreased levels of CytOX subunit I, IV and Vb, though the catalytic efficiency of the enzyme (TN for cytochrome c oxidase) remained nearly the same. Increased glycolytic flux and alterations in the kinetic characteristics of the CytOX might be the two mechanisms by which hypoxic cells maintain adequate ATP levels to sustain life processes. Reoxygenation nearly completely reversed hypoxia-mediated changes in CytOX mRNA contents, rate of mitochondrial transcription, and the catalytic activity of CytOX enzyme. Our results show adaptive changes in CytOX structure and activity during physiological hypoxia.

Published

2003

8. Tissue variant effects of heme inhibitors on the mouse cytochrome c oxidase gene expression and catalytic activity of the enzyme complex

Author

Nibedita Lenka, Shirish Damle, Camasamudram Vijayasarathy, and Narayan G. Avadhani

Subjects

Hemeproteins, Enzyme complex, Iron, Protein subunit, Mitochondria, Liver, Heme, Mitochondrion, Kidney, Biochemistry, Catalysis, Electron Transport Complex IV, Mice, chemistry.chemical_compound, Adenosine Triphosphate, Multienzyme Complexes, Animals, Cytochrome c oxidase, RNA, Messenger, Enzyme Inhibitors, Enzyme inducer, biology, Cytochrome c, Brain, Porphobilinogen Synthase, Cobalt, Cyclic AMP-Dependent Protein Kinases, Molecular biology, Enzyme assay, Heptanoates, Mitochondria, chemistry, Organ Specificity, Enzyme Induction, Heme Oxygenase (Decyclizing), biology.protein

Abstract

The in vivo effects of heme biosynthesis inhibitors, succinylacetone and CoCl2 on the cytochrome c oxidase (COX) gene expression and enzyme activity in different mouse tissues were investigated. Succinylacetone and CoCl2 showed tissue-specific differences in their ability to modulate heme aa3 content. A single dose of succinylacetone treatment for 8 h reduced the heme aa3 content of kidney mitochondria with no effect on the liver. CoCl2 treatment for 8 h, however, selectively affected the heme aa3 level in the liver. Reduced mitochondrial heme aa3 with both treatments was accompanied by approximately 50% reduced, mitochondrial genome-encoded COX I and II mRNAs and nuclear genome-encoded COX Vb mRNAs, but no change in COX IV mRNA level. Use of isolated mouse liver and brain mitochondrial systems showed a 50-80% reduction in mitochondrial transcription and translation rates in heme-depleted tissues. Blue native gel electrophoresis followed by immunoblot analysis showed that the complex from heme-depleted tissues contained a 30-50% reduction in levels of subunits I, IV, Vb and near normal levels of subunit VIc, indicating altered subunit content. Treatment of submitochondrial particles with protein kinase A and ATP resulted in partial dissociation of COX, suggesting a mechanistic basis for the reduced subunit content of the complex from heme-depleted tissues. Surprisingly, the enzyme from heme-depleted tissues showed twofold to fourfold higher turnover rates for cytochrome c oxidation, suggesting alterations in the kinetic characteristics of the enzyme following heme reduction. This is probably the first evidence that the tissue heme level regulates not only the mammalian COX gene expression, but also the catalytic activity of the enzyme, probably by affecting its stability.

Published

1999

9. Non-invasive evaluation of buccal respiratory chain enzyme dysfunction in mitochondrial disease: comparison with studies in muscle biopsy

Author

Sudip Sheth, Divya S. Khurana, Agustin Legido, Ignacio Valencia, Nidhi Shah, Teddy Kuruvilla, Shirish Damle, Leon Salganicoff, Harold Marks, and Michael J. Goldenthal

Subjects

Adult, Male, Pathology, medicine.medical_specialty, Mitochondrial Diseases, Adolescent, Endocrinology, Diabetes and Metabolism, Mitochondrial disease, Buccal swab, Respiratory chain, Citrate (si)-Synthase, Biology, Biochemistry, DNA, Mitochondrial, Oxidative Phosphorylation, Cohort Studies, Electron Transport, Young Adult, Endocrinology, stomatognathic system, Iron-Binding Proteins, Genetics, medicine, Citrate synthase, Humans, Child, Muscle, Skeletal, Molecular Biology, Muscle biopsy, Electron Transport Complex I, medicine.diagnostic_test, Mouth Mucosa, Skeletal muscle, Buccal administration, Middle Aged, medicine.disease, Mitochondria, Mitochondria, Muscle, medicine.anatomical_structure, Child, Preschool, Frataxin, biology.protein, Female

Abstract

Making a diagnosis of mitochondrial disease (MD) is extremely challenging and often employs the analysis of respiratory complex (RC) activities in biopsied skeletal muscle. Given both the invasive nature and expense of biopsied-muscle based testing for mitochondrial defects, buccal swab enzyme analysis has been explored as an alternative approach to the more invasive muscle biopsy. Case studies have recently suggested that buccal swabs from patients can be used to accurately assess mitochondrial enzyme activities including RC I and RC IV using a dipstick methodology combined with spectrophotometric analysis. In this study, forty patients with suspected MD who have previously been found to have significant defects in either RC I or RC IV in skeletal muscle were assessed by buccal swab analysis and compared to enzyme values obtained with unaffected controls (n=106) in the same age range. Buccal citrate synthase was used as an indicator of overall mitochondrial content, correlating well with overall buccal mitochondrial frataxin levels and was found to be elevated above control levels in 28% of the patients in this cohort. Of 26 cases with significant muscle RC I deficiency, 20 displayed significantly reduced levels of buccal RC I activity. All 7 of the patients with muscle RC IV deficiency showed significant buccal RC IV defect and 6 of the 7 patients with combined defects in muscle RC I and IV activity levels also exhibited analogous deficiencies in both buccal RC I and RC IV activities. In conclusion, the relatively high correlation (over 82%) of buccal and muscle RC deficiencies further supports the validity of this non-invasive approach as a potentially useful tool in the diagnosis of MD.

Published

2011