Your search keyword '"Vinik, A"' showing total 80 results

1. Programming a Ferroptosis‐to‐Apoptosis Transition Landscape Revealed Ferroptosis Biomarkers and Repressors for Cancer Therapy.

Author

Vinik, Yaron, Maimon, Avi, Dubey, Vinay, Raj, Harsha, Abramovitch, Ifat, Malitsky, Sergey, Itkin, Maxim, Ma'ayan, Avi, Westermann, Frank, Gottlieb, Eyal, Ruppin, Eytan, and Lev, Sima

Subjects

*TUMOR markers, *CANCER treatment, *BREAST, *BREAST cancer prognosis, *CANCER prognosis, *TRICARBOXYLIC acids

Abstract

Ferroptosis and apoptosis are key cell‐death pathways implicated in several human diseases including cancer. Ferroptosis is driven by iron‐dependent lipid peroxidation and currently has no characteristic biomarkers or gene signatures. Here a continuous phenotypic gradient between ferroptosis and apoptosis coupled to transcriptomic and metabolomic landscapes is established. The gradual ferroptosis‐to‐apoptosis transcriptomic landscape is used to generate a unique, unbiased transcriptomic predictor, the Gradient Gene Set (GGS), which classified ferroptosis and apoptosis with high accuracy. Further GGS optimization using multiple ferroptotic and apoptotic datasets revealed highly specific ferroptosis biomarkers, which are robustly validated in vitro and in vivo. A subset of the GGS is associated with poor prognosis in breast cancer patients and PDXs and contains different ferroptosis repressors. Depletion of one representative, PDGFA‐assaociated protein 1(PDAP1), is found to suppress basal‐like breast tumor growth in a mouse model. Omics and mechanistic studies revealed that ferroptosis is associated with enhanced lysosomal function, glutaminolysis, and the tricarboxylic acid (TCA) cycle, while its transition into apoptosis is attributed to enhanced endoplasmic reticulum(ER)‐stress and phosphatidylethanolamine (PE)‐to‐phosphatidylcholine (PC) metabolic shift. Collectively, this study highlights molecular mechanisms underlying ferroptosis execution, identified a highly predictive ferroptosis gene signature with prognostic value, ferroptosis versus apoptosis biomarkers, and ferroptosis repressors for breast cancer therapy. [ABSTRACT FROM AUTHOR]

Published

2024

2. Mouse Modeling Dissecting Macrophage–Breast Cancer Communication Uncovered Roles of PYK2 in Macrophage Recruitment and Breast Tumorigenesis.

Author

Müller, Anna‐Katharina, Köhler, Ulrike A., Trzebanski, Sébastien, Vinik, Yaron, Raj, Harsha Mohan, Girault, Jean‐Antoine, Ben‐Chetrit, Nir, Maraver, Antonio, Jung, Steffen, and Lev, Sima

Subjects

LABORATORY mice, PROTEIN-tyrosine kinases, BREAST cancer, TUMOR microenvironment, CANCER cells, PHENOTYPIC plasticity, MACROPHAGES

Abstract

Macrophage infiltration in mammary tumors is associated with enhanced tumor progression, metastasis, and poor clinical outcome, and considered as target for therapeutic intervention. By using different genetic mouse models, the authors show that ablation of the tyrosine kinase PYK2, either in breast cancer cells, only in the tumor microenvironment, or in both, markedly reduces the number of infiltrating tumor macrophages and concomitantly inhibits tumor angiogenesis and tumor growth. Strikingly, PYK2 ablation only in macrophages is sufficient to induce similar effects. These phenotypic changes are associated with reduced monocyte recruitment and a substantial decrease in tumor‐associated macrophages (TAMs). Mechanistically, the authors show that PYK2 mediates mutual communication between breast cancer cells and macrophages through critical effects on key receptor signaling. Specifically, PYK2 ablation inhibits Notch1 signaling and consequently reduces CCL2 secretion by breast cancer cells, and concurrently reduces the levels of CCR2, CXCR4, IL‐4Rα, and Stat6 activation in macrophages. These bidirectional effects modulate monocyte recruitment, macrophage polarization, and tumor angiogenesis. The expression of PYK2 is correlated with infiltrated macrophages in breast cancer patients, and its effects on macrophage infiltration and pro‐tumorigenic phenotype suggest that PYK2 targeting can be utilized as an effective strategy to modulate TAMs and possibly sensitize breast cancer to immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2022

3. Gene therapy for diabetic peripheral neuropathy: A randomized, placebo‐controlled phase III study of VM202, a plasmid DNA encoding human hepatocyte growth factor.

Author

Kessler, John A., Shaibani, Aziz, Sang, Christine N., Christiansen, Mark, Kudrow, David, Vinik, Aaron, and Shin, Nari

Subjects

HEPATOCYTE growth factor, DIABETIC neuropathies, PERIPHERAL neuropathy, GENE therapy, HUMAN DNA

Abstract

VM202 is a plasmid DNA encoding two isoforms of hepatocyte growth factor (HGF). A previous phase II study in subjects with painful diabetic peripheral neuropathy (DPN) showed significant reductions in pain. A phase III study was conducted to evaluate the safety and efficacy of VM202 in DPN. The trial was conducted in two parts, one for 9 months (DPN 3‐1) with 500 subjects (VM202: 336 subjects; and placebo: 164) and a preplanned subset of 101 subjects (VM202: 65 subjects; and placebo: 36) with a noninterventional extension to 12 months (DPN 3‐1b). VM202 or placebo was administered to calf muscles on days 0 and 14, and on days 90 and 104. The primary end point in DPN 3‐1 was change from baseline in the mean 24‐h Numerical Rating Scale (NRS) pain score. In DPN 3‐1b, the primary end point was safety, whereas the secondary efficacy end point was change in the mean pain score. VM202 was well‐tolerated in both studies without significant adverse events. VM202 failed to meet its efficacy end points in DPN 3‐1. In DPN 3‐1b, however, VM202 showed significant and clinically meaningful pain reduction versus placebo. Pain reduction in DPN 3‐1b was even greater in subjects not receiving gabapentin or pregabalin, confirming an observation noted in the phase II study. In DPN 3‐1b, symptomatic relief was maintained for 8 months after the last injection suggesting that VM202 treatment might change disease progression. Despite the perplexing discrepancy between the two studies, the safety and long‐lasting pain‐relieving effects of VM202 observed in DPN 3‐1b warrant another rigorous phase III study. Study HighlightsWHAT IS THE CURRENT KNOWLEDGE ON THE TOPIC?Current therapies for painful diabetic peripheral neuropathy (DPN) are palliative and do not target the underlying mechanisms. Moreover, symptomatic relief is often limited with existing neuropathic pain drugs. Thus, there is a great medical need for safer and effective treatments for DPN. WHAT QUESTION DID THIS STUDY ADDRESS?Can nonviral gene delivery of hepatocyte growth factor reduce pain in patients with DPN and potentially modify progression of the disorder? WHAT DOES THIS STUDY ADD TO OUR KNOWLEDGE?Nonviral gene therapy can be used safely and practically to treat DPN. HOW MIGHT THIS CHANGE CLINICAL PHARMACOLOGY OR TRANSLATIONAL SCIENCE?As the first gene medicine to enter advanced clinical trials for the treatment of DPN, this study provides the proof of concept of an entirely new potential approach to the disorder. [ABSTRACT FROM AUTHOR]

Published

2021

4. Modeling Heterogeneity of Triple‐Negative Breast Cancer Uncovers a Novel Combinatorial Treatment Overcoming Primary Drug Resistance.

Author

Lamballe, Fabienne, Ahmad, Fahmida, Vinik, Yaron, Castellanet, Olivier, Daian, Fabrice, Müller, Anna‐Katharina, Köhler, Ulrike A., Bailly, Anne‐Laure, Josselin, Emmanuelle, Castellano, Rémy, Cayrou, Christelle, Charafe‐Jauffret, Emmanuelle, Mills, Gordon B., Géli, Vincent, Borg, Jean‐Paul, Lev, Sima, and Maina, Flavio

Subjects

TRIPLE-negative breast cancer, DRUG resistance, MET receptor, HETEROGENEITY, BREAST cancer

Abstract

Triple‐negative breast cancer (TNBC) is a highly aggressive breast cancer subtype characterized by a remarkable molecular heterogeneity. Currently, there are no effective druggable targets and advanced preclinical models of the human disease. Here, a unique mouse model (MMTV‐R26Met mice) of mammary tumors driven by a subtle increase in the expression of the wild‐type MET receptor is generated. MMTV‐R26Met mice develop spontaneous, exclusive TNBC tumors, recapitulating primary resistance to treatment of patients. Proteomic profiling of MMTV‐R26Met tumors and machine learning approach show that the model faithfully recapitulates intertumoral heterogeneity of human TNBC. Further signaling network analysis highlights potential druggable targets, of which cotargeting of WEE1 and BCL‐XL synergistically kills TNBC cells and efficiently induces tumor regression. Mechanistically, BCL‐XL inhibition exacerbates the dependency of TNBC cells on WEE1 function, leading to Histone H3 and phosphoS33RPA32 upregulation, RRM2 downregulation, cell cycle perturbation, mitotic catastrophe, and apoptosis. This study introduces a unique, powerful mouse model for studying TNBC formation and evolution, its heterogeneity, and for identifying efficient therapeutic targets. [ABSTRACT FROM AUTHOR]

Published

2021

5. Effect of Powered Air-Purifying Respirators on Speech Recognition Among Health Care Workers.

Author

Kempfle, Judith S., Panda, Ashwin, Hottin, Mary, Vinik, Kevin, Kozin, Elliott D., Ito, Christopher J., and Remenschneider, Aaron K.

Abstract

Powered air-purifying respirators (PAPRs) are used as personalized protective equipment for health care personnel. PAPRs offer health care workers added protection when dealing with patients who have high-risk infectious disease such as COVID-19. Unfortunately, PAPRs can produce notable levels of background noise. We hypothesize that PAPR use may be associated with increased hearing thresholds and impaired word discrimination and may ultimately have a negative impact on effective communication. Herein, we (1) determined sound levels generated by PAPRs and (2) measured hearing thresholds and word discrimination with and without operational PAPRs. All participants had normal hearing. When the PAPR was operational, mean ± SD thresholds increased from 4.5 ± 3.6 to 38.6 ± 5.6 dB HL (P <.001). Word discrimination dropped from 100% in all participants in quiet to a mean 48% ± 14% with operational PAPR (P <.001). Thus, we find that use of PAPR hoods results in hearing impairment comparable to moderate to severe hearing loss, and we suspect that users will experience communication difficulties as a result. Level of Evidence. Prospective study. [ABSTRACT FROM AUTHOR]

Published

2021

6. Clinical measures in transthyretin familial amyloid polyneuropathy.

Author

Coelho, Teresa, Vinik, Aaron, Vinik, Etta J., Tripp, Tara, Packman, Jeff, and Grogan, Donna R.

Subjects

*NEURAL physiology, *TREATMENT of peripheral neuropathy, *PERIPHERAL neuropathy, *AMYLOID, *ANALYSIS of variance, *NEURONS, *NONPARAMETRIC statistics, *QUALITY of life, *CROSS-sectional method, *SEVERITY of illness index, *DISEASE progression, *PSYCHOLOGY, PERIPHERAL neuropathy diagnosis

Abstract

Introduction: This observational, cross-sectional, single-center study aimed to identify instruments capable of measuring disease progression in transthyretin familial amyloid polyneuropathy (TTR-FAP).Methods: The relationship between disease stage and Neuropathy Impairment Score-Lower Limbs (NIS-LL) and Norfolk Quality of Life-Diabetic Neuropathy (Norfolk QOL-DN) total score was assessed in 61 (stages 1-3) patients with TTR-FAP (V30M variant) and 16 healthy controls. Composite measures of large- and small-nerve fiber function, and modified body mass index (mBMI) were also assessed.Results: Ordinal-based NIS-LL and Norfolk QOL-DN scores discriminated between disease stages (P < 0.0001 for NIS-LL and Norfolk QOL-DN). Longer disease duration correlated with worse NIS-LL and Norfolk QOL-DN. Karnofsky performance score declined progressively by disease stage. Composite measures of nerve fiber function differentiated stage 1 from stage 2 disease. The mBMI declined with advancing disease.Conclusions: NIS-LL, Norfolk QOL-DN score, composite endpoints of nerve fiber function, and mBMI are valid, reliable measures of TTR-FAP severity. Muscle Nerve 55: 323-332, 2017. [ABSTRACT FROM AUTHOR]

Published

2017

7. Diabetic Cardiac Autonomic Neuropathy, Inflammation And Cardiovascular Disease

Author

Vinik, Aaron I., Erbas, Tomris, Casellini, Carolina M., and İç Hastalıkları

Subjects

Endocrinology & Metabolism

Abstract

One of the most overlooked of all serious complications of diabetes is cardiovascular autonomic neuropathy. There is now clear evidence that suggests activation of inflammatory cytokines in diabetic patients and that these correlate with abnormalities in sympathovagal balance. Dysfunction of the autonomic system predicts cardiovascular risk and sudden death in patients with type 2 diabetes. It also occurs in prediabetes, providing opportunities for early intervention. Simple tests that can be carried out at the bedside with real-time output of information within the scope of the practicing physician facilitate diagnosis and allow the application of sound strategies for management. The window of opportunity for aggressive control of all the traditional risk factors for cardiovascular events or sudden death with intensification of therapy is with short duration diabetes, the absence of cardiovascular disease and a history of severe hypoglycemic events. To this list we can now add autonomic dysfunction and neuropathy, which have become the most powerful predictors of risk for mortality. It seems prudent that practitioners should be encouraged to become familiar with this information and apply risk stratification in clinical practice. Several agents have become available for the correction of functional defects in the autonomic nervous system, and restoration of autonomic balance is now possible.

Published

2013

8. Structure‐Based Design of a Monosaccharide Ligand Targeting Galectin‐8.

Author

Bohari, Mohammad H., Yu, Xing, Kishor, Chandan, Patel, Brijesh, Go, Rob Marc, Eslampanah Seyedi, Hadieh A., Vinik, Yaron, Grice, I. Darren, Zick, Yehiel, and Blanchard, Helen

Published

2018

9. Ablation of the mammalian lectin galectin-8 induces bone defects in mice.

Author

Vinik, Yaron, Shatz-Azoulay, Hadas, Hiram-Bab, Sahar, Kandel, Leonid, Gabet, Yankel, Rivkin, Gurion, and Zick, Yehiel

Abstract

Mice overexpressing galectin-8 [gal-8 transgenic (Tg)], a secreted mammalian lectin, exhibit enhanced bone turnover and reduced bone mass, similar to cases of postmenopausal osteoporosis. Here, we show that gal-8 knockout (KO) mice have increased bone mass accrual at a young age but exhibit accelerated bone loss during adulthood. These phenotypes can be attributed to a gal-8-mediated increase in receptor activator of NF-κB ligand (RANKL) expression that promotes osteoclastogenesis, combined with direct inhibition of osteoblast differentiation, evident by reduced bone morphogenetic protein (BMP) signaling, reduced phosphorylation of receptor regulated mothers against decapentaplegic homolog (R-SMAD) and reduced expression of osteoblast differentiation markers osterix, osteocalcin, runt-related transcription factor 2 (RUNX2), dentin matrix acidic phosphoprotein-1 (DMP1), and alkaline phosphatase. At the same time, gal-8 promotes expression of estrogen receptor a (ESR1). Accordingly, the rate of bone loss is accelerated in ovariectomized, estrogen-deficient gal-8 Tg mice, whereas gal-8 KO mice, having low levels of ESR1, are refractory to ovariectomy. Finally, gal-8 mRNA positively correlates with the mRNA levels of osteoclastogenic markers RANKL, tartrate-resistant acid phosphatase, and cathepsin K in human femurs. Collectively, these findings identify gal-8 as a new physiologic player in the regulation of bone mass. [ABSTRACT FROM AUTHOR]

Published

2018

10. Norfolk QOL-DN: validation of a patient reported outcome measure in transthyretin familial amyloid polyneuropathy.

Author

Vinik, Etta J., Vinik, Aaron I., Paulson, James F., Merkies, Ingemar S. J., Packman, Jeff, Grogan, Donna R., and Coelho, Teresa

Subjects

*QUESTIONNAIRES, *ACADEMIC medical centers, *AMYLOID, *ANALYSIS of variance, *STATISTICAL correlation, *ELECTROPHYSIOLOGY, *FISHER exact test, *INTERVIEWING, *PERIPHERAL neuropathy, *POLYNEUROPATHIES, *QUALITY of life, *RESEARCH funding, *T-test (Statistics), *CROSS-sectional method, *SEVERITY of illness index, *DESCRIPTIVE statistics, RESEARCH evaluation

Abstract

The Norfolk Quality of Life-Diabetic Neuropathy ( QOL-DN) questionnaire is an instrument to assess QOL in diabetic polyneuropathy. The objective of this observational, cross-sectional study in 61 patients with V30M transthyretin familial amyloid polyneuropathy ( TTR-FAP) and 16 healthy volunteers was to validate the Norfolk QOL-DN for assessment of QOL in TTR-FAP. Comparisons were conducted to identify the best items to discriminate disease stages and assess which individual Norfolk domains (symptoms, large fiber, small fiber, autonomic, and activities of daily living) would be most affected by disease stage. Analysis of individual items revealed a significant pattern of discrimination among disease stages (p < 0.001). Total QOL scores increased (indicating worsening) with duration of symptoms, with a steeper increase observed earlier in the course of disease. Significant correlations were observed between each Norfolk domain and other measures of neurological function. Limitations include cross-sectional study design, low patient numbers in this rare disease, and the ordinal-based character of the metric used; future areas to explore include item response theory approaches such as Rasch analysis. These results suggest the Norfolk QOL-DN is a reliable indicator of the impact of disease severity on QOL in patients with TTR-FAP. [ABSTRACT FROM AUTHOR]

Published

2014

11. Content validity of symptom-based measures for diabetic, chemotherapy, and HIV peripheral neuropathy.

Author

Gewandter, Jennifer S., Burke, Laurie, Cavaletti, Guido, Dworkin, Robert H., Gibbons, Christopher, Gover, Tony D., Herrmann, David N., Mcarthur, Justin C., McDermott, Michael P., Rappaport, Bob A., Reeve, Bryce B., Russell, James W., Smith, A. Gordon, Smith, Shannon M., Turk, Dennis C., Vinik, Aaron I., and Freeman, Roy

Subjects

DIAGNOSIS of diabetic neuropathies, PERIPHERAL neuropathy diagnosis, HIV infection complications, DIABETIC neuropathies, PERIPHERAL neuropathy, RESEARCH funding, SYSTEMATIC reviews

Abstract

Introduction: No treatments for axonal peripheral neuropathy are approved by the United States Food and Drug Administration (FDA). Although patient- and clinician-reported outcomes are central to evaluating neuropathy symptoms, they can be difficult to assess accurately. The inability to identify efficacious treatments for peripheral neuropathies could be due to invalid or inadequate outcome measures.Methods: This systematic review examined the content validity of symptom-based measures of diabetic peripheral neuropathy, HIV neuropathy, and chemotherapy-induced peripheral neuropathy.Results: Use of all FDA-recommended methods to establish content validity was only reported for 2 of 18 measures. Multiple sensory and motor symptoms were included in measures for all 3 conditions; these included numbness, tingling, pain, allodynia, difficulty walking, and cramping. Autonomic symptoms were less frequently included.Conclusions: Given significant overlap in symptoms between neuropathy etiologies, a measure with content validity for multiple neuropathies with supplemental disease-specific modules could be of great value in the development of disease-modifying treatments for peripheral neuropathies. Muscle Nerve 55: 366-372, 2017. [ABSTRACT FROM AUTHOR]

Published

2017

12. Diabetes, peripheral neuropathy, and old age disability.

Author

Resnick, Helaine E., Stansberry, Kevin B., Harris, Tamar B., Tirivedi, Mahdvi, Smith, Kimberly, Morgan, Polly, Vinik, Aaaron I., Harris, Tamara B, and Vinik, Aaron I

Published

2002

13. Double-blind, placebo-controlled study of HGF gene therapy in diabetic neuropathy.

Author

Kessler, John A., Smith, A. Gordon, Cha, Bong‐Soo, Choi, Sung Hee, Wymer, James, Shaibani, Aziz, Ajroud‐Driss, Senda, and Vinik, Aaron

Subjects

GENE therapy, DIABETIC neuropathies, PLASMIDS, QUALITY of life, PREGABALIN, GABAPENTIN, THERAPEUTICS

Abstract

Objective To evaluate the safety and efficacy of a plasmid ( VM202) containing two human hepatocyte growth factor isoforms given by intramuscular injections in patients with painful diabetic neuropathy. Methods In a double-blind, placebo-controlled study, patients were randomized to receive injections of 8 or 16 mg VM202 per leg or placebo. Divided doses were administered on Day 0 and Day 14. The prospective primary outcome was change in the mean pain score measured by a 7 day pain diary. Secondary outcomes included a responder analysis, quality of life and pain measures, and intraepidermal nerve fiber density. Results There were no significant adverse events attributable to VM202. Eighty-four patients completed the study. Patients receiving 8 mg VM202 per leg improved the most in all efficacy measures including a significant ( P = 0.03) reduction at 3 months in the mean pain score and continued but not statistically significant reductions in pain at 6 and 9 months. Of these patients, 48.4% experienced a ≥50% reduction in pain compared to 17.6% of placebo patients. There were also significant improvements in the brief pain inventory for patients with diabetic peripheral neuropathy and the questionnaire portion of the Michigan Neuropathy Screening Instrument. Patients not on pregabalin or gabapentin had the largest reductions in pain. Interpretation VM202 was safe, well tolerated and effective indicating the feasibility of a nonviral gene therapy approach to painful diabetic neuropathy. Two days of treatment were sufficient to provide symptomatic relief with improvement in quality of life for 3 months. VM202 may be particularly beneficial for patients not taking gabapentin or pregabalin. [ABSTRACT FROM AUTHOR]

Published

2015

14. Immunohistochemical localization of neuron-specific enolase in gastroenteropancreatic neuroendocrine tumors. Correlation with tissue and serum levels of neuron-specific enolase.

Author

Simpson, Shannon, Vinik, Aaron I., Marangos, Paul J., Lloyd, Ricardo V., Simpson, S, Vinik, A I, Marangos, P J, and Lloyd, R V

Published

1984

15. Congenital malignant tumors.

Author

Vinik, Melvin, Altman, Donald H., Vinik, M, and Altman, D H

Published

1966

16. Erectile Dysfunction.

Author

Vinik, Aaron and Richardson, Donald

Abstract

Erectile dysfunction in diabetes is a common complication associated with a decreased quality of life and depression and is a marker of cardiovascular disease and early death. The prevalence of erectile dysfunction increases with advancing age. The pathophysiology is complex, with contributions from neuropathy, vasculopathy and endothelial dysfunction, both vasodilatory and vasoconstrictive. The symptoms are gradual in onset and progress with time. Diagnosis is made by a logical stepwise progression. The use of a questionnaire helps with recording a careful history. Vascular status should be evaluated and there should be a thorough examination of the somatic and autonomous nervous systems. A breakthrough in diagnosis was accomplished with the discovery of pharmacologically inducible erection by intracaversonal injection of a vasoactive compound. Three treatment options are described: no pharmacological treatment but hygienic measures including withdrawal from offending medications perhaps coupled with psychosexual counselling; medical treatment such as with sildenafil; and surgery. [ABSTRACT FROM PUBLISHER]

Published

2001

17. Sensory and Motor Peripheral Nerve Function and Incident Mobility Disability.

Author

Ward, Rachel E., Boudreau, Robert M., Caserotti, Paolo, Harris, Tamara B., Zivkovic, Sasa, Goodpaster, Bret H., Satterfield, Suzanne, Kritchevsky, Stephen B., Schwartz, Ann V., Vinik, Aaron I., Cauley, Jane A., Simonsick, Eleanor M., Newman, Anne B., and Strotmeyer, Elsa S.

Subjects

CONFIDENCE intervals, LONGITUDINAL method, MUSCLE strength, PERIPHERAL nervous system, NEUROLOGICAL disorders, RESEARCH funding, RISK assessment, BODY movement, PROPORTIONAL hazards models, DATA analysis software, DESCRIPTIVE statistics, DISEASE complications, OLD age

Abstract

Objectives To assess the relationship between sensorimotor nerve function and incident mobility disability over 10 years. Design Prospective cohort study with longitudinal analysis. Setting Two U. S. clinical sites. Participants Population-based sample of community-dwelling older adults with no mobility disability at 2000/01 examination (N = 1,680; mean age ± SD 76.5 ± 2.9, body mass index 27.1 ± 4.6; 50.2% female, 36.6% black, 10.7% with diabetes mellitus). Measurements Motor nerve conduction amplitude (poor <1 mV) and velocity (poor <40 m/s) were measured on the deep peroneal nerve. Sensory nerve function was measured using 10- and 1.4-g monofilaments and vibration detection threshold at the toe. Lower extremity symptoms included numbness or tingling and aching or burning pain. Incident mobility disability assessed semiannually over 8.5 years (interquartile range 4.5-9.6 years) was defined as two consecutive self-reports of a lot of difficulty or inability to walk one-quarter of a mile or climb 10 steps. Results Nerve impairments were detected in 55% of participants, and 30% developed mobility disability. Worse motor amplitude ( HR = 1.29 per SD, 95% CI = 1.16-1.44), vibration detection threshold ( HR = 1.13 per SD, 95% CI = 1.04-1.23), symptoms ( HR = 1.65, 95% CI = 1.26-2.17), two motor impairments ( HR = 2.10, 95% CI = 1.43-3.09), two sensory impairments ( HR = 1.91, 95% CI = 1.37-2.68), and three or more nerve impairments ( HR = 2.33, 95% CI = 1.54-3.53) predicted incident mobility disability after adjustment. Quadriceps strength mediated relationships between certain nerve impairments and mobility disability, although most remained significant. Conclusion Poor sensorimotor nerve function independently predicted mobility disability. Future work should investigate modifiable risk factors and interventions such as strength training for preventing disability and improving function in older adults with poor nerve function. [ABSTRACT FROM AUTHOR]

Published

2014

18. Diabetic cardiac autonomic neuropathy, inflammation and cardiovascular disease.

Author

Vinik, Aaron I, Erbas, Tomris, and Casellini, Carolina M

Subjects

*CARDIOVASCULAR diseases, *CYTOKINES, *PEOPLE with diabetes, *SUDDEN death, *NEUROPATHY, *HYPOGLYCEMIA, *DYSAUTONOMIA

Abstract

One of the most overlooked of all serious complications of diabetes is cardiovascular autonomic neuropathy. There is now clear evidence that suggests activation of inflammatory cytokines in diabetic patients and that these correlate with abnormalities in sympathovagal balance. Dysfunction of the autonomic system predicts cardiovascular risk and sudden death in patients with type 2 diabetes. It also occurs in prediabetes, providing opportunities for early intervention. Simple tests that can be carried out at the bedside with real-time output of information - within the scope of the practicing physician - facilitate diagnosis and allow the application of sound strategies for management. The window of opportunity for aggressive control of all the traditional risk factors for cardiovascular events or sudden death with intensification of therapy is with short duration diabetes, the absence of cardiovascular disease and a history of severe hypoglycemic events. To this list we can now add autonomic dysfunction and neuropathy, which have become the most powerful predictors of risk for mortality. It seems prudent that practitioners should be encouraged to become familiar with this information and apply risk stratification in clinical practice. Several agents have become available for the correction of functional defects in the autonomic nervous system, and restoration of autonomic balance is now possible. [ABSTRACT FROM AUTHOR]

Published

2013

19. Relationship Between Vitamin B12 and Sensory and Motor Peripheral Nerve Function in Older Adults.

Author

Leishear, Kira, Boudreau, Robert M., Studenski, Stephanie A., Ferrucci, Luigi, Rosano, Caterina, Rekeneire, Nathalie, Houston, Denise K., Kritchevsky, Stephen B., Schwartz, Ann V., Vinik, Aaron I., Hogervorst, Eva, Yaffe, Kristine, Harris, Tamara B., Newman, Anne B., and Strotmeyer, Elsa S.

Subjects

ANALYSIS of variance, BIOLOGICAL assay, CHI-squared test, CONFIDENCE intervals, STATISTICAL correlation, EPIDEMIOLOGY, FISHER exact test, LONGITUDINAL method, PERIPHERAL nervous system, NEURAL conduction, QUESTIONNAIRES, REGRESSION analysis, RESEARCH funding, STATISTICS, T-test (Statistics), VITAMIN B12, HOMOCYSTEINE, LOGISTIC regression analysis, DATA analysis, CROSS-sectional method, ACYCLIC acids, DATA analysis software, DESCRIPTIVE statistics

Abstract

Objectives To examine whether deficient B12 status or low serum B12 levels are associated with worse sensory and motor peripheral nerve function in older adults. Design Cross-sectional. Setting Health, Aging and Body Composition Study. Participants Two thousand two hundred and eighty-seven adults aged 72 to 83 (mean 76.5 ± 2.9; 51.4% female; 38.3% black). Measurements Low serum B12 was defined as serum B12 less than 260 pmol/ L, and deficient B12 status was defined as B12 less than 260 pmol/ L, methylmalonic acid ( MMA) greater than 271 nmol/ L, and MMA greater than 2-methylcitrate. Peripheral nerve function was assessed according to peroneal nerve conduction amplitude and velocity ( NCV) (motor), 1.4 g/10 g monofilament detection, average vibration threshold detection, and peripheral neuropathy symptoms (numbness, aching or burning pain, or both) (sensory). Results B12-deficient status was found in 7.0% of participants, and an additional 10.1% had low serum B12 levels. B12 deficient status was associated with greater insensitivity to light (1.4 g) touch (odds ratio = 1.50, 95% confidence interval = 1.06-2.13) and worse NCV (42.3 vs 43.5 m/s) (β = −1.16, P = .01) after multivariable adjustment for demographics, lifestyle factors, and health conditions. Associations were consistent for the alternative definition using low serum B12 only. No significant associations were found for deficient B12 status or the alternative low serum B12 definition and vibration detection, nerve conduction amplitude, or peripheral neuropathy symptoms. Conclusion Poor B12 (deficient B12 status and low serum B12) is associated with worse sensory and motor peripheral nerve function. Nerve function impairments may lead to physical function declines and disability in older adults, suggesting that prevention and treatment of low B12 levels may be important to evaluate. [ABSTRACT FROM AUTHOR]

Published

2012

20. Painful diabetic peripheral neuropathy: consensus recommendations on diagnosis, assessment and management.

Author

Tesfaye, S., Vileikyte, L., Rayman, G., Sindrup, S. H., Perkins, B. A., Baconja, M., Vinik, A. I., and Boulton, A. J. M.

Abstract

Painful diabetic peripheral neuropathy (DPN) is common, is associated with significant reduction in quality of life and poses major treatment challenges to the practising physician. Although poor glucose control and cardiovascular risk factors have been proven to contribute to the aetiology of DPN, risk factors specific for painful DPN remain unknown. A number of instruments have been tested to assess the character, intensity and impact of painful DPN on quality of life, activities of daily living and mood. Management of the patient with DPN must be tailored to individual requirements, taking into consideration the co-morbidities and other factors. Pharmacological agents with proven efficacy for painful DPN include tricyclic anti-depressants, the selective serotonin and noradrenaline re-uptake inhibitors, anti-convulsants, opiates, membrane stabilizers, the anti-oxidant alpha-lipoic acid and topical agents including capsaicin. Current first-line therapies for painful DPN include tricyclic anti-depressants, the serotonin and noradrenaline re-uptake inhibitor duloxetine and the anti-convulsants pregabalin and gabapentin. When prescribing any of these agents, other co-morbidities and costs must be taken into account. Second-line approaches include the use of opiates such as synthetic opioid tramadol, morphine and oxycodone-controlled release. There is a limited literature with regard to combination treatment. In extreme cases of painful DPN unresponsive to pharmacotherapy, occasional use of electrical spinal cord stimulation might be indicated. There are a number of unmet needs in the therapeutic management of painful DPN. These include the need for randomized controlled trials with active comparators and data on the long-term efficacy of agents used, as most trials have lasted for less than 6 months. Finally, there is a need for appropriately designed studies to investigate non-pharmacological approaches. Copyright © 2011 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2011

21. Autonomic imbalance: prophet of doom or scope for hope?

Author

Vinik, A. I., Maser, R. E., and Ziegler, D.

Subjects

*HYPERGLYCEMIA treatment, *AUTONOMIC nervous system diseases, *CARDIOVASCULAR diseases risk factors, *CYTOKINES, *DIABETES, *FAT cells, *HEART diseases, *HYPERGLYCEMIA, *INFLAMMATION, *SLEEP apnea syndromes, *LIFESTYLES

Abstract

It has long been recognized that cardiac autonomic neuropathy increases morbidity and mortality in diabetes and may have greater predictive power than traditional risk factors for cardiovascular events. Significant morbidity and mortality can now be attributable to autonomic imbalance between the sympathetic and parasympathetic nervous system regulation of cardiovascular function. New and emerging syndromes include orthostatic tachycardia, orthostatic bradycardia and an inability to use heart rate as a guide to exercise intensity because of the resting tachycardia. Recent studies have shown that autonomic imbalance may be a predictor of risk of sudden death with intensification of glycaemic control. This review examines an association of autonomic dysregulation and the role of inflammatory cytokines and adipocytokines that promote cardiovascular risk. In addition, conditions of autonomic imbalance associated with cardiovascular risk are discussed. Potential treatment for restoration of autonomic balance is outlined. [ABSTRACT FROM AUTHOR]

Published

2011

22. Gastroparesis and functional dyspepsia: excerpts from the AGA/ANMS meeting.

Author

PARKMAN, H. P., CAMILLERI, M., FARRUGIA, G., MCCALLUM, R. W., BHARUCHA, A. E., MAYER, E. A., TACK, J. F., SPILLER, R., HOROWITZ, M., VINIK, A. I., GALLIGAN, J. J., PASRICHA, P. J., KUO, B., SZARKA, L. A., MARCIANI, L., JONES, K., PARRISH, C. R., SANDRONI, P., ABELL, T., and ORDOG, T.

Subjects

INDIGESTION, ETIOLOGY of diseases, PATHOLOGICAL physiology, EPIDEMIOLOGY, GASTROENTEROLOGY, GASTROINTESTINAL diseases

Abstract

Background Despite the relatively high prevelance of gastroparesis and functional dyspepsia, the aetiology and pathophysiology of these disorders remain incompletely understood. Similarly, the diagnostic and treatment options for these two disorders are relatively limited despite recent advances in our understanding of both disorders. Purpose This manuscript reviews the advances in the understanding of the epidemiology, pathophysiology, diagnosis, and treatment of gastroparesis and functional dyspepsia as discussed at a recent conference sponsored by the American Gastroenterological Association (AGA) and the American Neurogastroenterology and Motility Society (ANMS). Particular focus is placed on discussing unmet needs and areas for future research. [ABSTRACT FROM AUTHOR]

Published

2010

23. Sensory and Motor Peripheral Nerve Function and Lower-Extremity Quadriceps Strength: The Health, Aging and Body Composition Study.

Author

Strotmeyer, Elsa S., De Rekeneire, Nathalie, Schwartz, Ann V., Resnick, Helaine E., Goodpaster, Bret H., Faulkner, Kimberly A., Shorr, Ronald I., Vinik, Aaron I., Harris, Tamara B., and Newman, Anne B.

Subjects

PERIPHERAL nervous system, QUADRICEPS muscle, MUSCLE strength, AGING, HUMAN body composition

Abstract

OBJECTIVES: To determine whether sensory and motor nerve function is associated cross-sectionally with quadriceps or ankle dorsiflexion strength in an older community-based population. DESIGN: Cross-sectional analyses within a longitudinal cohort study. SETTING: Two U.S. clinical sites. PARTICIPANTS: Two thousand fifty-nine Health, Aging and Body Composition Study (Health ABC) participants (49.5% male, 36.7% black, aged 73–82) in 2000/01. MEASUREMENTS: Quadriceps and ankle strength were measured using an isokinetic dynamometer. Sensory and motor peripheral nerve function in the legs and feet was assessed using 10-g and 1.4-g monofilaments, vibration threshold, and peroneal motor nerve conduction amplitude and velocity. RESULTS: Monofilament insensitivity, poorest vibration threshold quartile (>60 μ), and poorest motor nerve conduction amplitude quartile (<1.7 mV) were associated with 11%, 7%, and 8% lower quadriceps strength (all P<.01), respectively, than in the best peripheral nerve function categories in adjusted linear regression models. Monofilament insensitivity and lowest amplitude quartile were both associated with 17% lower ankle strength ( P<.01). Multivariate analyses were adjusted for demographic characteristics, diabetes mellitus, body composition, lifestyle factors, and chronic health conditions and included all peripheral nerve measures in the same model. Monofilament insensitivity (β=−7.19), vibration threshold (β=−0.097), and motor nerve conduction amplitude (β=2.01) each contributed independently to lower quadriceps strength (all P<.01). Monofilament insensitivity (β=−5.29) and amplitude (β=1.17) each contributed independently to lower ankle strength (all P<.01). Neither diabetes mellitus status nor lean mass explained the associations between peripheral nerve function and strength. CONCLUSION: Reduced sensory and motor peripheral nerve function is related to poorer lower extremity strength in older adults, suggesting a mechanism for the relationship with lower extremity disability. [ABSTRACT FROM AUTHOR]

Published

2009

24. Transplantation and beyond.

Author

Taylor-Fishwick, David A., Pittenger, Gary L., and Vinik, Aaron I.

Published

2008

25. Clinical features and morphological characterization of 10 patients with noninsulinoma pancreatogenous hypoglycaemia syndrome (NIPHS).

Author

Won, Justin G. S., Hsiao-Shan Tseng, An-Hang Yang, Kam-Tsun Tang, Tjin-Shing Jap, Chen Hsen Lee, Hong-Da Lin, Burcus, Niculina, Pittenger, Gary, and Vinik, Aaron

Subjects

ETIOLOGY of diseases, ISLANDS of Langerhans tumors, PANCREATIC secretions, CALCIUM, ENDOCRINE glands, PANCREAS

Abstract

Objective Noninsulinoma pancreatogenous hypoglycaemia syndrome (NIPHS), characterized by postprandial neuroglycopaenia, negative prolonged fasts and negative perioperative localization studies for insulinoma, but positive selective arterial calcium stimulation tests and nesidioblastosis in the gradient-guided resected pancreas, is a rare hypoglycaemic disorder of undetermined aetiology. We analysed the clinical, morphological and immunohistological features to further clarify the aetiology and pathogenesis of this rare disease. Patients Ten consecutive patients with NIPHS (nine men and one woman, aged 29–78 years) were included in the study. Six of the 10 received a gradient-guided subtotal (70%) or distal (50%) pancreatectomy. In the remaining four patients, diazoxide treatment was initiated and the precise mechanism of its action was assessed by meal tests. Results All of the patients showed a combination of postprandial neuroglycopaenia, negative prolonged fasts (except one patient) and negative localization studies for insulinoma, but positive calcium stimulation tests and nesidioblastosis in the gradient-guided resected pancreas. Immunohistological studies of the resected pancreatic tissues revealed neither an increased rate of proliferation of β-cells nor an abnormal synthesis and/or processing of either proinsulin or amylin. Evidence of overexpression of the two pancreatic differentiation factors, PDX-1 and Nkx-6·1, as well as the calcium sensing receptor (CaSR) was absent. Nevertheless, abnormal expression of islet neogenesis-associated protein (INGAP), a human cytokine expressed only in the presence of islet neogenesis, in ducts and/or islets, was identified in three of the five patients studied. All of the six patients who received a surgical operation were relieved of further neuroglycopaenic attacks, but one patient who received a subtotal pancreatectomy developed diabetes. In the remaining four patients who received diazoxide treatment, hypoglycaemic episodes were satisfactorily controlled with an attenuated response of β-cell peptides to meal stimulation. Conclusions Our results strengthen the existence of this unique clinical hypoglycaemic syndrome from β-cell hyperfunction as well as the value of the selective arterial calcium stimulation test in its correct diagnosis and localization. The mechanisms underlying β-cell hyperfunction and release of insulin to calcium, however, remain poorly characterized. Nevertheless, in a subset of patients with NIPHS, there exists some, as yet undefined, pancreatic humoral/paracrine factor(s) other than proinsulin, amylin, PDX-1, Nkx-6·1 and possibly glucagon-like peptide-1 (GLP-1) that are capable of inducing the INGAP gene and, if activated, will initiate ductal proliferation and islet neogenesis. As for the treatment, we recommend that diazoxide be tried first in each patient and, should it fail, a gradient-guided subtotal or distal pancreatectomy be attempted. [ABSTRACT FROM AUTHOR]

Published

2006

26. Treatment of gastroparesis: a multidisciplinary clinical review.

Author

Abell, T. L., Bernstein, R. K., Cutts, T., Farrugia, G., Forster, J., Hasler, W. L., McCallum, R. W., Olden, K. W., Parkman, H. P., Parrish, C. R., Pasricha, P. J., Prather, C. M., Soffer, C. M., Twillman, R., and Vinik, A. I.

Subjects

GASTROINTESTINAL diseases, THERAPEUTICS, GASTROENTEROLOGISTS, GUIDELINES, CLINICAL trials

Abstract

This clinical review on the treatment of patients with gastroparesis is a consensus document developed by the American Motility Society Task Force on Gastroparesis. It is a multidisciplinary effort with input from gastroenterologists and other specialists who are involved in the care of patients with gastroparesis. To provide practical guidelines for treatment, this document covers results of published research studies in the literature and areas developed by consensus agreement where clinical research trials remain lacking in the field of gastroparesis. [ABSTRACT FROM AUTHOR]

Published

2006

27. Effect of early addition of rosiglitazone to sulphonylurea therapy in older type 2 diabetes patients (>60 years): the Rosiglitazone Early vs. SULphonylurea Titration (RESULT) study.

Author

Rosenstock, J., Goldstein, B. J., Vinik, A. I., O'Neill, M. Colleen, Porter, L. E., Heise, M. A., Kravitz, B., Dirani, R. G., and Freed, M. I.

Subjects

MEDICAL care, THERAPEUTICS, ORAL therapy for diabetes, ORAL drug administration, DIABETES in old age, DISEASES in older people, PEOPLE with diabetes, DIABETES

Abstract

Aim: To compare the efficacy, safety and tolerability of adding rosiglitazone (RSG) vs. sulphonylurea (SU) dose escalation in older type 2 diabetes mellitus (T2DM) patients inadequately controlled on SU therapy. Methods: A total of 227 T2DM patients from 48 centres in the USA and Canada, aged ≥60 years, were randomized to receive RSG (4 mg) or placebo once daily in combination with glipizide 10 mg twice daily for 2 years in a double-blind, parallel-group study. Previous SU monotherapy was ¼ to ½ maximum recommended dose for ≥2 months prior to screening with fasting plasma glucose (FPG) ≥7.0 and ≤13.9 mmol/l. Treatment options were individualized, and escalation of study medication was specifically defined. Results: Disease progression (time to reach confirmed FPG ≥10 mmol/l while on maximum doses of both glipizide and study medication or placebo) was reported in 28.7% of patients uptitrating SU plus placebo compared with only 2.0% taking RSG and SU combination (p < 0.0001). RSG + SU significantly decreased HbA1c, FPG, insulin resistance, plasma free fatty acids and medical care utilization and improved treatment satisfaction compared with uptitrated SU. Conclusions: Addition of RSG to SU in older T2DM patients significantly improved glycaemic control and reduced disease progression compared with uptitrated SU alone but without increasing hypoglycaemia. These benefits were associated with increased patient treatment satisfaction and reduced medical care utilization with regards to emergency room visits and length of hospitalization. Early addition of RSG is an effective treatment option for older T2DM patients inadequately controlled on submaximal SU monotherapy. [ABSTRACT FROM AUTHOR]

Published

2006

28. Metabolic memory in diabetes-focus on insulin.

Author

LeRoith, Derek, Fonseca, Vivian, and Vinik, Aaron

Abstract

Large-scale clinical trials have demonstrated that metabolic control achieved early in the course of diabetes substantially reduces development and progression of diabetes and the associated microvascular complications. Additionally, prospective observational studies have demonstrated that atherogenic and inflammatory mediators are elevated even prior to the onset of diabetes and significantly contribute to subsequent development of macrovascular complications. Collectively, these data suggest that metabolic memories are stored early in the course of diabetes. We believe that insulin suppresses inflammation and also suppresses glucotoxicity and lipotoxicity (and the consequences thereof, such as the formation of advanced glycation end products and epigenetic phenomena), and thus has a pivotal and beneficial role. Comprehensive metabolic control, especially when instituted early, may alter the natural history of diabetic complications by affecting this metabolic memory. Thus, our overall goal is to understand in more detail the molecular mechanisms involved in these changes, thereby affording us opportunities to reduce the long-term effects of diabetes. Copyright © 2005 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2005

29. Cytochemical Quantification of Physiologic Regulation of Oxyntic Cell Carbonic Anhydrasea.

Author

VINIK, A. I. and HELDSINGER, A. A.

Published

1984

30. EFFECT OF BROMOCRIPTINE AND CHLOROTRIANISENE ON TNHIBITION OF LACTATION AND SERUM PROLACTIN A COMPARATIVE DOUBLE-BLIND STUDY.

Author

Utian, W. H., Begg, G., Vinik, A. I., Paul, M., and Shuman, L.

Published

1975

31. Substance P in the localization of a carcinoid tumor.

Author

Strodel, William E., Vinik, Aaron I., Jaffe, Bernard M., Eckhauser, Frederic E., and Thompson, Norman W.

Published

1984

32. Cervical metastases from small bowel carcinoid tumors.

Author

Marks, William H., Strodel, William E., Lloyd, Ricardo V., Eckhauser, Frederic E., Thompson, Norman W., and Vinik, Aaron I.

Published

1983

33. The Neuronal Toxic Factor in Serum of Type 1 Diabetic Patients is a Complement-fixing Autoantibody.

Author

Pittenger, G. L., Liu, D., and Vinik, A. I.

Published

1995

34. FAILURE OF ADRENERGIC α AND β RECEPTOR BLOCKADE TO ELEVATE THE TSH AND PROLACTIN RESPONSE TO TRH IN HYPERTHYROIDISM.

Author

EPSTEIN, S., PIMSTONE, B. L., VINIK, A. I., and McLAREN, H.

Published

1975

35. Plasma gut hormone levels in 37 patients with pheochromocytomas.

Author

Vinik, Aaron, Shapiro, Brahm, and Thompson, Norman

Abstract

Copyright of World Journal of Surgery is the property of Wiley-Blackwell and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

1986

36. MEN I pancreas: A histological and immunohistochemical study.

Author

Thompson, Norman, Lloyd, Ricardo, Nishiyama, Ronald, Vinik, Aaron, Strodel, William, Allo, Maria, Eckhauser, Frederic, Talpos, Gary, and Mervak, Tim

Abstract

Copyright of World Journal of Surgery is the property of Wiley-Blackwell and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

1984

37. MALIGNANT SOMATOSTATINOMA PRESENTING WITH DIABETIC KETOACIDOSIS.

Author

JACKSON, J. A., RAJU, B. U., FACHNIE, J. D., MELLINGER, R. C., JANAKIRAMAN, N., LLOYD, R. V., and VINIK, A. I.

Published

1987

38. Letters to the editor.

Author

Redmond, Janice M. T., McKenna, Malachi J., Vinik, Aaron I., Stansberry, Kevin B., Cohen, Ralph P., Stansberry, Kevin, and Rendell, Mark

Published

1996

39. Quantitative measurement of cutaneous perception in diabetic neuropathy.

Author

Vinik, Aaron I., Suwanwalaikorn, Sompongse, Stansberry, Kevin B., Holland, Marie T., McNitt, Patricia M., and Colen, Lawrence E.

Published

1995

40. PEPTIC ULCER AND GASTRIN IN PIGS.

Author

CASTLES, LINDSAY A., TERBLANCHE, JOHN, HOORN-HICKMAN, ROSEMARY VAN, and VINIK, AARON I.

Published

1978

41. The Toxic Effects of Serum from Patients with Type 1 Diabetes Mellitus on Mouse Neuroblastoma Cells: A New Mechanism for Development of Diabetic Autonomic Neuropathy.

Author

Pittenger, G.L., Liuy, D., and Vinik, A.I.

Published

1993

42. Kinetics of Insulin Secretion in Chronic Pancreatitis and Mild Maturity Onset Diabetes (Evidence for 'Gut Hormone' Action Beyond Glucoreceptor and Cyclic Adenosine Monophosphate Mediated Insulin Release).

Author

Botha, J. L., Vinik, A. I., Blake, K.C.H., and Jackson, W.P.U.

Published

1976

43. Vasoactive Intestinal Peptide Receptors in Human Platelet Membrane. Characterization of Binding and Functional Activity.

Author

ERCAL, N., O'DORISIO, M. S., VINIK, A., O'DORISIO, T. M., and KADROFSKE, M.

Published

1988

44. A 45‐Year‐Old Woman with Rash and Severe Weakness.

Author

Gao, Andrew F., Vinik, Ophir, and Munoz, David G.

Subjects

*LUPUS erythematosus, *INTERSTITIAL lung diseases, *BIOPSY, *INTRAVENOUS immunoglobulins, *IMMUNOHISTOCHEMISTRY

Published

2019

45. Circadian‐timed quick‐release bromocriptine lowers elevated resting heart rate in patients with type 2 diabetes mellitus.

Author

Chamarthi, Bindu, Vinik, Aaron, Ezrokhi, Michael, and Cincotta, Anthony H.

Subjects

SYMPATHETIC nervous system, CARDIOVASCULAR diseases, BLOOD pressure

Abstract

Objective: Sympathetic nervous system (SNS) overactivity is a risk factor for insulin resistance and cardiovascular disease (CVD). We evaluated the impact of bromocriptine‐QR, a dopamine‐agonist antidiabetes medication, on elevated resting heart rate (RHR) (a marker of SNS overactivity in metabolic syndrome), blood pressure (BP) and the relationship between bromocriptine‐QR's effects on RHR and HbA1c in type 2 diabetes subjects. Design and Subjects: RHR and BP changes were evaluated in this post hoc analysis of data from a randomized controlled trial in 1014 type 2 diabetes subjects randomized to bromocriptine‐QR vs placebo added to standard therapy (diet ± ≤2 oral antidiabetes medications) for 24 weeks without concomitant antihypertensive or antidiabetes medication changes, stratified by baseline RHR (bRHR). Results: In subjects with bRHR ≥70 beats/min, bromocriptine‐QR vs placebo reduced RHR by −3.4 beats/min and reduced BP (baseline 130/79; systolic, diastolic, mean arterial BP reductions [mm Hg]: −3.6 [P =.02], −1.9 [P =.05], −2.5 [P =.02]). RHR reductions increased with higher baseline HbA1c (bHbA1c) (−2.7 [P =.03], −5 [P =.002], −6.1 [P =.002] with bHbA1c ≤7, >7, ≥7.5%, respectively] in the bRHR ≥70 group and more so with bRHR ≥80 (−4.5 [P =.07], −7.8 [P =.015], −9.9 [P =.005]). Subjects with bRHR <70 had no significant change in RHR or BP. With bHbA1c ≥7.5%, %HbA1c reductions with bromocriptine‐QR vs placebo were −0.50 (P =.04), −0.73 (P =.005) and −1.22 (P =.008) with bRHR <70, ≥70 and ≥80, respectively. With bRHR ≥70, the magnitude of bromocriptine‐QR‐induced RHR reduction was an independent predictor of bromocriptine‐QR's HbA1c lowering effect. Conclusion: Bromocriptine‐QR lowers elevated RHR with concurrent decrease in BP and hyperglycaemia. These findings suggest a potential sympatholytic mechanism contributing to bromocriptine‐QR's antidiabetes effect and potentially its previously demonstrated effect to reduce CVD events. [ABSTRACT FROM AUTHOR]

Published

2020

46. G CELLS AND GASTRIN RELEASE FROM HUMAN ANTRAL MUCOSA IN VITRO.

Author

Askew, A. R., Grant, B. J., and Vinik, A. I.

Published

1980

47. Corrigendum: Structure‐Based Design of a Monosaccharide Ligand Targeting Galectin‐8.

Author

Bohari, Mohammad H., Yu, Xing, Kishor, Chandan, Patel, Brijesh, Go, Rob Marc, Eslampanah Seyedi, Hadieh A., Vinik, Yaron, Grice, I. Darren, Zick, Yehiel, and Blanchard, Helen

Published

2018

48. Poster 346 Measuring Symptoms and Small Fiber Function Objectively in CIPD: A Case Report.

Author

Nevoret, Marie‐Laure and Vinik, Aaron I.

Published

2014

49. Response Letter to Lawrence Solomon.

Author

Leishear, Kira, Studenski, Stephanie A., Ferrucci, Luigi, Rekeneire, Nathalie, Kritchevsky, Stephen B., Vinik, Aaron I., Hogervorst, Eva, Harris, Tamara B., Newman, Anne B., and Strotmeyer, Elsa S.

Subjects

VITAMIN B12 deficiency, PERIPHERAL nervous system, METFORMIN, OLD age, VITAMIN deficiency

Abstract

Kira Leishear et al. respond to a letter to the editor submitted in response to their article "Relationship Between Vitamin B12 and Sensory and Motor Peripheral Nerve Function in Older Adults".

Published

2013

50. Role of prostaglandin D2 and the autonomic nervous system in niacin-induced flushing (前列腺素D2与自主神经系统在烟酸引起的脸红中的作用)

Author

PARSON, Henri K., HARATI, Hadi, COOPER, Deona, and VINIK, Aaron I.

Subjects

PROSTAGLANDINS, BLUSHING, AUTONOMIC nervous system, NIACIN, ASPIRIN, PARASYMPATHETIC nervous system

Abstract

Copyright of Journal of Diabetes is the property of Wiley-Blackwell and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2013