PPAR‐gamma agonist pioglitazone modifies craving intensity and brain white matter integrity in patients with primary cocaine use disorder: a double‐blind randomized controlled pilot trial

Schmitz, Joy M.; Green, Charles E.; Hasan, Khader M.; Vincent, Jessica; Suchting, Robert; Weaver, Michael F.; Moeller, F. Gerard; Narayana, Ponnada A.; Cunningham, Kathryn A.; Dineley, Kelly T.; Lane, Scott D.

doi:10.1111/add.13868

Cited by 64 publications

(47 citation statements)

References 52 publications

(51 reference statements)

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“…In contrast, antioxidants level is increased. Net effect of mentioned changes leads to amelioration of neuroinflammation [62]. Furthermore, by activating of peroxisome proliferator activator receptor-g it regulates lipid and glucose metabolism [52,53,63].…”

Section: Discussionmentioning

confidence: 99%

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2018

IJDMD

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Diabetes mellitus (DM) is the most common cause of diabetic neuropathy (DN) comprises a heterogeneous group of disorders that can cause neuronal dysfunction throughout the human body. The incidence of diabetes and its complications is increasing to staggering proportions. In 2014 the WHO estimated an overall prevalence of 422 million (8, 5%). The incidence of diabetic neuropathy approaches 50% in most diabetic populations; there is no treatment, and its consequences in the form of foot ulceration and amputation.The recent studies suggest that the renin angiotensin aldosterone system (RAAS) plays a vital role in regulating glucose metabolism and blood pressure. In the same time the metabolic abnormalities associated with diabetes lead to activation RAAS, which might promote the formation of reactive oxygen species to lead the endothelial and neuronal dysfunctions. Furthermore, TNFα is part of the response of the organism to hypertension and is originally described as one of the central mediators of inflammation trough the activation of transcription factor NFκB an important factor in the control of cell proliferation, differentiation, and apoptosis. Methodology & Theoretical Orientation:The study is going on in parallel groups. The patients (enrolled on randomized principle) with DPN will be investigated. The enrolled subjects was divided into two main groups: group I with Type I and Type II DM, complicated by DPN to take Aliskiren and group II with the same pathology, proceeding with the treatment without Aliskiren but given Telmisartan, for certainty of Aliskiren efficacy. At the start of the trial and on completion of the six week period TNFα level and C-peptide will be determined.Findings: Telmisartan has less TNFα modulatory effects then Aliskiren, Namely, the symptoms of neuropathy a well as blood TNFα level and C-peptide level are not changed significantly. Conclusion & Significance: TNFα is involved in DPN pathogenesis formation and clinical manifestation. Aliskiren ameliorates symptoms in DPN patients by modulatory impact on TNFα, so we have results for clinical and pharmacological analysis of Aliskiren application in DPN. The involvements of RAAS system in developments of DNP needs further research study.Volume 3 | Issue 2 | 1 of 9 Int J Diabetes Metab Disord, 2018As it is discussed a number of different therapeutic approaches that target the various pathogenetic mechanisms of diabetic neuropathy have been the subject of clinical trials [44].

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Section: Discussionmentioning

confidence: 99%

Untitled

2018

IJDMD

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“…Participants for this project were recruited from the Greater Houston Metropolitan Area using local newspaper and radio advertisements. The data reported here constitute part of a larger clinical trial examining the effects 12-weeks of treatment with pioglitazone in participants with a primary cocaine use disorder (CUD) and a secondary alcohol use disorder (AUD), described in [31] (NCT02774343). For the present report, data were obtained from measures taken at baseline (Day 0), prior to initiation of the clinical trial, and included 22 CUD/AUD subjects who provided complete neuroimaging, eye tracking, and telomere data; two additional CUD/AUD subjects provided eye tracking and telomere data without DTI.…”

Section: Methodsmentioning

confidence: 99%

Measures of Possible Allostatic Load in Comorbid Cocaine and Alcohol Use Disorder: Brain White Matter Integrity, Telomere Length, and Anti-Saccade Performance

Lane

Tannous

Mwangi

et al. 2018

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34 Chronic cocaine and alcohol use impart significant stress on biological and cognitive systems, 35 resulting in changes consistent with an allostatic load model of neurocognitive impairment.36 The present study measured potential markers of allostatic load in individuals with comorbid 37 cocaine/alcohol use disorders (CUD/AUD) and control subjects. Measures of brain white 38 matter (WM) integrity, telomere length, and impulsivity/attentional bias were obtained. WM 39 integrity (CUD/AUD only) was indexed by diffusion tensor imaging metrics, including radial 40 diffusivity (RD) and fractional anisotropy (FA). Telomere length was indexed by T/S ratio.41 Impulsivity and attentional bias to drug cues were measured via eye-tracking, and were also 42 modeled using the Hierarchical Diffusion Drift Model (HDDM). Average whole-brain RD and 43 FA were associated with years of cocaine use (R 2 = 0.56 and 0.51, both p < .005) but not years 44 of alcohol use. CUD/AUD subjects showed more anti-saccade errors (p < .01), greater 45 attentional bias scores (p < .001), and higher HDDM drift rates on cocaine-cue trials 46 (Bayesian probability CUD/AUD > control = p > 0.99). Telomere length was shorter in 47 CUD/AUD, but the difference was not statistically significant. Within the CUD/AUD group, 48 exploratory regression using an elastic-net model determined that more years of cocaine use, , 49 older age, larger HDDM drift rate differences and shorter telomere length were all predictive 50 of white matter integrity as measured by RD (model R 2 = 0.79). Collectively, the results 51 provide modest support linking CUD/AUD to putative markers of allostatic load. 52 Cocaine and Allostasis -3 53 54 Introduction 55Allostasis implies a shift in homeostatic systems in response to acute or chronic 56 stressors (e.g., allostatic load), described by McEwen as "the price the body pays for being 57 forced to adapt to adverse psychosocial or physical situations" [1]. Exposure to extreme or 58 pervasive stressors can result in pathophysiological change. Examination of allostatic load has 59 commonly focused on changes in the regulation of stress hormones and the sequelae of such 60 changes [2,3], but the concept can apply broadly to effects on many homeostatic systems.61 Nearly two decades ago, Koob and colleagues proposed allostatic models of chronic cocaine 62 and alcohol intake based on preclinical work [4-6], but only modest attention has focused on 63 the allostasic framework in studying human substance use disorders (SUD). Here, we focus on 64 the effects of chronic SUD in adults with co-morbid cocaine and alcohol use disorders [7][8][9]. 65Cocaine use disorder (CUD) with co-occurring abuse of other substances, e.g., 66 marijuana and alcohol use disorder (AUD), is the norm rather than the exception [10].67 Individuals who use only cocaine are of putative scientific importance with regard to isolating 68 individual drug effects. However, such investigations are more precisely understood using 69 preclinical models that can isolate dose-respon...

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“…These findings go along with evidence indicating that the loss of hippocampal GABAergic inter-neurons is closely associated with the appearance of enhanced signs of tau-pathology(Levenga et al 2013). These processes may accelerate an ongoing pattern of hippocampal hyperactivity, micro/ macro-structural damage, atrophy, and the progression of cognitive and behavioral disorders(Gilani et al 2014; Jones et al 2016;Schmitz et al 2017;Schobel et al 2013).…”

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confidence: 99%

Functional signature of conversion in Mild Cognitive Impairment patients

Pizzi

Punzi

Sensi

2018

Preprint

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The entorhinal-hippocampal circuit is a strategic hub for memory but also the first site to be affected in the Alzheimer's Disease (AD)-related pathology. We investigated MRI patterns of brain atrophy and functional connectivity in a study cohort obtained from the Alzheimer's Disease Neuroimaging Initiative database including healthy control (HC), Mild Cognitive Impairment (MCI), and AD subjects. MCI individuals were clinically evaluated 24 months after the MRI scan, and the group further divided into a subset of subjects who either did (c-MCI) or did not (nc-MCI) convert to AD.Compared to HC subjects, AD patients exhibited a collapse of long-range connectivity from the hippocampus and entorhinal cortex, pronounced cortical/sub-cortical atrophy, and a dramatic decline in cognitive performances. c-MCI patients showed entorhinal and hippocampal hypo-connectivity, no signs of cortical thinning but evidence of right hippocampus atrophy. On the contrary, nc-MCI patients showed lack of brain atrophy, largely preserved cognitive functions, hippocampal and entorhinal hyperconnectivity with selected neocortical/sub-cortical regions mainly involved in memory processing and brain meta-stability. This hyper-connectivity can represent an early compensatory strategy to overcome the progression of cognitive impairment. This functional signature can also be employed for the diagnosis of c-MCI subjects.

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PPAR‐gamma agonist pioglitazone modifies craving intensity and brain white matter integrity in patients with primary cocaine use disorder: a double‐blind randomized controlled pilot trial

Cited by 64 publications

References 52 publications

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Measures of Possible Allostatic Load in Comorbid Cocaine and Alcohol Use Disorder: Brain White Matter Integrity, Telomere Length, and Anti-Saccade Performance

Functional signature of conversion in Mild Cognitive Impairment patients

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