Your search keyword '"Imbimbo, Bruno P."' showing total 90 results

1. Increases in amyloid-β42 slow cognitive and clinical decline in Alzheimer's disease trials.

Author

Abanto, Jesus, Dwivedi, Alok K, Imbimbo, Bruno P, and Espay, Alberto J

Subjects

ALZHEIMER'S disease, BIOMARKERS, MONOCLONAL antibodies, COGNITION disorders, AMYLOID

Abstract

Positive effects of new anti-amyloid-β (Aβ) monoclonal antibodies in Alzheimer's disease (AD) have been attributed to brain amyloid reduction. However, most anti-Aβ antibodies also increase the CSF levels of the 42-amino acid isoform (Aβ42). We evaluated the associations of changes in CSF Aβ42 and brain Aβ-PET with cognitive and clinical end points in randomized trials of anti-Aβ drugs that lowered (β- and γ-secretase inhibitors) or increased CSF Aβ42 levels (anti-Aβ monoclonal antibodies) to test the hypothesis that post-treatment increases in CSF Aβ42 levels are independently associated with cognitive and clinical outcomes. From long-term (≥12 months) randomized placebo-controlled clinical trials of anti-Aβ drugs published until November 2023, we calculated the post-treatment versus baseline difference in ADAS-Cog (cognitive subscale of the Alzheimer's Disease Assessment Scale) and CDR-SB (Clinical Dementia Rate-Sum of Boxes) and z -standardized changes in CSF Aβ42 and Aβ-PET Centiloids (CL). We estimated the effect size [regression coefficients (RCs) and confidence intervals (CIs)] and the heterogeneity (I2) of the associations between AD biomarkers and cognitive and clinical end points using random-effects meta-regression models. We included 25 966 subjects with AD from 24 trials. In random-effects analysis, increases in CSF Aβ42 were associated with slower decline in ADAS-Cog (RC: −0.55; 95% CI: −0.89, −0.21, P = 0.003, I2 = 61.4%) and CDR-SB (RC: −0.16; 95% CI: −0.26, −0.06, P = 0.002, I2 = 34.5%). Similarly, decreases in Aβ–PET were associated with slower decline in ADAS-Cog (RC: 0.69; 95% CI: 0.48, 0.89, P < 0.001, I2 = 0%) and CDR-SB (RC: 0.26; 95% CI: 0.18, 0.33, P < 0.001, I2 = 0%). Sensitivity analyses yielded similar results. Higher CSF Aβ42 levels after exposure to anti-Aβ drugs are independently associated with slowing cognitive impairment and clinical decline. Increases in Aβ42 may represent a mechanism of potential benefit of anti-Aβ monoclonal antibodies in AD. [ABSTRACT FROM AUTHOR]

Published

2024

2. Tracking neuroinflammatory biomarkers in Alzheimer's disease: a strategy for individualized therapeutic approaches?

Author

Lista, Simone, Imbimbo, Bruno P., Grasso, Margherita, Fidilio, Annamaria, Emanuele, Enzo, Minoretti, Piercarlo, López-Ortiz, Susana, Martín-Hernández, Juan, Gabelle, Audrey, Caruso, Giuseppe, Malaguti, Marco, Melchiorri, Daniela, Santos-Lozano, Alejandro, Imbimbo, Camillo, Heneka, Michael T., and Caraci, Filippo

Abstract

Background: Recent trials of anti-amyloid-β (Aβ) monoclonal antibodies, including lecanemab and donanemab, in early Alzheimer disease (AD) showed that these drugs have limited clinical benefits and their use comes with a significant risk of serious adverse events. Thus, it seems crucial to explore complementary therapeutic approaches. Genome-wide association studies identified robust associations between AD and several AD risk genes related to immune response, including but not restricted to CD33 and TREM2. Here, we critically reviewed the current knowledge on candidate neuroinflammatory biomarkers and their role in characterizing the pathophysiology of AD. Main body: Neuroinflammation is recognized to be a crucial and contributing component of AD pathogenesis. The fact that neuroinflammation is most likely present from earliest pre-stages of AD and co-occurs with the deposition of Aβ reinforces the need to precisely define the sequence and nature of neuroinflammatory events. Numerous clinical trials involving anti-inflammatory drugs previously yielded unfavorable outcomes in early and mild-to-moderate AD. Although the reasons behind these failures remain unclear, these may include the time and the target selected for intervention. Indeed, in our review, we observed a stage-dependent neuroinflammatory process in the AD brain. While the initial activation of glial cells counteracts early brain Aβ deposition, the downregulation in the functional state of microglia occurs at more advanced disease stages. To address this issue, personalized neuroinflammatory modulation therapy is required. The emergence of reliable blood-based neuroinflammatory biomarkers, particularly glial fibrillary acidic protein, a marker of reactive astrocytes, may facilitate the classification of AD patients based on the ATI(N) biomarker framework. This expands upon the traditional classification of Aβ ("A"), tau ("T"), and neurodegeneration ("N"), by incorporating a novel inflammatory component ("I"). Conclusions: The present review outlines the current knowledge on potential neuroinflammatory biomarkers and, importantly, emphasizes the role of longitudinal analyses, which are needed to accurately monitor the dynamics of cerebral inflammation. Such a precise information on time and place will be required before anti-inflammatory therapeutic interventions can be considered for clinical evaluation. We propose that an effective anti-neuroinflammatory therapy should specifically target microglia and astrocytes, while considering the individual ATI(N) status of patients. [ABSTRACT FROM AUTHOR]

Published

2024

3. Recalibrating the Risk-Benefit Profiles of Lecanemab and Donanemab: Scales, Immunoreactivity, and Changes in Amyloid-β42.

Author

Espay, Alberto J., Herrup, Karl, Imbimbo, Bruno P., Kepp, Kasper P., and Daly, Timothy

Subjects

LECANEMAB, ALZHEIMER'S disease, CEREBROSPINAL fluid, COGNITION, REPORTING of diseases

Abstract

Three recent anti-amyloid-β antibody trials for Alzheimer's disease reported similar effect sizes, used non-reactive saline as placebo, and showed large numbers of adverse events including imaging anomalies (ARIA) that correlate with cognitive changes. Conversely, all previous antibody trials were less reactive and pronounced ineffective. We argue that these observations point to unblinding bias, inflating apparent efficacy and thus altering the risk-benefit balance. Further, we highlight data demonstrating that beyond reducing amyloid, monoclonal antibodies increase monomeric amyloid-β42 in cerebrospinal fluid, which may explain potential benefits. We should recalibrate the efficacy of these antibodies and devote more resources into strategies beyond removing amyloid. [ABSTRACT FROM AUTHOR]

Published

2024

4. Are lecanemab and donanemab disease‐modifying therapies?

Author

Daly, Timothy, Kepp, Kasper P., and Imbimbo, Bruno P.

Published

2024

5. Are we close to using Alzheimer blood biomarkers in clinical practice.

Author

Imbimbo, Bruno P., Lista, Simone, Imbimbo, Camillo, and Nisticò, Robert

Published

2024

6. Plasma ATN(I) classification and precision pharmacology in Alzheimer's disease.

Author

Imbimbo, Bruno P., Watling, Mark, Imbimbo, Camillo, and Nisticò, Robert

Published

2023

7. Investigational treatments for neurodegenerative diseases caused by inheritance of gene mutations: lessons from recent clinical trials.

Author

Imbimbo, Bruno P., Triaca, Viviana, Imbimbo, Camillo, and Nisticò, Robert

Published

2023

8. Plasma Amyloid-β dynamics in late-life major depression: a longitudinal study.

Author

Pomara, Nunzio, Bruno, Davide, Plaska, Chelsea Reichert, Ramos-Cejudo, Jaime, Osorio, Ricardo S., Pillai, Anilkumar, Imbimbo, Bruno P., Zetterberg, Henrik, and Blennow, Kaj

Published

2022

9. A critical appraisal of tau‐targeting therapies for primary and secondary tauopathies.

Author

Imbimbo, Bruno P., Ippati, Stefania, Watling, Mark, and Balducci, Claudia

Published

2022

10. Sex‐ or depression‐specific relationships with CSF sAPPα, sAPPβ and their associations with CSF sTREM2 in older adults.

Author

Nunzio, Pomara, Plaska, Chelsea Reichert, Bruno, Davide, Ramos‐Cejudo, Jaime, Osorio, Ricardo S, Heslegrave, Amanda, Pillai, Anilkumar, Imbimbo, Bruno P, Zetterberg, Henrik, and Blennow, Kaj

Published

2023

11. A Path Toward Precision Medicine for Neuroinflammatory Mechanisms in Alzheimer's Disease.

Author

Hampel, Harald, Caraci, Filippo, Cuello, A. Claudio, Caruso, Giuseppe, Nisticò, Robert, Corbo, Massimo, Baldacci, Filippo, Toschi, Nicola, Garaci, Francesco, Chiesa, Patrizia A., Verdooner, Steven R., Akman-Anderson, Leyla, Hernández, Félix, Ávila, Jesús, Emanuele, Enzo, Valenzuela, Pedro L., Lucía, Alejandro, Watling, Mark, Imbimbo, Bruno P., and Vergallo, Andrea

Subjects

ALZHEIMER'S disease, INDIVIDUALIZED medicine, NEUROGLIA, INFLAMMATION, APOLIPOPROTEIN E4, SYSTEMS biology, CHRONIC traumatic encephalopathy, FRACTALKINE, NEURAL transmission

Abstract

Neuroinflammation commences decades before Alzheimer's disease (AD) clinical onset and represents one of the earliest pathomechanistic alterations throughout the AD continuum. Large-scale genome-wide association studies point out several genetic variants— TREM2, CD33, PILRA, CR1, MS4A, CLU, ABCA7, EPHA1 , and HLA-DRB5-HLA-DRB1 —potentially linked to neuroinflammation. Most of these genes are involved in proinflammatory intracellular signaling, cytokines/interleukins/cell turnover, synaptic activity, lipid metabolism, and vesicle trafficking. Proteomic studies indicate that a plethora of interconnected aberrant molecular pathways, set off and perpetuated by TNF-α, TGF-β, IL-1β, and the receptor protein TREM2, are involved in neuroinflammation. Microglia and astrocytes are key cellular drivers and regulators of neuroinflammation. Under physiological conditions, they are important for neurotransmission and synaptic homeostasis. In AD, there is a turning point throughout its pathophysiological evolution where glial cells sustain an overexpressed inflammatory response that synergizes with amyloid-β and tau accumulation, and drives synaptotoxicity and neurodegeneration in a self-reinforcing manner. Despite a strong therapeutic rationale, previous clinical trials investigating compounds with anti-inflammatory properties, including non-steroidal anti-inflammatory drugs (NSAIDs), did not achieve primary efficacy endpoints. It is conceivable that study design issues, including the lack of diagnostic accuracy and biomarkers for target population identification and proof of mechanism, may partially explain the negative outcomes. However, a recent meta-analysis indicates a potential biological effect of NSAIDs. In this regard, candidate fluid biomarkers of neuroinflammation are under analytical/clinical validation, i.e., TREM2, IL-1β, MCP-1, IL-6, TNF-α receptor complexes, TGF-β, and YKL-40. PET radio-ligands are investigated to accomplish in vivo and longitudinal regional exploration of neuroinflammation. Biomarkers tracking different molecular pathways (body fluid matrixes) along with brain neuroinflammatory endophenotypes (neuroimaging markers), can untangle temporal–spatial dynamics between neuroinflammation and other AD pathophysiological mechanisms. Robust biomarker–drug codevelopment pipelines are expected to enrich large-scale clinical trials testing new-generation compounds active, directly or indirectly, on neuroinflammatory targets and displaying putative disease-modifying effects: novel NSAIDs, AL002 (anti-TREM2 antibody), anti-Aβ protofibrils (BAN2401), and AL003 (anti-CD33 antibody). As a next step, taking advantage of breakthrough and multimodal techniques coupled with a systems biology approach is the path to pursue for developing individualized therapeutic strategies targeting neuroinflammation under the framework of precision medicine. [ABSTRACT FROM AUTHOR]

Published

2020

12. Time to test antibacterial therapy in Alzheimer's disease.

Author

Panza, Francesco, Lozupone, Madia, Solfrizzi, Vincenzo, Watling, Mark, and Imbimbo, Bruno P

Subjects

ALZHEIMER'S disease, HUMAN herpesvirus 1, ALZHEIMER'S patients, CEREBRAL amyloid angiopathy

Abstract

Alzheimer's disease is associated with cerebral accumulation of amyloid-β peptide and hyperphosphorylated tau. In the past 28 years, huge efforts have been made in attempting to treat the disease by reducing brain accumulation of amyloid-β in patients with Alzheimer's disease, with no success. While anti-amyloid-β therapies continue to be tested in prodromal patients with Alzheimer's disease and in subjects at risk of developing Alzheimer's disease, there is an urgent need to provide therapeutic support to patients with established Alzheimer's disease for whom current symptomatic treatment (acetylcholinesterase inhibitors and N-methyl d-aspartate antagonist) provide limited help. The possibility of an infectious aetiology for Alzheimer's disease has been repeatedly postulated over the past three decades. Infiltration of the brain by pathogens may act as a trigger or co-factor for Alzheimer's disease, with Herpes simplex virus type 1, Chlamydia pneumoniae, and Porphyromonas gingivalis being most frequently implicated. These pathogens may directly cross a weakened blood-brain barrier, reach the CNS and cause neurological damage by eliciting neuroinflammation. Alternatively, pathogens may cross a weakened intestinal barrier, reach vascular circulation and then cross blood-brain barrier or cause low grade chronic inflammation and subsequent neuroinflammation from the periphery. The gut microbiota comprises a complex community of microorganisms. Increased permeability of the gut and blood-brain barrier induced by microbiota dysbiosis may impact Alzheimer's disease pathogenesis. Inflammatory microorganisms in gut microbiota are associated with peripheral inflammation and brain amyloid-β deposition in subjects with cognitive impairment. Oral microbiota may also influence Alzheimer's disease risk through circulatory or neural access to the brain. At least two possibilities can be envisaged to explain the association of suspected pathogens and Alzheimer's disease. One is that patients with Alzheimer's disease are particularly prone to microbial infections. The other is that microbial infection is a contributing cause of Alzheimer's disease. Therapeutic trials with antivirals and/or antibacterials could resolve this dilemma. Indeed, antiviral agents are being tested in patients with Alzheimer's disease in double-blind placebo-controlled studies. Although combined antibiotic therapy was found to be effective in animal models of Alzheimer's disease, antibacterial drugs are not being widely investigated in patients with Alzheimer's disease. This is because it is not clear which bacterial populations in the gut of patients with Alzheimer's disease are overexpressed and if safe, selective antibacterials are available for them. On the other hand, a bacterial protease inhibitor targeting P. gingivalis toxins is now being tested in patients with Alzheimer's disease. Clinical studies are needed to test if countering bacterial infection may be beneficial in patients with established Alzheimer's disease. [ABSTRACT FROM AUTHOR]

Published

2019

13. Disease-modifying therapies for tauopathies: agents in the pipeline.

Author

Panza, Francesco, Imbimbo, Bruno P., Lozupone, Madia, Greco, Antonio, Seripa, Davide, Logroscino, Giancarlo, Daniele, Antonio, and Colosimo, Carlo

Abstract

Introduction: Tauopathies are heterogeneous clinicopathological entities characterized by abnormal neuronal and/or glial inclusions of the microtubule-binding protein tau. Primary tauopathies considered to be diseases correspond to a major class of frontotemporal lobar degeneration (FTLD) neuropathology (FTLD-Tau), including several forms of frontotemporal dementia (FTD) clinical syndromes. Little progress has been made in the past 20 years in developing effective disease-modifying drugs for primary tauopathies and available symptomatic treatments have limited efficacy. Areas covered: Potential disease-modifying drugs in clinical development to slow neuropathological progression of primary tauopathies. Expert opinion: Since the underlying pathology of primary tauopathies consists of abnormal tau protein aggregates, treatments are being developed to interfere with the aggregation process or to promote the clearance of this protein. Unfortunately, disease-modifying treatments remain years away as demonstrated by the recent negative Phase III findings of a tau aggregation inhibitor (LMTM) for treating the behavioral variant of FTD. Further evidence will come from ongoing Phase I/II trials on novel drugs and immunotherapeutics with various targets – prevention of deposition or removal of tau aggregates, inhibition of tau phosphorylation/acetylation, modulation of O-GlcNAcylation, activation of autophagy or ubiquitin-proteasome system pathways, and rescue of selected tau loss of function or suppression of tau gene expression. [ABSTRACT FROM AUTHOR]

Published

2019

14. Amyloid-β immunotherapy for alzheimer disease: Is it now a long shot?

Author

Panza, Francesco, Lozupone, Madia, Seripa, Davide, and Imbimbo, Bruno P.

Subjects

ALZHEIMER'S disease, MONOCLONAL antibodies, IMMUNOTHERAPY, PHYSIOLOGY, AMYLOID beta-protein, THERAPEUTIC use of monoclonal antibodies, BRAIN metabolism, BRAIN, DRUG therapy, PEPTIDES

Abstract

The amyloid-β (Aβ) cascade hypothesis of Alzheimer disease (AD) holds that brain accumulation of Aβ initiates the disease process. Accordingly, drug research has targeted Aβ production, clearance, and deposition as therapeutic strategies. Unfortunately, candidate drugs have failed to show clinical benefit in established, early, or prodromal disease, or in those with high AD risk. Currently, monoclonal antibodies specifically directed against the most neurotoxic Aβ forms are undergoing large-scale trials to confirm initially encouraging results. However, recent findings on the normal physiology of Aβ suggest that accumulation may be compensatory rather than the pathological initiator. If this is true, alternative strategies will be needed to defeat this devastating disease. ANN NEUROL 2019;85:303-315. [ABSTRACT FROM AUTHOR]

Published

2019

15. Are antibodies directed against amyloid-β (Aβ) oligomers the last call for the Aβ hypothesis of Alzheimer's disease?

Author

Panza, Francesco, Lozupone, Madia, Dibello, Vittorio, Greco, Antonio, Daniele, Antonio, Seripa, Davide, Logroscino, Giancarlo, and Imbimbo, Bruno P

Published

2019

16. Initial failures of anti-tau antibodies in Alzheimer's disease are reminiscent of the amyloid-β story.

Author

Imbimbo, Bruno P., Balducci, Claudia, Ippati, Stefania, and Watling, Mark

Published

2023

17. BACE inhibitors in clinical development for the treatment of Alzheimer’s disease.

Author

Panza, Francesco, Lozupone, Madia, Solfrizzi, Vincenzo, Sardone, Rodolfo, Piccininni, Carla, Dibello, Vittorio, Stallone, Roberta, Giannelli, Gianluigi, Bellomo, Antonello, Greco, Antonio, Daniele, Antonio, Seripa, Davide, Logroscino, Giancarlo, and Imbimbo, Bruno P.

Abstract

Introduction: The amyloid hypothesis of Alzheimer’s disease (AD) affirms that brain accumulation of amyloid-β (Aβ) oligomers and soluble aggregates represent the major pathological event of the disease. Several anti-Aβ small organic molecules, monoclonal antibodies and antigens were developed to interfere with Aβ production and clearance, including β-site amyloid precursor protein cleaving enzyme (BACE) inhibitors, blocking the first enzymatic step of Aβ formation. All these approaches, including BACE inhibitors, have failed in large randomized clinical trials (RCTs) in mild-to-moderate AD, but further studies are now being carried out in patients at early AD stages and in asymptomatic subjects at risk of developing AD. Areas covered: The paper provides a comprehensive review of BACE inhibitors for AD treatment, focusing on the most advanced compounds in Phase III RCTs. Expert commentary: BACE inhibitors inhibited robustly, and dose-dependently, Aβ formation in cerebrospinal fluid of AD patients, but without cognitive, clinical, or functional benefit in large RCTs. BACE inhibition may be not sufficient to decrease brain Aβ plaques and aggregates. Indeed, several BACE inhibitors were found to be poorly tolerated and some of them failed also in patients with prodromal AD. This may indicate that blocking the formation of nascent Aβ is not useful in AD. [ABSTRACT FROM AUTHOR]

Published

2018

18. Social Dysfunction in Older Age and Relationships with Cognition, Depression, and Apathy: The GreatAGE Study.

Author

Lozupone, Madia, Panza, Francesco, Piccininni, Marco, Copetti, Massimiliano, Sardone, Rodolfo, Imbimbo, Bruno P., Stella, Eleonora, D’Urso, Francesca, Barulli, Maria Rosaria, Battista, Petronilla, Grasso, Alessandra, Tortelli, Rosanna, Capozzo, Rosa, Coppola, Francesco, Abbrescia, Daniela Isabel, Bellomo, Antonello, Giannelli, Gianluigi, Quaranta, Nicola, Seripa, Davide, and Logroscino, Giancarlo

Subjects

COGNITIVE ability, COGNITION in old age, MENTAL depression, APATHY, SOCIAL isolation

Abstract

Background: Most studies focused on only one measure of social dysfunction in older age, without proper validation and distinction across different dimensions including subjectivity, structural, and functional aspects.Objective: We sought to validate the Social Dysfunction Rating Scale (SDRS) and its factorial structure, also determining the association of SDRS with cognitive functions, global psychopathology, and social deprivation.Methods: The SDRS was administered to 484 Italian community-dwelling elderly, recruited in the GreatAGE study, a population-based study on aging conducted in Castellana Grotte, Bari, Southern Italy. We determined objective and subjective psychometric properties of SDRS against the gold standard evaluation of social dysfunction according to the Semi-structured Clinical Diagnostic Interview for DSM-IV-TR Axis I Disorders (SCID-I) criterion.Results: The SDRS showed a moderate accuracy with an optimal cut-off of 26 maximized with higher sensitivity (0.74,95% CI:0.63-0.84) than specificity (0.57,95% CI:0.50-0.64). A five-factor structure was carried out and five dimensions of SDRS were identified (loneliness; social isolation; feeling of contribution/uselessness; lack of leisure activities; anxiety for the health). Education and global cognitive functions were inversely correlated to SDRS, while a direct association with global psychopathology, depression, and apathy was found. The prevalence of higher SDRS scores was major in subjects with current psychiatric disorders versus other subjects.∥Conclusion: The SDRS could be a valid instrument to capture both size and quality of social dysfunction, both in subjects with psychiatric disorders and in normal subjects. Several categories of social dysfunction differed only in the degree of health deprivation, not in social or material deprivation. [ABSTRACT FROM AUTHOR]

Published

2018

19. Relationships of Dietary Patterns, Foods, and Micro- and Macronutrients with Alzheimer's Disease and Late-Life Cognitive Disorders: A Systematic Review.

Author

Solfrizzi, Vincenzo, Custodero, Carlo, Lozupone, Madia, Imbimbo, Bruno P., Valiani., Vincenzo, Agosti, Pasquale, Schilardi, Andrea, D’Introno, Alessia, Montagna, Maddalena La, Calvani, Mariapaola, Guerra, Vito, Sardone, Rodolfo, Abbrescia, Daniela I., Bellomo, Antonello, Greco., Antonio, Daniele, Antonio, Seripa, Davide, Logroscino, Giancarlo, Sabbá, Carlo, and Panza, Francesco

Subjects

ALZHEIMER'S disease, BASAL ganglia diseases, COGNITION disorders, FOOD, DIET

Abstract

In the last decade, the association between diet and cognitive function or dementia has been largely investigated. In the present article, we systematically reviewed observational studies published in the last three years (2014-2016) on the relationship among dietary factors and late-life cognitive disorders at different levels of investigation (i.e., dietary patterns, foods and food-groups, and dietary micro- and macronutrients), and possible underlying mechanisms of the proposed associations. From the reviewed evidence, the National Institute on Aging-Alzheimer's Association guidelines for Alzheimer's disease (AD) and cognitive decline due to AD pathology introduced some evidence suggesting a direct relation between diet and changes in the brain structure and activity. There was also accumulating evidence that combinations of foods and nutrients into certain patterns may act synergistically to provide stronger health effects than those conferred by their individual dietary components. In particular, higher adherence to a Mediterranean-type diet was associated with decreased cognitive decline. Moreover, also other emerging healthy dietary patterns such as the Dietary Approach to Stop Hypertension (DASH) and the Mediterranean-DASH diet Intervention for Neurodegenerative Delay (MIND) diets were associated with slower rates of cognitive decline and significant reduction of AD rate. Furthermore, some foods or food groups traditionally considered harmful such as eggs and red meat have been partially rehabilitated, while there is still a negative correlation of cognitive functions with saturated fatty acids and a protective effect against cognitive decline of elevated fish consumption, high intake of monounsaturated fatty acids and polyunsaturated fatty acids (PUFA), particularly n-3 PUFA. [ABSTRACT FROM AUTHOR]

Published

2017

20. Midlife Metabolic Profile and the Risk of Late-Life Cognitive Decline.

Author

Tortelli, Rosanna, Lozupone, Madia, Guerra, Vito, Barulli, Maria Rosaria, Imbimbo, Bruno P., Capozzo, Rosa, Grasso, Alessandra, Tursi, Marianna, Di Dio, Cristina, Sardone, Rodolfo, Giannelli, Gianluigi, Seripa, Davide, Misciagna, Giovanni, Panza, Francesco, and Logroscino, Giancarlo

Subjects

MIDDLE age, METABOLIC syndrome, GLUCOSE, CHOLESTEROL, LIPOPROTEINS, DEMENTIA risk factors, ANALYSIS of variance, BLOOD pressure, FASTING, LONGITUDINAL method, METABOLISM, QUESTIONNAIRES, RADIOIMMUNOASSAY

Abstract

Among metabolic syndrome components, the effects of higher plasma glucose levels on cognitive decline (CD) have been considered in few studies. We evaluated the associations among midlife glycemia, total cholesterol, high-density lipoprotein cholesterol, triglycerides, midlife insulin resistance [homeostasis model assessment for insulin resistance (HOMA-index)], and CD in the older subjects of the population-based MICOL Study (Castellana Grotte, Italy) at baseline (M1) and at follow-ups seven (M2) and twenty years later (M3). At M1, a dementia risk score and a composite cardiovascular risk score for dementia were calculated. For 797 subjects out of 833, we obtained a Mini-Mental State Examination (MMSE) score at M3, subdividing these subjects in three cognitive functioning subgroups: normal cognition, mild CD, and moderate-severe CD. Mean fasting glycemia at baseline was significantly higher in moderate-severe CD subgroup (114.6±71.4 mg/dl) than in the normal cognition subgroup (101.2±20.6). Adjusting for gender, age, and other metabolic components, higher fasting glycemia values both at M1 [odds ratio (OR) = 1.31; 95% confidence interval (CI): 1.08-1.59] and M2 (OR = 1.26; 95% CI: 1.01-1.57) were associated with an increased risk of moderate-severe CD. Mean HOMA index value was significantly higher in the moderate-severe CD subgroup (5.7±9.4) compared to the normal cognition subgroup (2.9±1.4) at M1. The dementia risk probability (MMSE < 24) increased moving through higher categories of the dementia risk score and decreased as long as the cardiovascular score increased. The present findings highlighted the indication to control blood glucose levels, regardless of a diagnosis of diabetes mellitus, as early as midlife for prevention of late-life dementia. [ABSTRACT FROM AUTHOR]

Published

2017

21. CSP-1103 (CHF5074) stabilizes human transthyretin in healthy human subjects.

Author

Qiang, Lixia, Guan, Yanxia, Li, Xiangshun, Liu, Li, Mu, Yanshuang, Sugano, Aki, Takaoka, Yutaka, Sakaeda, Toshiyuki, Imbimbo, Bruno P., Yamamura, Ken-Ichi, Jin, Shoude, and Li, Zhenghua

Subjects

TRANSTHYRETIN, AMYLOIDOSIS, GENETIC disorders, BLOOD proteins, AMYLOID beta-protein, CYCLOOXYGENASES, TETRAMERS (Oligomers)

Abstract

Hereditary amyloid polyneuropathy is a type of protein misfolding disease. Transthyretin (TTR) is a homotetrameric serum protein and TTR tetramer dissociation is the limiting step in amyloid fibril formation. Thus, prevention of TTR dissociation is a promising therapeutic approach and some TTR stabilizers have been approved for the treatment of TTR amyloidosis. CSP-1103 (CHF5074) is a non-steroidal anti-inflammatory derivative that lacks cyclooxygenase inhibitory activity.In vitro, CSP-1103 stabilizes the TTR tetramer by binding to the thyroxine (T4) binding site. We have previously shown that serum TTR levels were increased by oral CSP-1103 administration through stabilization of TTR tetramers in humanized mice at both theTtrlocus and theRbp4locus. To determine whether CSP-1103 stabilizes TTR tetramers in humans, multiple CSP-1103 oral doses were administered for two weeks to 48 healthy human volunteers in a double-blind, placebo-controlled, parallel-group study. CSP-1103 treatment stabilized TTR tetramers in a dose-dependent manner under normal or denaturing stress conditions, thereby increasing serum TTR levels. Preincubation of serum with CSP-1103 or diflunisalin vitroincreased the TTR tetramer stability. Computer simulation analysis revealed that the binding affinities of CSP-1103 with TTR at pH 7.0 were similar to those of tafamidis, thus confirming that CSP-1103 has potent TTR-stabilizing activity. [ABSTRACT FROM AUTHOR]

Published

2017

22. Bipolar Disorder and Frontotemporal Dementia: An Intriguing Association.

Author

Papazacharias, Apostolos, Lozupone, Madia, Barulli, Maria Rosaria, Capozzo, Rosa, Imbimbo, Bruno P, Veneziani, Federica, De Blasi, Roberto, Nardini, Marcello, Seripa, Davide, Panza, Francesco, and Logroscino, Giancarlo

Subjects

MAGNETIC resonance imaging, BIPOLAR disorder, DISEASE progression, FRONTOTEMPORAL dementia, DISEASE complications

Abstract

Bipolar disorder (BD) could represent a prodromal state of frontotemporal dementia (FTD). Two patients affected by lifelong BD with a progressive decline of cognitive functions, behavioral, and neurological signs, reached the early diagnosis of FTD before the age of 60. They were diagnosed as affected by primary progressive aphasia and FTD with parkinsonism, respectively. A diagnosis of FTD should therefore be taken into account, in case of unexpected cognitive and behavioral decline in patients with a long history of BD. Follow-up studies with genetic, neuropsychological, and neuroimaging markers of these BD/FTD patients could further explore some of the underlying association, opening new viable therapeutic options. [ABSTRACT FROM AUTHOR]

Published

2017

23. Bipolar Disorder and Frontotemporal Dementia: An Intriguing Association.

Author

Papazachariasa, Apostolos, Veneziani, Federica, Nardini, Marcello, Lozupone, Madia, Logroscino, Giancarlo, Panza, Francesco, Barulli, Maria Rosaria, Capozzo, Rosa, Imbimbo, Bruno P., De Blasi, Roberto, and Seripa, Davide

Subjects

BIPOLAR disorder, FRONTOTEMPORAL dementia, COGNITIVE ability, PARKINSONIAN disorders, DEMENTIA

Abstract

Bipolar disorder (BD) could represent a prodromal state of frontotemporal dementia (FTD).Two patients affected by lifelong BD with a progressive decline of cognitive functions, behavioral, and neurological signs, reached the early diagnosis of FTD before the age of 60. They were diagnosed as affected by primary progressive aphasia and FTD with parkinsonism, respectively. A diagnosis of FTD should therefore be taken into account, in case of unexpected cognitive and behavioral decline in patients with a long history of BD. Follow-up studies with genetic, neuropsychological, and neuroimaging markers of these BD/FTD patients could further explore some of the underlying association, opening new viable therapeutic options. [ABSTRACT FROM AUTHOR]

Published

2017

24. Drug-induced reductions in brain amyloid-β levels may adversely affect cognition and behavior by a disruption of functional connectivity homeostasis.

Author

Imbimbo, Bruno P and Pomara, Nunzio

Published

2019

25. Amyloid deposition in a mouse model humanized at the transthyretin and retinol-binding protein 4 loci.

Author

Li, Xiangshun, Lyu, Yanyi, Shen, Jingling, Mu, Yanshuang, Qiang, Lixia, Liu, Li, Araki, Kimi, Imbimbo, Bruno P., Yamamura, Ken-ichi, Jin, Shoude, and Li, Zhenghua

Published

2018

26. Tau-based therapeutics for Alzheimer's disease: active and passive immunotherapy.

Author

Panza, Francesco, Solfrizzi, Vincenzo, Seripa, Davide, Imbimbo, Bruno P, Lozupone, Madia, Santamato, Andrea, Tortelli, Rosanna, Galizia, Ilaria, Prete, Camilla, Daniele, Antonio, Pilotto, Alberto, Greco, Antonio, and Logroscino, Giancarlo

Published

2016

27. Tau-Centric Targets and Drugs in Clinical Development for the Treatment of Alzheimer’s Disease.

Author

Panza, Francesco, Solfrizzi, Vincenzo, Seripa, Davide, Imbimbo, Bruno P., Lozupone, Madia, Santamato, Andrea, Zecca, Chiara, Barulli, Maria Rosaria, Bellomo, Antonello, Pilotto, Alberto, Daniele, Antonio, Greco, Antonio, and Logroscino, Giancarlo

Subjects

ALZHEIMER'S disease, BIOAVAILABILITY, CEREBRAL circulation, COGNITION, DEMENTIA, METHYLENE blue, NERVE tissue proteins, PHOSPHATASES, PHOSPHOTRANSFERASES, TOXICITY testing, DRUG development, CHEMICAL inhibitors, THERAPEUTICS

Abstract

The failure of several Phase II/III clinical trials in Alzheimer’s disease (AD) with drugs targeting β-amyloid accumulation in the brain fuelled an increasing interest in alternative treatments against tau pathology, including approaches targeting tau phosphatases/kinases, active and passive immunization, and anti-tau aggregation. The most advanced tau aggregation inhibitor (TAI) is methylthioninium (MT), a drug existing in equilibrium between a reduced (leuco-methylthioninium) and oxidized form (MT+). MT chloride (methylene blue) was investigated in a 24-week Phase II clinical trial in 321 patients with mild to moderate AD that failed to show significant positive effects in mild AD patients, although long-term observations (50 weeks) and biomarker studies suggested possible benefit. The dose of 138 mg/day showed potential benefits on cognitive performance of moderately affected AD patients and cerebral blood flow in mildly affected patients. Further clinical evidence will come from the large ongoing Phase III trials for the treatment of AD and the behavioral variant of frontotemporal dementia on a new form of this TAI, more bioavailable and less toxic at higher doses, called TRx0237. More recently, inhibitors of tau acetylation are being actively pursued based on impressive results in animal studies obtained by salsalate, a clinically used derivative of salicylic acid. [ABSTRACT FROM AUTHOR]

Published

2016

28. Tau-directed approaches for the treatment of Alzheimer’s disease: focus on leuco-methylthioninium.

Author

Seripa, Davide, Solfrizzi, Vincenzo, Imbimbo, Bruno P., Daniele, Antonio, Santamato, Andrea, Lozupone, Madia, Zuliani, Giovanni, Greco, Antonio, Logroscino, Giancarlo, and Panza, Francesco

Abstract

Small molecular weight compounds able to inhibit formation of tau oligomers and fibrils have already been tested for Alzheimer’s disease (AD) treatment. The most advanced tau aggregation inhibitor (TAI) is methylthioninium (MT), a drug existing in equilibrium between a reduced (leuco-methylthioninium) and oxidized form (MT+). MT chloride (also known as methylene blue) was investigated in a 24-week Phase II study in 321 mild-to-moderate AD patients at the doses of 69, 138, and 228 mg/day. This trial failed to show significant positive effects of MT in the overall patient population. The dose of 138 mg/day showed potential benefits on cognitive performance of moderately affected patients and cerebral blood flow in mildly affected patients. A follow-up compound (TRx0237) claimed to be more bioavailable and less toxic than MT, is now being developed. Phase III clinical trials on this novel TAI in AD and in the behavioral variant of frontotemporal dementia are underway. [ABSTRACT FROM PUBLISHER]

Published

2016

29. Age-related hearing impairment and frailty in Alzheimer's disease: interconnected associations and mechanisms.

Author

Panza, Francesco, Solfrizzi, Vincenzo, Seripa, Davide, Imbimbo, Bruno P., Capozzo, Rosa, Quaranta, Nicola, Pilotto, Alberto, and Logroscino, Giancarlo

Subjects

ALZHEIMER'S disease, DEMENTIA, MILD cognitive impairment, HEARING disorders, AGE factors in disease, WORD deafness, FRAGILITY (Psychology)

Abstract

The article discusses the age-related hearing impairment or presbycusis and frailty in Alzheimer's disease (AD). It examines the peripheral age-related dementia, central auditory processing dysfunction and mild cognitive impairment, as well as the link of cognition and dementia to frailty. It cites longitudinal population-based studies suggesting that peripheral and central auditory processing (CAP) dysfunctions appear to be associated with incident cognitive impairment and AD

Published

2015

30. CHF5074 (CSP-1103) stabilizes human transthyretin in mice humanized at the transthyretin and retinol-binding protein loci.

Author

Mu, Yanshuang, Jin, Shoude, Shen, Jingling, Sugano, Aki, Takaoka, Yutaka, Qiang, Lixia, Imbimbo, Bruno P., Yamamura, Ken-ichi, and Li, Zhenghua

Subjects

TRANSTHYRETIN, LABORATORY mice, RETINOL-binding proteins, PROTEIN folding, MATHEMATICAL bounds

Abstract

Familial amyloidotic polyneuropathy is one type of protein misfolding disease. Transthyretin (TTR) tetramer dissociation is the limiting step for amyloid fibril formation. CHF5074 (CSP-1103) stabilizes TTR tetramer in vitro by binding to the T4 binding site. Here, we used three strains of double humanized mice (mTtr hTTRVal30/hTTRVal30 , mTtr hTTRVal30/hTTRMet30 , and mTtr hTTRMet30/hTTRMet30 ) to assess whether CHF5074 stabilizes TTR tetramers in vivo. Treatment of mice with CHF5074 increased serum TTR levels by stabilizing TTR tetramers. Although the binding affinities of CHF5074 and diflunisal with TTRMet30 were similar, CHF5074 bound TTRVal30 more strongly than did diflunisal, suggesting the potent TTR-stabilizing activity of CHF5074. [ABSTRACT FROM AUTHOR]

Published

2015

31. Efficacy and safety studies of gantenerumab in patients with Alzheimer's disease.

Author

Panza, Francesco, Solfrizzi, Vincenzo, Imbimbo, Bruno P, Giannini, Michele, Santamato, Andrea, Seripa, Davide, and Logroscino, Giancarlo

Abstract

Among active and passive anti-β-amyloid (Aβ) immunotherapies for Alzheimer's disease (AD), bapineuzumab and solanezumab, two humanized monoclonal antibodies, failed to show significant clinical benefits in mild-to-moderate AD patients in large Phase III clinical trials. Another ongoing Phase III trial of solanezumab aims to confirm positive findings in mild AD patients. Gantenerumab is the first fully human anti-Aβ monoclonal antibody directed to both N-terminal and central regions of Aβ. A 6-month PET study in 16 AD patients showed that gantenerumab treatment dose-dependently reduced brain Aβ deposition, possibly stimulating microglial-mediated phagocytosis. Two ongoing Phase III trials of gantenerumab in patients with prodromal or mild dementia due to AD will determine if any reduction in brain Aβ levels will translate into clinical benefits. An ongoing secondary prevention trial of gantenerumab in presymptomatic subjects with genetic mutations for autosomal-dominant AD will verify the utility of anti-Aβ monoclonal antibodies as prevention therapy. [ABSTRACT FROM AUTHOR]

Published

2014

32. Is there still any hope for amyloid-based immunotherapy for Alzheimer's disease?

Author

Panza, Francesco, Logroscino, Giancarlo, Imbimbo, Bruno P, and Solfrizzi, Vincenzo

Published

2014

33. Amyloid-based immunotherapy for Alzheimer's disease in the time of prevention trials: the way forward.

Author

Panza, Francesco, Solfrizzi, Vincenzo, Imbimbo, Bruno P, Tortelli, Rosanna, Santamato, Andrea, and Logroscino, Giancarlo

Subjects

ALZHEIMER'S disease treatment, IMMUNOTHERAPY, AMYLOID, THERAPEUTIC use of monoclonal antibodies, VACCINES, DEMENTIA

Abstract

Both active and passive anti-β-amyloid (Aβ) immunotherapies for the treatment of Alzheimer's disease (AD) have demonstrated clearance of brain Aβ deposits. Among passive immunotherapeutics, two Phase III clinical trials in mild-to-moderate AD patients with bapineuzumab, a humanized monoclonal antibody directed at the N-terminal sequence of Aβ, were disappointing. Also solanezumab, directed at the mid-region of Aβ, failed in two Phase III trials in mild-to-moderate AD. Another Phase III trial with solanezumab is ongoing in mildly affected AD patients based on encouraging results in this subgroup. Second-generation active Aβ vaccines (CAD106, ACC-001, and Affitope AD02) and new passive anti-Aβ immunotherapies (gantenerumab and crenezumab) have been developed and are under clinical testing. These new anti-Aβ immunotherapies are being tested in prodromal AD, in presymptomatic subjects with AD-related mutations, or in asymptomatic subjects at risk of developing AD. These primary and secondary prevention trials will definitely test the Aβ cascade hypothesis of AD. [ABSTRACT FROM AUTHOR]

Published

2014

34. Pharmacokinetics and Pharmacodynamics of CHF5074 After Short-term Administration in Healthy Subjects.

Author

Imbimbo, Bruno P., Frigerio, Enrico, Breda, Massimo, Fiorentin, Francesco, Fernandez, Mercedes, Sivilia, Sandra, Giardino, Luciana, Calzà, Laura, Norris, Dottie, Casula, Daniela, and Shenouda, Magdy

Published

2013

35. Multi-target action of the novel anti-Alzheimer compound CHF5074: in vivo study of long term treatment in Tg2576 mice.

Author

Sivilia, Sandra, Lorenzini, Luca, Giuliani, Alessandro, Gusciglio, Marco, Fernandez, Mercedes, Baldassarro, Vito Antonio, Mangano, Chiara, Ferraro, Luca, Pietrini, Vladimiro, Baroc, Maria Francesca, Viscomi, Arturo R., Ottonello, Simone, Villetti, Gino, Imbimbo, Bruno P., Calzà, Laura, and Giardino, Luciana

Subjects

ALZHEIMER'S disease, DISEASES in older people, GLYCOPROTEINS, NEUROLOGICAL disorders, AMYLOID

Abstract

Background: Alzheimer disease is a multifactorial disorder characterized by the progressive deterioration of neuronal networks. The pathological hallmarks includes extracellular amyloid plaques and intraneuronal neurofibrillary tangles, but the primary cause is only partially understood. Thus, there is growing interest in developing agents that might target multiple mechanisms leading to neuronal degeneration. CHF5074 is a nonsteroidal anti-inflammatory derivative that has been shown to behave as a γ-secretase modulator in vitro and to inhibit plaque deposition and to reverse memory deficit in vivo in transgenic mouse models of Alzheimer's disease (AD). In the present study, the effects of a long-term (13-month) treatment with CHF5074 on indicators of brain functionality and neurodegeneration in transgenic AD mice (Tg2576) have been assessed and compared with those induced by a prototypical γ-secretase inhibitor (DAPT). Results: To this end, plaque-free, 6-month-old Tg2576 mice and wild-type littermates were fed with a diet containing CHF5074 (125 and 375 ppm/day), DAPT (375 ppm/day) or vehicle for 13 months. The measured indicators included object recognition memory, amyloid burden, brain oligomeric and plasma Aβ levels, intraneuronal Aβ, dendritic spine density/morphology, neuronal cyclin A positivity and activated microglia. Tg2576 mice fed with standard diet displayed an impairment of recognition memory. This deficit was completely reverted by the higher dose of CHF5074, while no effects were observed in DAPT-treated mice. Similarly, amyloid plaque burden, microglia activation and aberrant cell cycle events were significantly affected by CHF5074, but not DAPT, treatment. Both CHF5074 and DAPT reduced intraneuronal Aβ content, also increasing Aβ40 and Aβ42 plasma levels. Conclusions: This comparative analysis revealed a profoundly diverse range of clinically relevant effects differentiating the multifunctional anti-inflammatory derivative CHF5074 from the γ-secretase inhibitor DAPT and highlighted unique mechanisms and potential targets that may be crucial for neuroprotection in mouse models of AD. [ABSTRACT FROM AUTHOR]

Published

2013

36. CHF5074 restores visual memory ability and pre-synaptic cortical acetylcholine release in pre-plaque Tg2576 mice.

Author

Giuliani, Alessandro, Beggiato, Sarah, Baldassarro, Vito A., Mangano, Chiara, Giardino, Luciana, Imbimbo, Bruno P., Antonelli, Tiziana, Calzà, Laura, and Ferraro, Luca

Subjects

MICROGLIA, ACETYLCHOLINE, ALZHEIMER'S disease, LABORATORY mice, TRANSGENIC mice, GABA

Abstract

CHF5074, a new microglial modulator, attenuates memory deficit in Alzheimer's disease transgenic mice. In this study, the effect of an acute or subacute CHF5074 treatment on in vivo novel object recognition test and on [3H]Acetylcholine (ACh) and GABA release in pre-plaque (7-month-old) Tg2576 mice have been compared with those induced by the γ-secretase inhibitor LY450139 (semagacestat). Vehicle-treated Tg2576 mice displayed an impairment of recognition memory compared with wild-type animals. This impairment was recovered in transgenic animals acutely treated with CHF5074 (30 mg/kg), while LY450139 (1, 3, 10 mg/kg) was ineffective. In frontal cortex synaptosomes from vehicle-treated Tg2576 mice, K+-evoked [3H]ACh release was lower than that measured in wild-type mice. This reduction was absent in transgenic animals subacutely treated with CHF5074 (30 mg/kg daily for 8 days), while it was slightly, not significantly, amplified by LY450139 (3 mg/kg daily for 8 days). There were no differences between the groups on spontaneous [3H]ACh release as well as spontaneous and K+-evoked GABA release. These results suggest that CHF5074 has beneficial effects on visual memory and cortical cholinergic dysfunctions in pre-plaque Tg2576 mice. Together with previous findings, these data suggest that CHF5074 could be a possible candidate for early Alzheimer's disease therapeutic regimens. [ABSTRACT FROM AUTHOR]

Published

2013

37. Frailty syndrome and the risk of vascular dementia: The Italian Longitudinal Study on Aging

Author

Solfrizzi, Vincenzo, Scafato, Emanuele, Frisardi, Vincenza, Seripa, Davide, Logroscino, Giancarlo, Maggi, Stefania, Imbimbo, Bruno P., Galluzzo, Lucia, Baldereschi, Marzia, Gandin, Claudia, Di Carlo, Antonio, Inzitari, Domenico, Crepaldi, Gaetano, Pilotto, Alberto, and Panza, Francesco

Subjects

FRAGILITY (Psychology), VASCULAR dementia, ITALIANS, PSYCHOLOGICAL aspects of aging, LONGITUDINAL method, COGNITION, CLINICAL trials, HEALTH outcome assessment, DISEASES, DISEASE risk factors

Abstract

Abstract: Background: Frailty is a clinical syndrome generally associated with a greater risk for adverse outcomes such as falls, disability, institutionalization, and death. Cognition and dementia have already been considered as components of frailty, but the role of frailty as a possible determinant of dementia, Alzheimer’s disease (AD), and vascular dementia (VaD) has been poorly investigated. We estimated the predictive role of frailty syndrome on incident dementia and its subtypes in a nondemented, Italian, older population. Methods: We evaluated 2581 individuals recruited from the Italian Longitudinal Study on Aging sample population consisting of 5632 subjects aged 65 to 84 years and with a 3.9-year median follow-up. A phenotype of frailty according to a modified measurement of Cardiovascular Health Study criteria was operationalized. Dementia, AD, and VaD were classified using current published criteria. Results: Over a 3.5-year follow-up, 65 of 2581 (2.5%) older subjects, 16 among 252 frail individuals (6.3%), of which 9 were affected by VaD (3.6%), developed overall dementia. In a proportional hazards model, frailty syndrome was associated with a significantly increased risk of overall dementia (adjusted hazard ratio: 1.85; 95% confidence interval: 1.01–3.40) and, in particular, VaD (adjusted hazard ratio: 2.68; 95% confidence interval: 1.16–7.17). The risk of AD or other types of dementia did not significantly change in frail individuals in comparison with subjects without frailty syndrome. Conclusion: In our large population-based sample, frailty syndrome was a short-term predictor of overall dementia and VaD. [Copyright &y& Elsevier]

Published

2013

38. Receptor for Advanced Glycation End Products Contributes to Postnatal Pulmonary Development and Adult Lung Maintenance Program in Mice.

Author

Fineschi, Silvia, De Cunto, Giovanna, Facchinetti, Fabrizio, Civelli, Maurizio, Imbimbo, Bruno P., Carnini, Chiara, Villetti, Gino, Lunghi, Benedetta, Stochino, Stefania, Gibbons, Deena L., Hayday, Adrian, Lungarella, Giuseppe, and Cavarra, Eleonora

Published

2013

39. Metabolic-Cognitive Syndrome: Metabolic Approach for the Management of Alzheimer's Disease Risk.

Author

Frisardi, Vincenza, Imbimbo, Bruno, and Imbimbo, Bruno P.

Subjects

METABOLIC syndrome, DEMENTIA, MILD cognitive impairment, ALZHEIMER'S disease, GENETIC disorders

Abstract

The article discusses the metabolic syndrome (MetS) as a potential trigger of pathological molecular pathways dementia-linked. It mentions the existence of evidence which support the association of MetS and metabolic determinants with cognitive impairment and dementia. It mentions that although several studies suggested that MetS could be linked to the risk of vascular dementia, there are results which showed a possible role of MetS in developing Alzheimer's disease (AD).

Published

2012

40. Alcohol consumption in mild cognitive impairment and dementia: harmful or neuroprotective?

Author

Panza, Francesco, Frisardi, Vincenza, Seripa, Davide, Logroscino, Giancarlo, Santamato, Andrea, Imbimbo, Bruno P., Scafato, Emanuele, Pilotto, Alberto, and Solfrizzi, Vincenzo

Subjects

ALCOHOL drinking & health, MILD cognitive impairment, COGNITION disorder risk factors, TREATMENT of dementia, NEUROPROTECTIVE agents, PHYSIOLOGICAL effects of alcohol, COGNITION disorders in old age, THERAPEUTICS

Abstract

Objective: In several longitudinal studies, light-to-moderate drinking of alcoholic beverages has been proposed as being protective against the development of age-related changes in cognitive function, predementia syndromes, and cognitive decline of degenerative (Alzheimer's disease, AD) or vascular origin (vascular dementia). However, contrasting findings also exist. Method: The English literature published in this area before September 2011 was evaluated, and information relating to the various factors that may impact upon the relationship between alcohol consumption and dementia or predementia syndromes is presented in the succeeding texts. Results: Light-to-moderate alcohol consumption may be associated with a reduced risk of incident overall dementia and AD; however, protective benefits afforded to vascular dementia, cognitive decline, and predementia syndromes are less clear. The equivocal findings may relate to many of the studies being limited to cross-sectional designs, restrictions by age or gender, or incomplete ascertainment. Different outcomes, beverages, drinking patterns, and study follow-up periods or possible interactions with other lifestyle-related (e.g., smoking) or genetic factors (e.g., apolipoprotein E gene variation) may all contribute to the variability of findings. Conclusion: Protective effects of moderate alcohol consumption against cognitive decline are suggested to be more likely in the absence of the AD-associated apolipoprotein E ε4 allele and where wine is the beverage. At present, there is no indication that light-to-moderate alcohol drinking would be harmful to cognition and dementia, and attempts to define what might be deemed beneficial levels of alcohol intake in terms of cognitive performance would be highly problematic and contentious. Copyright © 2012 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2012

41. Solanezumab for the treatment of mild-to-moderate Alzheimer's disease.

Author

Imbimbo, Bruno P., Ottonello, Simone, Frisardi, Vincenza, Solfrizzi, Vincenzo, Greco, Antonio, Seripa, Davide, Pilotto, Alberto, and Panza, Francesco

Subjects

ALZHEIMER'S disease treatment, MONOCLONAL antibodies, AMYLOID beta-protein, PEPTIDES, DEMENTIA, IMMUNOTHERAPY, MILD cognitive impairment

Abstract

Solanezumab (LY2062430) is a humanized monoclonal antibody that binds to the central region of &bgr;-amyloid, a peptide believed to play a key role in the pathogenesis of Alzheimer's disease (AD). Eli Lilly & Co is developing an intravenous formulation of solanezumab for the treatment of mild-to-moderate AD. Acute and subchronic treatment with solanezumab of transgenic mice attenuated or reversed memory deficits with no effects on incidence or severity of cerebral amyloid angiopathy-associated microhemorrhages, a severe side effect associated with bapineuzumab, another monoclonal antibody. Phase II studies in AD patients have shown a good safety profile with encouraging indications on cerebrospinal and plasma biomarkers. The drug is currently being investigated in Phase III trials. While there is a strong hope that solanezumab may represent the first effective passive vaccine for AD treatment, skepticism still exists on the ability of the drug to slow the rate of deterioration in patients with fully established disease. INSET: Key issues. [ABSTRACT FROM AUTHOR]

Published

2012

42. Metabolic-Cognitive Syndrome: Metabolic Approach for the Management of Alzheimer's Disease Risk.

Author

Frisardi, Vincenza, Imbimbo, Bruno, and Imbimbo, Bruno P.

Subjects

ALZHEIMER'S disease, METABOLIC syndrome, DISEASES in older people, COGNITION disorders, METABOLIC disorders

Abstract

The article explores the possible link between metabolic syndrome (MetS) and Alzheimer's disease. Several studies have shown that MetS increases the risk for age-related cognitive decline. Molecular mechanisms underlying the mirror relationship between MetS and neurological disorders are not fully understood, but it is becoming increasingly evident that all cellular and biochemical alterations observed in MetS may represent a pathological bridge between MetS and various neurological disorders.

Published

2012

43. Therapeutic effect of CHF5074, a new γ-secretase modulator, in a mouse model of scrapie.

Author

Poli, Giorgio, Corda, Erica, Lucchini, Barbara, Puricelli, Maria, Martino, Piera Anna, Dall'Ara, Paola, Villetti, Gino, Bareggi, Silvio R., Corona, Cristiano, Costassa, Elena Vallino, Gazzuola, Paola, Iulini, Barbara, Mazza, Maria, Acutis, Pierluigi, Mantegazza, Paolo, Casalone, Cristina, and Imbimbo, Bruno P.

Published

2012

44. The γ-Secretase Modulator CHF5074 Restores Memory and Hippocampal Synaptic Plasticity in Plaque-Free Tg2576 Mice.

Author

Balducci, Claudia, Mehdawy, Bisan, Mare, Lydia, Giuliani, Alessandro, Lorenzini, Luca, Sivilia, Sandra, Giardino, Luciana, Calzà, Laura, Lanzillotta, Annamaria, Sarnico, Ilenia, Pizzi, Marina, Usiello, Alessandro, Viscomi, Arturo R., Ottonello, Simone, Villetti, Gino, Imbimbo, Bruno P., Nisticò, Giuseppe, Forloni, Gianluigi, and Nisticò, Robert

Subjects

ALZHEIMER'S disease, AMYLOID beta-protein, NONSTEROIDAL anti-inflammatory agents, MEMORY disorders, NEUROPLASTICITY

Abstract

Abnormal amyloid-β (Aβ) production and deposition is believed to represent one of the main causes of Alzheimer's disease (AD). γ-Secretase is the enzymatic complex responsible for Aβ generation from its precursor protein. Inhibition or modulation of γ-secretase represents an attractive therapeutic approach. CHF5074 is a new γ-secretase modulator that has been shown to inhibit brain plaque deposition and to attenuate memory deficit in adult AD transgenic mice after chronic treatment. To date, it is not known whether the positive behavioral effects of this compound also occur in young transgenic mice without plaque deposition. Here, we evaluated the effects of acute and subchronic treatment with CHF5074 on contextual and recognition memory and on hippocampal synaptic plasticity in plaque-free Tg2576 mice. We found that at 5 months of age, contextual memory impairment was significantly attenuated after acute subcutaneous administration of 30 mg/kg CHF5074. At 6 months of age, recognition memory impairment was fully reversed after a 4-week oral treatment in the diet (≈60 mg/kg/day). These cognitive effects were associated with a reversal of long-term potentiation (LTP) impairment in the hippocampus. A significant reduction in brain intraneuronal AβPP/Aβ levels and hyperphosphorylated tau, but no change in soluble or oligomeric Aβ levels was detected in Tg2576 mice showing functional recovery following CHF5074 treatment. We conclude that the beneficial effects of CHF5074 treatment in young transgenic mice occurred at a stage that precedes plaque formation and were associated with a reduction in intraneuronal AβPP/Aβ and hyperphosphorylated tau. [ABSTRACT FROM AUTHOR]

Published

2011

45. Gerontechnology for Demented Patients: Smart Homes for Smart Aging.

Author

Frisardi, Vincenza and Imbimbo, Bruno P.

Subjects

CARE of dementia patients, HOME automation, ALZHEIMER'S disease, INFORMATION & communication technologies, QUALITY of life

Abstract

In an aging world, maintaining good health and independence for as long as possible is essential. Instead of hospitalization or institutionalization, the elderly with chronic conditions, especially those with cognitive impairment, can be assisted in their own environment with numerous 'smart' devices that support them in their activity of daily living. A 'smart home' is a residence equipped with technology that facilitates monitoring of residents to improve quality of life and promote physical independence, as well as to reduce caregiver burden. Several projects worldwide have been conducted, but some ethical and legal issues are still unresolved and, at present, there is no evidence of the effects of smart homes on health outcomes. Randomized controlled trials are needed to understand the plus and minuses of these projects, but this will only be possible with a widespread proliferation and penetration of smart homes in the social network. [ABSTRACT FROM AUTHOR]

Published

2011

46. Nutraceutical Properties of Mediterranean Diet and Cognitive Decline: Possible Underlying Mechanisms.

Author

Frisardi, Vincenza, Panza, Francesco, Seripa, Davide, Imbimbo, Bruno P., Vendemiale, Gianluigi, Pilotto, Alberto, and Solfrizzi, Vincenzo

Subjects

FUNCTIONAL foods, DIET in disease, ALZHEIMER'S disease, DIET, DEMENTIA

Abstract

Recent prospective studies provided evidence that higher adherence to a Mediterranean-type diet could be associated with slower cognitive decline, reduced risk of progression from mild cognitive impairment to Alzheimer's disease (AD), reduced risk of AD, and decreased mortality in AD patients. Furthermore, the Mediterranean diet (MeDi) combines several foods, micro- and macronutrients already separately proposed as potential protective factors against dementia and predementia syndromes. At present, epidemiological evidence suggests a possible association between fish consumption, monounsaturated fatty acids, and polyunsaturated fatty acids (PUFA) (particularly, n-3 PUFA), and reduced risk of cognitive decline and dementia. Light to moderate alcohol use may be associated with a reduced risk of incident dementia and AD, while for vascular dementia, cognitive decline, and predementia syndromes, the current evidence is only suggestive of a protective effect. Finally, the limited epidemiological evidence available on fruit and vegetable consumption and cognition generally support a protective role of these macronutrients against cognitive decline, dementia, and AD. We reviewed evidence on the possible mechanisms underlying the suggested protective role of MeDi against age-related changes in cognitive function, predementia syndromes, and dementia, examining the possible role of macronutrients and food nutrients of the MeDi and their nutraceutical properties in modulating the risk of cognitive decline. Although vascular variables are likely to be in the causal pathway between MeDi and dementia syndromes and should be considered as possible mediators, other nonvascular biological mechanisms (i.e., metabolic, oxidative, and inflammatory) may be invoked to explain the complex epidemiological association between MeDi and cognitive decline. [ABSTRACT FROM AUTHOR]

Published

2010

47. Are γ-secretase inhibitors detrimental for Alzheimer's disease patients?

Author

Ross, Joel S. and Imbimbo, Bruno P.

Subjects

CLINICAL trials, ALZHEIMER'S disease treatment, SECRETASES, BASAL ganglia diseases, DEMENTIA

Abstract

The recent failure of semagacestat in two large Phase III studies questions the value of γ-secretase inhibitors in treating Alzheimer's disease. Understanding the reasons of this setback may be important for the future research on effective treatments for this devastating disease. [ABSTRACT FROM AUTHOR]

Published

2010

48. Peripheral antioxidant markers in mild cognitive impairment and its progression to dementia.

Author

Panza F, Solfrizzi V, Seripa D, Imbimbo BP, Pilotto A, Frisardi V, Panza, Francesco, Solfrizzi, Vincenzo, Seripa, Davide, Imbimbo, Bruno P, Pilotto, Alberto, and Frisardi, Vincenza

Subjects

COGNITION disorders diagnosis, REACTIVE oxygen species, ANIMALS, ANTIOXIDANTS, BIOMARKERS, CELLULAR signal transduction, COGNITION disorders, LONGITUDINAL method, DISEASE progression

Abstract

Mild cognitive impairment (MCI) is recognized as a prodromal phase of dementing disorders, and it has been suggested that oxidative stress may play a role in the pathogenesis of Alzheimer's disease (AD), and in predicting progression of MCI to AD. In the present article, on the basis of an increasing body of evidence from cross-sectional and longitudinal studies, we discussed the issue of the possible impact of antioxidant compounds from diet and supplementation on MCI and its progression to AD. [ABSTRACT FROM AUTHOR]

Published

2010

49. Peripheral Antioxidant Markers in Mild Cognitive Impairment and its Progression to Dementia.

Author

Panza, Francesco, Solfrizzi, Vincenzo, Seripa, Davide, Imbimbo, Bruno P., Pilotto, Alberto, and Frisardi, Vincenza

Abstract

Mild cognitive impairment (MCI) is recognized as a prodromal phase of dementing disorders, and it has been suggested that oxidative stress may play a role in the pathogenesis of Alzheimer's disease (AD), and in predicting progression of MCI to AD. In the present article, on the basis of an increasing body of evidence from cross-sectional and longitudinal studies, we discussed the issue of the possible impact of antioxidant compounds from diet and supplementation on MCI and its progression to AD. [ABSTRACT FROM AUTHOR]

Published

2010

50. Dietary Unsaturated Fatty Acids and Risk of Mild Cognitive Impairment.

Author

Panza, Francesco, Frisardi, Vincenza, Seripa, Davide, Imbimbo, Bruno P., Pilotto, Alberto, and Solfrizzi, Vincenzo

Subjects

ALZHEIMER'S disease, DEMENTIA, FATTY acids, VASCULAR dementia, COGNITIVE ability, EPIDEMIOLOGY

Abstract

An increasing body of epidemiological evidence suggested that elevated saturated fatty acids could have negative effects on age-related cognitive decline (ARCD) and mild cognitive impairment (MCI). Furthermore, a clear reduction of risk for cognitive decline has been found in population samples with elevated fish consumption, high intake of monounsaturated fatty acids, and polyunsaturated fatty acids (PUFA), particularly n-3 PUFA. In the present article, on the basis of increasing body of evidence from cross-sectional and longitudinal population-based studies, we discussed the issue of the possible impact of dietary PUFA (both n-6 and n-3) on ARCD, MCI, and Alzheimer's disease. [ABSTRACT FROM AUTHOR]

Published

2010