Link between Diabetes and Alzheimer’s Disease Due to the Shared Amyloid Aggregation and Deposition Involving Both Neurodegenerative Changes and Neurovascular Damages

Stanciu, Gabriela Dumitriţa; Bild, Veronica; Ababei, Daniela Carmen; Rusu, Răzvan Nicolae; Cobzaru, Alina; Păduraru, Luminiţa; Bulea, Delia

doi:10.3390/jcm9061713

Cited by 68 publications

(51 citation statements)

References 163 publications

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“…The detection of MIA associations with the previously enumerated transcript isoforms agrees with findings on behavior disorders, including reports that HCRT regulates sleep, feeding behavior, wakefulness, emotion, and stress response [41]. Similarly, RLN3 influences feeding behavior, stress responses, anxiety and memory [84], and AVP is a regulator of social behavior [85,86]. IGF1 has been associated with autism spectrum disorder symptoms [87][88][89], with IGF1-treatment proposed as an autism therapeutic intervention [88].…”

Section: Transcript Isoform Characterization Of Maternal Immune Activation Effectssupporting

confidence: 82%

Effects of maternal immune activation in porcine transcript isoforms of neuropeptide and receptor genes

Southey¹,

Zhang²,

Keever³

et al. 2021

Journal of Integrative Neuroscience

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Section: Transcript Isoform Characterization Of Maternal Immune Activation Effectssupporting

confidence: 82%

Effects of maternal immune activation in porcine transcript isoforms of neuropeptide and receptor genes

Southey¹,

Zhang²,

Keever³

et al. 2021

Journal of Integrative Neuroscience

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“…SAA, an apo-lipoprotein synthesized by the liver, is an acute phase reactant extensively studied in various acute pathologies in adults (cardiac, renal, degenerative disorders) [ 80 , 81 , 82 , 83 , 84 , 85 ]. Its levels rise early during the inflammatory response up to 1000 times higher than the baseline serum values but are significantly influenced by the patient’s hepatic function and nutritional status.…”

Section: Biomarkers Commonly Used or Under Consideration For Eos Dmentioning

confidence: 99%

Relevance of Biomarkers Currently in Use or Research for Practical Diagnosis Approach of Neonatal Early-Onset Sepsis

et al. 2020

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Neonatal early-onset sepsis (EOS) is defined as an invasive infection that occurs in the first 72 h of life. The incidence of EOS varies from 0.5–2% live births in developed countries, up to 9.8% live births in low resource settings, generating a high mortality rate, especially in extremely low birth weight neonates. Clinical signs are nonspecific, leading to a late diagnosis and high mortality. Currently, there are several markers used for sepsis evaluation, such as hematological indices, acute phase reactants, cytokines, which by themselves do not show acceptable sensitivity and specificity for the diagnosis of EOS in neonates. Newer and more selective markers have surfaced recently, such as presepsin and endocan, but they are currently only in the experimental research stages. This comprehensive review article is based on the role of biomarkers currently in use or in the research phase from a basic, translational, and clinical viewpoint that helps us to improve the quality of neonatal early-onset sepsis diagnosis and management.

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“…Alzheimer's disease neuropathology encompasses several interrelated features: (i) the progressive disorganization and dropout of neocortical synapses that involve loss of selective synaptic components, synaptic atrophy, "pruning" and synaptic loss; (ii) neuronal atrophy, cytoarchitectural deficits and neurite retraction and degeneration, neuronal cell death and loss of inter-neuronal communication; (iii) the progressive deposition and accumulation of amyloid-beta (Aβ) peptides and other insoluble end-stage oxidized lipoproteins into dense, pro-inflammatory senile plaque (SP) aggregates; (iv) the accumulation and aggregation of hyper-phosphorylated tau proteins into neurofibrillary tangles (NFT) that disrupt the normal neural cell cytoarchitecture; (v) neurovascular pathology; (vi) dysfunctional autophagy; (vii) progressive inflammatory neurodegeneration and anatomical targeting of specific anatomical regions of the brain and primarily the association neocortex and hippocampal CA1 regions; (viii) alterations in the innate-immune response and other immunological biomarkers; (ix) changes in the gastrointestinal tract (GI-tract) microbiome; (x) dysfunction and alterations in the glymphatic system of the CNS; (xi) multiple functional associations with diet, obesity, metabolic disease and diabetes; and (xii) blood lipoprotein composition and blood type (Lukiw et al, 1992;Lukiw, 2007;Cogswell et al, 2008;Lukiw, 2013a,b;Praticò, 2013;Hampel and Lista, 2013;Kim et al, 2014;Sherva et al, 2014;Canobbio et al, 2015;De Marco and Venneri, 2015;Jin et al, 2015;Verhülsdonk et al, 2015;Wang et al, 2015;Zhao et al, 2015;Blennow and Zetterberg, 2018;Hampel et al, 2018a,b,c;Arvanitakis et al, 2019;von Arnim et al, 2019;Cole and Seabrook, 2020;Dumurgier and Tzourio, 2020;Hampel et al, 2020a,b;Khoury and Grossberg, 2020;Lewczuk et al, 2020;McGurran et al, 2020;Rodriguez and Lachmann, 2020;Rossini et al, 2020;Stanciu et al, 2020;…”

Section: Traditional Pathophysiological Biomarkers For Ad Are Non-spementioning

confidence: 99%

microRNA-Based Biomarkers in Alzheimer’s Disease (AD)

et al. 2020

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Alzheimer's disease (AD) is a multifactorial, age-related neurological disease characterized by complex pathophysiological dynamics taking place at multiple biological levels, including molecular, genetic, epigenetic, cellular and large-scale brain networks. These alterations account for multiple pathophysiological mechanisms such as brain protein accumulation, neuroinflammatory/neuro-immune processes, synaptic dysfunction, and neurodegeneration that eventually lead to cognitive and behavioral decline. Alterations in microRNA (miRNA) signaling have been implicated in the epigenetics and molecular genetics of all neurobiological processes associated with AD pathophysiology. These changes encompass altered miRNA abundance, speciation and complexity in anatomical regions of the CNS targeted by the disease, including modified miRNA expression patterns in brain tissues, the systemic circulation, the extracellular fluid (ECF) and the cerebrospinal fluid (CSF). miRNAs have been investigated as candidate biomarkers for AD diagnosis, disease prediction, prognosis and therapeutic purposes because of their involvement in multiple brain signaling pathways in both health and disease. In this review we will: (i) highlight the significantly heterogeneous nature of miRNA expression and complexity in AD tissues and biofluids; (ii) address how information may be extracted from these data to be used as a diagnostic, prognostic and/or screening tools across the entire continuum of AD, from the preclinical stage, through the prodromal, i.e., mild cognitive impairment (MCI) phase all the way to clinically overt dementia; and (iii) consider how specific miRNA expression patterns could be categorized using miRNA reporters that span AD pathophysiological initiation and disease progression.

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Link between Diabetes and Alzheimer’s Disease Due to the Shared Amyloid Aggregation and Deposition Involving Both Neurodegenerative Changes and Neurovascular Damages

Cited by 68 publications

References 163 publications

Effects of maternal immune activation in porcine transcript isoforms of neuropeptide and receptor genes

Effects of maternal immune activation in porcine transcript isoforms of neuropeptide and receptor genes

Relevance of Biomarkers Currently in Use or Research for Practical Diagnosis Approach of Neonatal Early-Onset Sepsis

microRNA-Based Biomarkers in Alzheimer’s Disease (AD)

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