The Beneficial Effects of Combining Anti-Aβ Antibody NP106 and Curcumin Analog TML-6 on the Treatment of Alzheimer’s Disease in APP/PS1 Mice

Su, Ih‐Jen; Hsu, Chia‐Yu; Shen, Sheng‐Feng; Chao, Po-Kuan; Hsu, Ju Wei; Hsueh, Jung-Tsung; Liang, Jiajun; Hsu, Ying-Ting; Shie, Feng-Shiun

doi:10.3390/ijms23010556

Cited by 4 publications

(14 citation statements)

References 52 publications

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“…Microglial cells (MGs) are resident immune cells that exert multiple functions in a healthy and pathological brain. MGs are also involved in the pathogenesis of various diseases in the central nervous system, including ischemic stroke, traumatic brain injuries, Alzheimer’s disease, and brain tumors [ 1 , 2 , 3 , 4 , 5 ]. Therefore, insights into microglial regulation are essential in understanding the progress of such diseases.…”

Section: Introductionmentioning

confidence: 99%

Different Contacted Cell Types Contribute to Acquiring Different Properties in Brain Microglial Cells upon Intercellular Interaction

Nakano‐Doi

Kubo²,

Sonoda³

et al. 2023

IJMS

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Microglial cells (MGs), originally derived from progenitor cells in a yolk sac during early development, are glial cells located in a physiological and pathological brain. Since the brain contains various cell types, MGs could frequently interact with different cells, such as astrocytes (ACs), pericytes (PCs), and endothelial cells (ECs). However, how microglial traits are regulated via cell–cell interactions by ACs, PCs, or ECs and how they are different depending on the contacted cell types is unclear. This study aimed to clarify these questions by coculturing MGs with ACs, PCs, or ECs using mouse brain-derived cells, and microglial phenotypic changes were investigated under culture conditions that enabled direct cell–cell contact. Our results showed that ACs or PCs dose-dependently increased the number of MG, while ECs decreased it. Microarray and gene ontology analysis showed that cell fate-related genes (e.g., cell cycle, proliferation, growth, death, and apoptosis) of MGs were altered after a cell–cell contact with ACs, PCs, and ECs. Notably, microarray analysis showed that several genes, such as gap junction protein alpha 1 (Gja1), were prominently upregulated in MGs after coincubation with ACs, PCs, or ECs, regardless of cell types. Similarly, immunohistochemistry showed that an increased Gja1 expression was observed in MGs after coincubation with ACs, PCs, or ECs. Immunofluorescent and fluorescence-activated cell sorting analysis also showed that calcein-AM was transferred into MGs after coincubation with ACs, PCs, or ECs, confirming that intercellular interactions occurred between these cells. However, while Gja1 inhibition reduced the number of MGs after coincubation with ACs and PCs, this was increased after coincubation with ECs; this indicates that ACs and PCs positively regulate microglial numbers via Gja1, while ECs decrease it. Results show that ACs, PCs, or ECs exert both common and specific cell type-dependent effects on MGs through intercellular interactions. These findings also suggest that brain microglial phenotypes are different depending on their surrounding cell types, such as ACs, PCs, or ECs.

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Section: Introductionmentioning

confidence: 99%

Different Contacted Cell Types Contribute to Acquiring Different Properties in Brain Microglial Cells upon Intercellular Interaction

Nakano‐Doi

Kubo²,

Sonoda³

et al. 2023

IJMS

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“…The hypothesis from the study of Sun et al [ 20 ] is based on previous evidence that butyrate modulates abnormal GM, suggesting that after being produced in the colon, it can bypass portal circulation and reach the brain. Butyrate enhances the anti-inflammatory activity of peroxisome proliferator-activated receptor γ and exerts neuroprotective effects [ 26 ]. In addition, authors found decreased butyrate levels in APP/PS1 mice compared to wild-type (WT) but increased after treatment.…”

Section: Literature Reviewmentioning

confidence: 99%

“…Sun et al [ 20 ] suggest that greater microbe richness does not imply a healthy GM but instead could be attributed to varied harmful bacteria. However, treatment helps in having bacterial communities more akin to the WT mice [ 26 ]. After treatment, GM composition showed a significant increase of Deferribacteres, Alloprevotella and S24-7 and decrease of Helicobacteraceae [ 20 ].…”

Section: Literature Reviewmentioning

confidence: 99%

“…The reduction observed may occur via the increase of ADAM10 protein of AβPP, which cause the inhibition of Aβ production [ 24 ]. However, there are differences across studies on whether significant changes apply to the cortex and/or hippocampus, on the level of decrease in soluble forms of Aβ or tau phosphorylation, when measured using immunohistochemical assays with confocal imaging [ 24 , 26 ]. The reasons for these differences are unclear, according to Abdelhamid et al [ 24 ], probiotics may activate specific brain regions through the vagus afferent nerve.…”

Section: Literature Reviewmentioning

confidence: 99%

“…The reasons for these differences are unclear, according to Abdelhamid et al [ 24 ], probiotics may activate specific brain regions through the vagus afferent nerve. However, depending on the dose and the pharmacological approach, the treatment can cause more damage than improvement [ 25 , 26 ]. Significant increase in Aβ plaques and gastrointestinal burden have been observed when testing high doses of a classic Tibetan medicine called Byur dMar Nyer lNga Ril Bu ( BdNlRB ).…”

Section: Literature Reviewmentioning

confidence: 99%

See 2 more Smart Citations

Therapeutic Potential of Microbiota Modulation in Alzheimer’s Disease: A Review of Preclinical Studies

Benichou Haziot,

Birak

2023

ADR

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Alzheimer’s disease (AD) is the most common neurodegenerative disease, yet it currently lacks effective treatment due to its complex etiology. The pathological changes in AD have been linked to the neurotoxic immune responses following aggregation of Aβ and phosphorylated tau. The gut microbiota (GM) is increasingly studied for modulating neuroinflammation in neurodegenerative diseases and in vivo studies emerge for AD. This critical review selected 7 empirical preclinical studies from 2019 onwards assessing therapy approaches targeting GM modulating microglia neuroinflammation in AD mouse models. Results from probiotics, fecal microbiota transplantation, and drugs were compared and contrasted, including for cognition, neuroinflammation, and toxic aggregation of proteins. Studies consistently reported significant amelioration or prevention of cognitive deficits, decrease in microglial activation, and lower levels of pro-inflammatory cytokines, compared to AD mouse models. However, there were differences across papers for the brain regions affected, and changes in astrocytes were inconsistent. Aβ plaques deposition significantly decreased in all papers, apart from Byur dMar Nyer lNga Ril Bu (BdNlRB) treatment. Tau phosphorylation significantly declined in 5 studies. Effects in microbial diversity following treatment varied across studies. Findings are encouraging regarding the efficacy of study but information on the effect size is limited. Potentially, GM reverses GM derived abnormalities, decreasing neuroinflammation, which reduces AD toxic aggregations of proteins in the brain, resulting in cognitive improvements. Results support the hypothesis of AD being a multifactorial disease and the potential synergies through multi-target approaches. The use of AD mice models limits conclusions around effectiveness, as human translation is challenging.

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Bioactive chemicals in Helianthus tuberosus L may reduce beta-amyloid cytotoxicity as a potential novel treatment for Alzheimer's disease

Zhu

Cadet

Neuwirth

2023

Studies in Natural Products Chemistry

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The Beneficial Effects of Combining Anti-Aβ Antibody NP106 and Curcumin Analog TML-6 on the Treatment of Alzheimer’s Disease in APP/PS1 Mice

Cited by 4 publications

References 52 publications

Different Contacted Cell Types Contribute to Acquiring Different Properties in Brain Microglial Cells upon Intercellular Interaction

Different Contacted Cell Types Contribute to Acquiring Different Properties in Brain Microglial Cells upon Intercellular Interaction

Therapeutic Potential of Microbiota Modulation in Alzheimer’s Disease: A Review of Preclinical Studies

Bioactive chemicals in Helianthus tuberosus L may reduce beta-amyloid cytotoxicity as a potential novel treatment for Alzheimer's disease

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