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Host microbiota constantly control maturation and function of microglia in the CNS

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TLDR
It is determined that short-chain fatty acids (SCFA), microbiota-derived bacterial fermentation products, regulated microglia homeostasis and mice deficient for the SCFA receptor FFAR2 mirroredmicroglia defects found under GF conditions, suggesting that host bacteria vitally regulate microglian maturation and function.
Abstract
As the tissue macrophages of the CNS, microglia are critically involved in diseases of the CNS. However, it remains unknown what controls their maturation and activation under homeostatic conditions. We observed substantial contributions of the host microbiota to microglia homeostasis, as germ-free (GF) mice displayed global defects in microglia with altered cell proportions and an immature phenotype, leading to impaired innate immune responses. Temporal eradication of host microbiota severely changed microglia properties. Limited microbiota complexity also resulted in defective microglia. In contrast, recolonization with a complex microbiota partially restored microglia features. We determined that short-chain fatty acids (SCFA), microbiota-derived bacterial fermentation products, regulated microglia homeostasis. Accordingly, mice deficient for the SCFA receptor FFAR2 mirrored microglia defects found under GF conditions. These findings suggest that host bacteria vitally regulate microglia maturation and function, whereas microglia impairment can be rectified to some extent by complex microbiota.

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Sex-specific effects of microbiome perturbations on cerebral Aβ amyloidosis and microglia phenotypes

TL;DR: The microbiome plays a causal role in modulating Aβ burden and microglia phenotypes and an antibiotic cocktail leads to reductions in brain amyloidosis, altered morphology, and gene expression inmicroglia of male but not female transgenic mice that exhibit Aβ deposits.
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Gut reactions: How the blood-brain barrier connects the microbiome and the brain

TL;DR: This minireview examines the several ways the microbiome is known to interact with the CNS barriers and concludes that metastatic bacterial factors can signal T-cells to become more CNS penetrant, thus providing a novel intervention for treating CNS disease.
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The Microbiota-Gut-Brain Axis in Neuropsychiatric Disorders: Pathophysiological Mechanisms and Novel Treatments.

TL;DR: The microbiota–gut–brain axis might provide novel targets for prevention and treatment of neuropsychiatric disorders, however, further studies are required to substantiate the clinical use of probiotics, prebiotics and FMT.
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Peripheral immune system in aging and Alzheimer’s disease

TL;DR: This work summarizes the prominent molecular and cellular changes in the periphery of aging individuals and AD patients and reviews the knowledge gained in the past several years that implicate specific arms of the peripheral immune system and other types of immune responses in modulating AD progression.
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Microglia Gone Rogue: Impacts on Psychiatric Disorders across the Lifespan

TL;DR: Taking into account the recent identification of microglia-specific markers, and the availability of compounds that target these cells selectively in vivo, the prospect of disease intervention via the microglial route is considered.
References
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Journal ArticleDOI

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The gut microbiota shapes intestinal immune responses during health and disease

TL;DR: Findings indicating that developmental aspects of the adaptive immune system are influenced by bacterial colonization of the gut are discussed, and the possibility that the mammalian immune system, which seems to be designed to control microorganisms, is in fact controlled by microorganisms is raised.
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Fate Mapping Analysis Reveals That Adult Microglia Derive from Primitive Macrophages

TL;DR: Results identify microglia as an ontogenically distinct population in the mononuclear phagocyte system and have implications for the use of embryonically derived microglial progenitors for the treatment of various brain disorders.
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The Microbial Metabolites, Short-Chain Fatty Acids, Regulate Colonic Treg Cell Homeostasis

TL;DR: This study determined that short-chain fatty acids, gut microbiota–derived bacterial fermentation products, regulate the size and function of the colonic Treg pool and protect against colitis in a Ffar2-dependent manner in mice, revealing that a class of abundant microbial metabolites underlies adaptive immune microbiota coadaptation and promotes colonic homeostasis and health.
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