Regulation of Microglial Development: A Novel Role for Thyroid Hormone

Lima, Flávia Farias; Gervais, Annie; Colin, Catherine; Izembart, M; Neto, Vivaldo Moura; Mallat, Michel

doi:10.1523/jneurosci.21-06-02028.2001

Cited by 113 publications

(84 citation statements)

References 83 publications

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“…Microglial cells express the TRα1 and TRβ1 isoforms and are influenced by thyroid hormone (86). Microglial cell density and process formation are depressed in the parietal cortex of neonatal rats exposed to hypothyroid conditions from GD16 through lactation (86). In contrast, hyperthyroidism induced by T 3 injections to euthyroid and prenatally hypothyroid rat pups increased microglial cell survival and branching of the developing axonal fiber tracts of the corpus callosum.…”

Section: Thyroid Hormone Influence On Brain Developmentmentioning

confidence: 98%

“…A deficiency of GFAP during development inhibits the branching necessary for astrocyte-neuronal connections and decreases the long-term potentiation capacity, a factor essential to learning and memory (85). Microglial cells express the TRα1 and TRβ1 isoforms and are influenced by thyroid hormone (86). Microglial cell density and process formation are depressed in the parietal cortex of neonatal rats exposed to hypothyroid conditions from GD16 through lactation (86).…”

Section: Thyroid Hormone Influence On Brain Developmentmentioning

confidence: 99%

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A model of the development of the brain as a construct of the thyroid system.

Howdeshell

2002

Environ Health Perspect

330

229

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Thyroid hormone is essential for normal brain development. However, little is known about the molecular and cellular mechanisms that mediate thyroid hormone action on the developing brain or the developmental events selectively affected. Consequently, although a large number of environmental chemicals interfere with the thyroid system, there are few neurodevelopmental end points to recruit for toxicological studies. Therefore, my goal here is to review what is known about the relative timing of normal brain construction and thyroid system development, with special focus on the period of in utero development in humans and the comparable developmental period in laboratory rats. These data are presented as a timeline to aid in the identification of thyroid-sensitive end points in brain development and to highlight important data gaps. I discuss the known influence of certain synthetic chemicals on the thyroid system and include a brief review of the effects of developmental exposure to chemicals on thyroid system function. The relationship between the thyroid hormone and retinoic acid systems, as well as the thyroid hormone sensitivity of the developing cochlea, is also discussed.

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Section: Thyroid Hormone Influence On Brain Developmentmentioning

confidence: 98%

Section: Thyroid Hormone Influence On Brain Developmentmentioning

confidence: 99%

A model of the development of the brain as a construct of the thyroid system.

Howdeshell

2002

Environ Health Perspect

330

229

View full text Add to dashboard Cite

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“…Both murine and human microglia express high levels of LAT2 in addition to MCT10 and OATP4a1, allowing them to transport TH into the cell (Wirth et al 2009, Braun et al 2011. In addition, microglia express both TRα 1 and TRβ 1 (Lima et al 2001). Physiological TH concentrations appear to be crucial for microglial growth and morphological differentiation (Lima et al 2001).…”

Section: :2mentioning

confidence: 99%

“…In addition, microglia express both TRα 1 and TRβ 1 (Lima et al 2001). Physiological TH concentrations appear to be crucial for microglial growth and morphological differentiation (Lima et al 2001). Hypothyroid rats showed delayed microglial growth and differentiation, whereas hyperthyroid animals displayed the opposite phenotype with accelerated microglial growth and differentiation (Lima et al 2001).…”

Section: :2mentioning

confidence: 99%

“…Physiological TH concentrations appear to be crucial for microglial growth and morphological differentiation (Lima et al 2001). Hypothyroid rats showed delayed microglial growth and differentiation, whereas hyperthyroid animals displayed the opposite phenotype with accelerated microglial growth and differentiation (Lima et al 2001). A recent study by Mori and coworkers assessed in detail the effects of T 3 on microglial activation and the signalling pathways involved (Mori et al 2015).…”

Section: :2mentioning

confidence: 99%

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Thyroid hormone metabolism in innate immune cells

Spek

Fliers

Boelen

2017

Journal of Endocrinology

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Thyroid hormone (TH) metabolism and thyroid status have been linked to various aspects of the immune response. There is extensive literature available on the effects of thyroid hormone on innate immune cells. However, only recently have authors begun to study the mechanisms behind these effects and the role of intracellular TH metabolism in innate immune cell function during inflammation. This review provides an overview of the molecular machinery of intracellular TH metabolism present in neutrophils, macrophages and dendritic cells and the role and effects of intracellular TH metabolism in these cells. Circulating TH levels have a profound effect on neutrophil, macrophage and dendritic cell function. In general, increased TH levels result in an amplification of the pro-inflammatory response of these cells. The mechanisms behind these effects include both genomic and non-genomic effects of TH. Besides a pro-inflammatory effect induced by extracellular TH, the cellular response to pro-inflammatory stimuli appears to be dependent on functional intracellular TH metabolism. This is illustrated by the fact that the deiodinase enzymes and in some cell types also thyroid hormone receptors appear to be crucial for adequate innate immune cell function. This overview of the literature suggests that TH metabolism plays an important role in the host defence against infection through the modulation of innate immune cell function.

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Effects of electromagnetic fields on bone loss in hyperthyroidism rat model

Liu

Zhang

et al. 2016

Bioelectromagnetics

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Optimal therapeutics for hyperthyroidism-induced osteoporosis are still lacking. As a noninvasive treatment, electromagnetic fields (EMF) have been proven to be effective for treating osteoporosis in non-hyperthyroidism conditions. We herein systematically evaluated the reduced effects of EMF on osteoporosis in a hyperthyroidism rat model. With the use of Helmholtz coils and an EMF stimulator, 15 Hz/1 mT EMF was generated. Forty-eight 5-month-old male Sprague-Dawley rats were randomly divided into four different groups: control, levothyroxine treated (L-T4), EMF exposure + levothyroxine (EMF + L-T4), and EMF exposure without levothyroxine administration (EMF). All rats were treated with L-T4 (100 mg/day) except those in control and EMF groups. After 12 weeks, the results obtained from bone mineral density analyses and bone mechanical measurements showed significant differences between L-T4 and EMF + L-T4 groups. Micro CT and bone histomorphometric analyses indicated that trabecular bone mass and architecture in distal femur and proximal tibia were augmented and restored partially in EMF + L-T4 group. In addition, bone thyroid hormone receptors (THR) expression of hyperthyroidism rats was attenuated in EMF + L-T4 group, compared to control group, which was not observed in L-T4 group. According to these results, we concluded that 15 Hz/1 mT EMF significantly inhibited bone loss and micro architecture deterioration in hyperthyroidism rats, which might occur due to reduced THR expression caused by EMF exposure. Bioelectromagnetics. 38:137-150, 2017. © 2016 Wiley Periodicals, Inc.

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Regulation of Microglial Development: A Novel Role for Thyroid Hormone

Cited by 113 publications

References 83 publications

A model of the development of the brain as a construct of the thyroid system.

A model of the development of the brain as a construct of the thyroid system.

Thyroid hormone metabolism in innate immune cells

Effects of electromagnetic fields on bone loss in hyperthyroidism rat model

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